BACKGROUND OF THE INVENTION
Myocardial infarction (MI) is one of the most common diagnoses in hospitalized patients in industrialized countries. Myocardial Infarction generally occurs when there is an abrupt decrease in coronary blood flow following a thrombotic occlusionof a coronary artery previously narrowed by atherosclerosis. Infarction occurs when a coronary artery thrombus develops rapidly at a site a vascular injury, which is produced or facilitated by factors such as cigarette smoking, hypertension and lipidaccumulation. In most cases, infarction occurs when an atherosclerotic plaque fissures, ruptures or ulcerates and when conditions favor thrombogenesis. In rare cases, infarction may be due to coronary artery occlusion caused by coronary emboli,congenital abnormalities, coronary spasm, and a wide variety of systemic, particularly inflammatory diseases.
Although classical risk factors such as smoking, hyperlipidemia, hypertension, and diabetes are associated with many cases of coronary heart disease (CHD) and MI, many patients do not have involvement of these risk factors. In fact, manypatients who exhibit one or more of these risk factors do not develop MI. Family history has long been recognized as one of the major risk factors. Although some of the familial clustering of MI reflects the genetic contribution to the otherconventional risk factors, a large number of studies have suggested that there are significant genetic susceptibility factors, beyond those of the known risk factors (Friedlander Y, et al., Br Heart J. 1985; 53:382-7, Shea S. et al., J. Am. Coll. Cardiol. 1984; 4:793-801, and Hopkins P. N., et al., Am. J. Cardiol. 1988; 62:703-7). Major genetic susceptibility factors have not yet been identified.
SUMMARY OF THE INVENTION
As described herein, a locus on chromosome 13q12-13 has been identified as playing a major role in Myocardial Infarction (MI). The locus, herein after referred to as the MI locus, comprises nucleic acid that encodes 5-lipoxygenase activatingprotein (ALOX5AP or FLAP), herein after referred to as FLAP. The gene has also been shown to play a role in stroke.
The present invention relates to isolated nucleic acid molecules comprising a portion or the entire human FLAP nucleic acid or a variant thereof. In one embodiment, the nucleic acid molecule has at least one polymorphism that is correlated withthe incidence of myocardial infarction or stroke. Identification of nucleic acids and polymorphisms in this locus can pave the way for a better understanding of the disease process, which in turn can lead to improved diagnostic and therapeutic methods.
The invention further pertains to methods of diagnosing a susceptibility to myocardial infarction or stroke, comprising detecting an alteration in the expression or composition of a polypeptide encoded by a FLAP nucleic acid in a test sample, incomparison with the expression or composition of a polypeptide encoded by FLAP in a control sample, wherein the presence of an alteration in expression or composition of the polypeptide in the test sample is indicative of a susceptibility to myocardialinfarction or stroke.
The invention also relates to an isolated nucleic acid molecule comprising a FLAP nucleic acid, wherein the FLAP nucleic acid has a nucleic acid sequence of SEQ ID NO: 1 or SEQ ID NO: 3, or the complement of SEQ ID NO: 1 or SEQ ID NO: 3, whereinthe nucleic acid molecule comprises a polymorphism as indicated in Table 13.
In another embodiment, the invention relates to an isolated nucleic acid molecule having a polymorphism as indicated in Table 13, which hybridizes under high stringency conditions to a nucleic acid sequence of SEQ ID NO: 1 or SEQ ID NO: 3, or thecomplement of SEQ ID NO: 1 or SEQ ID NO: 3.
In yet another embodiment, a method for assaying for the presence of a first nucleic acid molecule in a sample is described, comprising contacting said sample with a second nucleic acid molecule, where the second nucleic acid molecule comprises anucleic acid sequence of SEQ ID NO: 1 or SEQ ID NO: 3, and hybridizes to the first nucleic acid under high stringency conditions.
The invention also relates to a vector comprising an isolated nucleic acid molecule of the invention operably linked to a regulatory sequence, as well as to a recombinant host cell comprising the vector. The invention also provides a method forpreparing a polypeptide encoded by an isolated nucleic acid molecule comprising culturing the recombinant host cell under conditions suitable for expression of said nucleic acid molecule.
Also contemplated by the invention is a method of assaying a sample for the presence of a polypeptide encoded by an isolated nucleic acid molecule of the invention, comprising contacting the sample with an antibody that specifically binds to thepolypeptide.
The invention further provides a method of identifying an agent that alters expression of a FLAP nucleic acid, comprising: contacting a solution containing a nucleic acid comprising the promoter region of the FLAP nucleic acid operably linked toa reporter gene with an agent to be tested; assessing the level of expression of the reporter gene; and comparing the level of expression with a level of expression of the reporter gene in the absence of the agent; wherein if the level of expression ofthe reporter gene in the presence of the agent differs, by an amount that is statistically significant, from the level of expression in the absence of the agent, then the agent is an agent that alters expression of the FLAP nucleic acid. An agentidentified by this method is also contemplated.
The invention additionally comprises a method of identifying an agent that alters expression of a FLAP nucleic acid, in which a solution containing a nucleic acid described herein or a derivative or fragment thereof is contacted with an agent tobe tested, and expression of the nucleic acid, derivative or fragment in the presence of the agent is assessed and compared with expression of the nucleic acid, derivative or fragment in the absence of the agent. If expression of the nucleic acid,derivative or fragment in the presence of the agent differs, by an amount that is statistically significant, from the expression in the absence of the agent, then the agent is an agent that alters expression of the FLAP nucleic acid. In certainembodiments, the expression of the nucleic acid, derivative or fragment in the presence of the agent comprises expression of one or more splicing variant(s) that differ in kind or in quantity from the expression of one or more splicing variant(s) theabsence of the agent. Agents identified by this method are also contemplated. Representative agents include antisense nucleic acid to a FLAP nucleic acid; a FLAP polypeptide; a FLAP nucleic acid receptor; a FLAP nucleic acid binding agent; apeptidomimetic; a fusion protein; a prodrug thereof; an antibody; and a ribozyme. A method of altering expression of a FLAP nucleic acid comprising contacting a cell containing a FLAP nucleic acid with such an agent is also contemplated.
The invention further pertains to a method of identifying a polypeptide which interacts with a FLAP polypeptide, employing a yeast two-hybrid system that uses a first vector which comprises a nucleic acid encoding a DNA binding domain and a FLAPpolypeptide, splicing variant, or a fragment or derivative thereof, and a second vector which comprises a nucleic acid encoding a transcription activation domain and a nucleic acid encoding a test polypeptide. If transcriptional activation occurs in theyeast two-hybrid system, the test polypeptide is a polypeptide which interacts with a FLAP polypeptide.
A transgenic animal comprising a nucleic acid of the invention such as an exogenous FLAP nucleic acid or a nucleic acid encoding a FLAP polypeptide is also contemplated.
In yet another embodiment, the invention relates to a method for assaying a sample for the presence of a FLAP nucleic acid, by contacting the sample with a nucleic acid comprising a contiguous nucleic acid sequence which is at least partiallycomplementary to a part of the sequence of said FLAP nucleic acid, under conditions appropriate for hybridization, and assessing whether hybridization has occurred between a FLAP nucleic acid and said nucleic acid, wherein if hybridization has occurred,a FLAP nucleic acid is present in the nucleic acid. In certain embodiments, the contiguous nucleic acid sequence is completely complementary to a part of the sequence of said FLAP nucleic acid and in other embodiments; amplification is of at least partof said FLAP nucleic acid.
In certain embodiments, the contiguous nucleic acid sequence is 100 or fewer nucleotides in length and is either: a) at least 80% identical to a contiguous sequence of nucleotides of SEQ ID NO: 1 or SEQ ID NO: 3; b) at least 80% identical to thecomplement of a contiguous sequence of nucleotides in of SEQ ID NO: 1 or SEQ ID NO: 3; or c) capable of selectively hybridizing to said FLAP nucleic acid.
The invention also pertains to a reagent for assaying a sample for the presence of a FLAP nucleic acid, the reagent comprising a nucleic acid comprising a contiguous nucleic acid sequence which is at least partially complementary to a part of thenucleic acid sequence of said FLAP nucleic acid. The reagent can comprise a contiguous nucleotide sequence which is completely complementary to a part of the nucleic acid sequence of said FLAP nucleic acid. A reagent kit for assaying a sample for thepresence of a FLAP nucleic acid is also described, including (e.g., in separate containers), one or more labeled nucleic acids comprising a contiguous nucleic acid sequence which is at least partially complementary to a part of the nucleic acid sequenceof said FLAP nucleic acid; and reagents for detection of said label. The labeled nucleic acid can comprise a contiguous nucleotide sequence which is completely complementary to a part of the nucleic acid sequence of said FLAP nucleic acid. Alsodescribed herein is a reagent kit for assaying a sample for the presence of a FLAP nucleic acid, comprising one or more nucleic acids comprising a contiguous nucleic acid sequence which is at least partially complementary to a part of the nucleic acidsequence of said FLAP nucleic acid, and which is capable of acting as a primer for said FLAP nucleic acid when maintained under conditions for primer extension.
The invention also provides for the use of a nucleic acid for assaying a sample for the presence of a FLAP nucleic acid, in which the nucleic acid is 100 or fewer nucleotides in length and is either: at least 80% identical to a contiguoussequence of nucleotides of SEQ ID NO: 1 or SEQ ID NO: 3; at least 80% identical to the complement of a contiguous sequence of nucleotides of SEQ ID NO: 1 or SEQ ID NO: 3; or capable of selectively hybridizing to said FLAP nucleic acid.
In yet another embodiment, the use of a first nucleic acid for assaying a sample for the presence of a FLAP nucleic acid that has at least one nucleotide difference from the first nucleic acid is described, in which the first nucleic acid is 100or fewer nucleotides in length and which is either: at least 80% identical to a contiguous sequence of nucleotides of SEQ ID NO: 1 or SEQ ID NO: 3 or one of the sequences shown in Table 13; at least 80% identical to the complement of a contiguoussequence of nucleotides of SEQ ID NO: 1 or SEQ ID NO: 3 one of the sequences shown in Table 13; or capable of selectively hybridizing to said FLAP nucleic acid.
The invention also relates to a method of diagnosing a susceptibility to myocardial infarction or stroke in an individual, comprising determining the presence or absence in the individual of certain single nucleotide polymorphisms (SNPs) or ofcertain "haplotypes" (combinations of genetic markers); the presence of the SNP or the haplotype is diagnostic of susceptibility to myocardial infarction or stroke. In one embodiment, a haplotype associated with a susceptibility to myocardial infarctionor stroke comprises markers SG13S99, SG13S25, SG13S377, SG13S106, SG13S32 and SG13S35 at the 13q12-13 locus. In one particular embodiment, the presence of the alleles T, G, G, G, A and G at SG13S99, SG13S25, SG13S377, SG13S106, SG13S32 and SG13S35,respectively (the B6 haplotype), is diagnostic of susceptibility to myocardial infarction or stroke. In another embodiment, a haplotype associated with a susceptibility to myocardial infarction or stroke comprises markers SG13S99, SG13S25, SG13S106,SG13S30 and SG13S42 at the 13q12-13 locus. In one particular embodiment, the presence of the alleles T, G, G, G and A at SG13S99, SG13S25, SG13S106, SG13S30 and SG13S42, respectively (the B5 haplotype), is diagnostic of susceptibility to myocardialinfarction or stroke. In a third embodiment, a haplotype associated with a susceptibility to myocardial infarction or stroke comprises markers SG13S25, SG13S106, SG13S30 and SG13S42 at the 13q12-13 locus. In one particular embodiment, the presence ofthe alleles G, G, G and A at SG13S25, SG13S106, SG13S30 and SG13S42, respectively (the B4 haplotype), is diagnostic of susceptibility to myocardial infarction or stroke. In a fourth embodiment, a haplotype associated with a susceptibility to myocardialinfarction or stroke comprises markers SG13S25, SG13S106, SG13S30 and SG13S32 at the 13q 12-13 locus. In one particular embodiment, the presence of the alleles G, G, G and A at SG13S25, SG13S106, SG13S30 and SG13S32, respectively (the Bs4 haplotype), isdiagnostic of susceptibility to myocardial infarction or stroke.
In a fifth embodiment, a haplotype associated with a susceptibility to myocardial infarction or stroke comprises markers SG13S99, SG13S25, SG13S114, SG13S89 and SG13S32 at the 13q12-13 locus. In one particular embodiment, the presence of thealleles T, G, T, G and A at SG13S99, SG13S25, SG13S114, SG13S89 and SG13S32, respectively (the A5 haplotype), is diagnostic of susceptibility to myocardial infarction or stroke. In a sixth embodiment, a haplotype associated with a susceptibility tomyocardial infarction or stroke comprises markers SG13S25, SG13S114, SG13S89 and SG13S32 at the 13q12-13 locus. In one particular embodiment, the presence of the alleles G, T, G and A at SG13S25, SG13S114, SG13S89 and SG13S32, respectively (the A4haplotype), is diagnostic of susceptibility to myocardial infarction or stroke. The presence or absence of the haplotype can be determined by various methods, including, for example, using enzymatic amplification, restriction fragment lengthpolymorphism analysis, sequence analysis or electrophoretic analysis of nucleic acid from the individual.
A further embodiment of the invention is a method for identification of susceptibility to myocardial infarction or stroke, by identifying haplotypes and/or SNPs that can be used to identify individuals at risk of developing MI or stroke. Incertain embodiments, haplotypes can comprise, for example, at least one of the polymorphisms as indicated in Table 13, or as shown in the haplotypes in Table 5, Table 7, Table 9, Table 14, and/or Table 15. In certain additional embodiments, thehaplotype can be one of haplotypes B4, BS4, B5, B6, A4, A5 or Hap B.
A method for the diagnosis and identification of susceptibility to myocardial infarction or stroke in an individual is also described, comprising: screening for a SNP or an at-risk haplotype in the FLAP nucleic acid that is more frequentlypresent in an individual susceptible to myocardial infarction or stroke compared to an individual who is not susceptible to myocardial infarction or stroke, wherein the SNP or the at-risk haplotype increases the risk significantly. In certainembodiments, the significant increase is at least about 20%, and in other embodiments, the significant increase is identified as an odds ratio of at least about 1.2.
An additional embodiment comprises methods for the diagnosis of increased risk of susceptibility to myocardial infarction or stroke in an individual, by screening for a SNP or an at-risk haplotype in the FLAP nucleic acid that is more frequentlypresent in an individual susceptible to myocardial infarction or stroke (affected), compared to the frequency of its presence in a healthy individual (control). The presence of the SNP or at-risk haplotype is indicative of a susceptibility to myocardialinfarction or stroke. In one embodiment, an at-risk haplotype has a p value <0.05. In certain other embodiments, the screening for the presence of an at-risk haplotype comprises screening for an at-risk haplotype within or near FLAP thatsignificantly correlates with a haplotype such as a halotype shown in Table 5; a haplotype shown in Table 7; a haplotype shown in Table 9; a haplotype shown in Table 14; a haplotype shown in Table 15; haplotype B4; haplotype Bs4; haplotype B5; haplotypeB6; haplotype A4; haplotype A5; or haplotype HapB. In other embodiments, screening for the presence of an at-risk haplotype comprises screening for an at-risk haplotype within or near FLAP that significantly correlates with susceptibility to myocardialinfarction or stroke.
A further embodiment comprises methods of diagnosing FLAP-associated myocardial infarction or stroke in an individual who has had a myocardial infarction and/or a stroke, by detecting a polymorphism in a FLAP nucleic acid, or an alteration in theexpression or composition of a polypeptide encoded by a flap nucleic acid, wherein the presence of the polymorphism in the nucleic acid or the alteration in expression or composition is indicative of FLAP-associated myocardial infarction or stroke. Additional embodiments of the invention include methods for identification of FLAP-associated myocardial infarction or stroke, by identifying haplotypes and/or SNPs associated with MI or stroke. The haplotypes can comprise, for example, at least one ofthe polymorphisms as indicated in Table 13, or as shown in the haplotypes in Table 5, Table 7, Table 9, Table 14, and/or Table 15. In certain additional embodiments, the haplotype can one of haplotypes B4, BS4, B5, B6, A4, A5 or Hap B.
BRIEFDESCRIPTION OF THE DRAWINGS
The foregoing and other objects, features and advantages of the invention will be apparent from the following more particular description of preferred embodiments of the invention.
FIG. 1 shows the results from a haplotype association analysis using 4 and 5 microsatellite markers. The p-value of the association is plotted on the y-axis and position of markers on the x-axis. Only haplotypes that show association with ap-value <10.sup.-5 are shown in the figure. The most significant microsatellite marker haplotype association is found using markers DG13S1103, DG13S166, DG13S1287, DG13S1061 and DG13S301, with alleles 4, 0, 2, 14 and 3, respectively (p-value of1.02.times.10.sup.-7). Carrier frequency of the haplotype is 7.3% in affected individuals and 0.3% in controls. These results are based on 437 patients and 721 controls. The area that is common to all the haploytypes shown in the figure includes onlyone gene, FLAP.
FIG. 2 shows the alleles of the markers defining the most significant microsatellite marker haplotypes. The area defined with a black square is a common area to all the most significantly associated haplotypes. The FLAP nucleic acid is locatedbetween markers DG13S166 and D13S1238. Two marker haplotype involving alleles 0 and -2 for markers DG13S166 and S13S1238, respectively, is found in excess in patients. Carrier frequency of this haploype is 27% in patients and 15.4% in controls p-value1.times.10.sup.-3).
FIG. 3 shows the relative location of key SNPs and exons of the ALOX5AP/FLAP gene. Haplotype length varies between 33 to 68 kb.
FIG. 4 shows the amino acid sequence of FLAP (SEQ ID NO: 2) and the mRNA of FLAP (SEQ ID NO: 3).
FIG. 5 shows linkage scan using framework microsatellite markers on chromosome 13 for male patients with ischemic stroke or TIA (n=342 in 164 families at 6 meiosis). The LOD score is expressed on the y axis and the distance from the pter inKosambi cM on the x axis.
FIGS. 6.1-6.82 shows the genomic sequence of the FLAP gene (SEQ ID NO: 1).
FIG. 7 shows a schematic view of the chromosome 13 linkage region showing the FLAP gene. (7.1) The linkage scan for female MI patients and the one LOD drop region that includes the FLAP gene; (7.2) Microsatellite association for all MI patients:single marker association (black dots) and two, three, four and five marker haplotype association. The arrows indicate the location of the most significant haplotype association across the FLAP gene in males and females. (7.3) The FLAP gene structure,with exons shown as cylinders, and the location of all the SNPs typed in the region (vertical lines). The vertical lines indicate the position of the microsatellites (shown in 9.2) and SNPs (shown in 10.3) used in the analysis.
FIGS. 8.1-8.40 show the sequences of the FLAP nucleic acid flanking the SNPs that were identified by sequencing samples from patients (SEQ ID NOs: 506-717).
FIG. 9 shows pairwise linkage disequilibrium (LD) between SNPs in a 60 kb region encompassing FLAP. The markers are plotted equidistantly. Two measures of LD are shown: D' in the upper left triangle and P values in the lower right triangle. Lines indicate the positions of the exons of FLAP and stars indicate the location of the markers of the at-risk haplotype A4. Scales for the LD strength are provided for both measures to the right.
DETAILED DESCRIPTION OF THE INVENTION
Extensive genealogical information has been combined with powerful gene sharing methods to map a susceptibility gene for myocardial infarction on chromosome 13q 12-13. A genome wide scan of 296 multiplex Icelandic families with 713 MI patientswas performed. Through a suggestive linkage to a locus on chromosome 13q12-13 for female MI patients and early onset MI patients, and a microsatellite marker association analysis, the gene encoding the 5-lipoxygenase activating protein (FLAP) wasidentified.
Subsequent to the mapping of the MI susceptibility gene to chromosome 13q12-13 the candidate locus was finely mapped with microsatellite markers. Patients with myocardial infarction and controls were initially genotyped with microsatellitemarkers with an average spacing between markers of less than 100 kb over a 7.6 Mb candidate region. Initial haplotype association analysis that included these microsatellite markers revealed several extended haplotypes composed of 4 and 5 microsatellitemarkers that were significantly associated with female MI (see FIGS. 1 and 2). A region common to all these extended haplotypes, is defined by markers DG13S166 and D13S1238. This region included only one gene, the FLAP nucleic acid sequence. The twomarker haplotype involving alleles 0 and -2 for markers DG13S166 and D13S1238, respectively, was found in excess in patients.
This was the first evidence that the FLAP gene might be involved in the pathogenesis of myocardial infarction.
Subsequent haplotype analysis that included more microsatellite markers in the candidate region on chromosome 13q12-13, now with a marker density of 1 microsatellite marker per 60 kb, showed decreased significance of the original haplotypeassociation. However, the haplotype association analysis using increased density of markers again pointed towards the FLAP gene. This analysis strongly suggested that a 300 kb region was involved in the susceptibility of myocardial infarction. This300 kb region included only two genes, the gene encoding highly charged protein (D13S106E) and the gene encoding 5-lipoxygenase activating protein (FLAP).
In view of the association results described above and because of the known role of the 5-lipoxygenease pathway in inflammatory processes, FLAP was an attractive candidate and therefore further efforts were focused on this gene.
SNP Haplotype Association to MI, and Subsequently to Stroke
In an effort to identify haplotypes involving only SNP markers that associate with MI, additional SNPs were identified by sequencing the FLAP gene and the region flanking the gene. A total of 48 SNPs in 1343 patients and 624 unrelated controlswere genotyped. Haplotype association analysis involving only these SNPs revealed two correlated series of SNP haplotypes that were in significant excess in patients, denoted as A and B in Table 7. The length of the haplotypes varied between 33 and 69kb, and the haplotypes covered one or two blocks of linkage disequilibrium. Both series of haplotypes contained the common allele G of the SNP SG13S25. All haplotypes in the A series contain the SNP SG13S114, while all haplotypes in the B seriescontain the SNP SG13S106. In the B series, the haplotypes B4, B5, and B6 have a relative risk (RR) greater than 2 and with allelic frequencies above 10%. The haplotypes in the A series have slightly lower RR and lower p-values, but higher frequency(15-16%). The haplotypes in series B and A are strongly correlated, i.e., the haplotypes in B define a subset of the haplotypes in A. Hence, haplotypes in series B are more specific than A. However, haplotypes in series A are more sensitive, i.e. theycapture more individuals with the putative mutation, as is observed in the population attributable risk which is less for B than for A. Furthermore, these haplotypes showed similar risk ratios and allelic frequencies for early-onset patients (defined asonset of first MI before the age of 55) and for both genders. In addition, analyzing various groups of patients with known risk factors, such as hypertension, high cholesterol, smoking and diabetes, did not reveal any significant correlation with thesehaplotypes, suggesting that the haplotypes in the FLAP gene represent an independent genetic susceptibility factor for MI.
The product of the FLAP gene is involved in an important inflammatory pathway, and could thus be a predisposing factor for plaque rupture in MI. Since MI and stroke are both considered to be atherothrombotic diseases the MI at-risk haplotypeswere assessed to determine whether they also were associated with stroke. Nineteen of the SNPs that defined the MI at-risk haplotypes (A and B series) were evaluated in stroke patients and unrelated controls. In the analysis, a subset of patients thatdid not have MI and were unrelated within 4 meiosis was used. The results from the haplotype association analysis are summarized in Table 9. The frequency of the at-risk haplotypes in all stroke patients was very similar to that of the MI patients andthe haplotype conferred a similar relative risk. The B4 haplotype, previously described for MI, is carried by 19% of all stroke patients and 11% of controls. Carriers of this haplotype have nearly twofold risk (RR=1.95, P=1.6 10-4) of having a stroke. Adding the fifth SNP (SG13S35) to the B4 haplotype increases the relative risk to 2.04 (p-value 5.8 10-5). The allelic frequency of this haplotype is 10.2% in stroke patients and 5.3% in controls. Also shown in Table 9 is a 4 SNP haplotype defined asBs4 that is highly correlated with the B4 haplotype (r2=0.93). Bs4 haplotype has a RR of 2.01, carrier frequency in patients of 19% and population attributable risk of 10%. This haplotype was tested with different subtypes of stroke (Table 9). Ofinterest is that all stroke subtypes have a considerably higher frequency of the `at-risk` haplotype than controls resulting in the increased relative risk.
The FLAP nucleic acid encodes a 5-lipoxygenase activating protein, which, in combination with 5-lipoxygenase (5-LO), is required for leukotriene synthesis. FLAP acts coordinately with 5-LO to catalyze the first step in the synthesis ofleukotrienes from arachidonic acid. It catalyzes the conversion of arachidonic acid to 5(S)-hydroperoxy-6-trans-8,11,14-cis-eicosatetraenoic acid (5-HPETE), and further to the allylic epoxide 5 (S)-trans7,9 trans 11,14-cis-eicosatetraenoic acid(leukotriene A4, LTA4).
The leukotrienes are a family of highly potent biological mediators of inflammatory processes produced primarily by bone marrow derived leukocytes such as monocytes, macrophages, and neurophils. Both FLAP and 5-LO are detected withinatherosclerosis lesions (Proc Natl Acad Sci USA. 2003 Feb. 4; 100(3):1238-43.), indicating that the vessel itself can be a source of leukotrienes. Inhibitors of FLAP function impede translocation of 5-LO from the cytoplasm to the cell membrane andinhibit activation of 5-LO and thereby decrease leukotriene synthesis.
Independent confirmation of FLAP association to MI was obtained in a British cohort of patients with sporadic MI. These findings support FLAP as the first specific gene isolated that confers substantial risk of the complex traits of MI andstroke.
As a result of these discoveries, genetic tests can now be developed to identify those that are at increased risk of developing myocardial infarction (MI) or stroke.
NUCLEIC ACIDS OF THE INVENTION
FLAP Nucleic Acids, Portions and Variants
Accordingly, the invention pertains to isolated nucleic acid molecules comprising a human FLAP nucleic acid. The term, "FLAP nucleic acid," as used herein, refers to an isolated nucleic acid molecule encoding FLAP polypeptide. The FLAP nucleicacid molecules of the present invention can be RNA, for example, mRNA, or DNA, such as cDNA and genomic DNA. DNA molecules can be double-stranded or single-stranded; single stranded RNA or DNA can be either the coding, or sense strand or the non-coding,or antisense strand. The nucleic acid molecule can include all or a portion of the coding sequence of the gene or nucleic acid and can further comprise additional non-coding sequences such as introns and non-coding 3' and 5' sequences (includingregulatory sequences, for example).
For example, a FLAP nucleic acid can consist of SEQ ID NOs: 1 or 3 or the complement thereof, or to a portion or fragment of such an isolated nucleic acid molecule (e.g., cDNA or the nucleic acid) that encodes FLAP polypeptide (e.g., apolypeptide such as SEQ ID NO: 2). In a preferred embodiment, the isolated nucleic acid molecule comprises a nucleic acid molecule selected from the group consisting of SEQ ID NOs: 1 or 3, or their complement thereof.
Additionally, the nucleic acid molecules of the invention can be fused to a marker sequence, for example, a sequence that encodes a polypeptide to assist in isolation or purification of the polypeptide. Such sequences include, but are notlimited to, those that encode a glutathione-S-transferase (GST) fusion protein and those that encode a hemagglutinin A (HA) polypeptide marker from influenza.
An "isolated" nucleic acid molecule, as used herein, is one that is separated from nucleic acids that normally flank the gene or nucleic acid sequence (as in genomic sequences) and/or has been completely or partially purified from othertranscribed sequences (e.g., as in an RNA library). For example, an isolated nucleic acid of the invention may be substantially isolated with respect to the complex cellular milieu in which it naturally occurs, or culture medium when produced byrecombinant techniques, or chemical precursors or other chemicals when chemically synthesized. In some instances, the isolated material will form part of a composition (for example, a crude extract containing other substances), buffer system or reagentmix. In other circumstances, the material may be purified to essential homogeneity, for example as determined by PAGE or column chromatography such as HPLC. In certain embodiments, an isolated nucleic acid molecule comprises at least about 50, 80 or90% (on a molar basis) of all macromolecular species present. With regard to genomic DNA, the term "isolated" also can refer to nucleic acid molecules that are separated from the chromosome with which the genomic DNA is naturally associated. Forexample, the isolated nucleic acid molecule can contain less than about 5 kb, including but not limited to 4 kb, 3 kb, 2 kb, 1 kb, 0.5 kb or 0.1 kb of nucleotides which flank the nucleic acid molecule in the genomic DNA of the cell from which the nucleicacid molecule is derived.
The nucleic acid molecule can be fused to other coding or regulatory sequences and still be considered isolated. Thus, recombinant DNA contained in a vector is included in the definition of "isolated" as used herein. Also, isolated nucleic acidmolecules include recombinant DNA molecules in heterologous host cells, as well as partially or substantially purified DNA molecules in solution. "Isolated" nucleic acid molecules also encompass in vivo and in vitro RNA transcripts of the DNA moleculesof the present invention. An isolated nucleic acid molecule or nucleic acid sequence can include a nucleic acid molecule or nucleic acid sequence that is synthesized chemically or by recombinant means. Therefore, recombinant DNA contained in a vectoris included in the definition of "isolated" as used herein. Also, isolated nucleotide sequences include recombinant DNA molecules in heterologous organisms, as well as partially or substantially purified DNA molecules in solution. In vivo and in vitroRNA transcripts of the DNA molecules of the present invention are also encompassed by "isolated" nucleotide sequences. Such isolated nucleotide sequences are useful in the manufacture of the encoded polypeptide, as probes for isolating homologoussequences (e.g., from other mammalian species), for gene mapping (e.g., by in situ hybridization with chromosomes), or for detecting expression of the nucleic acid in tissue (e.g., human tissue), such as by Northern blot analysis.
The present invention also pertains to nucleic acid molecules which are not necessarily found in nature but which encode a FLAP polypeptide (e.g., a polypeptide having an amino acid sequence comprising an amino acid sequence of SEQ ID NOs: 2), oranother splicing variant of a FLAP polypeptide or polymorphic variant thereof. Thus, for example, DNA molecules that comprise a sequence that is different from the naturally occurring nucleic acid sequence but which, due to the degeneracy of the geneticcode, encode a FLAP polypeptide of the present invention are also the subjects of this invention. The invention also encompasses nucleotide sequences encoding portions (fragments), or encoding variant polypeptides such as analogues or derivatives of aFLAP polypeptide. Such variants can be naturally occurring, such as in the case of allelic variation or single nucleotide polymorphisms, or non-naturally-occurring, such as those induced by various mutagens and mutagenic processes. Intended variationsinclude, but are not limited to, addition, deletion and substitution of one or more nucleotides that can result in conservative or non-conservative amino acid changes, including additions and deletions. Preferably, the nucleotide (and/or resultant aminoacid) changes are silent or conserved; that is, they do not alter the characteristics or activity of a FLAP polypeptide. In one preferred embodiment, the nucleotide sequences are fragments that comprise one or more polymorphic microsatellite markers. In another preferred embodiment, the nucleotide sequences are fragments that comprise one or more single nucleotide polymorphisms in a FLAP nucleic acid (e.g., the single nucleotide polymorphisms set forth in Table 13, below).
Other alterations of the nucleic acid molecules of the invention can include, for example, labeling, methylation, internucleotide modifications such as uncharged linkages (e.g., methyl phosphonates, phosphotriesters, phosphoamidates, carbamates),charged linkages (e.g., phosphorothioates, phosphorodithioates), pendent moieties (e.g., polypeptides), intercalators (e.g., acridine, psoralen), chelators, alkylators, and modified linkages (e.g., alpha anomeric nucleic acids). Also included aresynthetic molecules that mimic nucleic acid molecules in the ability to bind to a designated sequence via hydrogen bonding and other chemical interactions. Such molecules include, for example, those in which peptide linkages substitute for phosphatelinkages in the backbone of the molecule.
The invention also pertains to nucleic acid molecules that hybridize under high stringency hybridization conditions, such as for selective hybridization, to a nucleic acid sequence described herein (e.g., nucleic acid molecules which specificallyhybridize to a nucleic acid sequence encoding polypeptides described herein, and, optionally, have an activity of the polypeptide). In one embodiment, the invention includes variants described herein which hybridize under high stringency hybridizationconditions (e.g., for selective hybridization) to a nucleic acid sequence comprising a nucleic acid sequence selected from the group consisting of SEQ ID NOs: 1 or 3 or the complement thereof. In another embodiment, the invention includes variantsdescribed herein which hybridize under high stringency hybridization conditions (e.g., for selective hybridization) to a nucleic acid sequence encoding an amino acid sequence of SEQ ID NO: 2 or a polymorphic variant thereof. In a preferred embodiment,the variant that hybridizes under high stringency hybridizations has an activity of a FLAP.
Such nucleic acid molecules can be detected and/or isolated by specific hybridization (e.g., under high stringency conditions). "Specific hybridization," as used herein, refers to the ability of a first nucleic acid to hybridize to a secondnucleic acid in a manner such that the first nucleic acid does not hybridize to any nucleic acid other than to the second nucleic acid (e.g., when the first nucleic acid has a higher similarity to the second nucleic acid than to any other nucleic acid ina sample wherein the hybridization is to be performed). "Stringency conditions" for hybridization is a term of art which refers to the incubation and wash conditions, e.g., conditions of temperature and buffer concentration, which permit hybridizationof a particular nucleic acid to a second nucleic acid; the first nucleic acid may be perfectly (i.e., 100%) complementary to the second, or the first and second may share some degree of complementarity that is less than perfect (e.g., 70%, 75%, 85%,95%). For example, certain high stringency conditions can be used which distinguish perfectly complementary nucleic acids from those of less complementarity. "High stringency conditions", "moderate stringency conditions" and "low stringency conditions"for nucleic acid hybridizations are explained on pages 2.10.1-2.10.16 and pages 6.3.1-6.3.6 in Current Protocols in Molecular Biology (Ausubel, F. M. et al., "Current Protocols in Molecular Biology", John Wiley & Sons, (1998), the entire teachings ofwhich are incorporated by reference herein). The exact conditions which determine the stringency of hybridization depend not only on ionic strength (e.g., 0.2.times.SSC, 0.1.times.SSC), temperature (e.g., room temperature, 42.degree. C., 68.degree. C.) and the concentration of destabilizing agents such as formamide or denaturing agents such as SDS, but also on factors such as the length of the nucleic acid sequence, base composition, percent mismatch between hybridizing sequences and the frequencyof occurrence of subsets of that sequence within other non-identical sequences. Thus, equivalent conditions can be determined by varying one or more of these parameters while maintaining a similar degree of identity or similarity between the two nucleicacid molecules. Typically, conditions are used such that sequences at least about 60%, at least about 70%, at least about 80%, at least about 90% or at least about 95% or more identical to each other remain hybridized to one another. By varyinghybridization conditions from a level of stringency at which no hybridization occurs to a level at which hybridization is first observed, conditions which will allow a given sequence to hybridize (e.g., selectively) with the most similar sequences in thesample can be determined.
Exemplary conditions are described in Krause, M. H. and S. A. Aaronson, Methods in Enzymology 200: 546-556 (1991), and in, Ausubel, et al., "Current Protocols in Molecular Biology", John Wiley & Sons, (1998), which describes the determination ofwashing conditions for moderate or low stringency conditions. Washing is the step in which conditions are usually set so as to determine a minimum level of complementarity of the hybrids. Generally, starting from the lowest temperature at which onlyhomologous hybridization occurs, each .degree. C. by which the final wash temperature is reduced (holding SSC concentration constant) allows an increase by 1% in the maximum extent of mismatching among the sequences that hybridize. Generally, doublingthe concentration of SSC results in an increase in T.sub.m of -17.degree. C. Using these guidelines, the washing temperature can be determined empirically for high, moderate or low stringency, depending on the level of mismatch sought.
For example, a low stringency wash can comprise washing in a solution containing 0.2.times.SSC/0.1% SDS for 10 minutes at room temperature; a moderate stringency wash can comprise washing in a prewarmed solution (42.degree. C.) solutioncontaining 0.2.times.SSC/0.1% SDS for 15 minutes at 42.degree. C.; and a high stringency wash can comprise washing in prewarmed (68.degree. C.) solution containing 0.1.times.SSC/0.1% SDS for 15 minutes at 68.degree. C. Furthermore, washes can beperformed repeatedly or sequentially to obtain a desired result as known in the art. Equivalent conditions can be determined by varying one or more of the parameters given as an example, as known in the art, while maintaining a similar degree ofidentity or similarity between the target nucleic acid molecule and the primer or probe used.
The percent homology or identity of two nucleotide or amino acid sequences can be determined by aligning the sequences for optimal comparison purposes (e.g., gaps can be introduced in the sequence of a first sequence for optimal alignment). Thenucleotides or amino acids at corresponding positions are then compared, and the percent identity between the two sequences is a function of the number of identical positions shared by the sequences (i.e., % identity=# of identical positions/total # ofpositions.times.100). When a position in one sequence is occupied by the same nucleotide or amino acid residue as the corresponding position in the other sequence, then the molecules are homologous at that position. As used herein, nucleic acid oramino acid "homology" is equivalent to nucleic acid or amino acid "identity". In certain embodiments, the length of a sequence aligned for comparison purposes is at least 30%, for example, at least 40%, in certain embodiments at least 60%, and in otherembodiments at least 70%, 80%, 90% or 95% of the length of the reference sequence. The actual comparison of the two sequences can be accomplished by well-known methods, for example, using a mathematical algorithm. A preferred, non-limiting example ofsuch a mathematical algorithm is described in Karlin et al., Proc. Natl. Acad. Sci. USA 90:5873-5877 (1993). Such an algorithm is incorporated into the NBLAST and XBLAST programs (version 2.0) as described in Altschul et al., Nucleic Acids Res. 25:389-3402 (1997). When utilizing BLAST and Gapped BLAST programs, the default parameters of the respective programs (e.g., NBLAST) can be used. In one embodiment, parameters for sequence comparison can be set at score=100, wordlength=12, or can bevaried (e.g., W=5 or W=20).
Another preferred non-limiting example of a mathematical algorithm utilized for the comparison of sequences is the algorithm of Myers and Miller, CABIOS 4(1): 11-17 (1988). Such an algorithm is incorporated into the ALIGN program (version 2.0)which is part of the GCG sequence alignment software package (Accelrys, Cambridge, UK). When utilizing the ALIGN program for comparing amino acid sequences, a PAM120 weight residue table, a gap length penalty of 12, and a gap penalty of 4 can be used. Additional algorithms for sequence analysis are known in the art and include ADVANCE and ADAM as described in Torellis and Robotti, Comput. Appl. Biosci. 10:3-5 (1994); and FASTA described in Pearson and Lipman, Proc. Natl. Acad. Sci. USA85:2444-8 (1988).
In another embodiment, the percent identity between two amino acid sequences can be accomplished using the GAP program in the GCG software package using either a BLOSUM63 matrix or a PAM250 matrix, and a gap weight of 12, 10, 8, 6, or 4 and alength weight of 2, 3, or 4. In yet another embodiment, the percent identity between two nucleic acid sequences can be accomplished using the GAP program in the GCG software package using a gap weight of 50 and a length weight of 3.
The present invention also provides isolated nucleic acid molecules that contain a fragment or portion that hybridizes under highly stringent conditions to a nucleic acid sequence comprising SEQ ID NO: 1 or 3 or the complement of SEQ ID NO: 1 or3, and also provides isolated nucleic acid molecules that contain a fragment or portion that hybridizes under highly stringent conditions to a nucleic acid sequence encoding an amino acid sequence of the invention or polymorphic variant thereof. Thenucleic acid fragments of the invention are at least about 15, for example, at least about 18, 20, 23 or 25 nucleotides, and can be 30, 40, 50, 100, 200 or more nucleotides in length. Longer fragments, for example, 30 or more nucleotides in length,encoding antigenic polypeptides described herein are particularly useful, such as for the generation of antibodies as described below.
Probes and Primers
In a related aspect, the nucleic acid fragments of the invention are used as probes or primers in assays such as those described herein. "Probes" or "primers" are oligonucleotides that hybridize in a base-specific manner to a complementarystrand of nucleic acid molecules. Such probes and primers include polypeptide nucleic acids, as described in Nielsen et al. (Science 254:1497-1500 (1991)).
A probe or primer comprises a region of nucleic acid that hybridizes to at least about 15, for example about 20-25, and in certain embodiments about 40, 50 or 75, consecutive nucleotides of a nucleic acid of the invention, such as a nucleic acidcomprising a contiguous nucleic acid sequence of SEQ ID NOs: 1 or 3 or the complement of SEQ ID NOs: 1 or 3, or a nucleic acid sequence encoding an amino acid sequence of SEQ ID NO: 2 or polymorphic variant thereof. In preferred embodiments, a probe orprimer comprises 100 or fewer nucleotides, in certain embodiments, from 6 to 50 nucleotides, for example, from 12 to 30 nucleotides. In other embodiments, the probe or primer is at least 70% identical to the contiguous nucleic acid sequence or to thecomplement of the contiguous nucleotide sequence, for example, at least 80% identical, in certain embodiments at least 90% identical, and in other embodiments at least 95% identical, or even capable of selectively hybridizing to the contiguous nucleicacid sequence or to the complement of the contiguous nucleotide sequence. Often, the probe or primer further comprises a label, e.g., radioisotope, fluorescent compound, enzyme, or enzyme co-factor.
The nucleic acid molecules of the invention such as those described above can be identified and isolated using standard molecular biology techniques and the sequence information provided herein. For example, nucleic acid molecules can beamplified and isolated using the polymerase chain reaction and synthetic oligonucleotide primers based on one or more of SEQ ID NOs: 1 or 3, or the complement thereof, or designed based on nucleotides based on sequences encoding one or more of the aminoacid sequences provided herein. See generally PCR Technology: Principles and Applications for DNA Amplification (ed. H. A. Erlich, Freeman Press, NY, N.Y., 1992); PCR Protocols: A Guide to Methods and Applications (Eds. Innis et al., Academic Press,San Diego, Calif., 1990); Mattila et al., Nucl. Acids Res. 19:4967 (1991); Eckert et al., PCR Methods and Applications 1:17 (1991); PCR (eds. McPherson et al., IRL Press, Oxford); and U.S. Pat. No. 4,683,202. The nucleic acid molecules can beamplified using cDNA, mRNA or genomic DNA as a template, cloned into an appropriate vector and characterized by DNA sequence analysis.
Other suitable amplification methods include the ligase chain reaction (LCR) (see Wu and Wallace, Genomics 4:560 (1989), Landegren et al., Science 241:1077 (1988), transcription amplification (Kwoh et al., Proc. Natl. Acad. Sci. USA 86:1173(1989)), and self-sustained sequence replication (Guatelli et al., Proc. Nat. Acad. Sci. USA 87:1874 (1990)) and nucleic acid based sequence amplification (NASBA). The latter two amplification methods involve isothermal reactions based on isothermaltranscription, which produce both single stranded RNA (ssRNA) and double stranded DNA (dsDNA) as the amplification products in a ratio of about 30 or 100 to 1, respectively.
The amplified DNA can be labeled, for example, radiolabeled, and used as a probe for screening a cDNA library derived from human cells, mRNA in zap express, ZIPLOX or other suitable vector. Corresponding clones can be isolated, DNA can obtainedfollowing in vivo excision, and the cloned insert can be sequenced in either or both orientations by art recognized methods to identify the correct reading frame encoding a polypeptide of the appropriate molecular weight. For example, the directanalysis of the nucleic acid molecules of the present invention can be accomplished using well-known methods that are commercially available. See, for example, Sambrook et al., Molecular Cloning, A Laboratory Manual (2nd Ed., CSHP, New York 1989);Zyskind et al., Recombinant DNA Laboratory Manual, (Acad. Press, 1988)). Using these or similar methods, the polypeptide and the DNA encoding the polypeptide can be isolated, sequenced and further characterized.
Antisense nucleic acid molecules of the invention can be designed using the nucleotide sequences of SEQ ID NOs: 1 or 3 and/or the complement of one or more of SEQ ID NOs: 1 or 3 and/or a portion of one or more of SEQ ID NOs: 1 or 3 or thecomplement of one or more of SEQ ID NOs: 1 or 3 and/or a sequence encoding the amino acid sequences of SEQ ID NOs: 2 or encoding a portion of one or more of SEQ ID NOs: 1 or 3 or their complement. They can be constructed using chemical synthesis andenzymatic ligation reactions using procedures known in the art. For example, an antisense nucleic acid molecule (e.g., an antisense oligonucleotide) can be chemically synthesized using naturally occurring nucleotides or variously modified nucleotidesdesigned to increase the biological stability of the molecules or to increase the physical stability of the duplex formed between the antisense and sense nucleic acids, e.g., phosphorothioate derivatives and acridine substituted nucleotides can be used. Alternatively, the antisense nucleic acid molecule can be produced biologically using an expression vector into which a nucleic acid molecule has been subcloned in an antisense orientation (i.e., RNA transcribed from the inserted nucleic acid moleculewill be of an antisense orientation to a target nucleic acid of interest).
The nucleic acid sequences can also be used to compare with endogenous DNA sequences in patients to identify one or more of the disorders related to FLAP, and as probes, such as to hybridize and discover related DNA sequences or to subtract outknown sequences from a sample. The nucleic acid sequences can further be used to derive primers for genetic fingerprinting, to raise anti-polypeptide antibodies using DNA immunization techniques, and as an antigen to raise anti-DNA antibodies or elicitimmune responses. Portions or fragments of the nucleotide sequences identified herein (and the corresponding complete gene sequences) can be used in numerous ways as polynucleotide reagents. For example, these sequences can be used to: (i) map theirrespective genes on a chromosome; and, thus, locate gene regions or nucleic acid regions associated with genetic disease; (ii) identify an individual from a minute biological sample (tissue typing); and (iii) aid in forensic identification of abiological sample. Additionally, the nucleotide sequences of the invention can be used to identify and express recombinant polypeptides for analysis, characterization or therapeutic use, or as markers for tissues in which the corresponding polypeptideis expressed, either constitutively, during tissue differentiation, or in diseased states. The nucleic acid sequences can additionally be used as reagents in the screening and/or diagnostic assays described herein, and can also be included as componentsof kits (e.g., reagent kits) for use in the screening and/or diagnostic assays described herein.
Vectors
Another aspect of the invention pertains to nucleic acid constructs containing a nucleic acid molecule of SEQ ID NOs: 1 or 3 or the complement thereof (or a portion thereof). Yet another aspect of the invention pertains to nucleic acidconstructs containing a nucleic acid molecule encoding an amino acid of SEQ ID NO: 2 or polymorphic variant thereof. The constructs comprise a vector (e.g., an expression vector) into which a sequence of the invention has been inserted in a sense orantisense orientation. As used herein, the term "vector" refers to a nucleic acid molecule capable of transporting another nucleic acid to which it has been linked. One type of vector is a "plasmid", which refers to a circular double stranded DNA loopinto which additional DNA segments can be ligated. Another type of vector is a viral vector, wherein additional DNA segments can be ligated into the viral genome. Certain vectors are capable of autonomous replication in a host cell into which they areintroduced (e.g., bacterial vectors having a bacterial origin of replication and episomal mammalian vectors). Other vectors (e.g., non-episomal mammalian vectors) are integrated into the genome of a host cell upon introduction into the host cell, andthereby are replicated along with the host genome. Moreover, certain vectors, such as expression vectors, are capable of directing the expression of genes or nucleic acids to which they are operably linked. In general, expression vectors of utility inrecombinant DNA techniques are often in the form of plasmids. However, the invention is intended to include such other forms of expression vectors, such as viral vectors (e.g., replication defective retroviruses, adenoviruses and adeno-associatedviruses) that serve equivalent functions.
Preferred recombinant expression vectors of the invention comprise a nucleic acid molecule of the invention in a form suitable for expression of the nucleic acid molecule in a host cell. This means that the recombinant expression vectors includeone or more regulatory sequences, selected on the basis of the host cells to be used for expression, which is operably linked to the nucleic acid sequence to be expressed. Within a recombinant expression vector, "operably linked" or "operatively linked"is intended to mean that the nucleic acid sequence of interest is linked to the regulatory sequence(s) in a manner which allows for expression of the nucleic acid sequence (e.g., in an in vitro transcription/translation system or in a host cell when thevector is introduced into the host cell). The term "regulatory sequence" is intended to include promoters, enhancers and other expression control elements (e.g., polyadenylation signals). Such regulatory sequences are described, for example, inGoeddel, "Gene Expression Technology", Methods in Enzymology 185, Academic Press, San Diego, Calif. (1990). Regulatory sequences include those which direct constitutive expression of a nucleic acid sequence in many types of host cell and those whichdirect expression of the nucleic acid sequence only in certain host cells (e.g., tissue-specific regulatory sequences). It will be appreciated by those skilled in the art that the design of the expression vector can depend on such factors as the choiceof the host cell to be transformed and the level of expression of polypeptide desired. The expression vectors of the invention can be introduced into host cells to thereby produce polypeptides, including fusion polypeptides, encoded by nucleic acidmolecules as described herein.
The recombinant expression vectors of the invention can be designed for expression of a polypeptide of the invention in prokaryotic or eukaryotic cells, e.g., bacterial cells such as E. coli, insect cells (using baculovirus expression vectors),yeast cells or mammalian cells. Suitable host cells are discussed further in Goeddel, supra. Alternatively, the recombinant expression vector can be transcribed and translated in vitro, for example using T7 promoter regulatory sequences and T7polymerase.
Another aspect of the invention pertains to host cells into which a recombinant expression vector of the invention has been introduced. The terms "host cell" and "recombinant host cell" are used interchangeably herein. It is understood thatsuch terms refer not only to the particular subject cell but also to the progeny or potential progeny of such a cell. Because certain modifications may occur in succeeding generations due to either mutation or environmental influences, such progeny maynot, in fact, be identical to the parent cell, but are still included within the scope of the term as used herein.
A host cell can be any prokaryotic or eukaryotic cell. For example, a nucleic acid molecule of the invention can be expressed in bacterial cells (e.g., E. coli), insect cells, yeast or mammalian cells (such as Chinese hamster ovary cells (CHO)or COS cells). Other suitable host cells are known to those skilled in the art.
Vector DNA can be introduced into prokaryotic or eukaryotic cells via conventional transformation or transfection techniques. As used herein, the terms "transformation" and "transfection" are intended to refer to a variety of art-recognizedtechniques for introducing a foreign nucleic acid molecule (e.g., DNA) into a host cell, including calcium phosphate or calcium chloride co-precipitation, DEAE-dextran-mediated transfection, lipofection, or electroporation. Suitable methods fortransforming or transfecting host cells can be found in Sambrook, et al. (supra), and other laboratory manuals.
For stable transfection of mammalian cells, it is known that, depending upon the expression vector and transfection technique used, only a small fraction of cells may integrate the foreign DNA into their genome. In order to identify and selectthese integrants, a gene or nucleic acid that encodes a selectable marker (e.g., for resistance to antibiotics) is generally introduced into the host cells along with the gene or nucleic acid of interest. Preferred selectable markers include those thatconfer resistance to drugs, such as G418, hygromycin and methotrexate. Nucleic acid molecules encoding a selectable marker can be introduced into a host cell on the same vector as the nucleic acid molecule of the invention or can be introduced on aseparate vector. Cells stably transfected with the introduced nucleic acid molecule can be identified by drug selection (e.g., cells that have incorporated the selectable marker gene or nucleic acid will survive, while the other cells die).
A host cell of the invention, such as a prokaryotic host cell or eukaryotic host cell in culture can be used to produce (i.e., express) a polypeptide of the invention. Accordingly, the invention further provides methods for producing apolypeptide using the host cells of the invention. In one embodiment, the method comprises culturing the host cell of invention (into which a recombinant expression vector encoding a polypeptide of the invention has been introduced) in a suitable mediumsuch that the polypeptide is produced. In another embodiment, the method further comprises isolating the polypeptide from the medium or the host cell.
The host cells of the invention can also be used to produce nonhuman transgenic animals. For example, in one embodiment, a host cell of the invention is a fertilized oocyte or an embryonic stem cell into which a nucleic acid molecule of theinvention has been introduced (e.g., an exogenous FLAP nucleic acid, or an exogenous nucleic acid encoding a FLAP polypeptide). Such host cells can then be used to create non-human transgenic animals in which exogenous nucleotide sequences have beenintroduced into the genome or homologous recombinant animals in which endogenous nucleotide sequences have been altered. Such animals are useful for studying the function and/or activity of the nucleic acid sequence and polypeptide encoded by thesequence and for identifying and/or evaluating modulators of their activity. As used herein, a "transgenic animal" is a non-human animal, preferably a mammal, more preferably a rodent such as a rat or mouse, in which one or more of the cells of theanimal include a transgene. Other examples of transgenic animals include non-human primates, sheep, dogs, cows, goats, chickens and amphibians. A transgene is exogenous DNA which is integrated into the genome of a cell from which a transgenic animaldevelops and which remains in the genome of the mature animal, thereby directing the expression of an encoded gene product in one or more cell types or tissues of the transgenic animal. As used herein, an "homologous recombinant animal" is a non-humananimal, preferably a mammal, more preferably a mouse, in which an endogenous gene has been altered by homologous recombination between the endogenous gene and an exogenous DNA molecule introduced into a cell of the animal, e.g., an embryonic cell of theanimal, prior to development of the animal.
Methods for generating transgenic animals via embryo manipulation and microinjection, particularly animals such as mice, have become conventional in the art and are described, for example, in U.S. Pat. Nos. 4,736,866 and 4,870,009, 4,873,191and in Hogan, Manipulating the Mouse Embryo (Cold Spring Harbor Laboratory Press, Cold Spring Harbor, N.Y., 1986). Methods for constructing homologous recombination vectors and homologous recombinant animals are described further in Bradley, CurrentOpinion in BioTechnology 2:823-829 (1991) and in PCT Publication Nos. WO 90/11354, WO 91/01140, WO 92/0968, and WO 93/04169. Clones of the non-human transgenic animals described herein can also be produced according to the methods described in Wilmutet al., Nature 385:810-813 (1997) and PCT Publication Nos. WO 97/07668 and WO 97/07669.
POLYPEPTIDES OF THE INVENTION
The present invention also pertains to isolated polypeptides encoded by FLAP nucleic acids ("FLAP polypeptides"), and fragments and variants thereof, as well as polypeptides encoded by nucleotide sequences described herein (e.g., other splicingvariants). The term "polypeptide" refers to a polymer of amino acids, and not to a specific length; thus, peptides, oligopeptides and proteins are included within the definition of a polypeptide. As used herein, a polypeptide is said to be "isolated"or "purified" when it is substantially free of cellular material when it is isolated from recombinant and non-recombinant cells, or free of chemical precursors or other chemicals when it is chemically synthesized. A polypeptide, however, can be joinedto another polypeptide with which it is not normally associated in a cell (e.g., in a "fusion protein") and still be "isolated" or "purified."
The polypeptides of the invention can be purified to homogeneity. It is understood, however, that preparations in which the polypeptide is not purified to homogeneity are useful. The critical feature is that the preparation allows for thedesired function of the polypeptide, even in the presence of considerable amounts of other components. Thus, the invention encompasses various degrees of purity. In one embodiment, the language "substantially free of cellular material" includespreparations of the polypeptide having less than about 30% (by dry weight) other proteins (i.e., contaminating protein), less than about 20% other proteins, less than about 10% other proteins, or less than about 5% other proteins.
When a polypeptide is recombinantly produced, it can also be substantially free of culture medium, i.e., culture medium represents less than about 20%, less than about 10%, or less than about 5% of the volume of the polypeptide preparation. Thelanguage "substantially free of chemical precursors or other chemicals" includes preparations of the polypeptide in which it is separated from chemical precursors or other chemicals that are involved in its synthesis. In one embodiment, the language"substantially free of chemical precursors or other chemicals" includes preparations of the polypeptide having less than about 30% (by dry weight) chemical precursors or other chemicals, less than about 20% chemical precursors or other chemicals, lessthan about 10% chemical precursors or other chemicals, or less than about 5% chemical precursors or other chemicals.
In one embodiment, a polypeptide of the invention comprises an amino acid sequence encoded by a nucleic acid molecule comprising a nucleic acid sequence selected from the group consisting of SEQ ID NO: 1 or 3, or the complement of SEQ ID NO: 1 or3, or portions thereof, or a portion or polymorphic variant thereof. However, the polypeptides of the invention also encompass fragment and sequence variants. Variants include a substantially homologous polypeptide encoded by the same genetic locus inan organism, i.e., an allelic variant, as well as other splicing variants. Variants also encompass polypeptides derived from other genetic loci in an organism, but having substantial homology to a polypeptide encoded by a nucleic acid moleculecomprising a nucleic acid sequence selected from the group consisting of SEQ ID NOs: 1 or 3 or their complement, or portions thereof, or having substantial homology to a polypeptide encoded by a nucleic acid molecule comprising a nucleic acid sequenceselected from the group consisting of nucleotide sequences encoding SEQ ID NO: 2 or polymorphic variants thereof. Variants also include polypeptides substantially homologous or identical to these polypeptides but derived from another organism, i.e., anortholog. Variants also include polypeptides that are substantially homologous or identical to these polypeptides that are produced by chemical synthesis. Variants also include polypeptides that are substantially homologous or identical to thesepolypeptides that are produced by recombinant methods.
As used herein, two polypeptides (or a region of the polypeptides) are substantially homologous or identical when the amino acid sequences are at least about 45-55%, in certain embodiments at least about 70-75%, and in other embodiments at leastabout 80-85%, and in others greater than about 90% or more homologous or identical. A substantially homologous amino acid sequence, according to the present invention, will be encoded by a nucleic acid molecule hybridizing to SEQ ID NO: 1 or 3 orportion thereof, under stringent conditions as more particularly described above, or will be encoded by a nucleic acid molecule hybridizing to a nucleic acid sequence encoding SEQ ID NO: 2 or a portion thereof or polymorphic variant thereof, understringent conditions as more particularly described thereof.
The invention also encompasses polypeptides having a lower degree of identity but having sufficient similarity so as to perform one or more of the same functions performed by a polypeptide encoded by a nucleic acid molecule of the invention. Similarity is determined by conserved amino acid substitution. Such substitutions are those that substitute a given amino acid in a polypeptide by another amino acid of like characteristics. Conservative substitutions are likely to be phenotypicallysilent. Typically seen as conservative substitutions are the replacements, one for another, among the aliphatic amino acids Ala, Val, Leu and Ile; interchange of the hydroxyl residues Ser and Thr, exchange of the acidic residues Asp and Glu,substitution between the amide residues Asn and Gin, exchange of the basic residues Lys and Arg and replacements among the aromatic residues Phe and Tyr. Guidance concerning which amino acid changes are likely to be phenotypically silent are found inBowie et al., Science 247:1306-1310 (1990).
A variant polypeptide can differ in amino acid sequence by one or more substitutions, deletions, insertions, inversions, fusions, and truncations or a combination of any of these. Further, variant polypeptides can be fully functional or can lackfunction in one or more activities. Fully functional variants typically contain only conservative variation or variation in non-critical residues or in non-critical regions. Functional variants can also contain substitution of similar amino acids thatresult in no change or an insignificant change in function. Alternatively, such substitutions may positively or negatively affect function to some degree. Non-functional variants typically contain one or more non-conservative amino acid substitutions,deletions, insertions, inversions, or truncation or a substitution, insertion, inversion, or deletion in a critical residue or critical region.
Amino acids that are essential for function can be identified by methods known in the art, such as site-directed mutagenesis or alanine-scanning mutagenesis (Cunningham et al., Science 244:1081-1085 (1989)). The latter procedure introducessingle alanine mutations at every residue in the molecule. The resulting mutant molecules are then tested for biological activity in vitro, or in vitro proliferative activity. Sites that are critical for polypeptide activity can also be determined bystructural analysis such as crystallization, nuclear magnetic resonance or photoaffinity labeling (Smith et al., J. Mol. Biol. 224:899-904 (1992); de Vos et al., Science 255:306-312 (1992)).
The invention also includes fragments of the polypeptides of the invention. Fragments can be derived from a polypeptide encoded by a nucleic acid molecule comprising SEQ ID NO: 1 or 3, or the complement of SEQ ID NO: 1 or 3 (or other variants). However, the invention also encompasses fragments of the variants of the polypeptides described herein. As used herein, a fragment comprises at least 6 contiguous amino acids. Useful fragments include those that retain one or more of the biologicalactivities of the polypeptide as well as fragments that can be used as an immunogen to generate polypeptide-specific antibodies.
Biologically active fragments (peptides which are, for example, 6, 9, 12, 15, 16, 20, 30, 35, 36, 37, 38, 39, 40, 50, 100 or more amino acids in length) can comprise a domain, segment, or motif that has been identified by analysis of thepolypeptide sequence using well-known methods, e.g., signal peptides, extracellular domains, one or more transmembrane segments or loops, ligand binding regions, zinc finger domains, DNA binding domains, acylation sites, glycosylation sites, orphosphorylation sites.
Fragments can be discrete (not fused to other amino acids or polypeptides) or can be within a larger polypeptide. Further, several fragments can be comprised within a single larger polypeptide. In one embodiment a fragment designed forexpression in a host can have heterologous pre- and pro-polypeptide regions fused to the amino terminus of the polypeptide fragment and an additional region fused to the carboxyl terminus of the fragment.
The invention thus provides chimeric or fusion polypeptides. These comprise a polypeptide of the invention operatively linked to a heterologous protein or polypeptide having an amino acid sequence not substantially homologous to the polypeptide. "Operatively linked" indicates that the polypeptide and the heterologous protein are fused in-frame. The heterologous protein can be fused to the N-terminus or C-terminus of the polypeptide. In one embodiment the fusion polypeptide does not affectfunction of the polypeptide per se. For example, the fusion polypeptide can be a GST-fusion polypeptide in which the polypeptide sequences are fused to the C-terminus of the GST sequences. Other types of fusion polypeptides include, but are not limitedto, enzymatic fusion polypeptides, for example beta-galactosidase fusions, yeast two-hybrid GAL fusions, poly-His fusions and Ig fusions. Such fusion polypeptides, particularly poly-His fusions, can facilitate the purification of recombinantpolypeptide. In certain host cells (e.g., mammalian host cells), expression and/or secretion of a polypeptide can be increased using a heterologous signal sequence. Therefore, in another embodiment, the fusion polypeptide contains a heterologous signalsequence at its N-terminus.
EP-A-O 464 533 discloses fusion proteins comprising various portions of immunoglobulin constant regions. The Fc is useful in therapy and diagnosis and thus results, for example, in improved pharmacokinetic properties (EP-A 0232 262). In drugdiscovery, for example, human proteins have been fused with Fc portions for the purpose of high-throughput screening assays to identify antagonists. Bennett et al., Journal of Molecular Recognition, 8:52-58 (1995) and Johanson et al., The Journal ofBiological Chemistry, 270,16:9459-9471 (1995). Thus, this invention also encompasses soluble fusion polypeptides containing a polypeptide of the invention and various portions of the constant regions of heavy or light chains of immunoglobulins ofvarious subclasses (IgG, IgM, IgA, IgE).
A chimeric or fusion polypeptide can be produced by standard recombinant DNA techniques. For example, DNA fragments coding for the different polypeptide sequences are ligated together in-frame in accordance with conventional techniques. Inanother embodiment, the fusion gene can be synthesized by conventional techniques including automated DNA synthesizers. Alternatively, PCR amplification of nucleic acid fragments can be carried out using anchor primers which give rise to complementaryoverhangs between two consecutive nucleic acid fragments which can subsequently be annealed and re-amplified to generate a chimeric nucleic acid sequence (see Ausubel et al., Current Protocols in Molecular Biology, 1992). Moreover, many expressionvectors are commercially available that already encode a fusion moiety (e.g., a GST protein). A nucleic acid molecule encoding a polypeptide of the invention can be cloned into such an expression vector such that the fusion moiety is linked in-frame tothe polypeptide.
The isolated polypeptide can be purified from cells that naturally express it, purified from cells that have been altered to express it (recombinant), or synthesized using known protein synthesis methods. In one embodiment, the polypeptide isproduced by recombinant DNA techniques. For example, a nucleic acid molecule encoding the polypeptide is cloned into an expression vector, the expression vector introduced into a host cell and the polypeptide expressed in the host cell. The polypeptidecan then be isolated from the cells by an appropriate purification scheme using standard protein purification techniques.
The polypeptides of the present invention can be used to raise antibodies or to elicit an immune response. The polypeptides can also be used as a reagent, e.g., a labeled reagent, in assays to quantitatively determine levels of the polypeptideor a molecule to which it binds (e.g., a ligand) in biological fluids. The polypeptides can also be used as markers for cells or tissues in which the corresponding polypeptide is preferentially expressed, either constitutively, during tissuedifferentiation, or in diseased states. The polypeptides can be used to isolate a corresponding binding agent, e.g., ligand, such as, for example, in an interaction trap assay, and to screen for peptide or small molecule antagonists or agonists of thebinding interaction. For example, because members of the leukotriene pathway including FLAP bind to receptors, the leukotriene pathway polypeptides can be used to isolate such receptors.
ANTIBODIES OF THE INVENTION
Polyclonal and/or monoclonal antibodies that specifically bind one form of the polypeptide or nucleic acid product (e.g., a polypeptide encoded by a nucleic acid having a SNP as set forth in Table 13), but not to another form of the polypeptideor nucleic acid product, are also provided. Antibodies are also provided which bind a portion of either polypeptide encoded by nucleic acids of the invention (e.g., SEQ ID NO: 1 or SEQ ID NO: 3, or the complement of SEQ ID NO: 1 or SEQ ID NO: 3), or toa polypeptide encoded by nucleic acids of the invention that contain a polymorphic site or sites. The invention also provides antibodies to the polypeptides and polypeptide fragments of the invention, or a portion thereof, or having an amino acidsequence encoded by a nucleic acid molecule comprising all or a portion of SEQ ID NOs: 1 or 3, or the complement thereof, or another variant or portion thereof. The term "antibody" as used herein refers to immunoglobulin molecules and immunologicallyactive portions of immunoglobulin molecules, i.e., molecules that contain an antigen binding site that specifically binds an antigen. A molecule that specifically binds to a polypeptide of the invention is a molecule that binds to that polypeptide or afragment thereof, but does not substantially bind other molecules in a sample, e.g., a biological sample, which naturally contains the polypeptide. Examples of immunologically active portions of immunoglobulin molecules include F(ab) and F(ab').sub.2fragments which can be generated by treating the antibody with an enzyme such as pepsin. The invention provides polyclonal and monoclonal antibodies that bind to a polypeptide of the invention. The term "monoclonal antibody" or "monoclonal antibodycomposition", as used herein, refers to a population of antibody molecules that contain only one species of an antigen binding site capable of immunoreacting with a particular epitope of a polypeptide of the invention. A monoclonal antibody compositionthus typically displays a single binding affinity for a particular polypeptide of the invention with which it immunoreacts.
Polyclonal antibodies can be prepared as described above by immunizing a suitable subject with a desired immunogen, e.g., polypeptide of the invention or fragment thereof. The antibody titer in the immunized subject can be monitored over time bystandard techniques, such as with an enzyme linked immunosorbent assay (ELISA) using immobilized polypeptide. If desired, the antibody molecules directed against the polypeptide can be isolated from the mammal (e.g., from the blood) and further purifiedby well-known techniques, such as protein A chromatography to obtain the IgG fraction. At an appropriate time after immunization, e.g., when the antibody titers are highest, antibody-producing cells can be obtained from the subject and used to preparemonoclonal antibodies by standard techniques, such as the hybridoma technique originally described by Kohler and Milstein, Nature 256:495-497 (1975), the human B cell hybridoma technique (Kozbor et al., Immunol. Today 4:72 (1983)); the EBV-hybridomatechnique (Cole et al., Monoclonal Antibodies and Cancer Therapy, Alan R. Liss, 1985, Inc., pp. 77-96); or trioma techniques. The technology for producing hybridomas is well known (see generally Current Protocols in Immunology (1994) Coligan et al.(eds.) John Wiley & Sons, Inc., New York, N.Y.). Briefly, an immortal cell line (typically a myeloma) is fused to lymphocytes (typically splenocytes) from a mammal immunized with an immunogen as described above, and the culture supernatants of theresulting hybridoma cells are screened to identify a hybridoma producing a monoclonal antibody that binds a polypeptide of the invention.
Any of the many well known protocols used for fusing lymphocytes and immortalized cell lines can be applied for the purpose of generating a monoclonal antibody to a polypeptide of the invention (see, e.g., Current Protocols in Immunology, supra;Galfre et al., Nature 266:55052 (1977); R. H. Kenneth, in Monoclonal Antibodies: A New Dimension In Biological Analyses, Plenum Publishing Corp., New York, N.Y. (1980); and Lerner, Yale J. Biol. Med. 54:387-402 (1981). Moreover, the ordinarilyskilled worker will appreciate that there are many variations of such methods that also would be useful.
Alternative to preparing monoclonal antibody-secreting hybridomas, a monoclonal antibody to a polypeptide of the invention can be identified and isolated by screening a recombinant combinatorial immunoglobulin library (e.g., an antibody phagedisplay library) with the polypeptide to thereby isolate immunoglobulin library members that bind the polypeptide. Kits for generating and screening phage display libraries are commercially available (e.g., the Pharmacia Recombinant Phage AntibodySystem, Catalog No. 27-9400-01; and the Stratagene SurfZAP.TM. Phage Display Kit, Catalog No. 240612). Additionally, examples of methods and reagents particularly amenable for use in generating and screening antibody display library can be found in,for example, U.S. Pat. No. 5,223,409; PCT Publication No. WO 92/18619; PCT Publication No. WO 91/17271; PCT Publication No. WO 92/20791; PCT Publication No. WO 92/15679; PCT Publication No. WO 93/01288; PCT Publication No. WO 92/01047; PCT PublicationNo. WO 92/09690; PCT Publication No. WO 90/02809; Fuchs et al., Bio/Technology 9: 1370-1372 (1991); Hay et al., Hum. Antibod. Hybridomas 3:81-85 (1992); Huse et al., Science 246:1275-1281 (1989); Griffiths et al., EMBO J. 12:725-734 (1993).
Additionally, recombinant antibodies, such as chimeric and humanized monoclonal antibodies, comprising both human and non-human portions, which can be made using standard recombinant DNA techniques, are within the scope of the invention. Suchchimeric and humanized monoclonal antibodies can be produced by recombinant DNA techniques known in the art.
In general, antibodies of the invention (e.g., a monoclonal antibody) can be used to isolate a polypeptide of the invention by standard techniques, such as affinity chromatography or immunoprecipitation. A polypeptide-specific antibody canfacilitate the purification of natural polypeptide from cells and of recombinantly produced polypeptide expressed in host cells. Moreover, an antibody specific for a polypeptide of the invention can be used to detect the polypeptide (e.g., in a cellularlysate, cell supernatant, or tissue sample) in order to evaluate the abundance and pattern of expression of the polypeptide. Antibodies can be used diagnostically to monitor protein levels in tissue as part of a clinical testing procedure, e.g., to, forexample, determine the efficacy of a given treatment regimen. Detection can be facilitated by coupling the antibody to a detectable substance. Examples of detectable substances include various enzymes, prosthetic groups, fluorescent materials,luminescent materials, bioluminescent materials, and radioactive materials. Examples of suitable enzymes include horseradish peroxidase, alkaline phosphatase, .beta.-galactosidase, or acetylcholinesterase; examples of suitable prosthetic group complexesinclude streptavidin/biotin and avidin/biotin; examples of suitable fluorescent materials include umbelliferone, fluorescein, fluorescein isothiocyanate, rhodamine, dichlorotriazinylamine fluorescein, dansyl chloride or phycoerythrin; an example of aluminescent material includes luminol; examples of bioluminescent materials include luciferase, luciferin and aequorin, and examples of suitable radioactive material include .sup.125I, .sup.131I, .sup.35S or .sup.3H.
DIAGNOSTIC ASSAYS
Diagnosis Using Probes, Primers, Polypeptides, and Antibodies
The nucleic acids, probes, primers, polypeptides and antibodies described herein can be used in methods of diagnosis of a susceptibility to MI or stroke, or to a disease or condition associated with a gene such as FLAP, as well as in kits usefulfor diagnosis of a susceptibility to MI or stroke, or to a disease or condition associated with FLAP. In one embodiment, the kit useful for diagnosis of susceptibility to MI or stroke, or to a disease or condition associated with FLAP comprises primersas described herein, wherein the primers contain one or more of the SNPs identified in Table 13.
In one embodiment of the invention, diagnosis of susceptibility to MI or stroke (or diagnosis of or susceptibility to a disease or condition associated with FLAP), is made by detecting a polymorphism in a FLAP nucleic acid as described herein. The polymorphism can be an alteration in a FLAP nucleic acid, such as the insertion or deletion of a single nucleotide, or of more than one nucleotide, resulting in a frame shift alteration; the change of at least one nucleotide, resulting in a change inthe encoded amino acid; the change of at least one nucleotide, resulting in the generation of a premature stop codon; the deletion of several nucleotides, resulting in a deletion of one or more amino acids encoded by the nucleotides; the insertion of oneor several nucleotides, such as by unequal recombination or gene conversion, resulting in an interruption of the coding sequence of the gene or nucleic acid; duplication of all or a part of the gene or nucleic acid; transposition of all or a part of thegene or nucleic acid; or rearrangement of all or a part of the gene or nucleic acid. More than one such alteration may be present in a single gene or nucleic acid. Such sequence changes cause an alteration in the polypeptide encoded by a FLAP nucleicacid. For example, if the alteration is a frame shift alteration, the frame shift can result in a change in the encoded amino acids, and/or can result in the generation of a premature stop codon, causing generation of a truncated polypeptide. Alternatively, a polymorphism associated with a disease or condition associated with a FLAP nucleic acid or a susceptibility to a disease or condition associated with a FLAP nucleic acid can be a synonymous alteration in one or more nucleotides (i.e., analteration that does not result in a change in the polypeptide encoded by a FLAP nucleic acid). Such a polymorphism may alter splicing sites, affect the stability or transport of mRNA, or otherwise affect the transcription or translation of the nucleicacid. A FLAP nucleic acid that has any of the alteration described above is referred to herein as an "altered nucleic acid."
In a first method of diagnosing a susceptibility to MI or stroke, hybridization methods, such as Southern analysis, Northern analysis, or in situ hybridizations, can be used (see Current Protocols in Molecular Biology, Ausubel, F. et al., eds.,John Wiley & Sons, including all supplements through 1999). For example, a biological sample from a test subject (a "test sample") of genomic DNA, RNA, or cDNA, is obtained from an individual suspected of having, being susceptible to or predisposed for,or carrying a defect for, a susceptibility to a disease or condition associated with a FLAP nucleic acid (the "test individual"). The individual can be an adult, child, or fetus. The test sample can be from any source which contains genomic DNA, suchas a blood sample, sample of amniotic fluid, sample of cerebrospinal fluid, or tissue sample from skin, muscle, buccal or conjunctival mucosa, placenta, gastrointestinal tract or other organs. A test sample of DNA from fetal cells or tissue can beobtained by appropriate methods, such as by amniocentesis or chorionic villus sampling. The DNA, RNA, or cDNA sample is then examined to determine whether a polymorphism in a nucleic acid is present, and/or to determine which splicing variant(s) encodedby the FLAP is present. The presence of the polymorphism or splicing variant(s) can be indicated by hybridization of the nucleic acid in the genomic DNA, RNA, or cDNA to a nucleic acid probe. A "nucleic acid probe", as used herein, can be a DNA probeor an RNA probe; the nucleic acid probe can contain at least one polymorphism in a FLAP nucleic acid or contains a nucleic acid encoding a particular splicing variant of a FLAP nucleic acid. The probe can be any of the nucleic acid molecules describedabove (e.g., the nucleic acid, a fragment, a vector comprising the nucleic acid, a probe or primer, etc.).
To diagnose a susceptibility to MI or stroke (or a disease or condition associated with FLAP), the test sample containing a FLAP nucleic acid is contacted with at least one nucleic acid probe to form a hybridization sample. A preferred probe fordetecting mRNA or genomic DNA is a labeled nucleic acid probe capable of hybridizing to mRNA or genomic DNA sequences described herein. The nucleic acid probe can be, for example, a full-length nucleic acid molecule, or a portion thereof, such as anoligonucleotide of at least 15, 30, 50, 100, 250 or 500 nucleotides in length and sufficient to specifically hybridize under stringent conditions to appropriate mRNA or genomic DNA. For example, the nucleic acid probe can be all or a portion of one ofSEQ ID NOs: 1 and 3, or the complement thereof or a portion thereof; or can be a nucleic acid encoding all or a portion of one of SEQ ID NO: 2. Other suitable probes for use in the diagnostic assays of the invention are described above (see e.g., probesand primers discussed under the heading, "Nucleic Acids of the Invention").
The hybridization sample is maintained under conditions that are sufficient to allow specific hybridization of the nucleic acid probe to a FLAP nucleic acid. "Specific hybridization", as used herein, indicates exact hybridization (e.g., with nomismatches). Specific hybridization can be performed under high stringency conditions or moderate stringency conditions, for example, as described above. In a particularly preferred embodiment, the hybridization conditions for specific hybridizationare high stringency.
Specific hybridization, if present, is then detected using standard methods. If specific hybridization occurs between the nucleic acid probe and FLAP nucleic acid in the test sample, then the FLAP has the polymorphism, or is the splicingvariant, that is present in the nucleic acid probe. More than one nucleic acid probe can also be used concurrently in this method. Specific hybridization of any one of the nucleic acid probes is indicative of a polymorphism in the FLAP nucleic acid, orof the presence of a particular splicing variant encoding the FLAP nucleic acid, and is therefore diagnostic for a susceptibility to a disease or condition associated with FLAP (e.g., MI or stroke).
In Northern analysis (see Current Protocols in Molecular Biology, Ausubel, F. et al., eds., John Wiley & Sons, supra) the hybridization methods described above are used to identify the presence of a polymorphism or a particular splicing variant,associated with a disease or condition associated with or a susceptibility to a disease or condition associated with FLAP (e.g., MI or stroke). For Northern analysis, a test sample of RNA is obtained from the individual by appropriate means. Specifichybridization of a nucleic acid probe, as described above, to RNA from the individual is indicative of a polymorphism in a FLAP nucleic acid, or of the presence of a particular splicing variant encoded by a FLAP nucleic acid, and is therefore diagnosticfor susceptibility to a disease or condition associated with FLAP (e.g., MI or stroke).
For representative examples of use of nucleic acid probes, see, for example, U.S. Pat. Nos. 5,288,611 and 4,851,330. Alternatively, a peptide nucleic acid (PNA) probe can be used instead of a nucleic acid probe in the hybridization methodsdescribed above. PNA is a DNA mimic having a peptide-like, inorganic backbone, such as N-(2-aminoethyl)glycine units, with an organic base (A, G, C, T or U) attached to the glycine nitrogen via a methylene carbonyl linker (see, for example, Nielsen, P.E. et al., Bioconjugate Chemistry 5, American Chemical Society, p. 1 (1994). The PNA probe can be designed to specifically hybridize to a nucleic acid having a polymorphism associated with a susceptibility to a disease or condition associated with FLAP(e.g., MI or stroke). Hybridization of the PNA probe to a FLAP nucleic acid as described herein is diagnostic for the disease or condition or the susceptibility to the disease or condition.
In another method of the invention, mutation analysis by restriction digestion can be used to detect an altered nucleic acid, or nucleic acids containing a polymorphism(s), if the mutation or polymorphism in the nucleic acid results in thecreation or elimination of a restriction site. A test sample containing genomic DNA is obtained from the individual. Polymerase chain reaction (PCR) can be used to amplify a FLAP nucleic acid (and, if necessary, the flanking sequences) in the testsample of genomic DNA from the test individual. RFLP analysis is conducted as described (see Current Protocols in Molecular Biology, supra). The digestion pattern of the relevant DNA fragment indicates the presence or absence of the alteration orpolymorphism in the FLAP nucleic acid, and therefore indicates the presence or absence of the susceptibility to a disease or condition associated with FLAP (e.g., MI or stroke).
Sequence analysis can also be used to detect specific polymorphisms in the FLAP nucleic acid. A test sample of DNA or RNA is obtained from the test individual. PCR or other appropriate methods can be used to amplify the nucleic acid, and/or itsflanking sequences, if desired. The sequence of a FLAP nucleic acid, or a fragment of the nucleic acid, or cDNA, or fragment of the cDNA, or mRNA, or fragment of the mRNA, is determined, using standard methods. The sequence of the nucleic acid, nucleicacid fragment, cDNA, cDNA fragment, mRNA, or mRNA fragment is compared with the known nucleic acid sequence of the nucleic acid, cDNA (e.g., one or more of SEQ ID NOs: 1 or 3, and/or the complement of SEQ ID NO: 1 or 3), or a nucleic acid sequenceencoding SEQ ID NO: 2 or a fragment thereof) or mRNA, as appropriate. The presence of a polymorphism in the FLAP nucleic acid indicates that the individual has disease or a susceptibility to a disease associated with FLAP (e.g., MI or stroke).
Allele-specific oligonucleotides can also be used to detect the presence of polymorphism(s) in the FLAP nucleic acid, through the use of dot-blot hybridization of amplified oligonucleotides with allele-specific oligonucleotide (ASO) probes (see,for example, Saiki, R. et al., Nature 324:163-166 (1986)). An "allele-specific oligonucleotide" (also referred to herein as an "allele-specific oligonucleotide probe") is an oligonucleotide of approximately 10-50 base pairs, for example, approximately15-30 base pairs, that specifically hybridizes to a FLAP nucleic acid, and that contains a polymorphism associated with a susceptibility to a disease or condition associated with FLAP (e.g., MI or stroke). An allele-specific oligonucleotide probe thatis specific for particular polymorphisms in a FLAP nucleic acid can be prepared, using standard methods (see Current Protocols in Molecular Biology, supra). To identify polymorphisms in the nucleic acid associated with disease or susceptibility todisease, a test sample of DNA is obtained from the individual. PCR can be used to amplify all or a fragment of a FLAP nucleic acid, and its flanking sequences. The DNA containing the amplified FLAP nucleic acid (or fragment of the nucleic acid) isdot-blotted, using standard methods (see Current Protocols in Molecular Biology, supra), and the blot is contacted with the oligonucleotide probe. The presence of specific hybridization of the probe to the amplified FLAP is then detected. Specifichybridization of an allele-specific oligonucleotide probe to DNA from the individual is indicative of a polymorphism in the FLAP, and is therefore indicative of a susceptibility to a disease or condition associated with FLAP (e.g., MI or stroke).
An allele-specific primer hybridizes to a site on target DNA overlapping a polymorphism and only primes amplification of an allelic form to which the primer exhibits perfect complementarity. See Gibbs, Nucleic Acid Res. 17, 2427-2448 (1989). This primer is used in conjunction with a second primer which hybridizes at a distal site. Amplification proceeds from the two primers, resulting in a detectable product which indicates the particular allelic form is present. A control is usuallyperformed with a second pair of primers, one of which shows a single base mismatch at the polymorphic site and the other of which exhibits perfect complementarity to a distal site. The single-base mismatch prevents amplification and no detectableproduct is formed. The method works best when the mismatch is included in the 3'-most position of the oligonucleotide aligned with the polymorphism because this position is most destabilizing to elongation from the primer (see, e.g., WO 93/22456).
With the addition of such analogs as locked nucleic acids (LNAs), the size of primers and probes can be reduced to as few as 8 bases. LNAs are a novel class of bicyclic DNA analogs in which the 2' and 4' positions in the furanose ring are joinedvia an O-methylene (oxy-LNA), S-methylene (thio-LNA), or amino methylene (amino-LNA) moiety. Common to all of these LNA variants is an affinity toward complementary nucleic acids, which is by far the highest reported for a DNA analog. For example,particular all oxy-LNA nonamers have been shown to have melting temperatures of 64.degree. C. and 74.degree. C. when in complex with complementary DNA or RNA, respectively, as oposed to 28.degree. C. for both DNA and RNA for the corresponding DNAnonamer. Substantial increases in T.sub.m are also obtained when LNA monomers are used in combination with standard DNA or RNA monomers. For primers and probes, depending on where the LNA monomers are included (e.g., the 3' end, the 5' end, or in themiddle), the T.sub.m could be increased considerably.
In another embodiment, arrays of oligonucleotide probes that are complementary to target nucleic acid sequence segments from an individual, can be used to identify polymorphisms in a FLAP nucleic acid. For example, in one embodiment, anoligonucleotide array can be used. Oligonucleotide arrays typically comprise a plurality of different oligonucleotide probes that are coupled to a surface of a substrate in different known locations. These oligonucleotide arrays, also described as"Genechips.TM.," have been generally described in the art, for example, U.S. Pat. No. 5,143,854 and PCT patent publication Nos. WO 90/15070 and WO 92/10092. These arrays can generally be produced using mechanical synthesis methods or light directedsynthesis methods that incorporate a combination of photolithographic methods and solid phase oligonucleotide synthesis methods. See Fodor et al., Science 251:767-777 (1991); Pirrung et al., U.S. Pat. No. 5,143,854; (see also PCT Application WO90/15070); Fodor et al., PCT Publication WO 92/10092; and U.S. Pat. No. 5,424,186, the entire teachings of each of which are incorporated by reference herein. Techniques for the synthesis of these arrays using mechanical synthesis methods aredescribed in, e.g., U.S. Pat. No. 5,384,261, the entire teachings of which are incorporated by reference herein. In another example, linear arrays can be utilized.
Once an oligonucleotide array is prepared, a nucleic acid of interest is hybridized with the array and scanned for polymorphisms. Hybridization and scanning are generally carried out by methods described herein and also in, e.g., published PCTApplication Nos. WO 92/10092 and WO 95/11995, and U.S. Pat. No. 5,424,186, the entire teachings of which are incorporated by reference herein. In brief, a target nucleic acid sequence that includes one or more previously identified polymorphicmarkers is amplified using well-known amplification techniques, e.g., PCR. Typically, this involves the use of primer sequences that are complementary to the two strands of the target sequence both upstream and downstream from the polymorphism. Asymmetric PCR techniques may also be used. Amplified target, generally incorporating a label, is then hybridized with the array under appropriate conditions. Upon completion of hybridization and washing of the array, the array is scanned to determinethe position on the array to which the target sequence hybridizes. The hybridization data obtained from the scan is typically in the form of fluorescence intensities as a function of location on the array. In a reverse method, a probe, containing apolymorphism, can be coupled to a solid surface and PCR amplicons are then added to hybridize to these probes.
Although primarily described in terms of a single detection block, e.g., detection of a single polymorphism arrays can include multiple detection blocks, and thus be capable of analyzing multiple, specific polymorphisms. It will generally beunderstood that detection blocks may be grouped within a single array or in multiple, separate arrays so that varying, optimal conditions may be used during the hybridization of the target to the array. For example, it may often be desirable to providefor the detection of those polymorphisms that fall within G-C rich stretches of a genomic sequence, separately from those falling in A-T rich segments. This allows for the separate optimization of hybridization conditions for each situation.
Additional uses of oligonucleotide arrays for detection of polymorphisms can be found, for example, in U.S. Pat. Nos. 5,858,659 and 5,837,832, the entire teachings of which are incorporated by reference herein. Other methods of nucleic acidanalysis can be used to detect polymorphisms in a nucleic acid described herein, or variants encoded by a nucleic acid described herein. Representative methods include direct manual sequencing (Church and Gilbert, Proc. Natl. Acad. Sci. USA81:1991-1995 (1988); Sanger, F. et al., Proc. Natl. Acad. Sci., USA 74:5463-5467 (1977); Beavis et al. U.S. Pat. No. 5,288,644); automated fluorescent sequencing; single-stranded conformation polymorphism assays (SSCP); clamped denaturing gelelectrophoresis (CDGE); denaturing gradient gel electrophoresis (DGGE) (Sheffield, V. C. et al., Proc. Natl. Acad. Sci. USA 86:232-236 (1989)), mobility shift analysis (Orita, M. et al., Proc. Natl. Acad. Sci. USA 86:2766-2770 (1989)),restriction enzyme analysis (Flavell et al., Cell 15:25 (1978); Geever, et al., Proc. Natl. Acad. Sci. USA 78:5081 (1981)); heteroduplex analysis; chemical mismatch cleavage (CMC) (Cotton et al., Proc. Natl. Acad. Sci. USA 85:4397-4401 (1985));RNase protection assays (Myers, R. M. et al., Science 230:1242 (1985)); use of polypeptides which recognize nucleotide mismatches, such as E. coli mutS protein; allele-specific PCR, for example.
In one embodiment of the invention, diagnosis of a susceptibility to a disease or condition associated with FLAP (e.g., MI or stroke) can also be made by expression analysis by quantitative PCR (kinetic thermal cycling). Techniques utilizingTaqMan.RTM. can also be used to allow the identification of polymorphisms and whether a patient is homozygous or heterozygous. Techniques can assess the presence of an alteration in the expression or composition of the polypeptide encoded by a FLAPnucleic acid or splicing variants encoded by a FLAP nucleic acid. Further, the expression of the variants can be quantified as physically or functionally different.
In another embodiment of the invention, diagnosis of a susceptibility to MI or stroke (or of another disease or condition associated with FLAP) can also be made by examining expression and/or composition of a FLAP polypeptide, by a variety ofmethods, including enzyme linked immunosorbent assays (ELISAs), Western blots, immunoprecipitations and immunofluorescence. A test sample from an individual is assessed for the presence of an alteration in the expression and/or an alteration incomposition of the polypeptide encoded by a FLAP nucleic acid, or for the presence of a particular variant encoded by a FLAP nucleic acid. An alteration in expression of a polypeptide encoded by a FLAP nucleic acid can be, for example, an alteration inthe quantitative polypeptide expression (i.e., the amount of polypeptide produced); an alteration in the composition of a polypeptide encoded by a FLAP nucleic acid is an alteration in the qualitative polypeptide expression (e.g., expression of analtered FLAP polypeptide or of a different splicing variant). In a preferred embodiment, diagnosis of a susceptibility to a disease or condition associated with FLAP is made by detecting a particular splicing variant encoded by that FLAP variant, or aparticular pattern of splicing variants.
Both such alterations (quantitative and qualitative) can also be present. An "alteration" in the polypeptide expression or composition, refers to an alteration in expression or composition in a test sample, as compared with the expression orcomposition of polypeptide by a FLAP nucleic acid in a control sample. A control sample is a sample that corresponds to the test sample (e.g., is from the same type of cells), and is from an individual who is not affected by the disease or asusceptibility to a disease or condition associated with a FLAP nucleic acid. An alteration in the expression or composition of the polypeptide in the test sample, as compared with the control sample, is indicative of a susceptibility to a disease orcondition associated with FLAP (e.g., MI or stroke). Similarly, the presence of one or more different splicing variants in the test sample, or the presence of significantly different amounts of different splicing variants in the test sample, as comparedwith the control sample, is indicative of a susceptibility to a disease or condition associated with a FLAP nucleic acid. Various means of examining expression or composition of the polypeptide encoded by a FLAP nucleic acid can be used, including:spectroscopy, colorimetry, electrophoresis, isoelectric focusing and immunoassays (e.g., David et al., U.S. Pat. No. 4,376,110) such as immunoblotting (see also Current Protocols in Molecular Biology, particularly Chapter 10). For example, in oneembodiment, an antibody capable of binding to the polypeptide (e.g., as described above), preferably an antibody with a detectable label, can be used. Antibodies can be polyclonal, or more preferably, monoclonal. An intact antibody, or a fragmentthereof (e.g., Fab or F(ab').sub.2) can be used. The term "labeled", with regard to the probe or antibody, is intended to encompass direct labeling of the probe or antibody by coupling (i.e., physically linking) a detectable substance to the probe orantibody, as well as indirect labeling of the probe or antibody by reactivity with another reagent that is directly labeled. Examples of indirect labeling include detection of a primary antibody using a fluorescently labeled secondary antibody andend-labeling of a DNA probe with biotin such that it can be detected with fluorescently labeled streptavidin. Western blotting analysis, using an antibody as described above that specifically binds to a polypeptide encoded by an altered FLAP (e.g., by aFLAP having a SNP as shown in Table 13), or an antibody that specifically binds to a polypeptide encoded by a non-altered nucleic acid, or an antibody that specifically binds to a particular splicing variant encoded by a nucleic acid, can be used toidentify the presence in a test sample of a particular splicing variant or of a polypeptide encoded by a polymorphic or altered FLAP, or the absence in a test sample of a particular splicing variant or of a polypeptide encoded by a non-polymorphic ornon-altered nucleic acid. The presence of a polypeptide encoded by a polymorphic or altered nucleic acid, or the absence of a polypeptide encoded by a non-polymorphic or non-altered nucleic acid, is diagnostic for a susceptibility to a disease orcondition associated with FLAP, as is the presence (or absence) of particular splicing variants encoded by the FLAP nucleic acid.
In one embodiment of this method, the level or amount of polypeptide encoded by a FLAP nucleic acid in a test sample is compared with the level or amount of the polypeptide encoded by the FLAP in a control sample. A level or amount of thepolypeptide in the test sample that is higher or lower than the level or amount of the polypeptide in the control sample, such that the difference is statistically significant, is indicative of an alteration in the expression of the polypeptide encodedby the FLAP, and is diagnostic for disease or condition, or for a susceptibility to a disease or condition, associated with that FLAP. Alternatively, the composition of the polypeptide encoded by a FLAP nucleic acid in a test sample is compared with thecomposition of the polypeptide encoded by the FLAP in a control sample (e.g., the presence of different splicing variants). A difference in the composition of the polypeptide in the test sample, as compared with the composition of the polypeptide in thecontrol sample, is diagnostic for a susceptibility to a disease or condition associated with that FLAP. In another embodiment, both the level or amount and the composition of the polypeptide can be assessed in the test sample and in the control sample. A difference in the amount or level of the polypeptide in the test sample, compared to the control sample; a difference in composition in the test sample, compared to the control sample; or both a difference in the amount or level, and a difference inthe composition, is indicative of a susceptibility to a disease or condition, associated with FLAP (e.g., MI or stroke).
Diagnosis Utilizing at-Risk Haplotypes
The invention further pertains to a method for the diagnosis and identification of susceptibility to myocardial infarction or stroke in an individual, by identifying an at-risk haplotype in FLAP. As used herein, combinations of genetic markersare referred to herein as "haplotypes," and the present invention describes methods whereby detection of particular haplotypes is indicative of a susceptibility to myocardial infarction or stroke. In certain embodiments, the "haplotype" identified inthe methods of diagnosis can be a single marker, such as a single nucleotide polymorphism (SNP). In certain other embodiments, the "haplotype" can include more than one marker. The detection of the particular genetic markers that make up the particularhaplotypes can be performed by a variety of methods described herein and known in the art. For example, genetic markers can be detected at the nucleic acid level, e.g., by direct sequencing or at the amino acid level if the genetic marker affects thecoding sequence of FLAP, e.g., by immunoassays based on antibodies that recognize the FLAP protein or a particular FLAP variant protein.
In one embodiment of the invention, diagnosis of a susceptibility to MI or stroke is made by detecting a haplotype associated with FLAP as described herein. The FLAP-associated haplotypes (e.g., those described in Tables 5, 7, 9, 14 or 15),describe a set of genetic markers ("alleles") associated with FLAP. In a certain embodiment, the haplotype can comprise one or more alleles, two or more alleles, three or more alleles, four or more alleles, or five or more alleles. The genetic markersare particular "alleles" at "polymorphic sites" associated with FLAP. A nucleotide position at which more than one sequence is possible in a population (either a natural population or a synthetic population, e.g., a library of synthetic molecules), isreferred to herein as a "polymorphic site". Where a polymorphic site is a single nucleotide in length, the site is referred to as a single nucleotide polymorphism ("SNP"). For example, if at a particular chromosomal location, one member of a populationhas an adenine and another member of the population has a thymine at the same position, then this position is a polymorphic site, and, more specifically, the polymorphic site is a SNP. Polymorphic sites can allow for differences in sequences based onsubstitutions, insertions or deletions. Each version of the sequence with respect to the polymorphic site is referred to herein as an "allele" of the polymorphic site. Thus, in the previous example, the SNP allows for both an adenine allele and athymine allele.
Typically, a reference sequence is referred to for a particular sequence. Alleles that differ from the reference are referred to as "variant" alleles. For example, the reference FLAP sequence is described herein by SEQ ID NO: 1 (genomic) or SEQID NO: 3 (mRNA). The term, "variant FLAP", as used herein, refers to a FLAP sequence that differs from SEQ ID NO: 1 or SEQ ID NO: 3, but is otherwise substantially similar. The genetic markers that make up the haplotypes described herein include FLAPvariants. The variants of FLAP that are used to determine the haplotypes disclosed herein of the present invention are associated with a susceptibility to MI or stroke. Additional variants can include changes that affect a FLAP polypeptide, asdescribed above.
Haplotypes are a combination of genetic markers, e.g., particular alleles at polymorphic sites. The haplotypes described herein (e.g., in Tables 5, 7, 9, 14 or 15; haplotypes B4, Bs4, B5, B6, A4, A5; HapB) are found more frequently inindividuals having MI and/or stroke than in individuals not affected by these diseases. Therefore, these haplotypes have predictive value for detecting susceptibility to MI or stroke in an individual.
In one embodiment, the at-risk haplotype is one which confers a significant risk of MI or stroke. In one embodiment, significance associated with a haplotype is measured by an odds ratio. In a further embodiment, the significance is measured bya percentage. In one embodiment, a significant risk is measured as an odds ratio of at least about 1.2, including by not limited to: 1.2, 1.3, 1.4, 1.5, 1.6, 1.7, 1.8 and 1.9. In a further embodiment, an odds ratio of at least 1.2 is significant. In afurther embodiment, an odds ratio of at least about 1.5 is significant. In a further embodiment, a significant increase in risk is at least about 1.7 is significant. In a further embodiment, a significant increase in risk is at least about 20%,including but not limited to about 25%, 30%, 35%, 40%, 45%, 50%, 55%, 60%, 65%, 70%, 75%, 80%, 85%, 90%, 95%, and 98%. In a further embodiment, a significant increase in risk is at least about 50%. It is understood however, that identifying whether arisk is medically significant may also depend on a variety of factors, including the specific disease, the haplotype, and often, environmental factors.
The invention also pertains to methods of diagnosing a susceptibility to myocardial infarction or stroke in an individual, comprising screening for an at-risk haplotype in the FLAP nucleic acid that is more frequently present in an individualsusceptible to myocardial infarction or stroke (affected), compared to the frequency of its presence in a healthy individual (control), wherein the presence of the haplotype is indicative of susceptibility to myocardial infarction or stroke. As anexample of a simple test for correlation would be a Fisher-exact test on a two by two table. Given a cohort of chromosomes the two by two table is constructed out of the number of chromosomes that include both of the haplotypes, one of the haplotype butnot the other and neither of the haplotypes.
In certain embodiments, the screening for the presence of an at-risk haplotype comprises screening for an at-risk haplotype within or near FLAP that significantly correlates with a haplotype such as a haplotype shown in Table 5; a haplotype shownin Table 7; a haplotype shown in Table 9; a haplotype shown in Table 14; a haplotype shown in Table 15; haplotype B4; haplotype Bs4; haplotype B5; haplotype B6; haplotype A4; haplotype A5; or haplotype HapB. In other embodiments, screening for thepresence of an at-risk haplotype comprises screening for an at-risk haplotype within or near FLAP that significantly correlates with susceptibility to myocardial infarction or stroke.
In one particular embodiment, the at-risk haplotype is characterized by the presence of polymorphism(s) represented in Table 13. For example, SG13S99, where the SNP can be a "C" or a "T"; SG13S25, where the SNP can be a "G" or an "A"; SG13S377,where the SNP can be a "G" or an "A"; SG13S106, where the SNP can be a "G" or an "A"; SG13S114, where the SNP can be a "T" or an "A"; SG13S89, where the SNP can be a "G" or an "A"; SG13S30, where the SNP can be a "G" or a "T"; SG13S32, where the SNP canbe a "C" or an "A"; SG13S42, where the SNP can be a "G" or an "A"; and SG13S35, where the SNP can be a "G" or an "A". In another embodiment, the at-risk haplotype is selected from the group consisting of: haplotype B4, Bs4, B5, B6, A4 and A5. Theat-risk haplotype can also comprise a combination of the markers in the haplotypes B4, BS4, B5, B6, A4 and/or A5. In further embodiments, the at-risk haplotype can be haplotype HapB. In other embodiments, the at-risk haplotype comprises a polymorphismshown in any one of Tables 5, 7, 9, 14 or 15.
Standard techniques for genotyping for the presence of SNPs and/or microsatellite markers that are associated with myocardial infarctionor stroke can be used, such as fluorescent based techniques (Chen, et al., Genome Res. 9, 492 (1999), PCR,LCR, Nested PCR and other techniques for nucleic acid amplification. In a preferred embodiment, the method comprises assessing in an individual the presence or frequency of SNPs and/or microsatellites in the FLAP nucleic acid that are associated withmyocardial infarction or stroke, wherein an excess or higher frequency of the SNPs and/or microsatellites compared to a healthy control individual is indicative that the individual is susceptible to myocardial infarction or stroke.
Haplotype analysis involves defining a candidate susceptibility locus using LOD scores. The defined regions are then ultra-fine mapped with microsatellite markers with an average spacing between markers of less than 100 kb. All usablemicrosatellite markers that found in public databases and mapped within that region can be used. In addition, microsatellite markers identified within the deCODE genetics sequence assembly of the human genome can be used.
The frequencies of haplotypes in the patient and the control groups using an expectation-maximization algorithm can be estimated (Dempster A. et al., 1977. J. R. Stat. Soc. B, 39:1-389). An implementation of this algorithm that can handlemissing genotypes and uncertainty with the phase can be used. Under the null hypothesis, the patients and the controls are assumed to have identical frequencies. Using a likelihood approach, an alternative hypothesis where a candidateat-risk-haplotype, which can include the FLAP SNPs, is allowed to have a higher frequency in patients than controls, while the ratios of the frequencies of other haplotypes are assumed to be the same in both groups is tested. Likelihoods are maximizedseparately under both hypotheses and a corresponding 1-df likelihood ratio statistic is used to evaluate the statistic significance.
To look for at-risk-haplotypes in the 1-lod drop, for example, association of all possible combinations of genotyped markers is studied, provided those markers span a practical region. The combined patient and control groups can be randomlydivided into two sets, equal in size to the original group of patients and controls. The haplotype analysis is then repeated and the most significant p-value registered is determined. This randomization scheme can be repeated, for example, over 100times to construct an empirical distribution of p-values. In a preferred embodiment, a p-value of <0.05 is indicative of an at-risk haplotype.
A detailed discussion of haplotype analysis follows.
Haplotype Analysis
Our general approach to haplotype analysis involves using likelihood-based inference applied to NEsted MOdels. The method is implemented in our program NEMO, which allows for many polymorphic markers, SNPs and microsatellites. The method andsoftware are specifically designed for case-control studies where the purpose is to identify haplotype groups that confer different risks. It is also a tool for studying LD structures.
When investigating haplotypes constructed from many markers, apart from looking at each haplotype individually, meaningful summaries often require putting haplotypes into groups. A particular partition of the haplotype space is a model thatassumes haplotypes within a group have the same risk, while haplotypes in different groups can have different risks. Two models/partitions are nested when one, the alternative model, is a finer partition compared to the other, the null model, i.e, thealternative model allows some haplotypes assumed to have the same risk in the null model to have different risks. The models are nested in the classical sense that the null model is a special case of the alternative model. Hence traditional generalizedlikelihood ratio tests can be used to test the null model against the alternative model. Note that, with a multiplicative model, if haplotypes h.sub.i and h.sub.j are assumed to have the same risk, it corresponds to assuming thatf.sub.i/p.sub.i=f.sub.j/p.sub.j where f and p denote haplotype frequencies in the affected population and the control population respectively.
One common way to handle uncertainty in phase and missing genotypes is a two-step method of first estimating haplotype counts and then treating the estimated counts as the exact counts, a method that can sometimes be problematic (e.g., see theinformation measure section below) and may require randomization to properly evaluate statistical significance. In NEMO, maximum likelihood estimates, likelihood ratios and p-values are calculated directly, with the aid of the EM algorithm, for theobserved data treating it as a missing-data problem.
NEMO allows complete flexibility for partitions. For example, the first haplotype problem described in the Methods section on Statistical analysis considers testing whether h.sub.1 has the same risk as the other haplotypes h.sub.2, . . . ,h.sub.k. Here the alternative grouping is [h.sub.1], [h.sub.2, . . . , h.sub.k] and the null grouping is [h.sub.1, . . . , h.sub.k]. The second haplotype problem in the same section involves three haplotypes h.sub.1=G0, h.sub.2=GX and h.sub.3=AX, andthe focus is on comparing h.sub.1 and h.sub.2. The alternative grouping is [h.sub.1], [h.sub.2], [h.sub.3] and the null grouping is [h.sub.1, h.sub.2], [h.sub.3]. If composite alleles exist, one could collapse these alleles into one at the dataprocessing stage, and performed the test as described. This is a perfectly valid approach, and indeed, whether we collapse or not makes no difference if there were no missing information regarding phase. But, with the actual data, if each of thealleles making up a composite correlates differently with the SNP alleles, this will provide some partial information on phase. Collapsing at the data processing stage will unnecessarily increase the amount of missing information. Anested-models/partition framework can be used in this scenario. Let h.sub.2 be split into h.sub.2a, h.sub.2b, . . . , h.sub.2e, and h.sub.3 be split into h.sub.3a, h.sub.3b, . . . , h.sub.3e. Then the alternative grouping is [h.sub.1], [h.sub.2a,h.sub.2b, . . . ,h.sub.2e], [h.sub.3a, h.sub.3b, . . . , h.sub.3e] and the null grouping is [h.sub.1, h.sub.2a, h.sub.2b, . . . ,h.sub.2e], [h.sub.3a, h.sub.3b, . . . , h.sub.3e]. The same method can be used to handle composite where collapsing atthe data processing stage is not even an option since L.sub.C represents multiple haplotypes constructed from multiple SNPs. Alternatively, a 3-way test with the alternative grouping of [h.sub.1], [h.sub.2a, h.sub.2b, . . . ,h.sub.2e], [h.sub.3a,h.sub.3b, . . . , h.sub.3e] versus the null grouping of [h.sub.1, h.sub.2a, h.sub.2b . . . , h.sub.2e, h.sub.3a, h.sub.3b, . . . , h.sub.3e] could also be performed. Note that the generalized likelihood ratio test-statistic would have two degrees offreedom instead of one.
Measuring Information
Even though likelihood ratio tests based on likelihoods computed directly for the observed data, which have captured the information loss due to uncertainty in phase and missing genotypes, can be relied on to give valid p-values, it would stillbe of interest to know how much information had been lost due to the information being incomplete. Interestingly, one can measure information loss by considering a two-step procedure to evaluating statistical significance that appears natural buthappens to be systematically anti-conservative. Suppose we calculate the maximum likelihood estimates for the population haplotype frequencies calculated under the alternative hypothesis that there are differences between the affected population andcontrol population, and use these frequency estimates as estimates of the observed frequencies of haplotype counts in the affected sample and in the control sample. Suppose we then perform a likelihood ratio test treating these estimated haplotypecounts as though they are the actual counts. We could also perform a Fisher's exact test, but we would then need to round off these estimated counts since they are in general non-integers. This test will in general be anti-conservative because treatingthe estimated counts as if they were exact counts ignores the uncertainty with the counts, overestimates the effective sample size and underestimates the sampling variation. It means that the chi-square likelihood-ratio test statistic calculated thisway, denoted by .LAMBDA.*, will in general be bigger than .LAMBDA., the likelihood-ratio test-statistic calculated directly from the observed data as described in methods. But .LAMBDA.* is useful because the ratio .LAMBDA./.LAMBDA.* happens to be a goodmeasure of information, or 1-(.LAMBDA./.LAMBDA.*) is a measure of the fraction of information lost due to missing information. This information measure for haplotype analysis is described in Nicolae and Kong, Technical Report 537, Department ofStatistics, University of Statistics, University of Chicago, Revised for Biometrics (2003) as a natural extension of information measures defined for linkage analysis, and is implemented in NEMO.
Statistical Analysis.
For single marker association to the disease, the Fisher exact test can be used to calculate two-sided p-values for each individual allele. All p-values are presented unadjusted for multiple comparisons unless specifically indicated. Thepresented frequencies (for microsatellites, SNPs and haplotypes) are allelic frequencies as opposed to carrier frequencies. To minimize any bias due the relatedness of the patients who were recruited as families for the linkage analysis, first andsecond-degree relatives can be eliminated from the patient list. Furthermore, the test can be repeated for association correcting for any remaining relatedness among the patients, by extending a variance adjustment procedure (e.g., as described inRisch, N. & Teng, J., "The relative power of family-based and case-control designs for linkage disequilibrium studies of complex human diseases I. DNA pooling," Genome Res. 8:1278-1288 (1998)) for sibships so that it can be applied to general familialrelationships, and present both adjusted and unadjusted p-values for comparison. The differences are in general very small as expected. To assess the significance of single-marker association corrected for multiple testing we carried out arandomisation test using the same genotype data. Cohorts of patients and controls can be randomized and the association analysis redone multiple times (e.g., up to 500,000 times) and the p-value is the fraction of replications that produced a p-valuefor some marker allele that is lower than or equal to the p-value we observed using the original patient and control cohorts.
For both single-marker and haplotype analyses, relative risk (RR) and the population attributable risk (PAR) can be calculated assuming a multiplicative model (haplotype relative risk model), (Terwilliger, J. D. & Ott, J., Hum Hered, 42, 337-46(1992) and Falk, C. T. & Rubinstein, P, Ann Hum Genet 51 (Pt 3), 227-33 (1987)), i.e., that the risks of the two alleles/haplotypes a person carries multiply. For example, if RR is the risk of A relative to a, then the risk of a person homozygote AAwill be RR times that of a heterozygote Aa and RR.sup.2 times that of a homozygote aa. The multiplicative model has a nice property that simplifies analysis and computations--haplotypes are independent, i.e., in Hardy-Weinberg equilibrium, within theaffected population as well as within the control population. As a consequence, haplotype counts of the affecteds and controls each have multinomial distributions, but with different haplotype frequencies under the alternative hypothesis. Specifically,for two haplotypes h.sub.i and h.sub.j, risk(h.sub.i)/risk(h.sub.j)=(f.sub.i/p.sub.i)/(f.sub.j/p.sub.j), where f and p denote respectively frequencies in the affected population and in the control population. While there is some power loss if the truemodel is not multiplicative, the loss tends to be mild except for extreme cases. Most importantly, p-values are always valid since they are computed with respect to null hypothesis.
In general, haplotype frequencies are estimated by maximum likelihood and tests of differences between cases and controls are performed using a generalized likelihood ratio test (Rice, J. A. Mathematical Statistics and Data Analysis, 602(International Thomson Publishing, (1995)). deCODE's haplotype analysis program called NEMO, which stands for NEsted MOdels, can be used to calculate all the haplotype results. To handle uncertainties with phase and missing genotypes, it is emphasizedthat we do not use a common two-step approach to association tests, where haplotype counts are first estimated, possibly with the use of the EM algorithm, Dempster, (A. P., Laird, N. M. & Rubin, D. B., Journal of the Royal Statistical Society B, 39, 1-38(1971)) and then tests are performed treating the estimated counts as though they are true counts, a method that can sometimes be problematic and may require randomisation to properly evaluate statistical significance. Instead, with NEMO, maximumlikelihood estimates, likelihood ratios and p-values are computed with the aid of the EM-algorithm directly for the observed data, and hence the loss of information due to uncertainty with phase and missing genotypes is automatically captured by thelikelihood ratios. Even so, it is of interest to know how much information is retained, or lost, due to incomplete information. Described herein is such a measure that is natural under the likelihood framework. For a fixed set of markers, the simplesttests performed compare one selected haplotype against all the others. Call the selected haplotype h.sub.1 and the others h.sub.2, . . . , h.sub.k. Let p.sub.1, . . . , p.sub.k denote the population frequencies of the haplotypes in the controls, andf.sub.1, . . . , f.sub.k denote the population frequencies of the haplotypes in the affecteds. Under the null hypothesis, f.sub.i=p.sub.i for all i. The alternative model we use for the test assumes h.sub.2, . . . , h.sub.k to have the same risk whileh.sub.1 is allowed to have a different risk. This implies that while p.sub.1 can be different from f.sub.1, f.sub.i/(f.sub.2+ . . . +f.sub.k)=p .sub.i/(P.sub.2+ . . . +p.sub.k)=.beta..sub.i for i=2, . . . , k. Denoting f.sub.1/p.sub.1 by r, andnoting that .beta..sub.2+ . . . +.beta..sub.k=1, the test statistic based on generalized likelihood ratios is .LAMBDA.=2[l({circumflex over (r)}, {circumflex over (p)}.sub.1, {circumflex over (.beta.)}.sub.2, . . . , {circumflex over(.beta.)}.sub.k-1)-l(1, {tilde over (p)}.sub.1, {tilde over (.beta.)}.sub.2, . . . , {tilde over (.beta.)}.sub.k-1)] where l denotes log.sub.e likelihood and {tilde over ( )} and ^ denote maximum likelihood estimates under the null hypothesis andalternative hypothesis respectively. A has asymptotically a chi-square distribution with 1-df, under the null hypothesis. Slightly more complicated null and alternative hypotheses can also be used. For example, let h.sub.1 be G0, h.sub.2 be GX andh.sub.3 be AX. When comparing GO against GX, i.e., this is the test which gives estimated RR of 1.46 and p-value=0.0002, the null assumes G0 and GX have the same risk but AX is allowed to have a different risk. The alternative hypothesis allows, forexample, three haplotype groups to have different risks. This implies that, under the null hypothesis, there is a constraint that f.sub.1/p.sub.1=f.sub.2/p.sub.2, or w=[f.sub.1/p.sub.1]/[f.sub.2/p.sub.2]=1. The test statistic based on generalizedlikelihood ratios is .LAMBDA.=2[l({circumflex over (p)}.sub.1, {circumflex over (f)}.sub.1, {circumflex over (p)}.sub.2, w)-l({tilde over (p)}.sub.1, {tilde over (f)}.sub.1,{tilde over (p)}.sub.2, 1)] that again has asymptotically a chi-squaredistribution with 1-df under the null hypothesis. If there are composite haplotypes (for example, h.sub.2 and h.sub.3), that is handled in a natural manner under the nested models framework.
LD between pairs of SNPs can be calculated using the standard definition of D' and R.sup.2 (Lewontin, R., Genetics 49, 49-67 (1964) and Hill, W. G. & Robertson, A. Theor. Appl. Genet. 22, 226-231 (1968)). Using NEMO, frequencies of the twomarker allele combinations are estimated by maximum likelihood and deviation from linkage equilibrium is evaluated by a likelihood ratio test. The definitions of D' and R.sup.2 are extended to include microsatellites by averaging over the values for allpossible allele combination of the two markers weighted by the marginal allele probabilities. When plotting all marker combination to elucidate the LD structure in a particular region, we plot D' in the upper left corner and the p-value in the lowerright corner. In the LD plots the markers can be plotted equidistant rather than according to their physical location, if desired.
Statistical Methods for Linkage Analysis
Multipoint, affected-only allele-sharing methods can be used in the analyses to assess evidence for linkage. Results, both the LOD-score and the non-parametric linkage (NPL) score, can be obtained using the program Allegro (Gudbjartsson et al.,Nat. Genet. 25:12-3, 2000). Our baseline linkage analysis uses the S.sub.pairs scoring function (Whittemore, A. S., Halpern, J. (1994), Biometrics 50:118-27; Kruglyak L, et al. (1996), Am J Hum Genet 58:1347-63), the exponential allele-sharing model(Kong, A. and Cox, N. J. (1997), Am J Hum Genet 61:1179-88) and a family weighting scheme that is halfway, on the log-scale, between weighting each affected pair equally and weighting each family equally. The information measure we use is part of theAllegro program output and the information value equals zero if the marker genotypes are completely uninformative and equals one if the genotypes determine the exact amount of allele sharing by decent among the affected relatives (Gretarsdottir et al.,Am. J. Hom. Genet, 70:593-603, (2002)). We computed the P-values two different ways and here report the less significant result. The first P-value can be computed on the basis of large sample theory; the distribution of Z.sub.lr=(2[log.sub.e(10)LOD]) approximates a standard normal variable under the null hypothesis of no linkage (Kong, A. and Cox, N. J. (1997), Am J Hum Genet 61:1179-88). The second P-value can be calculated by comparing the observed LOD-score with its completedata sampling distribution under the null hypothesis (e.g., Gudbjartsson et al., Nat. Genet. 25:12-3, 2000). When the data consist of more than a few families, these two P-values tend to be very similar.
Kits
Kits (e.g., reagent kits) useful in the methods of diagnosis comprise components useful in any of the methods described herein, including for example, hybridization probes or primers as described herein (e.g., labeled probes or primers), reagentsfor detection of labeled molecules, restriction enzymes (e.g., for RFLP analysis), allele-specific oligonucleotides, antibodies which bind to altered or to non-altered (native) FLAP polypeptide, means for amplification of nucleic acids comprising a FLAP,or means for analyzing the nucleic acid sequence of a nucleic acid described herein, or for analyzing the amino acid sequence of a polypeptide as described herein, etc. In one embodiment, a kit for diagnosing susceptibility to MI or stroke can compriseprimers for nucleic acid amplification of a region in the FLAP nucleic acid comprising an at-risk haplotype that is more frequently present in an individual having MI or stroke or susceptible to MI or stroke. The primers can be designed using portionsof the nucleic acids flanking SNPs that are indicative of MI or stroke. In a particularly preferred embodiment, the primers are designed to amplify regions of the FLAP nucleic acid associated with an at-risk haplotype for MI or stroke, or moreparticularly the haplotypes defined by the following SNPs: SG13S99, SG13S25, SG13S377, SG13S106, SG13S114, SG13S89, SG13S30, SG13S32, SG13S42, and SG13S35, at the locus on chromosome 13q12-13. In other preferred embodiments, the primers are designed toamplify regions of the FLAP nucleic acid associated with a haplotype such as haplotype B4, Bs4, B5, B6, A4, A5, HapB, a haplotype shown in Table 5, and/or a haplotype shown in Table 7, and/or a haplotype shown in Table 9, and/or a haplotype shown inTable 14, and/or a haplotype shown in Table 15.
Diagnosis of Flap-Related Disease
Although the methods of diagnosis above have been described in the context of diagnosing susceptibility to MI or stroke, the methods can also be used to identify FLAP-associated MI and/or stroke. For example, individuals who have experienced MIand/or stroke can be assessed to determine whether the presence in'the individual of a polymorphism in a FLAP nucleic acid, or the presence of an at-risk haplotype in the individual, as described above, could have been a contributing factor to the MIand/or stroke. As used herein, the terms, "FLAP-associated MI" and "FLAP-associated stroke," refer to the occurrence of an MI or stroke in an individual who has a polymorphism in a FLAP nucleic acid or an at-risk FLAP haplotype. Identification ofFLAP-associated MI or stroke facilitates treatment planning, as treatment can be designed and therapeutics selected to target components of the FLAP pathway.
In one embodiment of the invention, diagnosis of FLAP-associated MI or stroke, is made by detecting a polymorphism in a FLAP nucleic acid as described herein. A polymorphism in a FLAP nucleic acid is described above. A test sample of genomicDNA, RNA, or cDNA, is obtained from an individual who has had at least one MI and/or stroke, to determine whether the MI or stroke is FLAP-associated. The DNA, RNA, or cDNA sample is then examined to determine whether a polymorphism in a nucleic acid ispresent, and/or to determine which splicing variant(s) encoded by the FLAP is present. If the FLAP nucleic acid has the polymorphism, or is the splicing variant associated with disease, then the presence of the polymorphism or the splicing variant isindicative of FLAP-associated MI or stroke.
For example, in one embodiment, hybridization methods, such as Southern analysis, Northern analysis, or in situ hybridizations, can be used to detect the polymorphism. In other embodiments, mutation analysis by restriction digestion or sequenceanalysis can also be used, as can allele-specific oligonucleotides, or quantitative PCR (kinetic thermal cycling). Diagnosis of FLAP-associated MI or stroke can also be made by examining expression and/or composition of a FLAP polypeptide, by a varietyof methods, including enzyme linked immunosorbent assays (ELISAs), Western blots, immunoprecipitations and immunofluorescence. A test sample from an individual is assessed for the presence of an alteration in the expression and/or an alteration incomposition of the polypeptide encoded by a FLAP nucleic acid, or for the presence of a particular variant encoded by a FLAP nucleic acid. An alteration in expression of a polypeptide encoded by a FLAP nucleic acid can be, for example, an alteration inthe quantitative polypeptide expression (i.e., the amount of polypeptide produced); an alteration in the composition of a polypeptide encoded by a FLAP nucleic acid is an alteration in the qualitative polypeptide expression (e.g., expression of analtered FLAP polypeptide or of a different splicing variant).
In other embodiments, the invention pertains to a method for the diagnosis and identification of FLAP-associated myocardial infarction or stroke in an individual, by identifying the presence of an at-risk haplotype in FLAP as described in detailherein. For example, the haplotypes described herein in Tables 14 and 15, are found more frequently in individuals having MI, or stroke than in individuals not affected by these diseases. Therefore, these haplotypes have predictive value for detectingFLAP-associated MI or stroke in an individual. In certain embodiments, an at-risk haplotype is characterized by the presence of polymorphism(s) shown in Table 13. In other embodiments, the at-risk haplotype is selected from the group consisting of:haplotype B4, Bs4, B5, B6, A4 and A5. The at-risk haplotype can also comprise a combination of the markers in the haplotypes B4, Bs4, B5, B6, A4 and/or A5. In further embodiments, the at-risk haplotype can be haplotype HapB. The methods describedherein can be used to assess a sample from an individual for the presence or absence of an at-risk haplotype; the presence of an at-risk haplotype is indicative of FLAP-associated MI or stroke.
In representative embodiments of the invention, a method of diagnosing FLAP-associated myocardial infarction or stroke in an individual who has had a myocardial infarction and/or a stroke, comprises detecting a polymorphism in a FLAP nucleicacid, wherein the presence of the polymorphism in the nucleic acid is indicative of FLAP-associated myocardial infarction or stroke. Alternatively, a method of diagnosing FLAP-associated myocardial infarction or stroke in an individual who has had amyocardial infarction and/or a stroke, comprises detecting an alteration in the expression or composition of a polypeptide encoded by a FLAP nucleic acid in a test sample, in comparison with the expression or composition of a polypeptide encoded by aFLAP nucleic acid in a control sample, wherein the presence of an alteration in expression or composition of the polypeptide in the test sample is indicative of FLAP-associated myocardial infarction or stroke. In addition, a method of diagnosingFLAP-associated myocardial infarction or stroke in an individual who has had a myocardial infarction and/or a stroke, comprises determining the presence or absence in the individual of a haplotype selected from haplotypes shown in Table 5, haplotypesshown in Table 7, haplotypes shown in Table 9, haplotypes shown in Table 14, and haplotypes shown in Table 15, wherein the presence of the haplotype is diagnostic of FLAP-associated myocardial infarction or stroke. Also, a method of diagnosingFLAP-associated myocardial infarction or stroke in an individual who has had a myocardial infarction and/or a stroke, comprises determining the presence or absence in the individual of haplotype B4, Bs4, B5, B6, A4, A5, or HapB, wherein the presence ofthe haplotype is diagnostic of FLAP-associated myocardial infarction or stroke.
SCREENING ASSAYS AND AGENTS IDENTIFIED THEREBY
The invention provides methods (also referred to herein as "screening assays") for identifying the presence of a nucleotide that hybridizes to a nucleic acid of the invention, as well as for identifying the presence of a polypeptide encoded by anucleic acid of the invention. In one embodiment, the presence (or absence) of a nucleic acid molecule of interest (e.g., a nucleic acid that has significant homology with a nucleic acid of the invention) in a sample can be assessed by contacting thesample with a nucleic acid comprising a nucleic acid of the invention (e.g., a nucleic acid having the sequence of one of SEQ ID NOs: 1 or 3 or the complement thereof, or a nucleic acid encoding an amino acid having the sequence of SEQ ID NO: 2, or afragment or variant of such nucleic acids), under stringent conditions as described above, and then assessing the sample for the presence (or absence) of hybridization. In a preferred embodiment, high stringency conditions are conditions appropriate forselective hybridization. In another embodiment, a sample containing a nucleic acid molecule of interest is contacted with a nucleic acid containing a contiguous nucleic acid sequence (e.g., a primer or a probe as described above) that is at leastpartially complementary to a part of the nucleic acid molecule of interest (e.g., a FLAP nucleic acid), and the contacted sample is assessed for the presence or absence of hybridization. In a preferred embodiment, the nucleic acid containing acontiguous nucleic acid sequence is completely complementary to a part of the nucleic acid molecule of interest.
In any of these embodiments, all or a portion of the nucleic acid of interest can be subjected to amplification prior to performing the hybridization.
In another embodiment, the presence (or absence) of a polypeptide of interest, such as a polypeptide of the invention or a fragment or variant thereof, in a sample can be assessed by contacting the sample with an antibody that specificallyhybridizes to the polypeptide of interest (e.g., an antibody such as those described above), and assessing the sample for the presence (or absence) of binding of the antibody to the polypeptide of interest.
In another embodiment, the invention provides methods for identifying agents (e.g., fusion proteins, polypeptides, peptidomimetics, prodrugs, receptors, binding agents, antibodies, small molecules or other drugs, or ribozymes which alter (e.g.,increase or decrease) the activity of the polypeptides described herein, or which otherwise interact with the polypeptides herein. For example, such agents can be agents which bind to polypeptides described herein (e.g., binding agent for members of theleukotriene pathway, such as FLAP binding agents); which have a stimulatory or inhibitory effect on, for example, activity of polypeptides of the invention; or which change (e.g., enhance or inhibit) the ability of the polypeptides of the invention tointeract with members of the leukotriene pathway binding agents (e.g., receptors or other binding agents); or which alter posttranslational processing of the leukotriene pathway member polypeptide, such as a FLAP polypeptide (e.g., agents that alterproteolytic processing to direct the polypeptide from where it is normally synthesized to another location in the cell, such as the cell surface; agents that alter proteolytic processing such that more polypeptide is released from the cell, etc.)
In one embodiment, the invention provides assays for screening candidate or test agents that bind to or modulate the activity of polypeptides described herein (or biologically active portion(s) thereof), as well as agents identifiable by theassays. Test agents can be obtained using any of the numerous approaches in combinatorial library methods known in the art, including: biological libraries; spatially addressable parallel solid phase or solution phase libraries; synthetic librarymethods requiring deconvolution; the `one-bead one-compound` library method; and synthetic library methods using affinity chromatography selection. The biological library approach is limited to polypeptide libraries, while the other four approaches areapplicable to polypeptide, non-peptide oligomer or small molecule libraries of compounds (Lam, K. S., Anticancer Drug Des. 12:145 (1997)).
In one embodiment, to identify agents which alter the activity of a FLAP polypeptide, a cell, cell lysate, or solution containing or expressing a FLAP polypeptide (e.g., SEQ ID NO: 2 or another splicing variant encoded by a FLAP nucleic acid,such as a nucleic acid comprising a SNP as shown in Table 13), or a fragment or derivative thereof (as described above), can be contacted with an agent to be tested; alternatively, the polypeptide can be contacted directly with the agent to be tested. The level (amount) of FLAP activity is assessed (e.g., the level (amount) of FLAP activity is measured, either directly or indirectly), and is compared with the level of activity in a control (i.e., the level of activity of the FLAP polypeptide or activefragment or derivative thereof in the absence of the agent to be tested). If the level of the activity in the presence of the agent differs, by an amount that is statistically significant, from the level of the activity in the absence of the agent, thenthe agent is an agent that alters the activity of a FLAP polypeptide. An increase in the level of FLAP activity in the presence of the agent relative to the activity in the absence of the agent, indicates that the agent is an agent that enhances (is anagonist of) FLAP activity. Similarly, a decrease in the level of FLAP activity in the presence of the agent, relative to the activity in the absence of the agent, indicates that the agent is an agent that inhibits (is an antagonist of) FLAP activity. In another embodiment, the level of activity of a FLAP polypeptide or derivative or fragment thereof in the presence of the agent to be tested, is compared with a control level that has previously been established. A statistically significant differencein the level of the activity in the presence of the agent from the control level indicates that the agent alters FLAP activity.
The present invention also relates to an assay for identifying agents which alter the expression of a FLAP nucleic acid (e.g., antisense nucleic acids, fusion proteins, polypeptides, peptidomimetics, prodrugs, receptors, binding agents,antibodies, small molecules or other drugs, or ribozymes; which alter (e.g., increase or decrease) expression (e.g., transcription or translation) of the nucleic acid or which otherwise interact with the nucleic acids described herein, as well as agentsidentifiable by the assays. For example, a solution containing a nucleic acid encoding a FLAP polypeptide (e.g., a FLAP nucleic acid) can be contacted with an agent to be tested. The solution can comprise, for example, cells containing the nucleic acidor cell lysate containing the nucleic acid; alternatively, the solution can be another solution that comprises elements necessary for transcription/translation of the nucleic acid. Cells not suspended in solution can also be employed, if desired. Thelevel and/or pattern of FLAP expression (e.g., the level and/or pattern of mRNA or of protein expressed, such as the level and/or pattern of different splicing variants) is assessed, and is compared with the level and/or pattern of expression in acontrol (i.e., the level and/or pattern of the FLAP expression in the absence of the agent to be tested). If the level and/or pattern in the presence of the agent differ, by an amount or in a manner that is statistically significant, from the leveland/or pattern in the absence of the agent, then the agent is an agent that alters the expression of the FLAP nucleic acid. Enhancement of FLAP expression indicates that the agent is an agonist of FLAP activity. Similarly, inhibition of FLAP expressionindicates that the agent is an antagonist of FLAP activity.
In another embodiment, the level and/or pattern of FLAP polypeptide(s) (e.g., different splicing variants) in the presence of the agent to be tested, is compared with a control level and/or pattern that have previously been established. A leveland/or pattern in the presence of the agent that differs from the control level and/or pattern by an amount or in a manner that is statistically significant indicates that the agent alters FLAP expression.
In another embodiment of the invention, agents which alter the expression of a FLAP nucleic acid or which otherwise interact with the nucleic acids described herein, can be identified using a cell, cell lysate, or solution containing a nucleicacid encoding the promoter region of the FLAP nucleic acid operably linked to a reporter gene. After contact with an agent to be tested, the level of expression of the reporter gene (e.g., the level of mRNA or of protein expressed) is assessed, and iscompared with the level of expression in a control (i.e., the level of the expression of the reporter gene in the absence of the agent to be tested). If the level in the presence of the agent differs, by an amount or in a manner that is statisticallysignificant, from the level in the absence of the agent, then the agent is an agent that alters the expression of the FLAP nucleic acid, as indicated by its ability to alter expression of a nucleic acid that is operably linked to the FLAP nucleic acidpromoter.
Enhancement of the expression of the reporter indicates that the agent is an agonist of FLAP activity. Similarly, inhibition of the expression of the reporter indicates that the agent is an antagonist of FLAP activity. In another embodiment,the level of expression of the reporter in the presence of the test agent, is compared with a control level that has previously been established. A level in the presence of the agent that differs from the control level by an amount or in a manner thatis statistically significant indicates that the agent alters expression.
Agents which alter the amounts of different splicing variants encoded by a FLAP nucleic acid (e.g., an agent which enhances activity of a first splicing variant, and which inhibits activity of a second splicing variant), as well as agents whichare agonists of activity of a first splicing variant and antagonists of activity of a second splicing variant, can easily be identified using these methods described above.
In other embodiments of the invention, assays can be used to assess the impact of a test agent on the activity of a polypeptide relative to a FLAP binding agent. For example, a cell that expresses a compound that interacts with a FLAP nucleicacid (herein referred to as a "FLAP binding agent", which can be a polypeptide or other molecule that interacts with a FLAP nucleic acid, such as a receptor, or another molecule, such as 5-LO) is contacted with a FLAP in the presence of a test agent, andthe ability of the test agent to alter the interaction between the FLAP and the FLAP binding agent is determined. Alternatively, a cell lysate or a solution containing the FLAP binding agent can be used. An agent which binds to the FLAP or the FLAPbinding agent can alter the interaction by interfering with, or enhancing the ability of the FLAP to bind to, associate with, or otherwise interact with the FLAP binding agent. Determining the ability of the test agent to bind to a FLAP nucleic acid ora FLAP nucleic acid binding agent can be accomplished, for example, by coupling the test agent with a radioisotope or enzymatic label such that binding of the test agent to the polypeptide can be determined by detecting the labeled with .sup.125I,.sup.35S, .sup.14C or .sup.3H, either directly or indirectly, and the radioisotope detected by direct counting of radioemmission or by scintillation counting. Alternatively, test agents can be enzymatically labeled with, for example, horseradishperoxidase, alkaline phosphatase, or luciferase, and the enzymatic label detected by determination of conversion of an appropriate substrate to product. It is also within the scope of this invention to determine the ability of a test agent to interactwith the polypeptide without the labeling of any of the interactants. For example, a microphysiometer can be used to detect the interaction of a test agent with a FLAP or a FLAP binding agent without the labeling of either the test agent, FLAP, or theFLAP binding agent. McConnell, H. M. et al., Science 257:1906-1912 (1992). As used herein, a "microphysiometer" (e.g., Cytosensor.TM.) is an analytical instrument that measures the rate at which a cell acidifies its environment using alight-addressable potentiometric sensor (LAPS). Changes in this acidification rate can be used as an indicator of the interaction between ligand and polypeptide.
Thus, these receptors can be used to screen for compounds that are agonists for use in treating a disease or condition associated with FLAP or a susceptibility to a disease or condition associated with FLAP, or antagonists for studying asusceptibility to a disease or condition associated with FLAP (e.g., MI or stroke). Drugs can be designed to regulate FLAP activation, that in turn can be used to regulate signaling pathways and transcription events of genes downstream or of proteins orpolypeptides interacting with FLAP (e.g., 5-LO).
In another embodiment of the invention, assays can be used to identify polypeptides that interact with one or more FLAP polypeptides, as described herein. For example, a yeast two-hybrid system such as that described by Fields and Song (Fields,S. and Song, O., Nature 340:245-246 (1989)) can be used to identify polypeptides that interact with one or more FLAP polypeptides. In such a yeast two-hybrid system, vectors are constructed based on the flexibility of a transcription factor that has twofunctional domains (a DNA binding domain and a transcription activation domain). If the two domains are separated but fused to two different proteins that interact with one another, transcriptional activation can be achieved, and transcription ofspecific markers (e.g., nutritional markers such as His and Ade, or color markers such as lacZ) can be used to identify the presence of interaction and transcriptional activation. For example, in the methods of the invention, a first vector is usedwhich includes a nucleic acid encoding a DNA binding domain and also a FLAP polypeptide, splicing variant, or fragment or derivative thereof, and a second vector is used which includes a nucleic acid encoding a transcription activation domain and also anucleic acid encoding a polypeptide which potentially may interact with the FLAP polypeptide, splicing variant, or fragment or derivative thereof (e.g., a FLAP polypeptide binding agent or receptor). Incubation of yeast containing the first vector andthe second vector under appropriate conditions (e.g., mating conditions such as used in the Matchmaker.TM. system from Clontech (Palo Alto, Calif., USA)) allows identification of colonies that express the markers of interest. These colonies can beexamined to identify the polypeptide(s) that interact with the FLAP polypeptide or fragment or derivative thereof. Such polypeptides may be useful as agents that alter the activity of expression of a FLAP polypeptide, as described above.
In more than one embodiment of the above assay methods of the present invention, it may be desirable to immobilize either the FLAP, the FLAP binding agent, or other components of the assay on a solid support, in order to facilitate separation ofcomplexed from uncomplexed forms of one or both of the polypeptides, as well as to accommodate automation of the assay. Binding of a test agent to the polypeptide, or interaction of the polypeptide with a binding agent in the presence and absence of atest agent, can be accomplished in any vessel suitable for containing the reactants. Examples of such vessels include microtitre plates, test tubes, and micro-centrifuge tubes. In one embodiment, a fusion protein (e.g., a glutathione-S-transferasefusion protein) can be provided which adds a domain that allows a FLAP nucleic acid or a FLAP binding agent to be bound to a matrix or other solid support.
In another embodiment, modulators of expression of nucleic acid molecules of the invention are identified in a method wherein a cell, cell lysate, or solution containing a nucleic acid encoding a FLAP nucleic acid is contacted with a test agentand the expression of appropriate mRNA or polypeptide (e.g., splicing variant(s)) in the cell, cell lysate, or solution, is determined. The level of expression of appropriate mRNA or polypeptide(s) in the presence of the test agent is compared to thelevel of expression of mRNA or polypeptide(s) in the absence of the test agent. The test agent can then be identified as a modulator of expression based on this comparison. For example, when expression of mRNA or polypeptide is greater (statisticallysignificantly greater) in the presence of the test agent than in its absence, the test agent is identified as a stimulator or enhancer of the mRNA or polypeptide expression. Alternatively, when expression of the mRNA or polypeptide is less(statistically significantly less) in the presence of the test agent than in its absence, the test agent is identified as an inhibitor of the mRNA or polypeptide expression. The level of mRNA or polypeptide expression in the cells can be determined bymethods described herein for detecting mRNA or polypeptide.
In yet another embodiment, the invention provides methods for identifying agents (e.g., fusion proteins, polypeptides, peptidomimetics, prodrugs, receptors, binding agents, antibodies, small molecules or other drugs, or ribozymes) which alter(e.g., increase or decrease) the activity of a member of leukotriene pathway binding agent, such as a FLAP binding agent (e.g., 5-LO), as described herein. For example, such agents can be agents which have a stimulatory or inhibitory effect on, forexample, the activity of a member of leukotriene pathway binding agent, such as a FLAP binding agent; which change (e.g., enhance or inhibit) the ability a member of leukotriene pathway binding agents, (e.g., receptors or other binding agents) tointeract with the polypeptides of the invention; or which alter posttranslational processing of the member of leukotriene pathway binding agent, (e.g., agents that alter proteolytic processing to direct the member of the leukotriene pathway binding agentfrom where it is normally synthesized to another location in the cell, such as the cell surface; agents that alter proteolytic processing such that more active binding agent is released from the cell, etc.).
For example, the invention provides assays for screening candidate or test agents that bind to or modulate the activity of a member of the leukotriene pathway (or enzymatically active portion(s) thereof), as well as agents identifiable by theassays. As described above, test agents can be obtained using any of the numerous approaches in combinatorial library methods known in the art, including: biological libraries; spatially addressable parallel solid phase or solution phase libraries;synthetic library methods requiring deconvolution; the `one-bead one-compound` library method; and synthetic library methods using affinity chromatography selection. The biological library approach is limited to polypeptide libraries, while the otherfour approaches are applicable to polypeptide, non-peptide oligomer or small molecule libraries of compounds (Lam, K. S. Anticancer Drug Des., 12:145 (1997)). In one embodiment, to identify agents which alter the activity of a member of the leukotrienepathway (such as a FLAP binding agent), a cell, cell lysate, or solution containing or expressing a binding agent (e.g., 5-LO, or a leukotriene pathway member receptor), or a fragment (e.g., an enzymatically active fragment) or derivative thereof, can becontacted with an agent to be tested; alternatively, the binding agent (or fragment or derivative thereof) can be contacted directly with the agent to be tested. The level (amount) of binding agent activity is assessed (either directly or indirectly),and is compared with the level of activity in a control (i.e., the level of activity in the absence of the agent to be tested). If the level of the activity in the presence of the agent differs, by an amount that is statistically significant, from thelevel of the activity in the absence of the agent, then the agent is an agent that alters the activity of the member of the leukotriene pathway. An increase in the level of the activity relative to a control, indicates that the agent is an agent thatenhances (is an agonist of) the activity. Similarly, a decrease in the level of activity relative to a control, indicates that the agent is an agent that inhibits (is an antagonist of) the activity. In another embodiment, the level of activity in thepresence of the agent to be tested, is compared with a control level that has previously been established. A level of the activity in the presence of the agent that differs from the control level by an amount that is statistically significant indicatesthat the agent alters the activity.
This invention further pertains to novel agents identified by the above-described screening assays. Accordingly, it is within the scope of this invention to further use an agent identified as described herein in an appropriate animal model. Forexample, an agent identified as described herein (e.g., a test agent that is a modulating agent, an antisense nucleic acid molecule, a specific antibody, or a polypeptide-binding agent) can be used in an animal model to determine the efficacy, toxicity,or side effects of treatment with such an agent. Alternatively, an agent identified as described herein can be used in an animal model to determine the mechanism of action of such an agent.
Furthermore, this invention pertains to uses of novel agents identified by the above-described screening assays for treatments as described herein. In addition, an agent identified as described herein can be used to alter activity of apolypeptide encoded by a FLAP nucleic acid, or to alter expression of a FLAP nucleic acid, by contacting the polypeptide or the nucleic acid (or contacting a cell comprising the polypeptide or the nucleic acid) with the agent identified as describedherein.
The present invention is now illustrated by the following Examples, which are not intended to be limiting in any way.
EXAMPLE 1
MI Susceptibility Gene Mapped to Chromosome 13 and Association Between MI and FLAP
Subjects and Methods
A genome wide scan of 296 multiplex Icelandic families with 713 MI patients was performed. Through the suggestive linkage to a locus on chromosome 13q12-13, the gene encoding the 5-lipoxygenase activating protein (FLAP) was identified, and a4-SNP haplotype within the gene was determined to confer a near 2-fold risk of MI and stroke. Male patients showed strongest association to the at-risk haplotype. Independent confirmation of FLAP association to MI was obtained in, a British cohort ofpatients with sporadic MI. These findings support FLAP as the first specific gene isolated that confers substantial risk of the complex traits of both MI and stroke.
Methods
Study Population
Patients entering the study were recruited from a registry that includes all MIs that occurred before the age of 75 (over 8,000 patients) in Iceland from 1981 to 2000. This registry is a part of the World Health Organization MONICA Project (TheWorld Health Organization MONICA Project, WHO MONICA Project Principal Investigators, J Clin Epidemiol 41, 105-14 (1988)). Diagnoses of all patients in the registry followed strict diagnostic rules based on signs, symptoms, electrocardiograms, cardiacenzymes, and necropsy findings.
Genotypes from 713 MI patients and 1741 of their first-degree relatives were used in the linkage analysis. For the microsatellite association study of the MI locus, 802 unrelated MI patients (n=233 females, n=624 males and n=302 early onset) and837 population-based controls were used. For the SNP association study in and around the FLAP gene 779 unrelated MI patients were genotyped (n=293 females, n=486 males and n=358 early onset). The control group for the SNP association study waspopulation based and comprised of 628 unrelated males and females in the age range of 30-85 years whose medical history was unknown. The stroke cohort used in this study has previously been described (Gretarsdottir, S. et al. Nat Genet 35, 131-8 (2003);Gretarsdottir, S. et al., Am J Hum Genet 70, 593-603 (2002)). For the stroke linkage analysis, genotypes from 342 male patients with ischemic stroke or TIA that were linked to at least one other male patient within and including 6 meioses in 164families were used. For the association studies, 702 patients with all forms of stroke (n=329 females and n=373 males) were analysed. Patients with stroke that also had MI were excluded. Controls used for the stroke association studies were the sameas used in the MI SNP association study (n=628).
The study was approved by the Data Protection Commission of Iceland and the National Bioethics Committee of Iceland. Informed consent was obtained from all study participants. Personal identifiers associated with medical information and bloodsamples were encrypted with a third party encryption system as previously described (Gulcher, J. R., Kristjansson, K., Gudbjartsson, H. & Stefansson, K., Eur J Hum Genet 8, 739-42 (2000)).
Statistical Analysis
A genome-wide scan was performed as previously described (Gretarsdottir, S. et al. Am J Hum Genet 70, 593-603 (2002)), using a set of approximately 1000 microsatellite markers. Multipoint, affected-only allele-sharing methods (Kong, A. & Cox, N.J., Am J Hum Genet 61, 1179-88 (1997)) were used to assess the evidence for linkage. All results were obtained using the program Allegro (Gudbjartsson, D. F., Jonasson, K., Frigge, M. L. & Kong, A. Allegro, Nat Genet 25, 12-3 (2000)) and the deCODEgenetic map (Kong, A. et al., Nat Genet 31, 241-7 (2002)). The S.sub.pairs scoring function (Whittemore, A. S. & Halpern, J., Biometrics 50, 118-27 (1994); Kruglyak, L., Daly, M. J., Reeve-Daly, M. P. & Lander, E. S., Am J Hum Genet 58, 1347-63 (1996))was used, as was the exponential allele-sharing model (Kong, A. & Cox, N. J. Am J Hum Genet 61, 1179-88 (1997)) to generate the relevant 1-df (degree of freedom) statistics. When combining the family scores to obtain an overall score, a weighting schemewas used that is halfway on a log scale between weighting each affected pair equally and weighting each family equally. In the analysis, all genotyped individuals who are not affected are treated as "unknown". Because of concern with small samplebehaviour, corresponding P values were usually computed in two different ways for comparison, and the less significant one was reported. The first P value is computed based on large sample theory; Z.sub.lr= (2 log.sub.e(10) LOD) and is distributedapproximately as a standard normal distribution under the null hypothesis of no linkage (Kong, A. & Cox, N. J. Am J Hum Genet 61, 1179-88 (1997)). A second P value is computed by comparing the observed LOD score to its complete data samplingdistribution under the null hypothesis (Gudbjartsson, D. F., Jonasson, K., Frigge, M. L. & Kong, A. Allegro, Nat Genet 25, 12-3 (2000)). When a data set consists of more than a handful of families, these two P values tend to be very similar. Theinformation measure that was used (Nicolae, D. University of Chicago (1999)), and is implemented in Allegro, is closely related to a classical measure of information (Dempster, A., Laird, N M, Rubin, D B., J R Stat Soc B 39, 1-38 (1977) and has aproperty that is between 0, if the marker genotypes are completely uninformative, and 1, if the genotypes determine the exact amount of allele sharing by descent among the affected relatives.
For single-marker association studies, Fisher's exact test was used to calculate two-sided P values for each allele. All P values were unadjusted for multiple comparisons unless specifically indicated. Allelic rather than carrier frequencieswere presented for microsatellites, SNPs and haplotypes. To minimize any bias due to the relatedness of the patients that were recruited as families for the linkage analysis, first and second-degree relatives were eliminated from the patient list. Forthe haplotype analysis, the program NEMO was used (Gretarsdottir, S. et al., Nat Genet 35, 131-8 (2003)), which handles missing genotypes and uncertainty with phase through a likelihood procedure, using the expectation-maximization algorithm as acomputational tool to estimate haplotype frequencies. Under the null hypothesis, the affected individuals and controls are assumed to have identical haplotype frequencies. Under the alternative hypotheses, the candidate at-risk haplotype is allowed tohave a higher frequency in the affected individuals than in controls, while the ratios of frequencies of all other haplotypes are assumed to be the same in both groups. Likelihoods are maximized separately under both hypotheses, and a corresponding 1-dflikelihood ratio statistic is used to evaluate statistical significance (id). Even though searches were only performed for haplotypes that increase the risk, all reported P values are two-sided unless otherwise stated. To assess the significance of thehaplotype association corrected for multiple testing, a randomisation test was carried out using the same genotype data. The cohorts of affected individuals and controls were randomized, and the analysis was repeated. This procedure was repeated up to1,000 times and the P value presented is the fraction of replications that produced a P value for a haplotype tested that is lower than or equal to the P value observed using the original patient and control cohorts.
For both single-marker and haplotype analysis, relative risk (RR) and population attributable risk was calculated assuming a multiplicative model (Terwilliger, J. D. & Ott, J. A., Hum Hered 42, 337-46 (1992); Falk, C. T. & Rubinstein, P., Ann HumGenet 51 (Pt 3), 227-33 (1987)) in which the risk of the two alleles of haplotypes a person carries multiply. We calculated LD between pairs of SNPs using the standard definition of D' (Lewontin, R. C., Genetics 50, 757-82 (1964)) and R.sup.2 (Hill, W.G. & Robertson, A., Genetics 60, 615-28 (1968)). Using NEMO, frequencies of the two marker allele combinations are estimated by maximum likelihood, and deviation from linkage equilibrium is evaluated by a likelihood ratio test. When plotting all SNPcombinations to elucidate the LD structure in a particular region, D' was plotted in the upper left corner and the P value in the lower right corner. In the LD plots presented, the markers are plotted equidistantly rather than according to theirphysical positions.
Identification of DNA Polymorphisms.
New polymorphic repeats (i.e., dinucleotide or trinucleotide repeats) were identified with the Sputnik program. For microsatellite alleles: the CEPH sample 1347-02 (Centre d'Etudes du Polymorphisme Humain, genomics repository) is used as areference. The lower allele of each microsatellite in this sample is set at 0 and all other alleles in other samples are numbered according in relation to this reference. Thus allele 1 is 1 bp longer than the lower allele in the CEPH sample, allele 2is 2 bp longer than the lower allele in the CEPH sample, allele 3 is 3 bp longer than the lower allele in the CEPH sample, allele 4 is 4 bp longer than the lower allele in the CEPH sample, allele -1 is 1 bp shorter than the lower allele in the CEPHsample, allele -2 is 2 bp shorter than the lower allele in the CEPH sample, and so on. Single nucleotide polymorphisms in the gene were detected by PCR sequencing exonic and intronic regions from patients and controls. Public single nucleotidepolymorphisms were obtained from the NCBI SNP database. SNPs were genotyped using a method for detecting SNPs with fluorescent polarization template-directed dye-terminator incorporation (SNP-FP-TDI assay) (Chen, X., Zehnbauer, B., Gnirke, A. & Kwok, P.Y., Proc Natl Acad Sci USA 94, 10756-61. (1997)) and TaqMan assays (Applied Biosystems).
British Study Population
The method of recruitment of 3 separate cohorts of British subjects has been described previously (Steeds, R., Adams, M., Smith, P., Channer, K. & Samani, N. J., Thromb Haemost 79, 980-4 (1998); Brouilette, S., Singh, R. K., Thompson, J. R.,Goodall, A. H. & Samani, N. J., Arterioscler Thromb Vasc Biol 23, 842-6 (2003)). In brief, in the first two cohorts, a total of 547 patients included those who were admitted to the coronary care units (CCU) of the Leicester Royal Infirmary, Leicester(July 1993-April 1994) and the Royal Hallamshire Hospital, Sheffield (November 1995-March 1997) and satisfied the World Health Organisation criteria for acute MI in terms of symptoms, elevations in cardiac enzymes or electrocardiographic changes(Nomenclature and criteria for diagnosis of ischemic heart disease. Report of the Joint International Society and Federation of Cardiology/World Health Organization task force on standardization of clinical nomenclature. Circulation 59, 607-9 (1979)). A total of 530 control subjects were recruited in each hospital from adult visitors to patients with non-cardiovascular disease on general medical, surgical, orthopaedic and obstetric wards to provide subjects likely to be representative of the sourcepopulation from which the subjects originated. Subjects who reported a history of coronary heart disease were excluded.
In the third cohort, 203 subjects were recruited retrospectively from the registries of 3 coronary care units in Leicester. All had suffered an MI according to WHO criteria before the age of 50 years. At the time of participation, patients wereat least 3 months from the acute event. The control cohort comprised 180 subjects with no personal or family history of premature coronary heart disease, matched for age, sex, and current smoking status with the cases. Control subjects were recruitedfrom 3 primary care practices located within the same geographical area. In all cohorts subjects were white of Northern European origin.
Results
Linkage Analysis
A genome wide scan was performed in search of MI susceptibility genes using a framework set of approximately 1000 microsatellite markers. The initial linkage analysis included 713 MI patients who fulfilled the WHO MONICA research criteria (TheWorld Health Organization MONICA Project, WHO MONICA Project Principal Investigators, J Clin Epidemiol 41, 105-14 (1988)) and were clustered in 296 extended families. The linkage analysis was also repeated for early onset, male and female patientsseparately. Description of the number of patients and families in each analysis are provided in Table 1.
TABLE-US-00001 TABLE 1 Number of patients that cluster into families and the corresponding number of families used in the linkage analysis Number of Number of Number of Genotyped Phenotype patients families pairs relatives.sup.a All MI patients713 296 863 1741 Males 575 248 724 1385 Females 140 56 108 366 Early onset 194 93 156 739 .sup.aGenotyped relatives were used to increase the information on IBD sharing among the patients in the linkage analysis.
None of these analyses yielded a locus of genome-wide significance. However, the most promising LOD score (LOD=2.86) was observed on chromosome 13q12-13 for female MI patients at the peak marker D13S289 (data not shown). This locus also had themost promising LOD score (LOD=2.03) for patients with early onset MI. After increasing the information on identity-by-descent sharing to over 90% by typing 14 additional microsatellite markers in a 30 centiMorgan (cM) region around D13S289, the LODscore from the female analysis dropped to 2.48 (P value=0.00036), while the highest LOD score remained at D13S289 (FIG. 7.1). In addition, in an independent linkage study of male patients with ischemic stroke or transient ischemic attack we observedlinkage to the same locus with a LOD score of 1.51 at the same peak marker (FIG. 5), further suggesting that a cardiovascular susceptibility factor might reside at this locus.
Microsatellite Association Study
The 7.6 Mb region that corresponds to a drop of one in LOD score in the female MI analysis, contains 40 known genes (Table 2).
TABLE-US-00002 TABLE 2 Genes residing within the one LOD drop region of the chromosome 13q12-13 linkage peak. LL_Symbol LL_gene_name USP12L1 ubiquitin specific protease 12 like 1 RPL21 ribosomal protein L21 GTF3A general transcription factorIIIA MTIF3 mitochondrial translational initiation factor 3 PDZRN1 PDZ domain containing ring finger 1 MGC9850 hypothetical protein MGC9850 POLR1D polymerase (RNA) I polypeptide D, 16 kDa GSH1 GS homeobox 1 IPF1 insulin promoter factor 1, homeodomaintranscription factor CDX2 caudal type homeo box transcription factor 2 FLT3 fms-related tyrosine kinase 3 LOC255967 hypothetical protein LOC255967 FLT1 fms-related tyrosine kinase 1 (vascular endothelial growth factor/vascular permeability factorreceptor) C13orf12 chromosome 13 open reading frame 12 LOC283537 hypothetical protein LOC283537 KIAA0774 KIAA0774 protein SLC7A1 solute carrier family 7 (cationic amino acid transporter, y+ system), member 1 UBL3 ubiquitin-like 3 MGC2599 hypotheticalprotein MGC2599 similar to katanin p60 subunit A 1 2599 HMGB1 high-mobility group box 1 D13S106E highly charged protein ALOX5AP arachidonate 5-lipoxygenase-activating protein FLJ14834 hypothetical protein FLJ14834 MGC40178 hypothetical protein MGC40178HSPH1 heat shock 105 kDa/110 kDa protein 1 B3GTL beta 3-glycosyltransferase-like GREAT similar to G protein coupled receptor affecting testicular descent (H. sapiens) LOC196549 similar to hypothetical protein FLJ20897 13CDNA73 hypothetical protein CG003BRCA2 breast cancer 2, early onset CG018 hypothetical gene CG018 PRO0297 PRO0297 protein LOC88523 CG016 CG012 hypothetical gene CG012 CG030 hypothetical gene CG030 CG005 hypothetical protein from BCRA2 region APRIN androgen-induced proliferationinhibitor KL Klotho STARD13 START domain containing 13 RFC3 replication factor C (activator 1) 3, 38 kDa
To determine which gene in this region most likely contributes to MI, 120 microsatellite markers were typed within this region, and a case-control association study was performed using 802 unrelated MI patients and 837 population-based controls. The association study was also repeated for each of the three phenotypes that were used in the linkage study, i.e. early onset, male and female MI patients. In addition to testing each marker individually, haplotypes constructed out of those markers forassociation were also tested. All usable microsatellite markers that were found in public databases and mapped within that region were used. In addition, microsatellite markers identified within the deCODE genetics sequence assembly of the human genomewere used (see Table 6).
The initial association analysis was performed when the average spacing between microsatellite markers was approximately 100 kb. This analysis revealed several extended haplotypes composed of 4 and 5 microsatellite markers that weresignificantly associated with female MI (see FIGS. 1 and 2 and Tables 13 and 14). A region common to all these extended haplotypes, is defined by markers DG13S166 and D13S1238. This region included only one gene, the FLAP nucleic acid sequence. Thetwo marker haplotype involving alleles 0 and -2 for markers DG13S166 and D13S1238, respectively, was found in excess in patients.
This was the first evidence that the FLAP gene might be involved in the pathogenesis of myocardial infarction.
Subsequent haplotype analysis that included more microsatellite markers in the candidate region on chromosome 13q12-13, now with a marker density of 1 microsatellite marker per 60 kb, showed decreased significance of the original haplotypeassociation. However, the haplotype association analysis using increased density of markers again pointed towards the FLAP gene. This analysis strongly suggested that a 300 kb region was involved in the susceptibility of myocardial infarction. Asshown in FIG. 7.2, the haplotype that showed association to all MI with the lowest P value (0.00009) covered a region that contains 2 known genes, including the gene encoding arachidonate 5-lipoxygenase-activating protein (FLAP) and a gene with anunknown function called highly charged protein. However, the haplotype association to female MI in this region was less significant (P value=0.005) than for all MI patients and to our surprise, the most significant haplotype association was observed formale MI patients (P value=0.000002). This male MI haplotype was the only haplotype that remained significant after adjusting for all haplotypes tested.
In view of the association results described above, FLAP was an attractive candidate and therefore efforts were focused on this gene.
Screening for Polymorphisms in FLAP and Linkage Disequilibrium Mapping
To determine whether variations within the FLAP gene significantly associate with M, I and to search for causal variations, the FLAP gene was sequenced in 93 patients and 93 controls. The sequenced region covers 60 kb containing the FLAP gene,including the 5 known exons and introns and the 26 kb region 5' to the first exon and 7 kb region 3' to the fifth exon. In all, 144 SNPs were identified, of those 96 were excluded from further analysis either because of low minor allele frequency orthey were completely correlated with other SNPs and thus redundant. FIG. 7 shows the distribution of the 48 SNPs, used for genotyping, relative to exons, introns and the 5' and 3' flanking regions of the FLAP gene. Only one SNP was identified within acoding sequence (exon 2). This SNP did not lead to amino acid substitution. The locations of these SNPs in the NCBI human genome assembly, build 34, are listed in Table 3.
TABLE-US-00003 TABLE 3 Locations of all genotyped SNPs in NCBI build 34 of the human genome assembly SNP name Build34 start SG13S381 29083350 SG13S366 29083518 SG13S1 29086224 SG13S2 29087473 SG13S367 29088090 SG13S10 29088473 SG13S3 29089044SG13S368 29089886 SG13S4 29090997 SG13S5 29091307 SG13S90 29091780 SG13S6 29092536 SG13S371 29093964 SG13S372 29094259 SG13S373 29096688 SG13S375 29096874 SG13S376 29096962 SG13S25 29097553 SG13S377 29101965 SG13S100 29104271 SG13S95 29106329 SG13S19129107830 SG13S106 29108579 SG13S114 29110096 SG13S121 29112174 SG13S122 29112264 SG13S43 29112455 SG13S192 29116308 SG13S88 29116401 SG13S137 29118118 SG13S86 29118815 SG13S87 29118873 SG13S39 29119740 SG13S26 29122253 SG13S27 29122283 SG13S29 29123643SG13S89 29124441 SG13S96 29124906 SG13S30 29125840 SG13S97 29129139 SG13S32 29130547 SG13S41 29134045 SG13S42 29135877 SG13S34 29137100 SG13S35 29138117 SG13S181 29138633 SG13S184 29139435 SG13S188 29140805
In addition to the SNPs, a polymorphism consisting of a monopolymer A repeat that has been described in the FLAP promoter region was typed (Koshino, T. et al., Mol Cell Biol Res Commun 2, 32-5 (1999)).
The linkage disequilibrium (LD) block structure defined by the 48 SNPs that were selected for further genotyping is shown in FIG. 9. A strong LD was detected across the FLAP region, although it appears that at least one recombination may haveoccurred dividing the region into two strongly correlated LD blocks.
Haplotype Association to MI
To perform a case-control association study the 48 selected SNPs and the monopolymer A repeat marker were genotyped in a set of 779 unrelated MI patients and 628 population-based controls. Each of the 49 markers was tested individually forassociation to the disease. Three SNPs, one located 3 kb upstream of the first exon and the other two 1 and 3 kb downstream of the first exon, showed nominally significant association to MI (Table 4).
TABLE-US-00004 TABLE 4 SNP allelic association in the MI cohort Pheno- Al- P # % # % type Marker lele value RR Pat. Pat. Ctrl Ctrl All SG13S106 G 0.0044 1.29 681 72.0 530 66.6 patients SG13S100 A 0.020 1.29 388 69.6 377 63.9 SG13S114 T 0.0211.21 764 70.0 602 65.8 Males SG13S106 G 0.0037 1.35 422 72.9 530 66.6 SG13S100 A 0.0099 1.36 292 70.7 377 63.9 SG13S114 T 0.026 1.24 477 70.4 602 65.8 Early SG13S100 A 0.0440 1.43 99 71.7 377 63.9 onset Nominally significant SNP association withcorresponding number of patients (# Pat.) and controls (#Ctrl). RR refers to relative risk.
However, after adjusting for the number of markers tested, these results were not significant. A search was then conducted for haplotypes that show association to the disease using the same cohorts. The result of haplotype association analysislimited to haplotype combinations constructed out of two, three or four SNPs are shown in Table 5. The resulting P values were adjusted for all the haplotypes we tested by randomizing the patients and controls (see Methods). Several haplotypes werefound that were significantly associated to the disease with an adjusted P value less that 0.05 (Table 5).
TABLE-US-00005 TABLE 5 SNP haplotypes that significantly associate with Icelandic MI patients SG13S4 SG13S6 SG13S372 SG13S25 SG13S377 SG13S100 SG13S95 SG13S114 SG13S192- SG13S137 SG13S86 SG13S87 SG13S39 G T G T A G T G A A G T T G T G G A G A GT G T G T T G A G G T A G T G T G G T G A G A G A A G A G T A G A A G T G G A G T G A G T G G A G A A G T A G A A G T C G T G T C G G A G T G T G G A G A G C G A G T A G A G T G T G G A G G A A SG13S27 SG13S89 SG13S96 SG13S32 SG13S41 SG13S42 SG13S34SG13S188 P value.sup.a P value.sup.b Pat.frq Ctrl.frq RR D'.sup.c G A 0.0000023 0.005 0.158 0.095 1.80 1.00 A 0.0000030 0.006 0.158 0.095 1.78 1.00 A T 0.0000032 0.007 0.157 0.094 1.79 1.00 A 0.0000046 0.012 0.158 0.083 2.07 0.89 A 0.0000047 0.012 0.1540.093 1.78 1.00 A 0.0000055 0.015 0.147 0.087 1.81 1.00 A T 0.0000061 0.017 0.157 0.083 2.07 0.89 G A 0.0000063 0.017 0.157 0.084 2.04 0.89 A 0.0000070 0.021 0.157 0.096 1.76 1.00 A A 0.0000075 0.022 0.149 0.089 1.78 1.00 A 0.0000083 0.024 0.208 0.1391.62 0.99 A 0.0000084 0.026 0.145 0.074 2.14 0.88 A 0.0000084 0.026 0.139 0.082 1.82 1.00 G A 0.0000091 0.028 0.156 0.096 1.75 1.00 A T 0.0000094 0.028 0.210 0.141 1.61 0.99 A 0.0000100 0.028 0.156 0.096 1.74 1.00 A A 0.0000101 0.028 0.215 0.133 1.800.81 A 0.0000105 0.028 0.157 0.084 2.03 0.89 A 0.0000108 0.029 0.214 0.133 1.78 0.81 A A 0.0000110 0.030 0.146 0.075 2.10 0.88 A 0.0000112 0.030 0.212 0.144 1.60 1.00 T 0.0000113 0.030 0.151 0.081 2.03 0.78 A 0.0000118 0.031 0.156 0.096 1.73 1.00 A T0.0000126 0.034 0.212 0.131 1.79 0.79 G A 0.0000129 0.035 0.211 0.144 1.59 1.00 G A 0.0000134 0.035 0.156 0.084 2.01 0.89 A 0.0000136 0.036 0.211 0.143 1.60 1.00 A 0.0000137 0.036 0.156 0.085 2.00 0.89 A 0.0000148 0.037 0.151 0.081 2.01 0.78 T 0.00001500.037 0.160 0.099 1.73 0.87 A 0.0000150 0.037 0.130 0.066 2.13 0.90 T 0.0000154 0.039 0.152 0.094 1.73 0.93 A A 0.0000154 0.040 0.155 0.097 1.70 1.00 A 0.0000157 0.040 0.141 0.085 1.76 1.00 A 0.0000158 0.040 0.152 0.084 1.94 0.90 G A 0.0000163 0.0400.210 0.143 1.59 0.99 A 0.0000166 0.041 0.200 0.134 1.61 0.92 G A 0.0000168 0.042 0.213 0.133 1.76 0.81 A 0.0000168 0.042 0.156 0.084 2.00 0.89 A 0.0000171 0.042 0.211 0.136 1.70 0.81 A 0.0000183 0.043 0.192 0.128 1.62 0.85 A 0.0000184 0.043 0.212 0.1321.77 0.81 A T 0.0000193 0.046 0.328 0.251 1.46 0.99 G T 0.0000194 0.046 0.175 0.115 1.64 0.98 A 0.0000202 0.048 0.210 0.136 1.70 0.81 0.0000209 0.049 0.151 0.082 2.00 0.76 .sup.aSingle test P values. .sup.bP values adjusted for all the SNP haplotypestested. .sup.cMeasure of correlation with haplotype A4.
The most significant association was observed for a four SNP haplotype spanning 33 kb, including the first four exons of the gene (FIG. 7.3), with a nominal P value of 0.0000023 and an adjusted P value of 0.005. This haplotype, labelledhaplotype A4, has haplotype frequency of 15.8% (carrier frequency 30.3%) in patients versus 9.5% (carrier frequency 17.9%) in controls (Table 6). The relative risk conferred by haplotype A4 compared to other haplotypes constructed out of the same SNPs,assuming a multiplicative model, was 1.8 and the corresponding population attributable risk (PAR) was 13.5%. As shown in Table 6, haplotype A4 was observed in higher frequency in male patients (carrier frequency 30.9%) than in female patients (carrierfrequency 25.7%). All the other haplotypes that were significantly associated with an adjusted P value less than 0.05, were highly correlated with haplotype A4 and should be considered variants of that haplotype (Table 5).
TABLE-US-00006 TABLE 6 Association of the A4 haplotype to MI and Stroke Phenotype (n) Frq. Pat. RR PAR P-value P-value.sup.a MI (779) 0.158 1.80 0.135 0.0000023 0.005 Males (486) 0.169 1.95 0.158 0.00000091 ND.sup.b Females (293) 0.138 1.530.094 0.0098 ND Early onset (358) 0.138 1.53 0.094 0.0058 ND Stroke (702).sup.c 0.149 1.67 0.116 0.000095 ND Males (373) 0.156 1.76 0.131 0.00018 ND Females (329) 0.141 1.55 0.098 0.0074 ND .sup.aP value adjusted for the number of haplotypes tested. .sup.bNot done. .sup.cExcluding known cases of MI. Shown is the FLAP A4 haplotype and corresponding number of patients (n), haplotype frequency in patients (Frq. pat.), relative risk (RR), population attributed risk (PAR) and P values. The A4haplotype is defined by the following SNPs: SG13S25, SG13S114, SG13S89 and SG13S32 (Table 5). The same controls (n = 628) are used for the association analysis in MI and stroke, as well as for the male, female and early onset analysis. The A4 frequencyin the control cohort is 0.095.
Additional SNP Haplotype Association to MI
Two correlated series of SNP haplotypes were observed in excess in patients, denoted as A and B in Table 7. The length of the haplotypes varies between 33 and 69 kb and cover one or two blocks of linkage disequilibrium. Both series ofhaplotypes contain the common allele G of the SNP SG13S25. All haplotypes in the A series (e.g., A4 haplotype) contain the SNP SG13S114, while all haplotypes in the B series contain the SNP SG13S106. In the B series, the haplotypes B4, BS4, B5, and B6have a relative risk (RR) greater than 2 and allelic frequencies above 10% (Table 7). The haplotypes in the A series have slightly lower RR and p-values, but higher allelic frequency (15-16%), and as such we also consider them interesting. Thehaplotypes in series B and A are strongly correlated, i.e. the B haplotypes define a subset of the A haplotypes. Hence, B haplotypes are more specific than A haplotypes. However, A haplotypes are more sensitive, i.e. they capture more individuals withthe putative mutation, as is observed in the population attributable risk which is less for B than for A. Furthermore, these haplotypes show similar risk ratios and allelic frequency for early-onset patients (defined as onset of first MI before the ageof 55). In addition, analyzing various groups of patients with known risk factors, such as hypertension, high cholesterol, smoking and diabetes, did not reveal any significant correlation with these haplotypes.
In conclusion, a series of correlated MI disease risk haplotypes has been identified, consisting of 4-6 SNPs, with relative risk greater than 2 and allelic frequency in MI patients greater than 10%. The length of the haplotypes varies between39-68 kb. These haplotypes are carried by 19% (B5) to 29% (A4) of MI patients. The results suggest that the `at risk` haplotypes in the FLAP gene represent a new major independent risk factor for MI.
TABLE-US-00007 TABLE 7 SNP haplotypes and the corresponding p-values p-val RR #aff aff.frq. carr.frq. #con con.frq. PAR SG13S99 SG13S25 SG13S3- 77 B4 4.80E-05 2.08 903 0.106 0.2 619 0.054 0.11 G B5 2.40E-05 2.2 910 0.101 0.19 623 0.049 0.11 TG B6 1.80E-06 2.22 913 0.131 0.24 623 0.063 0.14 T G G A4 5.10E-06 1.81 919 0.159 0.29 623 0.095 0.14 G A5 2.60E-06 1.91 920 0.15 0.28 624 0.085 0.14 T G SG13S106 SG13S114 SG13S89 SG13S30 SG13S32 SG13S42 SG13S35 B4 G G A B5 G G A B6 G A G A4 T G A A5 T GA Relative risk (RR), number of patients (#aff), allelic frequency in patients (aff.frq.), carrier frequency in patients (carr.frq.), number of controls (#con), allelic frequency in controls (con.frq.), population attributable risk (PAR). The patientsused for this analysis were all unrelated within 4 meioses.
Association of the A4 Haplotype to Stroke
In view of the linkage observed for stroke in male patients to the FLAP locus and since there is a high degree of co-morbidity among MI and stroke, with most of these cases occurring on the basis of an atherosclerotic disease, it was evaluatedwhether haplotype A4 also conferred risk of stroke. The SNPs defining haplotype A4 were typed on the Icelandic stroke patient cohort. First and second degree relatives and all known cases of MI were removed, and 702 stroke patients were tested forassociation. The results are also listed in Table 6, above. A significant association of haplotype A4 to stroke was observed, with a relative risk of 1.67 (P value=0.000095). In addition, it was determined whether haplotype A4 was primarily associatedwith a particular sub-phenotype of stroke, and found that both ischemic and hemorrhagic stroke were significantly associated with haplotype A4 (Table 8).
TABLE-US-00008 TABLE 8 Association of the A4 haplotype to subgroups of stroke Phenotype (n) Pat. Frq. RR PAR P-value Stroke.sup.a (702) 0.149 1.67 0.116 0.000095 Ischemic (484) 0.148 1.65 0.113 0.00053 TIA (148) 0.137 1.51 0.090 0.058Hemorrhagic (68) 0.167 1.91 0.153 0.024 .sup.aExcluding known cases of MI.
It should be noted that similar to the stronger association of Haplotype A4 to male MI compared to female MI, it also shows stronger association to male stroke (Table 6).
Table 9 shows that the haplotype A4 increases the risk of having a stroke to a similar extent as it increases the risk of having an MI. The `at risk` haplotype is carried by 28% of stroke patients and 17% of controls, meaning that the relativerisk of having stroke for the carriers of this haplotype is 1.7 (p-value=5.8 10.sup.-06). Also shown in Table 9 are the haplotype B series (B4 and Bs4). The Bs4 haplotype has 10% allelic frequency in stroke patients. Relative risk of having stroke forcarriers of Bs4 is estimated to be around 2.
TABLE-US-00009 TABLE 9 Haplotype relation to MI and Stroke p-val r #aff Aff.frq. #con con.frq. info SG13S25 SG13S106 SG13S114 SG13S8- 9 SG13S30 SG13S32 SG13S41 SG13S42 SG13S35 MI haplotypes All MI patients A4 5.3E-07 1.80 1407 0.16 614 0.090.82 G T G A B4 1.0E-04 1.87 1388 0.10 612 0.06 0.67 G G G A Males MI A4 2.5E-08 2.00 864 0.17 614 0.09 0.82 G T G A B4 1.1E-05 2.12 852 0.11 612 0.06 0.67 G G G A Females MI A4 1.9E-02 1.44 543 0.13 614 0.09 0.73 G T G A B4 7.9E-02 1.45 536 0.08 6120.06 0.60 G G G A Replication in stroke All stroke patients A4 5.8E-06 1.73 1238 0.15 614 0.09 0.80 G T G A B4 2.3E-04 1.83 1000 0.10 612 0.06 0.71 G G G A Males stroke A4 1.1E-06 1.91 710 0.17 614 0.09 0.79 G T G A B4 3.1E-05 2.11 574 0.11 612 0.06 0.72G G G A Females stroke A4 9.9E-03 1.49 528 0.13 614 0.10 0.74 G T G A B4 6.3E-02 1.47 426 0.08 612 0.06 0.70 G G G A All stroke excluding MI 8.4E-05 1.65 1054 0.15 614 0.09 0.78 G T G A Males stroke excluding MI 6.4E-05 1.78 573 0.16 614 0.09 0.75 G T GA Females stroke excluding MI 1.2E-02 1.49 481 0.14 614 0.10 0.72 G T G A Cardioembolic stroke 6.6E-04 1.87 248 0.16 614 0.10 0.74 G T G A Cardioembolic stroke excluding MI 3.8E-02 1.56 191 0.14 614 0.10 0.70 G T G A Large vessel stroke 8.0E-02 1.47 1500.13 614 0.09 0.83 G T G A Large vessel stroke excluding MI 2.9E-01 1.31 114 0.12 614 0.09 0.80 G T G A Small vessel stroke 7.2E-04 2.05 166 0.18 614 0.09 0.71 G T G A Small vessel stroke excluding MI 1.0E-04 2.31 152 0.20 614 0.10 0.71 G T G AHemorrhagic stroke 4.4E-02 1.73 97 0.15 614 0.09 0.72 G T G A Hemorrhagic stroke excluding MI 3.9E-02 1.78 92 0.16 614 0.09 0.71 G T G A Unknown cause stroke 1.3E-04 1.88 335 0.16 614 0.09 0.75 G T G A Unknown cause stroke excluding 6.5E-04 1.82 297 0.16614 0.09 0.72 G T G A MI MI and stroke together All patients with either MI or stroke Best haplo A4 4.1E-07 1.75 2659 0.15 614 0.09 0.82 G T G A B4 4.1E-05 1.85 2205 0.10 612 0.06 0.70 G G G A Males A4 1.4E-08 1.93 1437 0.17 614 0.09 0.82 G T G A B42.0E-06 2.11 1290 0.11 612 0.06 0.70 G G G A Females A4 3.6E-03 1.47 1024 0.13 614 0.09 0.77 G T G A B4 2.8E-02 1.48 915 0.08 612 0.06 0.66 G G G A Patients with both MI and stroke A4 6.1E-05 2.10 184 0.18 614 0.09 0.86 G T G A Patients and controlsunrelated in 4 meloses Stroke patients excluding MI B4 1.6E-04 1.95 624 0.102 612 0.055 0.74 G G G A 5.8E-05 2.04 624 0.102 612 0.053 0.76 G G G A G BS4 1.1E-04 2.01 624 0.103 611 0.054 0.72 6.6E-05 2.03 625 0.102 611 0.053 0.75 G G G A 4.3E-05 2.08 6250.101 611 0.051 0.76 G G G A A Patients with both stroke and MI 1.3E-02 1.99 183 0.099 611 0.052 0.65 G G G A A G Stroke Males 2.2E-05 2.18 574 0.108 611 0.053 0.71 Stroke Females 1.1E-02 1.71 426 0.089 611 0.054 0.69 Large vessel stroke 2.0E-01 1.50 1370.078 611 0.053 0.71 G G G A Cardoembolic stroke 7.9E-03 1.96 207 0.099 611 0/053 0.71 Small vessel stroke 1.2E-04 2.78 139 0.137 611 0.054 0.72 G G G A Hemorrhagic stroke 1.6E-03 2.9 83 0.143 611 0.053 0.63 G G G A Unknown cause stroke 9.0E-04 2.10 2800.109 611 0.055 0.70
Haplotype Association to FLAP in a British Cohort
In an independent study, it was determined whether variants in the FLAP gene also have impact on risk of MI in a population outside Iceland. The four SNPs, defining Haplotype A4, were typed in a cohort of 750 patients from the United Kingdom whohad sporadic MI, and in 728 British population controls. The patients and controls come from 3 separate study cohorts recruited in Leicester and Sheffield. No significant differences were found in the frequency of the haplotype between patients andcontrols (16.9% versus 15.3%, respectively). However, when 9 additional SNPs, distributed across the FLAP gene, were typed in the British cohort and a search was performed for other haplotypes that might be associated with MI, two SNPs showedassociation to MI with a nominally significant P value (data not shown). Moreover, three and four SNP haplotype combinations increased the risk of MI in the British cohort further and the most significant association was observed for a four SNPhaplotype with a nominal P value=0.00037 (Table 10).
TABLE-US-00010 TABLE 10 Association of the HapB haplotype to British MI patients Phenotype (n) Frq. Pat. RR PAR P-value P-value.sup.a MI (750) 0.075 1.95 0.072 0.00037 0.046 Males (546) 0.075 1.97 0.072 0.00093 ND Females (204) 0.073 1.900.068 0.021 ND .sup.aP value adjusted for the number of haplotypes tested using 1,000 randomization tests. Shown are the results for HapB that shows the strongest association in British MI cohort. HapB is defined by the following SNPs: SG13S377,SG13S114, SG13S41 and SG13S35 (that have the following alleles A, A, A and G, respectively. In all three phenotypes shown the same set of n = 728 British controls is used and the frequency of HapB in the control cohort is 0.040. Number of patients (n),haplotype frequency in patients (Frq. pat.), relative risk (RR) and population attributed risk (PAR).
This was called haplotype HapB. The haplotype frequency of HapB is 7.5% in the MI patient cohort (carrier frequency 14.4%), compared to 4.0% (carrier frequency 7.8%) in controls, conferring a relative risk of 1.95 (Table 10). This haplotyperemained significant after adjusting for all haplotypes tested, using 1000 randomisation steps, with an adjusted P value=0.046. No other SNP haplotype had an adjusted P value less than 0.05. The two at-risk haplotypes haplotype A4 and HapB appear to bemutually exclusive with no instance where the same chromosome carries both haplotypes.
Discussion
These results show that variants of the gene encoding FLAP associate with increased risk of MI and stroke. In the Icelandic cohort, a haplotype that spans the FLAP gene is carried by 30% of all MI patients and almost doubles the risk of MI. These findings were subsequently replicated in an independent cohort of stroke patients. In addition, another haplotype that spans the FLAP gene is associated with MI in a British cohort. Suggestive linkage to chromosome 13q 12-13 was observed withseveral different phenotypes, including female MI, early onset MI of both sexes, and ischemic stroke or TIA in males. However, surprisingly, the strongest haplotype association was observed to males with MI or stroke. Therefore, there may be othervariants or haplotypes within the FLAP gene, or in other genes within the linkage region, that also may confer risk to these cardiovascular phenotypes.
These data also show that the at-risk haplotype of the FLAP gene has increased frequency in all subgroups of stroke, including ischemic, TIA, and hemorrhagic stroke.
Association was not found between Haplotype A4 and MI in a British cohort. However, significant association to MI was found with a different variant over the FLAP gene. The fact that different haplotypes of the gene are found conferring risk toMI in a second population is not surprising. A common disease like MI associates with many different mutations or sequence variations, and the frequencies of these disease associated variants may differ between populations. Furthermore, the samemutations may be seen arising on different haplotypic backgrounds.
TABLE-US-00011 TABLE 11 The marker map for chromosome 13 used in the linkage analysis. Location (cM) Marker 6 D13S175 9.8 D13S1243 13.5 D13S1304 17.2 D13S217 21.5 D13S289 25.1 D13S171 28.9 D13S219 32.9 D13S218 38.3 D13S263 42.8 D13S326 45.6D13S153 49.4 D13S1320 52.6 D13S1296 55.9 D13S156 59.8 D13S1306 63.9 D13S170 68.7 D13S265 73 D13S167 76.3 D13S1241 79.5 D13S1298 81.6 D13S1267 84.7 D13S1256 85.1 D13S158 87 D13S274 93.5 D13S173 96.7 D13S778 102.7 D13S1315 110.6 D13S285 115 D13S293 A LODscore suggestive of linkage of 2.5 was found at marker D13S289.
TABLE-US-00012 TABLE 12 Marker Map for the second step of Linkage Analysis Location (cM) Marker 1.758 D13S175 9.235 D13S787 11.565 D13S1243 16.898 D13S221 17.454 D13S1304 18.011 D13S1254 18.59 D13S625 19.308 D13S1244 19.768 D13S243 22.234D13S1250 22.642 D13S1242 22.879 D13S217 25.013 D13S1299 28.136 D13S289 28.678 D13S290 29.134 D13S1287 30.073 D13S260 31.98 D13S171 32.859 D13S267 33.069 D13S1293 33.07 D13S620 34.131 D13S220 36.427 D13S219 39.458 D13S1808 40.441 D13S218 41.113 D13S128841.996 D13S1253 42.585 D13S1248 44.288 D13S1233 44.377 D13S263 45.535 D13S325 45.536 D13S1270 45.537 D13S1276 49.149 D13S326 49.532 D13S1272 52.421 D13S168 52.674 D13S287 60.536 D13S1320 64.272 D13S1296 71.287 D13S156 76.828 D13S1306 77.86 D13S170 82.828D13S265 91.199 D13S1241 93.863 D13S1298 97.735 D13S779 100.547 D13S1256 102.277 D13S274 111.885 D13S173 112.198 D13S796 115.619 D13S778 119.036 D13S1315 126.898 D13S285 131.962 D13S293
The inclusion of additional microsatellite markers increased the information on sharing by descent from 0.7 to 0.8, around the markers that gave the highest LOD scores. Table 13 shows the exons with positions that encode the FLAP protein,markers and SNPs identified within the genomic sequence by the methods described herein.
TABLE-US-00013 NCBI NCBI build34; build34; start on stop on chr. 13 chr. 13 SNP/marker/ public (bp) (bp) exon name alias1 alias2 SNP Variation 28932432 28932432 SG13S421 DG00AAFQR rs1556428 A/G 28960356 28960356 SG13S417 SNP13B_R1028729rs1028729 C/T 28965803 28965803 SG13S418 SNP13B_Y1323898 rs1323898 A/G 28974627 28974627 SG13S44 A/G 28975101 28975101 SG13S45 C/G 28975315 28975315 SG13S46 A/G 28975353 28975353 SG13S50 C/T 28975774 28975774 SG13S52 A/G 28985244 28985244 SG13S53rs1408167 A/C 28985303 28985303 SG13S55 rs1408169 A/G 28985423 28985423 SG13S56 G/T 28985734 28985734 SG13S57 rs6490471 C/T 28985902 28985902 SG13S58 rs6490472 A/G 29003869 29003869 SG13S59 C/G 29004696 29004696 SG13S60 A/G 29007670 29007670 SG13S419SNP13B_K912392 rs912392 C/T 29015410 29015410 SG13S61 C/T 29025792 29025792 SG13S62 C/T 29026202 29026202 SG13S63 rs7997114 A/G 29026668 29026668 SG13S64 A/G 29038707 29038707 SG13S65 A/G 29042180 29042180 SG13S420 DG00AAFIV rs2248564 A/T 2904935529049355 SG13S66 A/G 29049446 29049446 SG13S67 C/T 29050416 29050416 SG13S69 A/C 29059348 29059348 SG13S70 A/G 29059383 29059383 SG13S71 A/G 29059402 29059402 SG13S72 G/T 29063702 29063949 D13S289 29064359 29064753 DG13S166 29066272 29066272 SG13S73 A/G29070551 29070551 SG13S99 SNP_13_Y1323892 DG00AAFIU rs1323892 C/T 29081983 29081983 SG13S382 FLA267479 A/G 29082200 29082200 SG13S383 FLA267696 A/G 29082357 29082357 SG13S384 FLA267853 A/G 29083350 29083350 SG13S381 FLA268846 DG00AAJER C/G 2908351829083518 SG13S366 FLA269014 DG00AAJES rs4312166 A/G 29085102 29085102 SG13S385 FLA270742 C/T 29085190 29085190 SG13S386 FLA270830 A/G 29086224 29086224 SG13S1 FLA271864 C/T 29087473 29087473 SG13S2 FLA273371 A/G 29088090 29088090 SG13S367 FLA273988DG00AAJEU rs4474551 A/G 29088186 29088186 SG13S388 FLA274084 A/G 29088473 29088473 SG13S10 FLA274371 A/T 29089044 29089044 SG13S3 FLA274942 C/T 29089886 29089886 SG13S368 FLA275784 DG00AAJEV C/T 29090025 29090025 SG13S369 FLA275923 DG00AAJEW G/T29090054 29090054 SG13S370 FLA275952 DG00AAJEX A/G 29090997 29090997 SG13S4 FLA276895 G/C 29091307 29091307 SG13S5 FLA277205 rs4238133 G/T 29091580 29091580 SG13S389 FLA277478 A/G 29091780 29091780 SG13S90 FLA277678 A/C 29092287 29092287 SG13S390FLA278185 rs5004913 A/G 29092536 29092536 SG13S6 FLA278434 A/G 29092594 29092594 SG13S391 FLA278492 A/G 29092947 29092947 SG13S392 FLA278845 G/T 29093964 29093964 SG13S371 FLA279888 DG00AAJEY rs4409939 A/G 29094259 29094259 SG13S372 FLA280183 DG00AAJEZA/G 29094999 29094999 SG13S393 FLA280923 A/T 29096688 29096688 SG13S373 FLA282612 DG00AAJFA A/G 29096813 29096813 SG13S374 FLA282737 DG00AAJFB A/G 29096874 29096874 SG13S375 FLA282798 DG00AAJFC C/T 29096962 29096962 SG13S376 FLA282886 DG00AAJFD A/G29097476 29097476 SG13S394 FLA283400 C/G 29097553 29097553 SG13S25 FLA283477 A/G 29098486 29098486 SG13S395 FLA284410 A/G 29098891 29098891 SG13S396 FLA284815 A/C 29098979 29098979 SG13S397 FLA284903 C/T 29101965 29101965 SG13S377 FLA287889 DG00AAJFF A/G29103909 29103909 SG13S189 FLA289833 C/G 29104271 29104271 SG13S100 FLA290195 DG00AAHIK rs4073259 A/G 29104629 29104629 SG13S398 FLA290553 C/G 29104646 29104646 SG13S94 FLA290570 rs4073261 C/T 29105099 29105099 SG13S101 FLA291023 rs4075474 C/T 2910632929106329 SG13S95 FLA292253 G/T 29106652 29106652 SG13S102 FLA292576 A/T 29107138 29107138 SG13S103 FLA293062 C/T 29107404 29107404 SG13S104 FLA293328 A/G 29107668 29107812 EXON1 29107830 29107830 SG13S191 FLA293754 DG00AAFJT rs4769055 A/C 2910839829108398 SG13S105 FLA294322 A/G 29108579 29108579 SG13S106 FLA294503 DG00AAHII A/G 29108919 29108919 SG13S107 FLA294843 rs4075131 A/G 29108972 29108972 SG13S108 FLA294896 rs4075132 C/T 29109112 29109112 SG13S109 FLA295036 A/G 29109182 29109182 SG13S110FLA295106 A/G 29109344 29109344 SG13S111 FLA295268 rs4597169 C/T 29109557 29109557 SG13S112 FLA295481 C/T 29109773 29109773 SG13S113 FLA295697 rs4293222 C/G 29110096 29110096 SG13S114 FLA296020 DG00AAHID A/T 29110178 29110178 SG13S115 FLA296102 A/T29110508 29110508 SG13S116 FLA296432 rs4769871 C/T 29110630 29110630 SG13S117 FLA296554 rs4769872 A/G 29110689 29110689 SG13S118 FLA296613 rs4769873 C/T 29110862 29110862 SG13S119 FLA296786 A/G 29111889 29111889 SG13S120 FLA297813 C/T 29112174 29112174SG13S121 FLA298098 DG00AAHIJ rs4503649 A/G 29112264 29112264 SG13S122 FLA298188 DG00AAHIH A/G 29112306 29112306 SG13S123 FLA298230 C/T 29112455 29112455 SG13S43 FLA298379 rs3885907 A/C 29112583 29112583 SG13S399 FLA298507 A/C 29112680 29112680 SG13S124FLA298604 rs3922435 C/T 29113139 29113139 SG13S125 FLA299063 A/G 29114056 29114056 SG13S400 FLA299980 A/G 29114738 29114738 SG13S126 FLA300662 A/G 29114940 29114940 SG13S127 FLA300864 A/G 29115878 29115878 SG13S128 FLA302094 rs4254165 A/G 2911602029116020 SG13S129 FLA302236 rs4360791 A/G 29116068 29116068 SG13S130 FLA302284 G/T 29116196 29116296 EXON2 29116249 29116249 SG13S190 FLA302465 C/T 29116308 29116308 SG13S192 FLA302524 B_SNP_302524 rs3803277 A/C 29116344 29116344 SG13S193 FLA302560 A/G29116401 29116401 SG13S88 FLA302617 B_SNP_302617 rs3803278 C/T 29116688 29116688 SG13S131 FLA302904 C/T 29117133 29117133 SG13S132 FLA303349 A/C 29117546 29117546 SG13S133 FLA303762 rs4356336 C/T 29117553 29117553 SG13S38 FLA303769 rs4584668 A/T 2911758029117580 SG13S134 FLA303796 C/T 29117741 29117741 SG13S135 FLA303957 rs4238137 C/T 29117954 29117954 SG13S136 FLA304170 rs4147063 C/T 29118118 29118118 SG13S137 FLA304334 DG00AAHIG rs4147064 C/T 29118815 29118815 SG13S86 FLA305031 A/G 29118873 29118873SG13S87 FLA305089 DG00AAHOJ A/G 29119069 29119069 SG13S138 FLA305285 C/T 29119138 29119138 SG13S139 FLA305354 C/G 29119289 29119289 SG13S140 FLA305505 A/G/T 29119462 29119462 SG13S141 FLA305678 C/T 29119740 29119740 SG13S39 FLA305956 G/T 2912093929120939 SG13S142 FLA307155 rs4387455 C/T 29120949 29120949 SG13S143 FLA307165 rs4254166 C/T 29121342 29121342 SG13S144 FLA307558 rs4075692 A/G 29121572 29121572 SG13S145 FLA307788 C/G 29121988 29121988 SG13S146 FLA308204 C/T 29122253 29122253 SG13S26FLA308469 C/T 29122283 29122283 SG13S27 FLA308499 A/G 29122294 29122294 SG13S147 FLA308510 C/T 29122298 29122298 SG13S28 FLA308514 G/T 29122311 29122311 SG13S148 FLA308527 G/T 29123370 29123370 SG13S98 FLA309586 G/T 29123635 29123635 SG13S149 FLA309851A/G 29123643 29123643 SG13S29 FLA309859 A/C 29124188 29124259 EXON3 29124441 29124441 SG13S89 FLA310657 B_SNP_310657 rs4769874 A/G 29124906 29124906 SG13S96 FLA311122 rs4072653 A/G 29125032 29125032 SG13S150 FLA311248 C/G 29125521 29125521 SG13S401FLA311737 C/T 29125822 29125822 SG13S151 FLA312038 C/T 29125840 29125840 SG13S30 FLA312056 G/T 29127301 29127301 SG13S31 FLA313550 C/T 29128080 29128162 EXON4 29128284 29128284 SG13S152 FLA314500 C/G 29128316 29128316 SG13S402 FLA314532 rs4468448 C/T29128798 29128798 SG13S403 FLA315014 rs4399410 A/G 29129016 29129016 SG13S153 FLA315232 A/T 29129139 29129139 SG13S97 FLA315355 A/G 29129154 29129154 SG13S154 FLA315370 C/T 29129395 29129395 SG13S40 FLA315611 G/T 29129915 29129915 SG13S155 FLA316131rs4769875 A/G 29130192 29130192 SG13S156 FLA316408 A/C 29130256 29130256 SG13S157 FLA316472 A/G 29130299 29130299 SG13S158 FLA316515 A/C 29130353 29130353 SG13S159 FLA316569 G/T 29130391 29130391 SG13S160 FLA316607 C/T 29130547 29130547 SG13S32FLA316763 A/C 29131280 29131280 SG13S161 FLA317496 A/G 29131403 29131403 SG13S162 FLA317619 A/G 29131404 29131404 SG13S163 FLA317620 C/T 29131431 29131431 SG13S164 FLA317647 rs4769058 C/T 29131517 29131517 SG13S165 FLA317733 A/T 29131528 29131528SG13S166 FLA317744 rs4769059 C/T 29131599 29131599 SG13S167 FLA317815 rs4769876 A/G 29132003 29132003 SG13S168 FLA318219 A/C 29133753 29133753 SG13S33 FLA319969 G/T 29134045 29134045 SG13S41 FLA320261 A/G 29134177 29134177 SG13S169 FLA320393 A/G 2913437929134379 SG13S404 FLA320595 rs4427651 G/T 29135558 29135558 SG13S170 FLA321774 rs3935645 C/T 29135640 29135640 SG13S171 FLA321856 rs3935644 A/G 29135750 29135750 SG13S172 FLA321966 A/G 29135809 29135809 SG13S173 FLA322025 A/T 29135877 29135877 SG13S42FLA322093 rs4769060 A/G 29136080 29136556 EXON5 29136290 29136290 SG13S194 FLA322506 C/T 29136462 29136462 SG13S195 FLA322678 rs1132340 A/G 29136797 29136797 SG13S174 FLA323013 A/G 29137100 29137100 SG13S34 FLA323316 G/T 29137150 29137150 SG13S175FLA323366 A/G 29137607 29137607 SG13S176 FLA323823 A/G 29137651 29137651 SG13S177 FLA323867 C/T 29137905 29137905 SG13S178 FLA324121 C/G 29138117 29138117 SG13S35 FLA324333 A/G 29138375 29138375 SG13S179 FLA324591 A/G 29138385 29138385 SG13S180 FLA324601C/T 29138633 29138633 SG13S181 FLA324849 DG00AAHIF rs4420371 C/G 29139153 29139153 SG13S182 FLA325369 C/T 29139277 29139277 SG13S183 FLA325493 rs4466940 C/T 29139435 29139435 SG13S184 FLA325651 DG00AAHOI rs4445746 A/G 29139971 29139971 SG13S185 FLA326187A/G 29140441 29140441 SG13S405 FLA326657 A/G 29140649 29140649 SG13S91 FLA326865 A/G 29140695 29140695 SG13S186 FLA326911 rs4769877 A/T 29140703 29140703 SG13S187 FLA326919 A/G 29140805 29140805 SG13S188 FLA327021 DG00AAJFE A/G 29141049 29141049SG13S406 FLA327265 C/T 29142392 29142392 SG13S92 FLA328644 rs4429158 C/T 29142397 29142397 SG13S93 FLA328649 A/G 29142712 29142712 SG13S36 FLA328964 C/T 29144013 29144013 SG13S407 FLA330265 C/T 29144203 29144203 SG13S408 FLA330455 C/T 29144234 29144589D13S1238 29144255 29144255 SG13S7 FLA330507 C/T 29144877 29144877 SG13S37 FLA331129 A/G 29144982 29144982 SG13S409 FLA331234 A/G 29144983 29144983 SG13S8 FLA331235 rs4491352 A/C 29145122 29145122 SG13S410 FLA331374 rs4319601 C/T 29145143 29145143SG13S411 FLA331395 A/G 29145171 29145171 SG13S9 FLA331423 C/T 29145221 29145221 SG13S412 FLA331473 rs4769062 A/G 29145265 29145265 SG13S413 FLA331517 rs4238138 C/T minor allele start position in end position in minor allele frequency (%) SEQ ID NO: 1 SEQID NO: 1 G 10.32 432 432 G 30.46 28356 28356 T 37.38 33803 33803 G 0.545 42627 42627 G 1.111 43101 43101 G 0.328 43315 43315 C 0.495 43353 43353 A 6.993 43774 43774 C 30.876 53244 53244 G 6.731 53303 53303 T 0.353 53423 53423 C 31.356 53734 53734 A30.935 53902 53902 G 5.492 71869 71869 A 1.812 72696 72696 G 35.00 75670 75670 C 1.314 83410 83410 T 3.521 93792 93792 A 30.031 94202 94202
A 1.724 94668 94668 A 0.369 106707 106707 A 13.66 110180 110180 A 20.779 117355 117355 T 5.965 117446 117446 A 16.923 118416 118416 A 34.364 127348 127348 A 8.537 127383 127383 T 25.536 127402 127402 131702 131949 132359 132753 A 37.302 134272134272 C 6.25 138551 138551 A 0.49 149983 149983 A 14.08 150200 150200 G 0.62 150357 150357 G 14.01 151350 151350 T 0.58 151518 151518 C 30.21 153102 153102 A 10.95 153190 153190 G 30.00 154224 154224 A 27.95 155473 155473 G 2.41 156090 156090 A 0.39156186 156186 T 10.23 156473 156473 T 15.17 157044 157044 T 13.60 157886 157886 G 12.44 158025 158025 A 13.45 158054 158054 G 14.59 158997 158997 T 26.84 159307 159307 A 12.73 159580 159580 C 43.67 159780 159780 A 12.18 160287 160287 A 8.38 160536 160536G 0.62 160594 160594 T 12.34 160947 160947 G 25.34 161964 161964 C 0.24 162259 162259 T 25.66 162999 162999 A 14.84 164688 164688 G 12.37 164813 164813 C 14.55 164874 164874 G 11.99 164962 164962 C 14.66 165476 165476 A 12.21 165553 165553 A 0.79 166486166486 C 10.15 166891 166891 C 3.53 166979 166979 A 12.45 169965 169965 C 0.62 171909 171909 G 31.55 172271 172271 G 4.94 172629 172629 C 15.51 172646 172646 T 27.91 173099 173099 G 14.74 174329 174329 T 1.17 174652 174652 T 1.28 175138 175138 A 2.17175404 175404 175668 175812 A 30.11 175830 175830 G 0.66 176398 176398 A 28.31 176579 176579 G 14.85 176919 176919 C 1.21 176972 176972 A 1.04 177112 177112 G 0.88 177182 177182 C 1.14 177344 177344 T 7.10 177557 177557 C 22.52 177773 177773 A 20.86178096 178096 T 13.83 178178 178178 T 4.05 178508 178508 A 4.07 178630 178630 T 4.07 178689 178689 A 1.06 178862 178862 C 16.00 179889 179889 G 49.36 180174 180174 A 29.75 180264 180264 T 5.06 180306 180306 C 46.23 180455 180455 C 1.59 180583 180583 T1.45 180680 180680 G 11.32 181139 181139 A 3.25 182056 182056 A 34.12 182738 182738 G 29.63 182940 182940 A 45.68 183878 183878 G 36.65 184020 184020 G 8.07 184068 184068 184196 184296 T 1.02 184249 184249 A 49.57 184308 184308 A 0.58 184344 184344 C24.71 184401 184401 T 7.19 184688 184688 A 1.10 185133 185133 T 37.65 185546 185546 A 45.50 185553 185553 T 1.22 185580 185580 T 0.89 185741 185741 T 36.69 185954 185954 T 29.11 186118 186118 A 30.19 186815 186815 G 3.29 186873 186873 T 36.96 187069187069 G 36.63 187138 187138 T 37.34 187289 187289 C 1.15 187462 187462 T 9.91 187740 187740 C 3.36 188939 188939 T 36.24 188949 188949 A 31.58 189342 189342 G 0.45 189572 189572 T 1.14 189988 189988 T 46.57 190253 190253 A 10.34 190283 190283 T 8.00190294 190294 T 33.71 190298 190298 T 2.29 190311 190311 G 1.19 191370 191370 A 1.01 191635 191635 A 47.88 191643 191643 192188 192259 A 4.68 192441 192441 G 29.72 192906 192906 C 8.22 193032 193032 C 21.10 193521 193521 T 8.57 193822 193822 T 23.23193840 193840 T 24.20 195301 195301 196080 196162 C 23.89 196284 196284 T 19.33 196316 196316 G 11.50 196798 196798 T 3.08 197016 197016 A 9.72 197139 197139 T 0.98 197154 197154 T 2.24 197395 197395 A 1.43 197915 197915 A 1.80 198192 198192 G 2.38198256 198256 A 0.61 198299 198299 G 2.55 198353 198353 T 0.83 198391 198391 C 48.50 198547 198547 G 2.44 199280 199280 G 2.45 199403 199403 C 2.45 199404 199404 C 2.55 199431 199431 T 20.00 199517 199517 T 2.46 199528 199528 A 3.50 199599 199599 C 8.39200003 200003 T 8.99 201753 201753 G 5.41 202045 202045 G 4.12 202177 202177 G 38.33 202379 202379 C 32.77 203558 203558 G 48.03 203640 203640 G 1.67 203750 203750 A 0.68 203809 203809 G 42.44 203877 203877 204080 204556 T 0.30 204290 204290 G 2.46204462 204462 G 0.56 204797 204797 G 30.23 205100 205100 A 2.40 205150 205150 A 2.24 205607 205607 T 1.64 205651 205651 C 1.40 205905 205905 A 9.52 206117 206117 A 48.14 206375 206375 T 2.50 206385 206385 C 49.41 206633 206633 T 2.36 207153 207153 T12.07 207277 207277 A 16.67 207435 207435 G 7.66 207971 207971 A 9.66 208441 208441 A 7.78 208649 208649 A 25.71 208695 208695 A 1.43 208703 208703 G 4.71 208805 208805 T 0.56 209049 209049 T 8.33 210392 210392 A 7.23 210397 210397 C 15.88 210712 210712T 3.29 212013 212013 T 0.30 212203 212203 212234 212589 T 16.28 212255 212255 G 16.70 212877 212877 A 1.93 212982 212982 C 30.64 212983 212983 T 20.57 213122 213122 A 1.54 213143 213143 C 16.37 213171 213171 A 7.42 213221 213221 T 1.91 213265 213265
TABLE-US-00014 TABLE 14 Extended 4 microsatellite marker haplotypes in the initial haplotype analysis. 4 markers: pos.rr-frqgt1perc Length p-val RR N_af P_al P_ca N_ct P_al P_ca Alleles Markers 0.88 4.71E-06 6.23 428 0.065 0.125 721 0.011 0.0220 -12 -6 0 DG13S80 DG13S83 DG13S1110 DG13S163 0.82 8.60E-06 INF 438 0.032 0.062 720 0 0 0 4 2 14 DG13S1111 DG13S1103 D13S1287 DG13S1061 0.67 6.98E-06 19.91 435 0.03 0.059 721 0.002 0.003 8 6 0 8 DG13S1103 DG13S163 D13S290 DG13S1061 0.767 4.85E-06 26.72436 0.048 0.094 721 0.002 0.004 0 0 2 12 DG13S1101 DG13S166 D13S1287 DG13S1061 0.515 1.93E-06 INF 422 0.048 0.094 721 0 0 2 0 0 6 DG13S166 DG13S163 D13S290 DG13S1061 0.864 1.68E-06 INF 424 0.024 0.048 717 0 0 0 2 0 -16 DG13S166 DG13S163 DG13S1061DG13S293 0.927 5.38E-06 INF 435 0.034 0.067 720 0 0 4 2 14 3 DG13S1103 D13S1287 DG13S1061 DG13S301
Length=length of haplotype in Mb. P-val=p-value. RR=Relative risk. N af=Number of patients. P al=allelic frequency of haplotype. P ca=carrier frequency of haplotype. N ct=number of controls. Alleles=alleles in the haplotype. Markers=markers in the haplotype.
TABLE-US-00015 TABLE 15 Extended 5 microsatellite marker haplotypes in the initial haplotype analysis. 5markers: pos.rr-frqgt1perc Length p-val RR N_af P_al P_ca N_ct P_al P_ca Alleles Markers 0.851 7.45E-06 15.43 413 0.034 0.067 715 0.0020.005 0 18 0 0 0 DG13S79 D13S1299 DG13S87 D13S1246 DG13S166 0.964 8.07E-06 INF 437 0.023 0.045 721 0 0 0 -12 6 8 6 DG13S79 DG13S83 DG13S1104 DG13S1103 DG13S163 0.964 2.38E-06 INF 437 0.026 0.052 720 0 0 0 6 0 8 6 DG13S79 DG13S1104 DG13S172 DG13S1103DG13S163 0.931 7.05E-06 5.8 429 0.068 0.131 721 0.012 0.025 0 -6 0 0 -2 DG13S79 DG13S1110 DG13S175 DG13S166 D13S1238 0.964 8.13E-06 INF 434 0.021 0.041 721 0 0 0 3 8 2 6 DG13S79 DG13S1098 DG13S1103 DG13S166 DG13S163 0.597 9.78E-06 4.58 428 0.074 0.143717 0.017 0.034 -6 0 0 0 -2 DG13S1110 DG13S89 DG13S175 DG13S166 D13S1238 0.896 6.92E-06 INF 428 0.026 0.051 721 0 0 -12 -6 0 -2 2 DG13S83 DG13S1110 DG13S166 D13S1238 D13S290 0.722 2.18E-06 INF 453 0.026 0.051 738 0 0 -6 0 0 -2 2 DG13S1110 D13S289DG13S166 D13S1238 D13S290 0.982 7.88E-06 INF 437 0.028 0.055 721 0 0 0 0 4 2 14 DG13S87 DG13S175 DG13S1103 D13S1287 DG13S1061 0.841 8.88E-06 INF 438 0.032 0.062 720 0 0 0 0 4 2 14 DG13S89 DG13S1111 DG13S1103 D13S1287 DG13S1061 0.841 9.67E-07 INF 4350.029 0.057 721 0 0 0 8 6 0 8 DG13S89 DG13S1103 DG13S163 D13S290 DG13S1061 0.982 7.90E-06 18.63 437 0.026 0.052 721 0.001 0.003 0 4 0 2 14 DG13S87 DG13S1103 DG13S166 D13S1287 DG13S1061 0.841 3.52E-06 28.52 436 0.048 0.094 721 0.002 0.004 0 0 0 2 12DG13S89 DG13S1101 DG13S166 D13S1287 DG13S1061 0.705 5.28E-06 INF 435 0.027 0.053 721 0 0 0 8 6 0 8 DG13S175 DG13S1103 DG13S163 D13S290 DG13S1061 0.841 4.21E-06 INF 422 0.048 0.093 721 0 0 0 2 0 0 6 DG13S89 DG13S166 DG13S163 D13S290 DG13S1061 0.7674.02E-06 28.11 436 0.049 0.095 721 0.002 0.004 0 0 0 2 12 DG13S1101 DG13S175 DG13S166 D13S1287 DG13S1061 0.767 1.29E-06 31.07 436 0.047 0.092 721 0.002 0.003 0 0 0 2 12 DG13S1101 DG13S172 DG13S166 D13S1287 DG13S1061 0.705 4.25E-07 INF 422 0.048 0.093 7210 0 0 2 0 0 6 DG13S175 DG13S166 DG13S163 D13S290 DG13S1061 0.683 6.58E-06 INF 437 0.029 0.056 721 0 0 0 4 0 2 14 DG13S172 DG13S1103 DG13S166 D13S1287 DG13S1061 0.767 2.85E-06 32.43 436 0.044 0.087 721 0.001 0.003 0 0 0 2 12 DG13S1101 DG13S166 D13S290D13S1287 DG13S1061 0.865 9.58E-06 18.39 451 0.023 0.045 739 0.001 0.003 0 0 2 2 -16 D13S289 DG13S166 DG13S163 D13S1287 DG13S293 0.865 5.08E-06 INF 453 0.019 0.038 739 0 0 0 0 2 0 -16 D13S289 DG13S166 DG13S163 DG13S1061 DG13S293 0.927 1.02E-07 27.65 4370.037 0.073 721 0.001 0.003 4 0 2 14 3 DG13S1103 DG13S166 D13S1287 DG13S1061 DG13S301 Length = length of haplotype in Mb. P-val = p-value. RR = Relative risk. N af = Number of patients. P al = allelic frequency of haplotype. P ca = carrier frequencyof haplotype. N ct = number of controls. Alleles = alleles in the haplotype. Markers = markers in the haplotype
TABLE-US-00016 TABLE 16 Basepair position of microsatellite markers (start and stop of the amplimersin NCBI sequence assembly build 34 and primer sequences (forward and reverse). basepair basepair Marker start stop name forward primer reverseprimer position position DG13S2393 CCTTTGCTTTGTTCCTATTTCTTT TCCCATTGCCCAGAGTTAAT 22831401 22831787 - (SEQ ID NO. 4) (SEQ ID NO. 5) DG13S2070 TCCTCATGTCTTCACCTAGAAGC CCACTCATGAGGGAGCTGTT 23020439 23020651 (SEQ ID NO. 6) (SEQ ID NO. 7) DG13S2071TGTCACAGGCACACACTCTCT GAGTATGGCTGCTGCTCCTC 23066973 23067076 (SEQ ID NO. 8) (SEQ ID NO. 9) DG13S2072 ATGGCTCACACTGGCCTAAA TGAACAGACCAATAATAGTGCAG 23136964 23137114 (SEQ ID NO. 10) (SEQ ID NO. 11) DG13S2078 AAGCCACCCTTTAAACAGCA GCTGAGGAAGCAACTCCACT23591927 23592081 (SEQ ID NO. 12) (SEQ ID NO. 13) DG13S2079 GCTCTGAATTCCCTGGCATA TTAGCCCTAGTCCCACTCTCC 23646974 23647183 (SEQ ID NO. 14) (SEQ ID NO. 15) DG13S2082 CAAGAGGCCTGCATAAGGAA AGATTGCCGGTGGCTTAAAT 23807898 23808174 (SEQ ID NO. 16) (SEQ ID NO. 17)DG13S2083 TGTCTGTTCCCGTCTGTCTG TTCATCCTCTGCCAAATTCC 23882291 23882532 (SEQ ID NO. 18) (SEQ ID NO. 19) DG13S2086 GGCATGTATTCACTGCCTGA AAACCCATTCTTCTTCCTCTTAC 24069346 24069771 (SEQ ID NO. 20) (SEQ ID NO. 21) DG13S2089 TATGTGTTCAGCCCAGACCTCCCCTGCCATGTGCATTTAC 24274920 24275129 (SEQ ID NO. 22) (SEQ ID NO. 23) DG13S44 CATTTCGGAAGGCAAAGAAA TTGCAATGAGGAATGAAGCA 24413148 24413382 (SEQ ID NO. 24) (SEQ ID NO. 25) DG13S2095 TCCATTATCCATCTGTTCATTCA GAAGAATTAATTGTAGGAGGCAAGA 24621830 24622- 121 (SEQID NO. 26) (SEQ ID NO. 27) DG13S46 CTGACATCACCACATTGATCG CATACACAGCCATGTGGAATTA 24652046 24652291 (SEQ ID NO. 28) (SEQ ID NO. 29) DG13S2101 ACGGTGATGACGCCTACATT TCACATGGACCAATTACCTAGAA 24863557 24863744 (SEQ ID NO. 30) (SEQ ID NO. 31) D13S1254AAATTACTTCATCTTGACGATAACA CTATTGGGGACTGCAGAGAG 25316434 25316657 (SEQ ID NO. 32) (SEQ ID NO. 33) DG13S55 AGCCAGTGTCCACAAGGAAG GAGGGTGAGACACATCTCTGG 25337471 25337753 (SEQ ID NO. 34) (SEQ ID NO. 35) DG13S54 AATCGTGCCTCAGTTCCATC CCACCAGGAACAACACACAC25377308 25377463 (SEQ ID NO. 36) (SEQ ID NO. 37) D13S625 TTGCTCTCCAGCCTGGGC TTCCTCTGGCTGCCTGCG 25391207 25391395 (SEQ ID NO. 38) (SEQ ID NO. 39) DG13S2695 TCCTGCATGAGAAGGAACTG CGACATTCACTGTGGCTCTT 25415551 25415807 (SEQ ID NO. 40) (SEQ ID NO. 41)DG13S1479 TTTGATTCCGTGGTCCATTA TTATTTGGTCGGTGCACCTTT 25459039 25459368 (SEQ ID NO. 42) (SEQ ID NO. 43) DG13S2696 GGTGCACCGACCAAATAAGT CCAGCTTATTCTCTCTGCCTTC 25459351 25459478 (SEQ ID NO. 44) (SEQ ID NO. 45) DG13S1440 GGTAGGTTGAAATGGGCTAACATCATGACAAGGTGTTGGATTT 25520858 25520987 (SEQ ID NO. 46) (SEQ ID NO. 47) DG13S1890 CCTCCTCTGCCATGAAGCTA CTATTTGGTCTGCGGGTTGT 25672727 25673140 (SEQ ID NO. 48) (SEQ ID NO. 49) DG13S1540 TACTGGGTTATCGCCTGACC CCAATGGACCTCTTGGACAT 25704358 25704504 (SEQ IDNO. 50) (SEQ ID NO. 51) DG13S59 TTTCGGCACAGTCCTCAATA CAGCTGGGTGTGGTGACAT 25720194 25720421 (SEQ ID NO. 52) (SEQ ID NO. 53) DG13S1545 CAGAGAGGAACAGGCAGAGG AGTGGCTGGGAAGCCTTATT 25760018 25760404 (SEQ ID NO. 54) (SEQ ID NO. 55) DG13S1524AGGTGAGAGAACAAACCTGTCTT GCCTTCCTTCTAAGGCCAAC 25843657 25843768 (SEQ ID NO. 56) (SEQ ID NO. 57) DG13S1529 CTGTAGACTTTATCCCTGACTTACTG CAATGAATGATGAAGATTCCACTC 26098943 260- 99063 (SEQ ID NO. 58) (SEQ ID NO. 59) DG13S1908 TGACACCATGTCTTACTGTTTGCGAGGATACAATGAGAACCAAATCTC 26110282 26110- 493 (SEQ ID NO. 60) (SEQ ID NO. 61) DG13S2525 CAGGATCATCAGCCAGGTTT GCTGCATGTCACTAGGCATT 26123233 26123381 (SEQ ID NO. 62) (SEQ ID NO. 63) DG13S1546 CCACAGAATGCTCCAAAGGT GAGTTCAAGTGATGGATGACGA 26159644 26159995(SEQ ID NO. 64) (SEQ ID NO. 65) DG13S1444 CAGATAGATGAATAGGTGGATGGA CACTGTTCCAAGTGCTTTGC 26207544 26207727 (SEQ ID NO. 66) (SEQ ID NO. 67) DG13S66 TATGCGTTGTGTGCTGTG GGGCCTTAGATTCTTGTAGTGG 26279746 26279962 (SEQ ID NO. 68) (SEQ ID NO. 69) DG13S1907TGTCCAGACTGCCTCCTACA TGCAACACCTGGTTCACAAT 26378401 26378521 (SEQ ID NO. 70) (SEQ ID NO. 71) DG13S68 TTTGCGAGTCCTTGTGGAGT ACAGTCCGCTCCCTCCTAAT 26511587 26511825 (SEQ ID NO. 72) (SEQ ID NO. 73) DG13S69 ATGCTTGGCCCTCAGTTT TTGGCAACCCAAGCTAATATG 2651818826518483 (SEQ ID NO. 74) (SEQ ID NO. 75) D13S1250 CTCCACAGTGACAGTGAGG GAGAGGTTCCCAATCCC 26721525 26721686 (SEQ ID NO. 76) (SEQ ID NO. 77) DG13S574 CAGCTCCTGGCCATATTTCT GAGCCATTTCTCTGGGTCTG 26853541 26853693 (SEQ ID NO. 78) (SEQ ID NO. 79) DG13S73 GGTCCGTGTCAACCCTTAGA CAGGTTGATGGGAGGGAAA 26878938 26879133 (SEQ ID NO. 80) (SEQ ID NO. 81) DG13S1532 CGGGAAATGACAGTGAGACC TGCCTAGATTCTCCCGTAAG 26899505 26899652 (SEQ ID NO. 82) (SEQ ID NO. 83) D13S1242 GTGCCCAGCCAGATTC GCCCCCAGTCAGGTTT 26943073 26943316(SEQ ID NO. 84) (SEQ ID NO. 85) DG13S576 TTTCTCTCTCCACGGAATGAA AACCCATTCTCACAGGGTGTA 27121599 27121797 (SEQ ID NO. 86) (SEQ ID NO. 87) DG13S1917 AGGAGTGTGGCAGCTTTGAG TGGATTCCCGTGAGTACCAG 27135092 27135232 (SEQ ID NO. 88) (SEQ ID NO. 89) D13S217ATGCTGGGATCACAGGC AACCTGGTGGACTTTTGCT 27169880 27170051 (SEQ ID NO. 90) (SEQ ID NO. 91) DG13S581 AGCATTTCCAATGGTGCTTT CATGTTGATATGCCTGAAGGA 27318359 27318725 (SEQ ID NO. 92) (SEQ ID NO. 93) DG13S1471 CACTGTCTGCTGCCACTCAT AGAGATTATGTGATGTACCCTCTCTAT27403303 274035- 44 (SEQ ID NO. 94) (SEQ ID NO. 95) DG13S2505 TGATGAAGATCTGGGCGTTA TGCCTGTGCTCACTCACTCT 27493479 27493626 (SEQ ID NO. 96) (SEQ ID NO. 97) D13S120 ATGACCTAGAAATGATACTGGC CAGACACCACAACACACATT 27540983 27541093 (SEQ ID NO. 98) (SEQ ID NO.99) D13S1486 TGGTTTAAAAACCTCATGCC ATCCCAAACTCTGTACTTATGTAGG 27623349 27623496 (SEQ ID NO. 100) (SEQ ID NO. 101) DG13S1495 CCTTGGCTGTTGTGACTGGT CACTCAGGTGGGAGGATCAC 27668199 27668471 (SEQ ID NO. 102) (SEQ ID NO. 103) DG13S1845 CACTTTGCCAGTAGCCTTGATTGGGAAAGTTAACCCAGAGA 27788787 27789056 (SEQ ID NO. 104) (SEQ ID NO. 105) DG13S1030 TTTGGGAAGAGCCATGAGAC CTCTGGGCATTGGAGGATTA 27872811 27873164 (SEQ ID NO. 106) (SEQ ID NO. 107) DG13S584 GGGAGACAAGTCAGGTGAGG CTGAGTATGGAGTCTTCATCATTATC 27924334 27924484-(SEQ ID NO. 108) (SEQ ID NO. 109) DG13S79 TGCTACTAGATTTGACCAACCA GACTTGTAAAGGATTTAGTGATTTCG 28213368 2821349- 5 (SEQ ID NO. 110) (SEQ ID NO. 111) DG13S80 GTGGAAGGCCTCTCTCTGTG TGCTTCTTGAGGGAAAGCAT 28297121 28297353 (SEQ ID NO. 112) (SEQ ID NO. 113)DG13S1934 CCTTCAGAGGATTTCCCTTTC CTGGTTTGACTCCAGCTTCA 28461787 28462194 (SEQ ID NO. 114) (SEQ ID NO. 115) DG13S1104 CCTGGCACGGAATAGACACT GGCCTCCTTTGCTCTGAAG 28497694 28498071 (SEQ ID NO. 116) (SEQ ID NO. 117) DG13S1097 CATCCCTGTGGCTGATTAAGAAACAGTTCCAGCCCGTTCTA 28532382 28532543 (SEQ ID NO. 118) (SEQ ID NO. 119) DG13S1110 TTTCAAAGGAATATCCAAGTGC TGGCGTACCATATAAACAGTTCTC 28547636 2854790- 0 (SEQ ID NO. 120) (SEQ ID NO. 121) DG13S87 TTCAATGAAGGTGCCGAAGT TGTCTATCCCAAAGCTGCAA 28597688 28597905(SEQ ID NO. 122) (SEQ ID NO. 123) DG13S2400 GCTCAGTCCAAGTTCATGCTC TGGGATTGGGTTCTGGATAC 28671947 28672231 (SEQ ID NO. 124) (SEQ ID NO. 125) DG13S3114 CCTACTTTCCATCTCCTCCTTG TGGAGTAAGTTGGAGAATTGTTGA 28678081 2867824- 8 (SEQ ID NO. 126) (SEQ ID NO. 127)DG13S1111 GCAAGACTCTGTTGAAGAAGAAGA TCCCTCTGTTTGAGTTTCTCG 28760422 28760531- (SEQ ID NO. 128) (SEQ ID NO. 129) DG13S3122 CCTTGGGCAGTCAGAGAAAC CCCGTGAAGTCTGAGAGGTG 28778662 28778906 (SEQ ID NO. 130) (SEQ ID NO. 131) DG13S1101 AGGCACAGTCGCTCATGTCAAACTTTAGCTAATGGTGGTCAAA 28812542 28812874 (SEQ ID NO. 132) (SEQ ID NO. 133) D13S1246 GAGCATGTGTGACTTTCATATTCAG AGTGGCTATTCATTGCTACAGG 28903534 2890373- 8 (SEQ ID NO. 134) (SEQ ID NO. 135) DG13S1103 TTGCTGGATGCTGGTTTCTA AAAGAGAGAGAGAAAGAGAAAGAAAGA28910502 289107- 65 (SEQ ID NO. 136) (SEQ ID NO. 137) DG13S3147 AAAGTGGATGCAGTTGAGGTTT GCTAGCCATTACAGACAACCAA 29018341 29018591 (SEQ ID NO. 138) (SEQ ID NO. 139) DG13S3150 CAGGGCTCCATGTATCCATAA CAATCTTTGGCTTTGGGTTT 29042766 29042948 (SEQ ID NO. 140) (SEQID NO. 141) D13S289 CTGGTTGAGCGGCATT TGCAGCCTGGATGACA 29063702 29063949 (SEQ ID NO. 142) (SEQ ID NO. 143) DG13S166 CCTATGGAAGCATAGGGAAGAA CCCACTTCTGAGTCTCCTGAT 29064359 29064753 (SEQ ID NO. 144) (SEQ ID NO. 145) DG13S3156 GGGAAATGGAGCTGCTGTTAGAGTGGGTGAGTGCAAGGAT 29111037 29111416 (SEQ ID NO. 146) (SEQ ID NO. 147) D13S1238 CTCTCAGCAGGCATCCA GCCAACGTAATTGACACCA 29144427 29144579 (SEQ ID NO. 148) (SEQ ID NO. 149) DG13S2605 TGAAAGGAAGGTCCCTGAGTT CCCTGCTTTGCACAAGTTATC 29145896 29146055 (SEQ IDNO. 150) (SEQ ID NO. 151) DG13S163 CACATGAGGCTGTATGTGGA TGTGCAGGAATGAGAAGTCG 29177152 29177313 (SEQ ID NO. 152) (SEQ ID NO. 153) D13S290 CCTTAGGCCCCATAATCT CAAATTCCTCAATTGCAAAAT 29227323 29227512 (SEQ ID NO. 154) (SEQ ID NO. 155)
D13S1229 GGTCATTCAGGGAGCCATTC CCATTATATTTCACCAAGAGGCTGC 29282262 29282396 (SEQ ID NO. 156) (SEQ ID NO. 157) DG13S2358 AGTCAAGGCTGACAGGGAAG GCTCTCAGCCCTCAATGTGT 29342275 29342399 (SEQ ID NO. 158) (SEQ ID NO. 159) DG13S2658 ATTTGGGTTCCTCTCCCAATACAAACTCTTGCTGCTGGTG 29348162 29348426 (SEQ ID NO. 160) (SEQ ID NO. 161) DG13S1460 TGCCTGGTCATCTACCCATT TCTACTGCAGCGCTGATCTT 29389048 29389297 (SEQ ID NO. 162) (SEQ ID NO. 163) DG13S2434 TCCTTCCAGAAGGTTTGCAT TGCAAAGTTGTTCAAGAGAGACA 29485254 29485392 (SEQID NO. 164) (SEQ ID NO. 165) DG13S1448 CAGCAGGAAGATGGACAGGT CACACTGCATCACACATACCC 29499404 29499531 (SEQ ID NO. 166) (SEQ ID NO. 167) D13S1287 TATGCCAGTATGCCTGCT GTCACATCAGTCCATTTGC 29513830 29514063 (SEQ ID NO. 168) (SEQ ID NO. 169) DG13S2665GGTTTATGTCTGTGTGTGTGTGC TGAGGGATGTCAGAGAAATATGC 29747845 2974798- 4 (SEQ ID NO. 170) (SEQ ID NO. 171) DG13S1904 TGATGAAATTGCCTAGTGATGC GGATCCAATCGTACGCTACC 29767797 29767922 (SEQ ID NO. 172) (SEQ ID NO. 173) DG13S1490 ACCTAAACACCACGGACTGGCAGGTATCGACATTCTTCCAAA 29908555 29908958 (SEQ ID NO. 174) (SEQ ID NO. 175) DG13S2637 GGTGATCTAGGGAATTATTTGTCTTC TTGGCCACTAAGGTCCAGAT 29941956 2994212- 0 (SEQ ID NO. 176) (SEQ ID NO. 177) DG13S96 CCTTTGAGGCTGGATCTGTT TTTCCTTATCATTCATTCCCTCA 3016643330166650 (SEQ ID NO. 178) (SEQ ID NO. 179) D13S260 AGATATTGTCTCCGTTCCATGA CCCAGATATAAGGACCTGGCTA 30234833 30234997 (SEQ ID NO. 180) (SEQ ID NO. 181) DG13S17 TTTAAGCCCTGTGGAATGTATTT GACATTGCAGGTCAAGTAGGG 30288392 30288544 (SEQ ID NO. 182) (SEQ ID NO. 183)DG13S306 TGCATAAGGCTGGAGACAGA CACAGCAGATGGGAGCAAA 30404049 30404203 (SEQ ID NO. 184) (SEQ ID NO. 185) DG13S2486 AGCCAGTTGTCTTTCATCCTG TGCCTGTGCTTGTATATTCTGTG 30411508 30411755 (SEQ ID NO. 186) (SEQ ID NO. 187) DG13S18 GTGCATGTGCATACCAGACCGGCAAGATGACCTCTGGAAA 30456875 30457193 (SEQ ID NO. 188) (SEQ ID NO. 189) DG13S1062 TTTGTGTTCCAGGTGAGAATTG GAACCATATCCCAAGGCACT 30551596 30551715 (SEQ ID NO. 190) (SEQ ID NO. 191) DG13S1093 TTGTTCCCACATTCATTCTACA TTAAACTCGTGGCAAAGACG 30625918 30626190(SEQ ID NO. 192) (SEQ ID NO. 193) DG13S1059 CACCATGCCTGGCTCTTT AACTTCTCCAGTTGTGTGGTTG 30822917 30823246 (SEQ ID NO. 194) (SEQ ID NO. 195) D13S171 CCTACCATTGACACTCTCAG TAGGGCCATCCATTCT 31051937 31052167 (SEQ ID NO. 196) (SEQ ID NO. 197) DG13S2359TCTGTGTGTATTGTGTACTCCTCTG TCACACAATTTGAACCAATCCT 31073673 310738- 49 (SEQ ID NO. 198) (SEQ ID NO. 199) DG13S1092 ACCAAGATATGAAGGCCAAA CCTCCAGCTAGAACAATGTGAA 31113759 31113934 (SEQ ID NO. 200) (SEQ ID NO. 201) DG13S2629 TGATCATGTCAGCAGCAGAAGAGTAACAGGTGAGGGCATGG 31179791 31179953 (SEQ ID NO. 202) (SEQ ID NO. 203) DG13S1449 TGTCCATAGCTGTAGCCCTGT CTCAATCGGGCATCTTTAGGC 31199228 31199498 (SEQ ID NO. 204) (SEQ ID NO. 205) DG13S312 CAAACAAACAAACAAGCAAACC TGGACGTTTCTTTCAGTGAGG 31280202 31280550(SEQ ID NO. 206) (SEQ ID NO. 207) DG13S1511 TGATAACTTACCAGCATGTGAGC TCACCTCACCTAAGGATCTGC 31321562 31321854 (SEQ ID NO. 208) (SEQ ID NO. 209) DG13S2454 GCTAGCAAATCTCTCAACTTCCA TCTTCTCCATGCTGCTTCCT 31352662 31352803 (SEQ ID NO. 210) (SEQ ID NO. 211)DG13S314 CATGCAATTGCCCAATAGAG TTGGGCTTGTCTACCTAGTTCA 31379760 31380086 (SEQ ID NO. 212) (SEQ ID NO. 213) DG13S1071 GCTGCACGTATTTGTTGGTG AAACAGCAGAAATGGGAACC 31447431 31447669 (SEQ ID NO. 214) (SEQ ID NO. 215) DG13S1068 CCGTGGGCTATCAATTTCTGAAGATGCAATCTGGTTTCCAA 31553333 31553570 (SEQ ID NO. 216) (SEQ ID NO. 217) DG13S1077 CCCAAGACTGAGGAGGTCAA GCTGACGGAGAGGAAAGAGA 31569360 31569733 (SEQ ID NO. 218) (SEQ ID NO. 219) DG13S2343 TCACAAAGCAAGCAATCACA TGATGGATGCACCATGTTTA 31653489 31653608 (SEQID NO. 220) (SEQ ID NO. 221) DG13S316 TGAGAAGCCTGGGCATTAAG ACAAGCTCATCCAGGGAAAG 31708002 31708244 (SEQ ID NO. 222) (SEQ ID NO. 223) DG13S1558 AGAGCTGATCTGGCCGAAG GGTGGACACAGAATCCACACT 31986248 31986627 (SEQ ID NO. 224) (SEQ ID NO. 225) D13S267GGCCTGAAAGGTATCCTC TCCCACCATAAGCACAAG 32062233 32062380 (SEQ ID NO. 226) (SEQ ID NO. 227) DG13S1478 TCAACCTAGGATTGGCATTACA TCTAGGATTTGTGCCTTTCCA 32157761 32158137 (SEQ ID NO. 228) (SEQ ID NO. 229) DG13S1551 ATTCGTGCAGCTGTTTCTGC GCATGACATTGTAAATGGAGGA32364898 32365153 (SEQ ID NO. 230) (SEQ ID NO. 231) DG13S1884 GGTGGGAATGTGTGACTGAA CCAGGTACAACATTCTCCTGAT 32451203 32451315 (SEQ ID NO. 232) (SEQ ID NO. 233) D13S1293 TGCAGGTGGGAGTCAA AAATAACAAGAAGTGACCTTCCTA 32536337 32536467 (SEQ ID NO. 234) (SEQ IDNO. 235) DG13S1518 AAAGGATGCATTCGGTTAGAG ACTGTCCTGTGCCTGTGCTT 32588965 32589321 (SEQ ID NO. 236) (SEQ ID NO. 237) D13S620 GTCCACCTAATGGCTCATTC CAAGAAGCACTCATGTTTGTG 32627749 32627947 (SEQ ID NO. 238) (SEQ ID NO. 239) DG13S1866 AGCCTGTGATTGGCTGAGAGGCTTACAGCTGCCTCCTTT 32633306 32633709 (SEQ ID NO. 240) (SEQ ID NO. 241) DG13S1927 CCCACAGAGCACTTTGTTAGA GCCTCCCTTAAGCTGTTATGC 32691932 32692304 (SEQ ID NO. 242) (SEQ ID NO. 243) DG13S1503 CACTCTTTACTGCCAATCACTCC GCCGTGTGGGTGTATGAAT 32699827 32700058(SEQ ID NO. 244) (SEQ ID NO. 245) DG13S332 TTGTACCAGGAACCAAAGACAA CACAGACAGAGGCACATTGA 32764576 32764751 (SEQ ID NO. 246) (SEQ ID NO. 247) DG13S333 GCTCTGGTCACTCCTGCTGT CATGCCTGGCTGATTGTTT 32872275 32872720 (SEQ ID NO. 248) (SEQ ID NO. 249) D13S220CCAACATCGGGAACTG TGCATTCTTTAAGTCCATGTC 32967602 32967793 (SEQ ID NO. 250) (SEQ ID NO. 251) DG13S1919 CAGCAACTGACAACTCATCCA CCTCAATCCTCAGCTCCAAC 33014255 33014477 (SEQ ID NO. 252) (SEQ ID NO. 253) DG13S2383 TGATTGGTTCTGTTGTTGCTG AGCCCAAGGCTCTTGTGAG33053369 33053553 (SEQ ID NO. 254) (SEQ ID NO. 255) DG13S1439 TCCTTCACAGCTTCAAACTCA AGTGAGAAGCTTCCATACTGGT 33070030 33070264 (SEQ ID NO. 256) (SEQ ID NO. 257) DG13S335 GCCAACCGTTAGACAAATGA CTACATGTGCACCACAACACC 33102278 33102478 (SEQ ID NO. 258) (SEQ IDNO. 259) DG13S340 AGTTTATTGCCGCCGAGAG ACCCACCACATTCACAAGC 33124866 33125238 (SEQ ID NO. 260) (SEQ ID NO. 261) DG13S1496 CGATTGCCATGTCTCTTTGA GAGATCTGGCCTGGATTTGT 33215915 33216066 (SEQ ID NO. 262) (SEQ ID NO. 263) DG13S347 TCATTGTCAGCACAGAATGAACTGGAGGGAGGGAAGAAAGAGA 33280351 33280688 (SEQ ID NO. 264) (SEQ ID NO. 265) DG13S339 GGGAAGAGGAGATTTGACTTGTT GGAACACCATCATTCCAACC 33352425 33352656 (SEQ ID NO. 266) (SEQ ID NO. 267) DG13S1926 TACAAGCTCCACCGTCCTTC TGAGTTGCTGCCTCTTCAAA 33388692 33388919 (SEQID NO. 268) (SEQ ID NO. 269) DG13S1469 TGCTAATGGGCCAAGGAATA GCTAAATGTCCTCATGAATAGCC 33416571 33416940 (SEQ ID NO. 270) (SEQ ID NO. 271) DG13S351 TGTCCTGCAGACAGATGGTC CCTCCGGAGTAGCTGGATTA 33497762 33498055 (SEQ ID NO. 272) (SEQ ID NO. 273) DG13S26GAGACTGGCCCTCATTCTTG AAGAAGCCAGAGACAAAGAAATACA 33584096 33584425 (SEQ ID NO. 274) (SEQ ID NO. 275) DG13S30 CATCTATCTTTGGATTCAGTGGTG TGCTCCCAACATCTTACCAG 33731684 33732071 (SEQ ID NO. 276) (SEQ ID NO. 277) DG13S1435 TGTCCTCTGGTCATTTCTATGGTCATGAATGAGAAGTGATGAATGG 33762069 3376228- 5 (SEQ ID NO. 278) (SEQ ID NO. 279) DG13S356 CAGACACTGTAAACTGGCTTCG GCCACATTGCTATCAGCGTA 33908746 33908957 (SEQ ID NO. 280) (SEQ ID NO. 281) DG13S2316 ATGTGCTGTGGTCCAGATTT CCTACTACTGCAATTACTCCCTACC 3391378733913954- (SEQ ID NO. 282) (SEQ ID NO. 283) DG13S357 TGTCATAGGCTTGCGGTATTT TTGGTAGGGTCCTTTCCTTT 33935177 33935378 (SEQ ID NO. 284) (SEQ ID NO. 285) DG13S1032 GCCTGCTCACTGTTGTTTGA CGGTTATCAGAGACTGGTGGT 33967059 33967269 (SEQ ID NO. 286) (SEQ ID NO. 287)DG13S1557 GGCTTATTTCATGTACGGCTA GGTTAAACTCTACTTAGTCCTGATGC 33996100 339962- 49 (SEQ ID NO. 288) (SEQ ID NO. 289) DG13S1925 GAACTCTGCAGGCACCTCTT CCTGAAGCGCTTGTACTGAA 34079148 34079570 (SEQ ID NO. 290) (SEQ ID NO. 291) DG13S360 TTGGCTTCTCGCTCTTTCTTAGCCATCAGTCACATGCAAA 34138872 34139221 (SEQ ID NO. 292) (SEQ ID NO. 293) DG13S1522 AGATCTCCAGGGCAGAGGAC CCTTCCTCCCTCCTTCTCTC 34195314 34195659 (SEQ ID NO. 294) (SEQ ID NO. 295) DG13S2324 CAGTCAAATGTCTCAACCTTCC CTAGCAACATGGCCAAGAAA 34224040 34224206 (SEQID NO. 296) (SEQ ID NO. 297) DG13S1517 CGTCATTGATCCCAATCATCT GGCTGATAGCCTCCCTTGTA 34271358 34271587 (SEQ ID NO. 298) (SEQ ID NO. 299) DG13S364 ACCTTTCAAGCTTCCGGTTT TTCCATCCGTCCATCTATCC 34323307 34323478 (SEQ ID NO. 300) (SEQ ID NO. 301) DG13S1036TTAAAGTCACTTGTCTGTGGTCA TTTGTAGGAATCAAGTCAAATAATGTA 34525065 345- 25280 (SEQ ID NO. 302) (SEQ ID NO. 303) DG13S1037 CTTTCGGAAGCTTGAGCCTA CCCAAGACCACTGCCATATT 34616658 34616926 (SEQ ID NO. 304) (SEQ ID NO. 305) DG13S1854 TGACAGGTTTGGGTATATTGGATGCTTAATGTAGTGGCAGCA 34622055 34622151 (SEQ ID NO. 306) (SEQ ID NO. 307) DG13S1038 TCCTGCCTTTGTGAATTCCT GTTGAATGAGGTGGGCATTA 34702405 34702738 (SEQ ID NO. 308) (SEQ ID NO. 309) DG13S2366 TTGGGAATAAATCAGGTGTTGA GCAGCAGCTCAGCATTTCTC 34735455 34735583 (SEQID NO. 310) (SEQ ID NO. 311) DG13S1039 CCATTTAATCCTCCAGCCATT GCTCCACCTTGTTACCCTGA 34743651 34743817 (SEQ ID NO. 312) (SEQ ID NO. 313) DG13S1840 ACAACCCTGGAATCTGGACT GAAGGAAAGGAAAGGAAAGAAA 34805466 34805682 (SEQ ID NO. 314) (SEQ ID NO. 315) DG13S369TGACAAGACTGAAACTTCATCAG GATGCTTGCTTTGGGAGGTA 34815499 34815755 (SEQ ID NO. 316) (SEQ ID NO. 317) DG13S2481 CAGGTTAGAGCCCATCCAAG AGGCTCAGCTTCATCCACAT 34867728 34867872
(SEQ ID NO. 318) (SEQ ID NO. 319) D13S219 AAGCAAATATGCAAAATTGC TCCTTCTGTTTCTTGACTTAACA 34956581 34956707 (SEQ ID NO. 320) (SEQ ID NO. 321) DG13S2351 GGGAACAGGTCACAGGTCAT GGAAGACTGGGTGGTCACAG 35099146 35099320 (SEQ ID NO. 322) (SEQ ID NO. 323)DG13S384 TTCCTTCTGCTTGTGAGCTG TACCCTCACCTTCCTCATGC 35499548 35499763 (SEQ ID NO. 324) (SEQ ID NO. 325) DG13S1507 GAAGACATTGGCAGGTCTGG GAGCCCTCATGTTGGGATAA 35557977 35558206 (SEQ ID NO. 326) (SEQ ID NO. 327) DG13S1512 TTGTTGATTCTCCCATTCTGTGTCACCTACCTCATCTCATACTCAAA 35668964 356692- 01 (SEQ ID NO. 328) (SEQ ID NO. 329) DG13S1556 TCTTCCGGACAAGTTTCCAA TGGGTCATTCTGGACATTCA 35791215 35791467 (SEQ ID NO. 330) (SEQ ID NO. 331) DG13S388 GCAAATGAGGCTGGTAAGGT TGCACTGTGGTAGAGGGAAA 35817061 35817320(SEQ ID NO. 332) (SEQ ID NO. 333) DG13S1442 CAACATACTCCTATGCCTAGAAAGAAA CTCACCAGGCAGAAACAGGT 35842967 358433- 35 (SEQ ID NO. 334) (SEQ ID NO. 335) DG13S1045 CCCAATGGCATGCTTCACT GGTTCTCCCAGCATTGGTT 35928180 35928324 (SEQ ID NO. 336) (SEQ ID NO. 337)DG13S2452 AAGGCCTCTGGGTAGGTAGG AAGCAATCCTTATGGGCTCT 35948528 35948826 (SEQ ID NO. 338) (SEQ ID NO. 339) DG13S2350 CCAGGTAATCAGAAGCCTCA TTCCGTTAAATCCAGCCATC 36011840 36011961 (SEQ ID NO. 340) (SEQ ID NO. 341) DG13S2483 CAGGGACTGCAGTGTCTCAAATGCCACATTTGCCTCTCTC 36027396 36027703 (SEQ ID NO. 342) (SEQ ID NO. 343) DG13S1100 CCACCTTCCACTTAATACAAACTTC GAAGCAATCCATTCCAAGAAA 36056838 3605711- 5 (SEQ ID NO. 344) (SEQ ID NO. 345) DG13S1501 GTCCTGAGGGTGTCCAGGTA GCTGGAGAACTCCTATTCTGCT 3621576136215909 (SEQ ID NO. 346) (SEQ ID NO. 347) DG13S1868 TGGAGCTATTGCGGTTCTCT TCAAATCTCTCTTTCCTCCTCCT 36313203 36313417 (SEQ ID NO. 348) (SEQ ID NO. 349) DG13S395 CAGTTCCAGCTACGGGAGAA CCGCATTTAGGCAAGTCTCA 36317151 36317507 (SEQ ID NO. 350) (SEQ ID NO. 351)D13S1491 AAGCACACACAGATGCTAGG CCTCAGCCTCCATAATCTCA 36361442 36361571 (SEQ ID NO. 352) (SEQ ID NO. 353) DG13S400 GTACAGAGCCCACCTTCTGG TCACTATGCTGCAAGGCAAG 36369862 36370134 (SEQ ID NO. 354) (SEQ ID NO. 355) D13S894 GGTGCTTGCTGTAAATATAATTGCACTACAGCAGATTGCACCA 36536509 36536706 (SEQ ID NO. 356) (SEQ ID NO. 357) D13S218 GATTTGAAAATGAGCAGTCC GTCGGGCACTACGTTTATCT 36830331 36830519 (SEQ ID NO. 358) (SEQ ID NO. 359) DG13S1553 TGGGTGAAGATGCTACCTGA CCCTTCTTCCTTTCCCTCTC 36898814 36899040 (SEQ IDNO. 360) (SEQ ID NO. 361) DG13S411 TGCCAGGTCTGAGTTGTAAGC CAGCATGAGACCCTGTCAAA 36908058 36908265 (SEQ ID NO. 362) (SEQ ID NO. 363) DG13S1870 GAAAGAAAGAAAGAAAGAAGAAAGAAA AATCACCAAACCTGGAAGCA 36927423 369276- 32 (SEQ ID NO. 364) (SEQ ID NO. 365) DG13S1870GAAAGAAAGAAAGAAAGAAGAAAGAAA AATCACCAAACCTGGAAGCA 36927485 369276- 32 (SEQ ID NO. 366) (SEQ ID NO. 367) DG13S39 TCTGAGTTAAACACTTGAGTTGCTG CCAGTAAATGGCAGTGTGGTT 36957292 36957640 (SEQ ID NO. 368) (SEQ ID NO. 369 DG13S2415 TGTCATGGATATTTCTACATAAACCAATGAAGATGGTTATTGCTTCCTTC 36984719 369- 84955 (SEQ ID NO. 370) (SEQ ID NO. 371) DG13S412 CGCTTTGTTTGGTTTGGTTT ATGCAGTTGTCCCACATGCT 37036929 37037137 (SEQ ID NO. 372) (SEQ ID NO. 373) DG13S414 TCCTGCACTCCAAAGGAAAC AACTCTGGTTTAATTCAGCTTTGTC 37047489 37047713(SEQ ID NO. 374) (SEQ ID NO. 375) DG13S1872 TTCTTGAGGGCATAAAGCTGA CACACTCACCAGGCACTCTG 37119505 37119608 (SEQ ID NO. 376) (SEQ ID NO. 377) DG13S416 CAGGTTTGATGAAGGAAATATGC GGGATCCTCTGCATTTCTCTAA 37125983 37126184 (SEQ ID NO. 378) (SEQ ID NO. 379)DG13S2607 TTTGCCAAATCAACCTTCAG CCTGCTTCACACCTCTGACC 37317455 37317831 (SEQ ID NO. 380) (SEQ ID NO. 381) DG13S1898 ACTCACACACAACCACCACA GCTACTGGTGGGTCGTAAGC 37318932 37319055 (SEQ ID NO. 382) (SEQ ID NO. 383) D13S1288 TTCAGAGACCATCACGGCCTGGAAAAATCAGTTGAATCCTACG 37321295 37321486 (SEQ ID NO. 384) (SEQ ID NO. 385) DG13S2567 AGGAAAGCCGAGAAAGCATA CATGTATCCACATGCCCAGA 37416093 37416462 (SEQ ID NO. 386) (SEQ ID NO. 387) DG13S418 CCTTCAGCGCAGCTACATCT AGAACTGCGAGGTCCAAGTG 37473016 37473380(SEQ ID NO. 388) (SEQ ID NO. 389) DG13S419 GGGAGAAAGAGAGGTAGGAAGG TTCCCAAGTTAGCAGCATCC 37532947 37533123 (SEQ ID NO. 390) (SEQ ID NO. 391) DG13S1051 TTCTAGAGGAGTCTATTTCTTTACTGG GGAGCTGTCACTTGAGCTTTG 37694432 37694- 579 (SEQ ID NO. 392) (SEQ ID NO. 393)DG13S1841 CCGTGACCTACAGGGAACAT GGCATCGGGTGTTTCTATTC 37715601 37715829 (SEQ ID NO. 394) (SEQ ID NO. 395) DG13S1052 AGACCTGCCTGTGTTCTGGT GGAGTGAAATAAGTGGAACTGGA 37831275 37831438 (SEQ ID NO. 396) (SEQ ID NO. 397) DG13S1053 CATTAAATGAGTCATAAAGGTCATGGAACATTGTTGCTTTGCTGGA 37935190 3793531- 1 (SEQ ID NO. 398) (SEQ ID NO. 399) DG13S423 GGCCTTAGCTCAGTTTCTGG TGCAAAGACATTTGCGGATA 37941221 37941411 (SEQ ID NO. 400) (SEQ ID NO. 401) D13S1253 CCTGCATTTGTGTACGTGT CAGAGCCGTGGTAGTATATTTTT 37944396 37944533 (SEQID NO. 402) (SEQ ID NO. 403) DG13S2539 GGAACCAGTCATTTGGGTGT TTATTGCTCCCTCGTCCAAG 38050898 38051253 (SEQ ID NO. 404) (SEQ ID NO. 405) DG13S2509 TGCCTTAAGGTCTATTATTTCCTTTC ACCAATGCAGGAAGACTCAA 38067039 3806718- 6 (SEQ ID NO. 406) (SEQ ID NO. 407) DG13S1863CTGATGAAAGGACACACATGC TGCATTAACTATGCAGCTTGAAA 38092085 38092353 (SEQ ID NO. 408) (SEQ ID NO. 409) DG13S2510 GTCGTGCAATCCCGAGAG GGATTCCTGCTGGCTCTTCT 38197807 38198059 (SEQ ID NO. 410) (SEQ ID NO. 411) DG13S1909 CTGGTGTGGTCAGGAAATGAGTGCTAAACACATGTGAGTGAGAG 38309328 38309442 (SEQ ID NO. 412) (SEQ ID NO. 413) DG13S428 TTTGACCATGCTTTCTCTTTGA GCTTGATGACTCCCTGCTGT 38346716 38347069 (SEQ ID NO. 414) (SEQ ID NO. 415) DG13S1858 AAGCCATTGAAAGGCAGGTA GGGACTTTCCGGCTTCTATT 38371574 38371742(SEQ ID NO. 416) (SEQ ID NO. 417) DG13S1911 GGTTTGGGAACCATTCTCCT GCAGAGAAGGGATTTACTCCAG 38475656 38475877 (SEQ ID NO. 418) (SEQ ID NO. 419) DG13S433 ACTTGACATGGAGCAAGCTG AGCTCATCATGCTGTAAGGAG 38516056 38516191 (SEQ ID NO. 420) (SEQ ID NO. 421) DG13S2421CACAGGCTCTCACATTCTCG TGACACTCATCCCTCTGCTG 38534972 38535357 (SEQ ID NO. 422) (SEQ ID NO. 423) DG13S2375 TGAGTTTCATAAGTTTACTACCTGCTG GGCAGGGAGAAAGGACAAAT 38548257 385484- 40 (SEQ ID NO. 424) (SEQ ID NO. 425) D13S1248 TCCCTTATGTGGGATTAGTTGACAGACATGGAACTGAGATTTTTT 38558005 38558267 (SEQ ID NO. 426) (SEQ ID NO. 427) DG13S1856 TGTTCCATCTCTCTACCCATGT TCAATGTTCTTATTGAGTGGGAAA 38577323 3857750- 6 (SEQ ID NO. 428) (SEQ ID NO. 429) DG13S435 ATATCCACCCACCCACACAT TAGCTCTGAGGGCAGAGACC 3859104338591261 (SEQ ID NO. 430) (SEQ ID NO. 431) DG13S2459 CCGTCCTTCCTCCACTGAT AGAGCACTGAGGGAGCAAAT 38596056 38596299 (SEQ ID NO. 432) (SEQ ID NO. 433) DG13S438 AGCTACAGCACGAGGCAGTT TTTGAATTGAGTTGCTGTTCG 38676957 38677248 (SEQ ID NO. 434) (SEQ ID NO. 435)DG13S1865 TGTACACCACCAACCATTCTG GGGAAGAAAGGCAAATAGCA 38684800 38684904 (SEQ ID NO. 436) (SEQ ID NO. 437) DG13S2354 GGATTGGCAATTAGCAGGTC GCCTGGTCAAAGATAACAGACG 38773862 38774026 (SEQ ID NO. 438) (SEQ ID NO. 439) DG13S2534 CCTGATTAAGCTGGCCTTTGATCCTTCTGGGACCCTCATC 38801698 38801951 (SEQ ID NO. 440) (SEQ ID NO. 441) DG13S1903 GCTTTGCTTCCTTCTTGGTG CAACATTACGGCCAGTCTCA 38802843 38803052 (SEQ ID NO. 442) (SEQ ID NO. 443) DG13S1896 GGTGCATCTGATAAGCCAAA GCTGTCTTGGACACAGTGGA 38815291 38815405 (SEQ IDNO. 444) (SEQ ID NO. 445) DG13S443 CACCATCATCATCTGGTTGG GAGCTCATTGAAAGGCAGGA 38838839 38839093 (SEQ ID NO. 446) (SEQ ID NO. 447) DG13S445 CCATCCATCTATCCATTTATCTCTG GGATTTATCCTTGCCCTGCT 38840399 38840584 (SEQ ID NO. 448) (SEQ ID NO. 449) DG13S447CTATCATCCATCCATCCTATTTG TTAGGGCAGCTACCTGGAAA 38840751 38840928 (SEQ ID NO. 450) (SEQ ID NO. 451) D13S1233 AGGACTANAGATGAATGCTC GACATGACTCCATGTTTGGT 38875108 38875292 (SEQ ID NO. 452) (SEQ ID NO. 453) DG13S2320 CCTCACCTTGCAATTTCCTG CTGACTTGCCTGTTGGCATA38957405 38957570 (SEQ ID NO. 454) (SEQ ID NO. 455) DG13S451 TTTGGGATCTTGAAGACCTTT TTGTGGCATGTCCTTGGTT 39032835 39033191 (SEQ ID NO. 456) (SEQ ID NO. 457) DG13S180 TGTACACTGCAAACATTGCTAAA TTGTCCTTTCATTATGACGTGTCT 39233968 3923435- 0 (SEQ ID NO. 458) (SEQID NO. 459) DG13S458 AAGCCTGAAAGGATACACACAAA CAGGATCCCAGACTTTCCAG 39475899 39476187 (SEQ ID NO. 460) (SEQ ID NO. 461) DG13S2547 GGTGAATCCCACCCTCATAC TTGGTATGTTTCCTATTGTTGCAT 39612492 39612849 (SEQ ID NO. 462) (SEQ ID NO. 463) D13S244GAACCAGTGAGTTTTTATTAC AGACACAGCATATAATACATG 39665226 39665353 (SEQ ID NO. 464) (SEQ ID NO. 465) DG13S2435 TGAAGCTTTGTGGCTTGTTG GACTGAGTCCACAGCCCATT 39863067 39863301 (SEQ ID NO. 466) (SEQ ID NO. 467) D13S263 CCTGGCCTGTTAGTTTTTATTGTTACCCAGTCTTGGGTATGTTTTTA 39878976 39879126- (SEQ ID NO. 468) (SEQ ID NO. 469) DG13S188 CCACCATGCAAGAACAGATG GCTTTGCACTTGGCTGTCTT 39935769 39936103 (SEQ ID NO. 470) (SEQ ID NO. 471) DG13S189 TTGCATGAAGTAAAGTATCCCTGT CACAAACCACAAGATGATTGG 39968676 39969030(SEQ ID NO. 472) (SEQ ID NO. 473) DG13S190 GGGCATCATGTCTACAACTCA ACCAAGGGCACTTGCTGATA 40027542 40027801 (SEQ ID NO. 474) (SEQ ID NO. 475) DG13S2370 AGGATGAAGAGGGAGGAAGG CCAGACTGATCTTCCTTAATTAGTTG 40159684 4015981-
2 (SEQ ID NO. 476) (SEQ ID NO. 477) DG13S196 CCTCCTCTTTCTGCTGCTGT AGCCAAAGAACCCAAAGAAAC 40251445 40251793 (SEQ ID NO. 478) (SEQ ID NO. 479) DG13S2457 GCCCTACTTTGCCTCAGAAA GCAACTCATGCCAGCCTCTA 40376042 40376447 (SEQ ID NO. 480) (SEQ ID NO. 481)DG13S2445 AACTGTGTTAATGATGGGCAAA AACGAGCGCATGAAACCTAT 40422793 40423200 (SEQ ID NO. 482) (SEQ ID NO. 483) DG13S211 CCTGGTCAATTGAACCCAAA TGAAGGAAGATAAAGCAGGGTAA 40434073 40434172 (SEQ ID NO. 484) (SEQ ID NO. 485) DG13S472 CTCTCTCTGGCCCTCTCTTGGGTAACTTGCCATTCTTCTACCA 40476985 40477395 (SEQ ID NO. 486) (SEQ ID NO. 487) DG13S207 ACTCCACCTGAAGGGAGAAA TGGAAGCCACTAATTGGAGAA 40545942 40546202 (SEQ ID NO. 488) (SEQ ID NO. 489) DG13S200 AATGGATGGATACCTCCTTATCA CTCATTGTGGCTTTCTGTGC 40737337 40737570(SEQ ID NO. 490) (SEQ ID NO. 491) DG13S198 GTACCCACACCTCACCAAGC CGTAGCTCACATTCCCAACA 40811813 40812059 (SEQ ID NO. 492) (SEQ ID NO. 493) DG13S215 GGCGAGTGAAAGAGAGGACA GGGTGGTAATTCCCAGATGA 40871695 40871992 (SEQ ID NO. 494) (SEQ ID NO. 495) DG13S221TCTGCAACAGCCAGAATCAA TGTCTGTTGGCAACTTTCTGTC 41107773 41108117 (SEQ ID NO. 496) (SEQ ID NO. 497) DG13S219 AGGTGAACCCAGTCCAGCTA TCTTAGGCAAAGGAGCCAGT 41127591 41127734 (SEQ ID NO. 498) (SEQ ID NO. 499) D13S1270 ACATGAGCACTGGTGACTG GGCCTCAAATGTTTTAAGCA41161654 41161831 (SEQ ID NO. 500) (SEQ ID NO. 501) DG13S225 TTCTGGGTGTTCGCTATTCC TTTCCTGTCCAGTCCTGACC 41212951 41213310 (SEQ ID NO. 502) (SEQ ID NO. 503) D13S1276 GTTTTGCAGGTCTAGGTCACAC AGGATAGCTTGAGCCCG 41213917 41214090 (SEQ ID NO. 504) (SEQ ID NO.505)
All references cited herein are incorporated by reference in their entirety. While this invention has been particularly shown and described with references to preferred embodiments thereof, it will be understood by those skilled in the art thatvarious changes in form and details may be made therein without departing from the scope of the invention encompassed by the appended claims.
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74 Homo sapiens agatg aatatgcatt cattcaccaa aatctcatattcccaaaaag caggaaaggt 6agtga gatggatgat gccttcacat gactcagatg tcacgtgttt ctcaccattg cccccaa ggcaccccct cccagcattt accagaatgt gtgtgtaact atttacagtg tgtgtaa ttatttgatt gtttctcttg tatcctgtag caatgagggt agagattata 24cctaccactgcagct ccaggatcca gcttcacaaa catttgttga atgaatgaat 3aaagag gacaccccca aagaggctgc aagggaaaaa gctacaaaga cagaagcacc 36aaagt agggtcatgt aagtcaaagc aggaaaaaag ttccatggtg gggtggtcag 42tctaa tgccacgaag gcacaaagta ggataaaggt taaaaatcagcctttggttt 48aatat gaagcttatc ggtagcctta gcgagaacaa ttccatcagg gagcagaagc 54gcagt gggttgagtc atcaagcagg cataaggaag tagggatacc ccattataag 6tctttc aagaagctca aatctgaagg ttaggagaat taggtcagta gctagaagga 66ggagt cgaggggctgtttttcctcc caaggagtat aaaggtgtaa cgttgcatga 72cttca gacaaaggcc gatatcaata gagaagttaa aacgcacgcc tcaagatttg 78gcttg gggttgggct taaagaggta ggagcatatt tcctatccta ggacagagaa 84aagaa aggataggtt cccatggaga taaatttcta agtgttaaag aagaggctca9attcta gcatgatagg ctcacttttt tctttttcca tgaaggagat ggcaaagtca 96catga gaaaggtgac aatactgatg ggttgaagag cgatggacat ttgaaataac cttagacc agtagaggct ggagttcata aatcagaact ggctacaggt tatatatgtt tttttttt tctccaacag cataagataacagagcgaag tctgtagaaa tgaaagaaga cagatgag gatagctgga gctagtgcaa ggagggaagc accacggtgg gagccaggta ccctggat ttataattca tactgaattc caacaacaga agggctctaa gcaggagagt cagatttc agaagactga gacacatttg gtaaaaaaaa gtaggaggaa aacctgattc gaattagg gcagccaata gacggcagta ttttcagaaa ggagggaatg gtcaacagtg tttctagt ctggagctca ggaggaagag gcaactctac ctgatggtat taagatcatg ggtagctg agatcaccta gcttgtgtgt gtcaaatgag aaaagaagaa agaataggag gttcccca ggaacacaga cattaagtggggctgtggtg acaacacaag aagagaggct caaaggag cctgagcagc tgtcatgaga gaggtaggat ggtggactcg gagaagaggc aagatgtt cttaaaggaa ggacactgct gccaagtagt cagccaattg gtgacaaaga gaccctgt tgcgagaaaa aaagtcagtg aagtagtagg aacgatgaca gatgacactg ttgaagac tgaggagaga gaagtgtaag agtggaagca gagggcagac cactcttctg acactgaa gaggcatagt tagaaataaa ggggagtcgc cagaaaggaa tttgtggcta caagaggt tttctttaag actgaaatac ataagcatga tttaaatgct gctgggatgg ttcacaga cctggaagac agaagacaaagcggatcatc aagatagtgg aatttactga tgagagag gaaaatccca tccacaggaa atgcagacat gagggagggg ccagaaggac 2gaaaaca tcagcaactg gtcccccaac ttctgagtga atgtggagat ataatcaggt 2ggactgc atcatctccc tggttaatga tggagtcaga gaaaagagtg tcttatacag 2ttgtgat atacttggcc gggcgcagtg gctcacgcct gtaatctaag cactttggga 222aggca ggcggatcac ctgaggtcag gagttcatga ctggcctggt caacatggca 228ccacc tctactaaaa acaaaagcct gtaatcccag ctactaggga ggctgaggca 234atcgc ttgaacccag gaggcagaggttgcagtgag ccaaggtcgc accactgtac 24gcctgg gcaacagagc tagactcagt ctcaaaaaaa aaaaaaaaag atgtatttat 246ctgta taaatttctg tgtaagaaat actctctcat atagaagtaa atttatatat 252tatat agaaccacta taaaatactc aggtttataa aatttatata taaacttgtt 258ataaa attccatgta aatgactata aagtactctt atatgaaaag tatatgaatt 264atata tcaacttact tttatattac agtatttttg ttatacagaa gtttatatag 27aataaa tatttctcaa gaacgatttc acataataga agtataaatt atccatttcc 276tgaaa aagaaaagca gttccacaccagtgacaggg ctacgaatct aagaggtaca 282ttcat tcttagagac actgaggtca gggcatggcc aacacatctg aagctgatag 288gcgct gggttggttg gagacggtac ggtattacta ttacaatggc agacgcttgg 294ataac tagccaatca gggggaaaga ttctggtttc ctctgttatt atctgaacta 3tgttccc aaagggttaa gatggtttat ggaaggcaca agatcagcaa accataaagg 3agcacta agaaggaagg aagtagacca agtgttaatg gcgatgccat gtaagagcca 3ctgcgat gtatgttcta catggtttgg ggggtaaaaa aaatgtcagc ctccagagca 3ggcttta agcctcaagt actgttaacagtagagttta ctagtctaca gcaggaatta 324agtaa ttctaaggcc aattactcag gcaagtttta ctagaacaag gaagctctgc 33aggtca aatcgatttc tgcatttata gaagcatcta gatgttctct gttcaaacaa 336taaaa tccccacaca ttttatttct gacagagtgt tccctatatt gcctggccag 342ataac attgcttggc tattattaat aaaacattgc tgtggctggg cgcagtggct 348ctgta atcctggcac tttgggaggc tgaggcagga ggatcactta actccaggag 354cagca gcctgggcaa catagcaaga tcccatctct ctaaaaaatt ttaaaattag 36gtgtgg tggcagacac ctgtagtcccagctcctcag gaagctgagg tgggaggatc 366agccc aagcaggttg aggctgcagc gtgctgtgac tgtgccactg cactccagcc 372aacac actgagagag actctgtctc aaaaaaatac atcaaataaa aattaaaagc 378tcttt cttttggtac attacagcca tgcacttcaa aggctagcac aattattttt 384gttct atatttagat tctagttaga agtaacctag gaccttcatg ttagaggtgt 39ggcaaa actgttatgt gagtgaaacg tttaatcaat tgaggataaa gatgcctcat 396atgaa gatgtggttt aaggatttta tgcacccagt tcatttatta acaacttgtt 4gctttat tagctgggtc tctactttataactgtgttc tttaatttac aagacaataa 4ttaaaat ggtaaatggg aaacctatct tgcttttcaa taaataattt attttaataa 4cgtgggc atggtggcca aaacatttta gctgtgaaaa taatttcaat tcatattttt 42aatcaa tattaaaagg tgatatattc tcaaatgaaa agtggacaaa tgatcagtta 426catga ttaagaaact aaccatgagc cacgtgcagt ggctcatgcc tgtaatccca 432ctggg aggccgcggt gagcggattg cttgagccca ggagttcaag accaggctgg 438atggc aaaaacccgg ctctactaaa aatgcaaaaa aaaaaaaaaa aaaaaaaatt 444gggtt ttggtggctt atgcctgcagtcccagctac tcgggaggct gactcgggag 45aggcac aagaatcatt tgaacccagg aggcagaggt tgcaatgagc tgagaataca 456gcact ccagcctggg caacagagag agagagactc agtctcaaaa aacaaacaaa 462aaaca aaccgctgcc ctgtgcttgg agagatctgt ttacctttac cactaaagac 468gaagt aaattttaga aggtttataa tacctaaaag taatcacttc tgtcttatga 474tctgc tgagattttt ctattgtggc cactagtggc aatattccag aagtcatatt 48gaatat ctttagtgga ttcagcagtt tttcaaatat gtacttttat ctctccaaca 486gattg caatttttca aattaacctcatgatataaa caactgtact ctatgatgcc 492gtaca gaaactggag gcagaaagag aagttgaatg tctaagaatc ggtaattcta 498caaca tagaccattc agcattagtg gttctaacaa tcccactgca aaatgagttg 5atgtgta acactttagt gaactaaagc ataaagaacc atggtctcct aatgcagcaa 5aaaacac atgatagcta caattaatga agtacatagt cctggctggg cactatggta 5cctttac atagattatc tcttaaatta ttaaccccgt tttagagatg agaacattcg 522aggaa ggttatgtaa gttatataaa aatcacaaaa taagagacag agctaagatt 528ccaag tgtgaccagg ttcatatcaagcttccattt ttgaatttat attagaggtc 534ctcac ctttgtcctt ttaaaataat ttttggctct gtgacctaca caggcaagct 54tttaca aacaacccac acatctagat ggtcactgtc tcaccgccca cttttaccat 546ctcct agtgagctgt caaggggaat gctataattt tggaggttct aaatctgagg 552agaaa gaaagaaatt gtaaaaagca ggcattactc aggggcatag attgtcaggc 558tgtca tgcttatagg taacctccca gggccaaaaa tatatgtgcc caaactgcct 564tttcc tgtcacttca taatactgcc tgaaatcctg ccaaattaga acttcatttg 57gcttgt caatttttaa cgcataagcaaatcacctgg agatcttgtt aaaatgcaaa 576attag gttaggtctg ggtctgcatg tctgatatgc ttccagaggg cactgatgct 582tccat ggaccacact taaagaagca aaaaagatgt ctgatattta ctctctggct 588ggagt gcttctcatt taagtgagat ctctttgtgc atcataatgg gagggatgag 594aagca gcaaattaag agtgagttaa gtgtctacct cacttcccta ctatctgtaa 6gcaggtt tgggcactgt ggtcaaccag aaaattcttt ccaggaccac aacccttgag 6atgttgc aaagatgcaa ggacaactta gaaataattt ccagcactgg tggcactgga 6ctgtcag tggtgctggt ggcagggtcctattcagact gtggtttacc tgcctggccc 6tggttat gggccatttt ctgagtacca tggagcatcg cccagctgac aagggcttgt 624accct tggtgcgcag aagggaagct tggctgctac taagtttggt gcaaagtaat 63gttttg ccattaatat ttgatacagt gagtccctac tttcctcagg tgaaactaga 636agggg acacgctcaa gttctcatta tacagtacta agtttcaaaa atcagcaatt 642aaaca catgctctac agcagtggtc ggcaaacttt ttctgtaagg ggccagagag 648gtttt agagtttctg ggccacatat ggtttctgtt ccagctataa actctgccac 654ggcaa aagcaaccct ccacaatacatacatgaata ggtgtgttcc aaaaaaactt 66tgtgga ccctgaaatt tgaatttcat aaacttttca tgtgtcatga aatattcttt 666ttttc ccaacctttt aaagatgtaa caaccatttt tagcctgtag gccatataga 672gcagt gggctgggtt tgctgaccct tgctctgaag caatgatatc tcgatccaat 678cccac aaatttttct ccttgaaacc atgcatttaa ttctcatctc ttcttaccat 684taaga agttattcta tataacaaag agattgtacc cacccaagcc agcatttaga 69gtcatt tgcttcctca aaattttggt ctttataaaa atcaattaaa gcaccttaaa 696agcag tgatgaaata tttgaaataattggctaatt aaacatcacc taaatagaaa 7tgataag aaccacaaat gcgaaaagga atcatgtagt aactaatgtg gaggatatct 7tttagag atttgatgaa cacgagtttt gatttaaaaa aatttgtgca atactcactg 7tggtggg gagcttgcta tgcaagttgg tagaaaaatt tatcctaaag tcacagttct 72cactct ggattttctc gagctaacta ccattccaaa ctattttagg cacagttact 726caaga atcaggcaaa ttgccctggt attagcactg ttctttctgt ggtcacaagt 732tactg tggtgaataa aattagatga tttctttagt ctttcctttt tcagcccctg 738aattt ccagtgctcc attcaaagaaaaaccaaaaa tgtccagaat ataaccttat 744aactt gttaaccact gatttcactt gttaaccaaa tttttttttt tttttttttg 75tgaatc tcactctgtc accaggctgg agtgcagtgg catgatcttg gttcactgca 756cgcct cctgggtact ggttcaagca attctcctgc ctcagtctcc cgagtagctg 762acagg tgtgcacccc cacacccagc taattttttt gtacttttag tagagatggg 768accat gttggccggg ctagtcttaa actcctgacc tcgtgatccg cccgcctcgg 774caaag tgctgggatt gcaggcatga accactgcgc ccagcctgtt aaccaaattt 78tcacac acacttgagg cccagtaaatgcctgctgaa aagagggtgc tggtggtgag 786tgagg ggctaacata ctgatagctg ctgaaatctt ctacagctct ttcttgttag 792tccat cacggctccc aggcccacac cacatgaagg aacttctagc tctcttgctt 798ttacc caaatgtagt tagcaagtcc tgggaactaa acagcattga cacacttgaa 8gacaatt aggcaaatcc caactgctgt gctcctgcag ctaaagatga agactcgtcc 8gggcagt tgattaattg tacctagaaa attaatttca atggtcccat gacaacatac 8cagtgaa gctctagtgt tccccctggg tggaatcttc caggatgtat agtctcccat 822ctcat cctcccattt ttccagattctggttcttct ctcttaccta gtgtgtagtg 828aatgg tggtccccca aaaagatatg tccatgtgtt aaccctggaa actgtggatg 834ttatt tggaaaaatg gggccaggtg cagtggtgtg catgtgtagt cccagaactt 84aagcca aggtgggaga atcgttggag cccaggagtt caagaacagc ccaggcaaca 846agacc cccgtctcta taagcaataa aaaattagct aggtgtggtg gcatgcacct 852tccag ctacttgaga ggctgaggca gaaggactgc tcaagcccaa ggagttcaag 858agtga gctatgatca tgtcacccca ctccagcctg ggtgacagag tcagactccc 864cagga gaaaagaaaa aaaggtctttgtaaatgtaa taaagaatct tgagataaga 87cctgat ttaggatgga ccctaaatcc aatgacattt gtccttacaa aagaaaggta 876aactg tgagacagac acagagggga gggccttgtg aagcaggaag catagatgca 882aagtc aaggaatgcc aaggactgtc tacaaccaga agccaggaga gatgcatggg 888ttctc cctcacagcc tccagaactt ctggcctcca ggactgtgaa gaatcaattt 894gtttt aagccaccaa gtttgtgtgt catttgttat ggcaatggca gtattaggac 9aatacac agtataaaaa aataaaaata gggccaggcg tggtggctca gacctataac 9agcactt tgggaggcta aggcggggagatcacttgag gtcaggagtt tgagaccaac 9gccaaca tggtgaaacc ccatctctat taaaaataaa aattagttgg gcatggtggt 9catctgt aatcccagtt actcaggagg ctgaggcaga agaatcgctt gaacccagga 924aggtt gtagtgaatg ccactgcact ccagcctggg tgacagagct agactccttc 93taggac acagccaagt cttacgtagc aaaaagaagt tgttaaaggt ctgtagttct 936aagca acacaggcat gtacctatga attatatgat tataaaagtg ctcggacagg 942ttcaa acttggcctc tttccaccaa ctgtgtactg tttctcattc cataactaga 948tgtct ttatatcctg tcaaaaaagtgaatttttgt gggctaagac attatccctg 954aatgc accagtctta gtgtaaacaa gcctagttcc tttttcattt tggctgtcta 96gcattt gtatatgcta ggcagtgtac taggcacctt aaatacatta ccttgtttaa 966acagg attctgggag gtaggcatta tccccatttt atagatgaga acactgagaa 972tgttc ataagtgcgt cacttgtctg agatgacata tttactaagt agcagaacca 978cgagc tactcagtct gatttccaaa gcccctgctc ttaatcacat caacttcttt 984atcac ctttcccaga gtgcgctctc atggataaag agcagaagta taagttacta 99gcagaa aactgtagag gtgggaagattagataaaaa atgtaaataa gaaggcttta 996ccaaa atcaaatgta aatactttat aacctgaatc agtgcttgtg ttcatgaggc agaggtcgt gcattttatc tctaggtctg gtgatgccaa tcctgatcta cagccagcag aacagttcc ctagcctgcc tagaagtttg taaatgcatg ggctttggta ggaggaagac agagaaagc agaacagatt attacaaacc cagtgcattc ccccttgatg ggtcaacagc atttctttg taagtgaagg acagcacact ggttttgatg actcacgaga gagtaggagg aaaaagaag tctgaggcat tgcctggaag cctcgctctg cttaaacaag tacactaatg ctcatgcct gttactccca gcactttggaaggccaagat gggtggatca cttgaggcca gagtttaag cccagcctgg tcaacatagc gagacctttt ctctattaaa aataaagaag aagaaagta ataatgattc aagttctcat tctctacaaa attcacttat gactttccaa tgctagtga aaacttttag gtattgcaaa actgccttaa tgcataacgg gattctcatt tacttagtc taagatgact ttttcacttt gaacttctgc atctttatga tcgcttagct tctgacaag caatttcagt aagtgtttat caatttgcat ccacacgctg acacataggg tctacttac atatccttca tgtaattgag cttttgtaaa tcatctttct acatggtaca ttctgattt tgtgtgcagc tttcttgtttaagcactgta ttaaatgctc tgcttcctac cccttagga acaatgagaa taaaagcgta atgttggtta cttcttcata tcaaaggaag tcatctcct ggttattaaa agctattatt aaatggccat ctttttgtgc ccctgtgtta gcactctac caagatacca ttaaatagat aagggccaca ctccatagag atgatggttc atattctgt attttctggg ggagttctaa tttcatgcaa ttccttcttc ttaaataaag caattctct aaatatatta cctaatgtgc tttcactttc atattcttgt aagatttttc cataaatca attctcaaaa aatagtatca taggcctttt aaaaatagtc atgttcaaaa tcaggctca tgaataaatg tgtgcattcattacatatat tttcataaat tcaaatttaa agaataaga gtagctagaa ggtggaagaa aaatcttatt ctgattagga atgcacaatc caagaaaat ttgtgatata tatagtcatt ttattctgta ttgttttatt ttgattttgg aagacaaga aacaatgtag aaagtttgac aacttaaaaa agtaatatga gtgtgagaaa tcctcttcc aggattagca aaaaaatggt tttttttttt tttttttccg agatggagtc cgctctctc gcccaggctg gagtgcagtg gcgcaatctt ggctcactgc aacctccgcc cccgggttc aggtgattct cttgcctcag cctcccaagt agctgggact acaggcatgt ccaccatgc ccggctaatt ttttttatttttagtagaga cggggtttca ccatgctggc aggctggtc ttgaactcct gaccttgtga tctgcccgcc ttagcctccc aaagtgctgg attacaggc gtgagccacc gtacccagcc taaatggcca agttttatta tggacaatta gctgtagaa taaaaatcta cttttaatag ctggcatagt gcctagtggt tttgaagcca aagcaggtt tacaaaaaac atttaaatcc atctgaatct acagaaaact aagattacct agcagaaaa tgaaaatagt tcaggattaa ggaagattaa caaatgaaga gtatatgtat ttagaagta ttactttata tttttatagt ataataataa tatttacgtt cctacactta aatgagttt cgtatatata ttaaaataatttaatggatt agtatgttta tatttgcttt agtaaattt ggtgtatgat aaactcagtt gtctacattg tgagactaca cctgaggcaa ttctgtgtt gatatatacc tgaatagcag atattacttg ggagcaaata aaatagcttc ggcctaatt ttgcaagttc atgatgggag agtaagcatg acttcaaaga actgactttg gttaaaact tgaagaatga atgtgacaac agcaagtata aaacaatgcc aggcagaggt ggactgttc atgggtatca gggtaagtgt gttgataaat gctcaaagta ggaaatacct tcttccccc acacatgtca gaaaataact gcaatagaat gcaacgacat ctcagagata agtgttcaa cttagctctc agagaccgttcagttacatt ttgtaatgac attggaattg ttgcatttt gaaggcaatt ctaaatgcaa agtcttcatt ttgttgatag aagctgggtt tttattatg aaatttcaaa aattaagtaa aatatctaat taggattata ccagcaaagg aaatttaga attcaagact tcatgatcca tggtaagatt attttaatgc aactctgcta ttaactgaa atttccttta actctcacat ctgcctttta cttcttaaga catttttcta tatttcacc agagcaagat atcagaaggg taaatctctt accaatgaac tttgctaatt ttagtgact ccgttgaccc tggtgtaagg atcaggaaca aagtgaatga aatacatttt atacatttc tgctttctct aattccaaagaccactctaa agaataagtt atttgtgggt ttatctgaa acttgggatt aaaagagacc gtgattaccc ttcagggatt ttggcaaaac taagccatt tcatctgaag agcaaagcaa gcctcccaca ctcttggctt attctcacaa tatctagat atctagcaac aaaactcttg agtagtttgt taactacaga tgccaagggc gacagtttc actttcagtt ttcagaatat cttttgtttc agtggtgtaa gcacaccatc gaatctcta ctatttaaaa taattaagtt ataattgtaa cttccattag atgtagtact aaaggaatc tagaagacac aactcattaa ttataggaat ttgactgcaa attcttctgg gggtctgaa ttgcaaagga ggcatctttgtaagtcagac tcaactcatt actctgtgat caggctcct ccaaatggca gcagaaacgt attactctct agaaacacta cagtagtgct caatttcag ggttctgtag agataaggac aaattgacag aaacacattc ttagaaggac gtatcattt aaaataaaaa tactgtcata attgtacacc aggatagctt ctccataata attctttat gattttctga tttttagaaa tcagaattga actttttaat gtgaaaaaaa gagagaatt gtttcaaaat aggaccacat ttctgtgtat aattttaaaa gtttaaaaat tttgattag tagactgata aactgaaaca tttttgataa gcttttcatt acatacaaac atataattt gtaaaaaatt ggaaattattcaaaacttca cataactaaa gtgaccaaat aatactgga gaggaaagaa aaggagtcaa atgaatctag cattttcttt tttttttttt tttggagaa agggtctcac tgtgccaccc aggtgggagt gcaatggcac gatcatggct actgcagcc tcaactttat gggcttaggt gatcctccca cctcggcctc ccaagtagca ggactacag gcatgcgcca acacgtccag ctaatttttt tggtattttt tgcagagacg ggtttcacc aggttgccgt ggctgatctg gaactcctgg tctcaagtga tctacccaac cagcctccc aaagtgctgg gattacaggc gtgagccacc gcacccggcc taatctagca tttctaaaa ggaaggaccc agcagtgaacggcaatatca ataatcatgt tcaagactat agacatgca agctggggat gaatgggtgg aaggggaaaa tgatgaataa atgatgaaca aagtataga cccagtggat ttgagatgcc caagatgcca gtgagatatt caaagtttaa tcaaaagcc acttcccata tgaaatcctg acaaacactc ctacgtccaa ctggaattaa ttctcttct gggctcccac agcactctgt atttttctaa tagcataaca ctattttgtt gtagatatt tctctgatag cattactatc tttcctcttt atcacaactg tttgaagttc tttgcctct tgcatccact gttgcccaat cccactgctg gaaggctcat cttattaagt ctgtattcc tagtgctaac acactgtctaccatagatga tgttcaataa atggttgcta atgaattct cttgtgataa tagcactatg gcaacataat cgacggtaaa aatttcttct aatgtttac ttttagcaga atgcattcat ttatcaactt tcattgagaa tatgctaatt ccatgaccc tgctaggaaa taggaaaata aagatgaatg taataaggtg ctcattctac gaaagtctt gactagtgga gaattatgga tccaactttt catgaaatgc cttcagtggt agaattctc atatttggaa taaaaaatgt tatgggttgt gccaagatac ctacatactt ataattttg tagagggctg tccttactgc agaaatgtat actactatag tcatatgtgg aattctttt tatgatgcta actgcatgctaaccagactt tttaatttaa tacttgcatt aataaacca tgctaggaat ccaggaatct
agcttggttt attttccata caatgtactc ttgtaatat gcatatacta cataaaaatt ctattaatgg cctcgtacta aagatgtgtc gttggggaa tcagttattc tgtataattt tatcttaatt gatatattaa aatctaccaa aatataaac tccgagtaaa agtatctgca tggtgtgcat atgtttattattttaagtgt agcgtatac attttcatgc cataaagtta taaaatgaaa aaatagtagc cttttatatt agttcatgc ttatgtagtt agtaaaaaca agaaagcaat taacatacaa accatgatgg ggttaaact tgcttcagtt tgtgtttttt aaaatttgaa agtgagaaat acagctcgaa tcagctcat attttcagtaagtactgatg aggatgtact ggccctattg actacgctga cccattaaa atatttgtga gtctaaaggt tcatatgacg ctgttccttc actctagcaa aggccatac atgtcttaca tagggactct gttcaattca ttaatacctc ctgaagtgct aacatcgtg gttcatttat agtagatact caatacatac tccattaactgaattctaag taaactgtc tgttactgac agaaattttc acttaaggga gtctccgtgg ctgaaggcaa tttgaaatc ctgtaaaaga acccactcct ctccccaagt aatgaagttt gtcagtttca gcctgtaat aaggtactga cttaaaatta attttctaat aatacagtac tgctatgtat taatgtggg gttagtcaatgataggaaaa aaacataaga cagagtcaca tttaaaaatg gtgcttagg tgcatggtga cacctgcctg tagtccagct attccagggg ctgaggcagg agatccctt gagctcacga gtttgaggct gcagtaagcc actgcactca gcctgggcaa agagtgaga ccctgtctct aaaaaaaatt cgttttaagt gtgctcaggacataacagga ccgctggta acatgccatt tccactgtga atatggtaag gacagaatcc ctgtctctag ccctcttcc actagtcaat ctcatcatca ccatcaaggc caacattggt attctctcct tgagacaaa gtctttgaca ttttctatac tatactatgt cttcctctcc ccaaatgcat tacaaataa aatttgaatgcttctttctc catttagtgt aatttttttt ataacataga ccaattttc aaaccccaca atggtggatt ttatttgatg tattgtaaaa agcgctggat gaagtcaaa tggcttggga gacctaaatt ctactcctgc ctgtaccatg aaagagacaa tcccaaggc tttgcagggc ttcagcttcc ttgtttgtag aataaagaattataaaatca ctcttttgg tcctactggg caataaaaag ctatgattct aagcctgttc ccttttctca ctaagaata caaatttgat acaaagaggc cgcagaatgt gtcaaacact ccctgttgcc ggaattctc tcttcctttg ggttcaggga taaaggtatg ttatttctta agtctccctt gctttcttc tgcttgcctcgtaaatattt ttccatcttg gcagtcctac atgtcttctc ctctacatg ttttccctag gtgatgtgac ccagcctgtg gcttccactg ccatccacac cgtcgctgc ctctctccac atcagcatcg caactatctc ctggaagctt tccaagtgct aactacagt aacctcaacc gaactgctgt tcattcaccc cacaggcttgcccctcctct catctttgt gagaacctga gagtcatcct aaactcctcc ttccacctca ctccccacat aaatcgatt accaacttgt gctgatttta tcttcaaata ctctccagaa ttgtcgctgt atggactga atatttgtgt tcccccaaat tcatatgtcc taatccctga tgtgactgta ttagagacg tgacctctaaggagtaatta aggttcagtg aggtcaaagg tggagccctg tctgatagg atcagtgtcc ttataagaag agactagagc tgggcacagg ggctcacacc gtaatccca gtattttggg aggctgaggt gggaagatca ctcaaggaga ggagtctgag ccagcctgg gcaacagagt gagactccat ctctacaaga aaataaaatagtcagacaca tggtacaca cctgtggtcc cagctcctca ggaggctgag gcaggaggat ggcttgagcc aggaatttg aggctgcagc aagctatgat cacacctctg cactccagcc tgggtgacag atgagaccc agtctcttta aaaaaaaaaa aaaaaaaggc catatatagc ccagaagagc tcctcacca aaacccaatcctgatagcac ctggaggact tccagcctcc agagctgtga aaaatttct gttgcttgca ccgcccagtc tgtggtattt tgctgtggca gcccaagctg ctcatcagt gaccttctct ctgttaccgc agagtagctc atcatcctct cttccctaga tccagccac tctctcacat ctacctacct agcagtatca ctgtgggttagagtcagatc ctgcggatt aagtcctcat tctgccactg cctgtgtaaa tctgagcaag ttacttaatc ctctgtgtg tcagtaacct ccctgtgaaa tgaggctaat aatagcaggg ttgtttcaac aggcgatac atgcataatg cttacaacac agcttggcac attataagca ttcaacgaaa gtgagctac tattatctcatccgttatca gaataaacca cctaagccac aaggctgccc catcatcct catgttttaa aacacttcag tgggctcccc accatcaaca ggataaagtc aagcttcct tagcatttct tagaggctcc atatgaatcc ccaagttcca ctacaggaac caggtgaac tttccactcc aacctcaggc tccttcgtgt cactcctcatccacatggag taagcagca agagactccg tgcagttcct ggtggttccc tgaccctcag gcagactctc ccagccctc tgcctgcaac gtccttgccc tttgcttccc ttggccagct cccattcatt tccttgatt ctgcttggaa gtttccctct caggaaggct ttatgaacct tagtgtaggt atgaaccca tctttgctcctttcatacct tttgcaagcc tttatttatt atgacactta ccattatca tactgaagtg acctgttggt gtgtctttgt tccccactag acagaaaact aagatcaga gaccagttct tgttcttttt tttttttttt tttttttttt ttgtatcaca tgtttagca gcctgctata tggtaaatgt cagtaaatgt tccacaaactgaatggaatt agctctgga atctagacca tcttttccat acccatcact cctgtcttag ttgaagtcct atttcccat ttgaagcaat gcaaaggatt tcctaactct aatctctctt ttcttcacac atcctttaa acagccgaca gaatggtcat cctaaagcac atatatccta tcttacatat ctagattcg gaacctctctgggcttctca ccatataaga agaaagtcta acctccttag aaggtgcat aggtcttcaa tgggctccac ctcacttctc tatatatacc tatactcttg tacactaaa cttctttctt actgttgctg gaacaagttc aacgctttca aacctccctg ctttgcata tgcagttcat tctgtcagga atgcccttct ctcttatgcctgggatattc cattcattc catatgacct atttcataag tcactcctta atgaagcctt tcttagatat cactggggc aatcagctgc ttgctcctgt ttccacagca cattgttcac acagatagca aggacttac cacaagttat tataattttg tctgtcttgc ccatttgaat ccaagggcaa gacggaatc attctcatctttgtatgtcc tgggaactag aactgtacct gagacataat aacacttga tatgtttgta atttttaaat aagttaatga acggaatggc tagaaaaagt agaagaaac tctggcttac tgtatatcat actgtcatac taaaaatata tactgaagac gaatcacat tatatcatca cttttcacgc tataggccat gatccattatgaaaaagagg tagtaaaaa aatcacaggg cacaattttt gtttctgtca cacacatgtg tacctgtata tggactgga atgtaaaacg catgttccat tgtagaacgt ggttttaaaa gaggcttgga aacactgca tatggtcatt tcttagttta gtacaattta ttattttcgt aataacctca ctataatat aagtctaccatgaagcattt tggggagatt aaatgagatg tgaaaagtaa tgtgttaga tagactgaat tcatatcata gcttgctctg atactttaca aaacatttaa cttacccac aagttttagt ttcctcacta aagtcaccct gaggacagta atgggatctt ctcacagag tattgtgagg aatacataag agaacgtacg taaatgcctggcacttagta ttattcaat aaatcttagc aatgatgatg ataacaacat ggtacctggc acataagaga ttaaaaatt agtttcttca gtcaaatgtg cttacattga tagttgatac taactggggt aaaaggtca ttgctggcat ctcagaaaga tagattacag tgaaataaaa aatgactact 2ttaaaatg aatgaagacttatttacaaa gtcatgttca tctggtacaa taatgaagtc 2tcaattgg gagaaaatga caaataatac aagtgaatat acaatcttac ttaagacgaa 2aaatagga caccaggcta actatcagtc tcctaaacca caactttatt tctgatacaa 2agacagtg agacaatcag ggcttccctc aaataaatta cttaatctctcttcaattca 2tttgcatc tgtaaatata aataactaca atttcacagt atttccattt aaaaagttct 2tgcaacat cagaaacaag aacttagtag gtgttcaaaa agaaatataa gttctgcttt 2tagccagc aaatagttgc ctgtttctag ccctcacttc ttttctccta aatccctata 2gcatttat ttaacttaaagtgctggatg tggcactacg agaaagaaaa agatatttgg 2atcttgtt aaaatcatta gacatcccag gctatctgga atcaccttgg gctcacagtt 2acatcagc tatggcttgt tttatttaaa aattcatcca ctgatgcatg ataatggaat 2acaggaga gcaatttacc aaaaaaaaga aatttattga tttataatgtgagatattaa 2tagccaca aatatttatt gagcatctcc tacatgccag ggaatggact atatatggca 2aaaacaga taccaatcat ttatatcagg catttttttc taatagaagg atattcgcag 2gacaatgc atagcaccat gccttgcacg taacagacat ttaataacta ttagttgaat 2aattggag actagaatgatacataaaga ggcaagaaag agcaaagata agcctttctg 2aatttcta tcatgttttg ctcaatagct tgtctttatc cactgcttgt atttttccat 2agctaatc ctcattggtc gttagaattg agacaccctt tccttgaaat caggagctat 2gaggccat tcttcctact gggcattttc tttctgggac agggtctcactctgtcacct 2gctggagt gcatcatagc tcactataac cttgaagtcc tgggctcaag gaatcctctt 2caaagagg tgggattaca ggcatgagtc accatgccag cctatttggc atttctactg 2gacaaagc agacttacag cagtaggtct acctgcctaa tacaaaaaga aaaaaaagaa 2ttaacaaa caaatgagggaatcagatcc agaaagtgat tcttataact tagattactt 2agtagatc tataatctgc tctagatcca ctgcatacag tgggcccttc ttatcatatt 2ataaatag cacttttctc agcccagctt ttgatgatag ctgaacagac taacagtttg 2taacaaag gctagagaag gggatagcaa ataatggccc acaggctgaatcctgcctgc 2ctcatttt tgcaaagttt tattagaata cggtcatttc cactcatttt cacactgtca 2ggctgctt ttgcgctaca gcagcagagc tgggtggttg gggcaggggt cacatggcta 2aaagacta aaatacttat catctgacct tttacagaaa gtttgctgat ccttggagtg 2caagtatt ctatattgttgattaagaac agaaccacaa gtattagaag ttagaccagc 2gtggtaaa gctgatcatc tactaatata atggaaattg gggttcccaa tcaggactct 2ctttgata gaaggccatc ttaacgagga gggagacacc tgcaggcaaa gtcagaattt 2tgcaggaa aagttttgag tccatttccc cttgtgaaca agtgctcagctatgcatttc 2ctttagta accatgcttc tatacctggt tctccttggc aaagatttct ttcttcagta 22ctcaaga ctttctggga aggtagggag atatgggggt aaaagtgtcc caggacttac 22aggaagt gttttatgat tatctgatag aatcactgta tcatggtaga gaaggcaaac 22atataat ctgaaaatagaggtgagggt gaacaaatgg gcactaaaag tgaactcagc 222ggaagg tagcaaaaca agacatcagt caaagatatg gggtgattca gacctaagga 2226taatg tgggatgttt ccgtgtgcca ggagctggac acttaagcaa gaggagatcc 2232tgttg ctaaaaccat ggcctccata ctttattgga attagcacaacttatccttg 2238ttcat tttgcaatca aaatctttaa aaacacatta tttaaaaata cattatttta 2244tagaa tgaaaattat gatatcattt aggtggttta aaaaacatcc accagccggg 225gtggct catgcctgta atcccagcac tttgggagtc cgaggcgggc agatcacgag 2256gagat tgagaccatcctggctgaca cggtgaaacc ccgtctccac taaaaataca 2262ttaac cgggcgtggt ggcgggtgcc tgtggtccca gctactcggg aggctgaggc 2268aatgg catgaacccg ggaggtggag gttgcagtga gctgagatcg tgccactgca 2274gcctg ggtgacagag caagactcca tctaaaaaaa aaaaacaaaaaccatccacc 228tgggaa gaagtgatga aaaattacag tccaagaaga agggccatag ctgtttaaat 2286ggtat atttgttatc taatataacc ccacgtaacg acaggtattt aacaaatgtt 2292tgaat ttgacgattc catttccctt acatcccata tgcaatccat cagcacccca 2298aaccc atcagtacatcctgtcagca ttggctccca aatataacct aaatctaaca 23atcctac tatctctgct gctacaactt tagtctgaaa tctcataatc tcccacttgt 23actgtag atgactctga atgagtcttc ttgcttccat tccacacagc atccatactg 23tattttt tttttcaatt ttttgtagag acggggtctt gccatgttgcccaggctggt 2322actcc tggcttcaag ggatcctccc acctcaacct cccaaagtga taggatttca 2328gagcc actgtgccta accctgactg atctttctaa gcataaatct aataatgccc 2334ttgat taaacccttc aatgaattca cattaagcaa acaacctggc caggtgtgat 234catgcc tgtaatctcagcactttggg agaccaagat gggaggatca cttgaggcca 2346tcaac atcagcttag acaacatggt gaaactacat ctctacaaaa aatacaagaa 2352tgggc atggtggtgc acctatagtc ccagctactc gggcggctga gctgggagga 2358tgagc cctggaggtc aaggcagcag tgagctgtga ttatgccactacacttcagc 2364tgaag tgagacctgg tctccaaaaa aaaaaaaaaa aaaaaaaaga agcagggcaa 237gctcac acctgtaatc ccatcacttt gggaggccaa ggcaggcctc ctggatcatg 2376aagag atcgagacca tcctggccaa catggtgaaa ccccatctct actaaaaata 2382attag ctgggcatggtggcatgcac ctgtagtctc aggtacttgg gaggctgagg 2388gaatt gcttgaaccc gggaggcgaa ggttgcagtg agccaagatt gcctggtgac 2394gagcg agactctgtc tcaaaaaaaa aaaaaaaaag aaagaaagaa agaaagaaag 24gaagaaa tccttagtcc tgtcttaact acttgagagg ctgagggaggaggatcactt 24cctagga atttgaggct ccagtgagct atgacagcac cacggtgctc tggtctggag 24gtgagac cttgtctcta aagaagagaa aagaaaagaa tgaatgaatg aacaaaaaga 24aaggaaa ggaaaagaag agagagagag agagaggaag aaaggaagga aggaaacaaa 2424ataaa ataataaataaataaaccca aatccaactt ctttacccta atcaacaagg 243aataat ctcatgccaa ctaagtctct gaacagctcc ttccattcta ttgccagatt 2436atctt tcagccacaa gaccttttta tcttcctttt accagccaaa cacaatccta 2442gaaca tgtgcacttt ttcttttctc tgacttgaat ctcctccacccattatataa 2448gctca aagaggcttt tcttgacaac ttagcgaaag tatttatccc agtcattctc 2454catta ttccaattta ttttctccat agtacatttc agcacataaa gatttcctta 246gtgctt gttgcctttc cccaacctcc taaaatgtca gcattccttg agggcagaga 2466tcatt cctgtatcatcagcacctaa gacagttcct ggaacatacc aagtacttaa 2472atttg tttattgact agctatgaca cattttactt atataatttc attttctcag 2478tgaac actttgaaat gtaattaatt actgattttt gcagtatttt ctaattattt 2484aaata tttactattt tggtcaacca gaattcttac attgttttagcacccagata 249ctaaaa atgcttacaa ttaacacaat tttatctagc aatatgtatt tatcactaga 2496tgcac tgaactcttc ttcattaata aaaagcaatc caggctgggt gcagtggttc 25cctgtaa tcctagcata gtggaaggcc gaggagggag gatcacttga taccaggaat 25agaccag cctggccaacatggcaaaac cccatctcta taaaaaacac aaaaattagc 25gtataat agcagacatc tatagtccca gctactcagg aggctgagag gtgggaggac 252tgaccc caggagattg aggttgcagt gagccgtgat tgtgtcactg cactccagcc 2526tacag aatgatacct catctaaaaa aaaaaaaaaa ttagccaggcatggtggcat 2532tgtag tcccagctac tcaggaggct aaggtgggag ggtcacctga gcctggaagg 2538actgc agtgagccct gggtagcccg cgccactgca ctccagccct gagtgacaga 2544agttt caaaaaaaca caaaaaacag aaaacaaaac aaacaaacaa aaaaacccaa 255ttgctg aaatgttaaatccattataa agaaaagtac aggggtgggc atggtggttc 2556tgtaa tcccagcact ttgggaggcc aaggtgggca gatcacttaa ggtcaggaat 2562aacag cctggctaac acagtgaaaa atgcaaaata caaaataagc cgggagtggt 2568atgcc tgtaatccca gctactcggg aggctgaggg gggagaatcgcttgaacctg 2574tggag gttgcagtca gccaagatcg aactccagcc tgggtaacag agactccatc 258aaaaaa aaagtaaaaa gtatatagtt gattctgcag ggacttaaaa aagtataaat 2586tttta acatcacaaa gctctgatat ctgcaggttt atgactaact actagctcac 2592tgaat acacgtatgtaaacaggctc tatacaatct acaatcccag actaagggga 2598ctgtc ctgtcactgt ggtctccaac ccttggccca tttctttcct cttgaccaca 26cttctca ggagttgctt gtttcctctt gatccactta tctttagccc actccaatct 26atcggtt ctcagtactc tccactaaaa ctgcttttat gaaggccatcaatgacgttc 26ctgccaa atccagcaga cacctcctgt tttctaattt tttttattgt tattttttaa 2622tgggt cttgctctgt cacccaggct ggaatgcagt gatgccatca tagctcactg 2628ttaac ctccctgagt tcaagagatc cttctacctc agctgggact acaggcatgc 2634tatgc ctggctaattactcaatctt taacatagct gataattccc tccttgaaac 264tcaact tttaagaaac cctgttattt tcctcctaca tttttagcca gttcttctat 2646tctcc ttatctgacc tctaaatgtt aagaacatta acaaagactg aacctagttt 2652tcccc ttactgtact gctcctgggc gatgtcaatc agtcccattgctttagatac 2658gttga aacactgaaa tcactggttt tttttgtttt tttttttttt tttttttttt 2664atgga gtttcgctct gttgcccagg ctggagtgca gtggtgcaat ctcggctcac 267agttcc acctcctggg ctcaagcaat tttcctgcct cagtctcccg agtactggga 2676ggtgt gtgccaccatacccagctaa tttttctatt ttagtagaga tggggtttca 2682tgtcc aggctggtct taaactcctg acctcaggtg atctgcccac cttggcctcc 2688gttgg gaaaagatat cccaatcttt ttcctatgat ttcttaattg atctacttga 2694ccact tggactttta ataggcatct caaacttaat gtgttcaaaataaacctcgt 27tttccct cccaaacctg tccctacctc cctcaataac taatattatc attcttatat 27tatattg aataaatgtt tgttccccca agtatttgtt gctataaatt tatgaagaat 27tttctca ctagttatta taattaaaat gtaatattta ttttctttaa aaactttact 27taggatt attattttttaaacagggac caacaataaa taacttctct acttgattaa 2724gggct tcctcttgtg ctccctcagg actatttctt tgtaaaaaca ataggctaaa 273tactgg tgtcaaagaa atcataatct cacaacttta taaatacagc atgtggcaag 2736ttccc atcttatata gtaataaaat tttcagctgt gccatggctaaaagtttacc 2742agttg gaattttaaa ttagaggtag tcatctttct ttctttttaa agaaatggag 2748ctatg ttgcccaggc tggagtgcag tggctatttg caggcatgac cacagcacgc 2754catcc tggcctcaag caattctcct gcctcagctt gccaagtagc tgggactaca 276cctgcc accacacccagcagaaatat ttagctttct gaatttctca agtgtgtgta 2766gagac tagtggggtc cttaaccaag attcacagga tttttagtga tttattaaat 2772ggatt tgtatctacc agcatgttct ttgaggtaca ggtatgtctt ttatatctcc 2778tagtt cattacaatg ctaaatacta agatgtgatg ctcacacactacagaatagc 2784aaatg aactacttat tctcataggg ctattataat taacaaattc ttgtatcacc 279cattat caacaacaac atgataggat ttccttttat cttgaagagt ctggaaaaag 2796cagag agatatttct gaggaacaaa ctggtaatga gggagctact gtgtccatta 28tactcct tctagaagctcaatacataa tgactaatct ctggaaaaaa gcaagtgtga 28tggaagg ctcttcttca aactatgcaa aatgaatcaa tcagcagtga acaaatttat 28ccaaaca aattcctaca aaaattacca tcatatgctg tcatgcatgt ctgccagtct 282atcata ttatttaaga aacaaacatt tattgaagat ttatcatgtgctcagcactg 2826gagga aataaagagc ataatatcta ttcttagaaa ataacattaa cacaaataga 2832agaaa ccataatgtt aaaaatatta catagtaaca cagaaagaca atgtataatt 2838tacgc actaaagcaa agataacata atttataaat tatgaggtac agaatagtta 2844tgaaa attaaaataatcaggaaaaa cttcatgaag atgagatctg ggctggatcc 285ggatag gcaggtggat catgtagaac aggggaaagg agttcctgat cggggataca 2856tgtaa aaactcggag acaggactga gcgtgaaatg ttaatgggac agtaaagaaa 2862ctctg cagcggggga aaaaacagaa taatgggaaa ctgcatggttaaaaggtttg 2868aagat agtgcttgga cacaaaagat cttaaagttg agtcaaaaga gtacaatgaa 2874tagaa atagaagata aaacacaatt aggccgggtg cagcggctca tgcctgtaat 288gcactt tgggaggcca aggtgggtag atcacttgag gtcaagagtt tgagaccagc 2886caaca tggtgaaaccccgtctctac taaaaataca gaaattagcc gtgaatgatg 2892tgcct gtagtcccag ctatttggga ggctgaggca ggagactcgc ttgaatctgg 2898ggagg ttgcagtgag ccgacatcgc gccactgcac tccagcctgg gtgacagagc 29cctctgt ttaaaaaaaa acggtaaaaa taaataacat ttactattgttttctgatga 29atatggc ctctaattgt aaagctgaat gcctagttta ccactttttt tttttttttg 29cggagtc ttgctcttgt tgcccaggct ggagggcaat ggcacgatct tggctcacca 2922tctgt ctcccaggtt taagcgattc tccagcctca gcctcccgag tagctgggat 2928gcatg tgccatcatgctcagctaat tttgtatttt tagtagagat ggggtttctc 2934tggtc aggctggtct caaactccca acctcaggtg atccacccgc ctcagcctcc 294gggctg ggattacagg cgtgaaccac cgcgcccggc ctatcattct tattttatgc 2946gaaac taaggctcaa caagattaaa gctgtctagg gtcacaaagattgtaagtgg 2952ctaga attcaaaatg agacctgctt gactcctaag cctgtaccat ttctactata 2958agtga agtagatggg ttgaagaaat atttaggagg tgaaatttca aaagtgtaca 2964aagag aagacatata tggaaaccta aattttcaca cagtaaagtg tcaataataa 297ataatg ccaaaatgacagaggctgtg catggtggct catgcctgta atcccagcac 2976gaggc tgaggcagga agatcacttg agcccaggag tttgacacca acctggccaa 2982cgaaa ccccatctct actaaaaata caaaaaatta gctggtaatg gtggtacaca 2988aatcc cagctactca ggaggctgag gcattagagt cacttgaacctgggaggcag 2994gccat gagccaagat tgtgccactg cactctagcc tgggcaacag agtgagactc 3tctcaaaa aaaaaaaaag gaagactcga gggctagaac cctgaaattg ggaatgaaca 3actggctg aaaatgtttc ttgcacctga
taaaaatctt gaagaagaat gctttaaata 3taagaaag gagagagaga ggtgggcagt gagaggagac caccctaagt aatcagagat 3cttacgtt ggttactcag gctggtctct gaatctgatt ataaatgaaa tagagattac 3aaaacaaa gggctgtaag gtagcactgt ccagcagcac tttctatgatggaaatcttc 3tatctgca ctgtccaata aggtgtagct gctagcacat gtggccactg agtacttaga 3atagctac gacaaccgag aggctgaatt ttaaatttaa tttaatgaat tcaaacaaat 3atttttaa tacagcactt taaattttat ttttaaattt taatctatta tttatttaga 3ctgggtta tgagactggctaatttttgt atttttggta gagacggcgt ttcaccatgt 3cccaagtt agtctcaaac tcccgggctc aagtgatcca cctgccttgg cctccccgca 3gtgctgag aatacaggtg tgagtcacca cgcccggcct aaacttaaat ttaaatagcc 3gtgcgggt agtggctacc atactgcaca tgcaactgta agatgtagaagtcagatgtg 3caaagaaa tgacaagccg ttcaatgctg ttagagaatg aaattcaagg ttccaatgat 3gaacttgt gtcccctcaa attcgtatgt tgaaatctta atcctcaatg caacagtatt 3gaatttgg ggctttagga ggtaatttgg ttttgagggt ggagccctca tgaataggat 3gcacctga ggtagcctctttgacccttc caccatgtga ggacacacca cgaaggcacc 3gttggaag cagagagtga gcactcccaa gacactgaat ctgccacatc ttgattttgg 3ttctcagc ctacagaact gtgagcaata aatatctgct gtttataaat tatccagtgt 3agtatttt gttatagcag cctgaataga ctaagacaaa ggtggactaaggcaggataa 3ggttagaa aaggaggcag ggcctttttt tttttttttt tttttttgag acaaagcctc 3tctcaccc aggctggagt gcaatggcat gatcttggct cactgcaacc tccacctcca 3gttcaagc aattctcctg tctcagcctc ccaagtagct gggattacag gtgtgcacca 3acacccag ctaatcttttgtatttttag tagagacggg gtttcactat gttggccagg 3agtcttga actcttgacc ttaaatgatc cacccgcctc ggcctcccaa agtgctggga 3acaggtgt gaaccatcgc gcctggccga ggcacagtgt ttttacagag aagcctgttt 3ggtttaat catataaaat gtatgatatc cagtaagttt tgatataaaaaagaaacacc 3gcgatttt atataatata ttgtgctaag gaattttaag cactctacat tctgctctct 3gctctgta aagagcacca gggatttttt tttttttttt ctttttgaac agggtcttgc 3tgtcagcc aggctggagt gcagtggcac aatcttggct cactgcaacc tctgcctctc 3gctcagcg attctcccacctcagcctcc tgagtggttg ggaccacagg cgcatgccac 3catctggc taattttttg tagagatggg gttttgccat gttgcccagg ctggtcttta 3tcctgggc tcaagcgatc ctcccacctt ggcctaccac gcatgcctgg ccacaacagg 3tttttaaa tgtaagacta cctagtcaac tcttattcta tattaacaatatagacaaga 3taacctct aagtaatctc tatttcattt ataatcagat tcagaggttc tcttatgctt 32aatattg tcctactgtg ggtagcgcaa taactaaggt aatctgaaag accagttata 32tatacta tagttaaatg catttcaact gcatgggaga aagcaactgt gttctttcct 32aatttta acagaaggaaaattgtcaaa attagcttat ttagaatgtc ctatcagaga 3222tttga ttaaaatata tttttaatca ataaaatatt tctctttggt caatacttgt 3228tagaa taatatctag ccacaaaatt aaaaaaaaaa cattttcccc tatattacat 3234gatct tcttgaattt ctgttatcta ggtgctttta aaagtcatatttctgataat 324aatcac agctcctttt ctttggcata tttagttact gtattaagaa aatgtacaac 3246attta gaatgggtaa ttattatatt ctctttattc ttatattgaa aatgacatga 3252accag tcttcccagg taatataatt taagttaaag aacatctaca tactacaacc 3258ccatt cccctatgttatgtttggaa aaacatagaa gtatctttag tagtactctt 3264ttatc ccaggttcag catattggta ttttatttcc aggtttaagt tacagtattt 327cacccc aagtttaata aactattccc tgcagaaacc tgacaagtga agttgtggct 3276tatgt tagtcttcag ataaaatgaa ttgtttaaga atttgctaaagatctcaaag 3282ttctt aaatctaaag aaagtcagga acaaagccac aaccaggacc atagcatcag 3288ggaaa gttgctttgt cttcaaactt aaaaaacatt ttccatttta aaataatttt 3294ttacc tgtgatactg ttgaaaatta tgaaaaaaca gataatttaa aatttagtgc 33tttttaa aaaaaaaaaaaaagcgaatc cctgggacac ttcatatagt gcaaaacaac 33tcaagaa ttcaagcatt gaaagaaata atctcttatc ccccagtctc tgaaagggat 33ctttact actgttccca tctttatgtc catatgtacc taaggcttat ctcccactta 33gtgagaa actattcagt atggcttagt catttttaat gcaagagaataggtaaaaat 3324gcacc agccagagtt ttttctttgc agatagatgt gactcttaca ggagcagcag 333ttccca ctttgggcgg aaagcagcat ttaggtattc cccctccagt gcagttacag 3336ccccc cgtagaagct gctcctgtcc tctgtggcat gtcagcctct gattatcttt 3342aacaa tatggcatattaagtctctt ttatgccctt ctttgtattc ccaggtacca 3348atgtc aggataacaa gaatttggta atgtttgttg aataaattta gcagaagttg 3354aaaat cctgtttcta cagaaagata ccactggctt ttggggagcc cgagttcatg 336aactaa agaaagccac aaaagttcac ctcaatgcca agacatttcttgatttttga 3366cagtt gtcgaaccac ccatctatag aaacttgaaa gactaaaaac tatcttactc 3372atttt ctaggaagtt gattctacaa cacattttgg ttttccaatt tggcttctaa 3378atttc aaagtttctg tggcctaaat tttgttttac attgatcctt tgaatggact 3384ttcca cattttagaacatttaaaaa gatatctaca acccgagtct aatcataaaa 339tcagac agatccaaaa tgtggaacat tccactaaaa aaggagtggg gagaggtctt 3396ttcca aaaatatcaa tgccataaaa gacaaagacg gctatggaaa tgttacagat 34aggagac taaagttaaa tgcaagaaag gaaaaaatgg catataggacagtattgaat 34ctgacaa aactggatta caatagtaga gtatcaatgt taaacttgct gaagttgcta 34gtatttc ttaggaatta ttcacctaag aatttaggca cacagatatg atgtatgtaa 342ccctta aatggcttag aaaaaaatgt gtgtatattc atttacatac gtatctacac 3426tgtat tagcggaagagagcaaggca cacatgtgca taagtgataa agcaaatgag 3432atctt tatttttaaa tttaattttg taagtttcag ctttttaaaa ttttagattc 3438ataca cgtgcagtta ttacttgggt atattgtgtg aagctgaggt ttggacctct 3444tcctg ttgccacaac agtgaacaca gtacccagca cgcagtttttcagcccttgc 345tccctc ccgctctccc tccttgcttt tggagttccc agtgtctact gttcccatct 3456tccat gtgtacccaa gacttatctc ccacttacaa gtgagagcat gcagtattta 3462cttgt tctgcgttag ttccgttagg ataattgcct ccagttacat tcatgtcact 3468ggatt tgatttcattctttttaatg gctgtgtagt attccatgtt gtataggtaa 3474tttct ttatccactc atcaattaat gggcacttac attgatttca tgtgtttgct 348tgaacg gtgctgcaat gaacatctga gcgcaggtgt ctttctggca gaatgattta 3486ctgtg ggtatatacc cagtaatggg attgctagct cagataagtatttctatttt 3492gctct ccacaggggt agaactaatt tgcattccca ccaacggcgt gtaagtgttc 3498tctcc acggcctcgc caacatacgt tcttttctga tttttaatag tagccatttt 35ctggtaa gagatggtgt ctcattgtag tttggctttg catccaaatg agacaaaatc 35atgacag gtgaatctaggtaaaaggca tacagacgtt ctttgtgttg tttttttaac 35catttga agttattttc aaatgaaaaa taaaagcaag caaaaaaagg tcattcttca 3522taaac tcttcaaaga ttaccacccc cttcaacagt ttttcctggt tctagtgagt 3528cccat ttgtttagat ctttgttgaa atgtagtctc agataaaaaattgtattttt 3534tttta catatttcaa acaatctaaa ttctttttaa atgaaactca ttaaaaatac 354tttgtt tctaaataaa atggtagagg taatttgcac ctttccaaac agaagcaata 3546aaccc agatgttcta gccacgatcc aagtcaacca cattcaatct aagaagtaat 3552gctgt aacgacttctgtaaggccta caaaaatgag ttcagacaca agctctgctc 3558aaatc tagtggcaga tgatatatac aatgatctga gaaaaaggca gaatcaacaa 3564gtatt tttatctatt gctgcgtagc atatttcctt aactttagta gcttgaaaca 357acattt attatttcat aaagtttctg tggtcagaaa tccaggagcagcttaactgg 3576tctgg ctcagctgta gacaagatgt cggctgggac ggccatcctt tgagggctct 3582ctttg agggctgcac gatccaattg caaggtggct cactcacata ctaggcaagt 3588ctggg tgctgggagg agaccttagt ttcttatcac atggacctct ccacagggct 3594aatgt cctcatgaccttccccatag tgagtattcc aagacaggaa agtggaagcc 36atgtctt tcatgaccta gcctcaaaag tgacatactg tcatttacac aatattctac 36ctgtaca agttaatcct atttagtctg ggaggggact gcataagggc atgagtaaca 36ggcaaga atccttgggg gccatcttgg aagctggcta cacagaagagaaaacaccag 36agtgcga agaaggtgca attaaactca attccttggt atgccaatgg taagaaatat 3624gatct ctggggtgta acctttttaa tttagttctt cactgaataa tctggccagt 363gtaata caaaatacgg cactctgaca atattctctc cctttataat caattacaca 3636atata tataaagaaagacttacaaa gtcacaagta attgtttggt attattttta 3642acata ctagggccct acaattagca ttcacaaaca tcactccatg ttggccagat 3648tgtct ttatagtggt ttaccatacg cgccttagca tgaagttaca tgtggtttcc 3654catca gatgctccaa atgcaaaaaa tgtctcacca cagtcacagaatcatggaat 366aagtta cctggggttt ctgaaaatct catgggaaca actcacgaga attaaggctt 3666agtga tttatcaaag aacaaaacca gcaagacttg agtttagaac tcgcagcaga 3672gacta gaacctgttg aaataggcaa tgtagaaacc cagactaagg cacattctct 3678tttac tatgcaagtatgcttagata ctccttagca aacagcaggc cttgagtaaa 3684tcaga actgaataca caaaggatac agaacggaat acactaacaa tagtgcatga 369ctcatt tctgtaatag aaatgaatta attctgatcc atctataatt tattattgct 3696attaa cggaaggcat aggaaagatg actggaatag tgtaactagtacaaacaagt 37acacttg actgaacctc attacactgc aattgcatat tatatagtat gtaggtgaac 37tactggg ttagtcagtg gacctacatt tgaatactgg ttctgctcct agacagctgt 37atttgaa tgacttcttt atactttcat agtttctctg ttcttctctg taaaacaaag 372agaaga tattatgggttagattatgc cccttacaaa agatgctgaa gtcctaaact 3726acctg tgaatgtgac tttatttgga aatagggtct ttgcaagtga taaagaagag 3732ggagt gacctaatcc aatacgacca gtgtccttat aaaaaaaagg aaatttggat 3738tacac acaaacaagg agaatatcaa atgaacatga aggcagagaccggggcggta 3744acaag ccaagggaca ccaaagattt tcagcaaatc accagaagtt aggaagagtc 375gacagg ttctcacagt cctcagaaga aacccaccat gtcaatacat cattttggac 3756gtctt cagaaccgta agaaaataaa tttttgttgt tcaagctacc caatttgtgg 3762tgtta cagcagtcctagcaaactaa tacaaatgag ctcttaacac tggtctaaaa 3768taatc ctatgaaatg ctacaaatgt ttgggaagat ttctcatact caactgttta 3774tacca caagcctgtc agttgaagat acaaacagac cctctataat cctctatact 378tgcaag gaacagcaca ctttttctgc aaaaggtcag atagtaaacattttaggctt 3786gccaa acaaggtttc tgttacattt tttttttata actccttaaa aatgtaaaaa 3792ctcat cccaacggac tacaggaaca gacctcaggt cacatttgac tcatagcctg 3798tggtg tgtagggtta acaagcctcc tttccctggg ctcctttttc tttcagcatt 38agccaaa ggaaactatctttttcaaat cattttctct cctaggtggg acatcttaca 38gcccagg catgcttccg atagccttag agtagctgtc ccttcctcag aattactgtc 38ttggcta gaagttagca actttttaca tttttccttc aattcctttc cattaagaag 3822atgca ccggcaaatt acttgtgact atcaatgaca tactctcagaagcaccagta 3828gtgtt gtttctaaac ccattctaat agacacatac cccaaggtta tgctgtttgt 3834cacaa aatgacttac atctagagat ttaaataatt aatgtacttt tcataactac 384tacagt agatctgata atggcagagc taagcacata tacagaaagt agggcaaggg 3846gactc attttaaagcaatgttacaa gatcgtcact gttgcttttc atttttctaa 3852gccac tgctgttttc tcactaaagg aaatgtttta tgtaaagtga ataacagtac 3858ataaa ataagtgctc aataaatgtt aaggccttct ctccctcttc aactggcctc 3864ttttc acaaagtgaa atagaaaaac aacatggaag ataatcctgttgcttaggaa 387aactaa agcttgctag acaaaataca cctgaaaata taggaagtga gctatagctg 3876tatgc atgtatgttg gaacaggaca agatagtgta gggtggggtg aagaggacag 3882tggaa ggaaaggggc tacagccttg gtggcaaaat aaaggataag acgactcttt 3888tggtc tatttcaaatgctgggttgt gaaacttaat ttgattactt catgagaaac 3894ctata atccatccct gatttttcta caacaaaaat ttattattta ttttatgttt 39tgtagat cttttatata tatacatgta cacacgtata tgtatatatt atatatgcat 39catatat atgtgtatat acatatataa tatattgtgt gtgtatgtgtgtgtatatat 39tttttta aaggaatggg gtctcactat gttgcccagg ctggacttga actcctgggc 39agcaatc ctccacctca gcctcccaag tagcaaccaa cagttttagt tttgaaaaaa 3924aatat taaacaccca tgtgtaaggg ttggtactgg gccctgtgtt agtttgcatg 393gtcgta acgtaacactacaggccggg cacaacggct cacgcctgta atcccagtac 3936gaggc caaggtgggc ggatcacctg aggtcaggag tttgagacca gtctgaccaa 3942agaaa ccccgtctct actaaaaata caaaattagc catgtgtggt ggctcatgcc 3948tccca gctacttggg agactgaggc aggagaatcg cttgaacctgggaggcggag 3954gatga gctgagatca ggccattgta ctccagcctg ggcaacaaga gcaaaactct 396caaaaa caaaaaaaca aaaacaaaaa aaccctgata acactacaga ctgggtagct 3966aacag aaatttattt tctcacagtt ctggaggctg gaaatctaag ataaagttgt 3972ggttt ggtttctgaggcctctctcc ttaacttgca gatggctgct ttcttgaaat 3978cacat agctgtccct ctgtctgttt ctggtgtctc cccacgtatc caaatttcct 3984tataa agatactagt catattggat tagggtccac cataaagacc tcatttaaac 399tcacct ttttacggcc ctgtgtccaa atacagtcac attccgagttccaggggatt 3996ttcaa cctatgaatt gggggtgggg cacaattcag cccgtaacag gcctagacct 4atttgtca acactacagt tagatttata gtatagtaac tgcatctgtg ctcatctaaa 4tcataccc aaatgaaata atatagcatg atgatctgaa tttattaaag gcaatttttc 4atagaaac ccaaatctataaattatata caaactgtgg taagttactc gataccttgc 4ggactcat ctatggtggt agatagacca caaagagtac cactgaaaga tccctttcct 4tcacagtt tcctcactgg cttgccacaa aacctaaaat tcttctattc tttcattggc 4tttatttc ccctgaaaat gtaaataatc tctggcagag caatctattaagtgatcatc 4ccactaac accttagggt agaacagctc agatcacagt cttaaaataa attccatcag 4tgaaattt tctttattac tgctccgcta ctggaatgtt agatcactgt ctgctttaat 4taattctg gtgtaggtca ttcaaatttt gtttaagata ataagacaaa tagcaggtat 4aaacattc cgtcatctaataaagcaacc cgagaacagt aagaagaacg tgatgaaatt 4catttttg agtacctgct aggaatcaag tattctgcta gatattttag aaatcatctc 4ttcaatcc taaaaattat tctgtataat agtataggtt gagtattcct aatccaaaaa 4tgaagctt tttttttcct gagacggagt tttgctcttg ttgaccaggctggagtgcaa 4gcgcaatc ctgactcact gcaacctccg cctcctgggt tcaagtgatt agggatactc 4ctggctaa atataatgca aatatttcaa aatctgaaaa aacccaaatc tgaaacactt 4ggtcccaa acatttcagg caagggacac tcaagttgta ttaatcccat tttacagaag 4gaaacagg ctcagataaatgaacatctc agagcttgtt gatagcaaag gagagattga 4ctgtcagg cctctgatcc caagccaagc catcacttcc cctgtgactt gcatgtatac 4ccagatgg cctgaagtaa ctgaagatcc acaaaagaag taaaaataac cttaactaat 4cattctac cactgtgatt tgtttctgcc ccaccctcac tgatcaatgtactttgtaat 4ccgccacc cttaagaagg ttctttataa tttcccccac ccttaagaag gttctttgta 4tctcccca cccttgagaa tgtaatttgt gagatccacc gctgcccgca aaacattgct 4taacttca ccacctatcc caaaacctat aagaagtaat gataatccac caccctttgc 4actctctt ttctgactcagcccgcctgc acccaggtga aataaatagc catgttgctc 4acaaagcc tgtttggtgt ctcttcacat ggacacgcat gaaagaaacc ctacctggtt 4gtgtctta cctgttgggg gcctgtggtc aaactactag tacggagttt tagtgtcctc 4tttaaaaa tgagggttgt ggccgggcgc ggtggctcac gcctgtaatcccagcacttt 4gaggccga ggcgggcgga tcacgaggtc aagagatcga gaccatcccg gctaaaacgg 4aaaccccg tctctactaa aaatacaaaa aaattagccg ggcgtagtgg cgggcgcctg 4gtcccagc tacttgggag gctgaggcag gagaatggcg tgaacccggg aggcggagct 4cagtgagc cgagatcccgccactgcact ccagcctggg cgacagagcg agactccgtc 4aaaaaaaa aaaaaaaaaa aaaaaaaaaa aaaaaaaaaa aaaaatgagg gttgtaaggt 4ctacctac tttttatagc attgtagtga agttgaaatg aattaatcca catatattat 42gtggtag aatgcagcag aactgatgat gtatgacttc taagactagtccttaagaga 42gcagttt ttgcttttgc cctcttggaa cactcctgtt gccatgttaa gaaaaactct 42gagacta tgaaggaaga gagcatactc ggggcagggg ggtgaacagg acgtgcacat 42cgagcgt acaagccagg tgacaccagt accacagcct cagacatgtc accggggata 4224accac agcctcagacatgtcaccgg ggacaccagc accacagcct cagacatgtc 423gggaca ccagcaccac ggcctcagac atgtcaccca gggacaccag caccagcacc 4236ctcag acatgtcatc ggggacacca gccccatggt ctcagacatg tccctgaggc 4242tagac ccttcaaccc cagcccagct gctaactgac tacagccacatgaacagaac 4248gagac cagaggaaac ttccagtcac ctaccagatc atgacaaata ataaacgatg 4254taaac cacaaagatt tggagcagca tttgttacac aaaattagac aactattaca 426gactaa aaacatgttc atttacaata ctaaattaga agtgtaagaa tgggagaaaa 4266atact ttaaaagtcattttttcctc caaaaacttc caactttgaa aaactgattt 4272atgca taaaaattaa aataacctta gaatttatat gagtagcata gccagctggc 4278tatct gttgtactca acacttcaat aatcactgat gttttagaac tcttcagatt 4284ctctt gcccttgctt tagtctggtt taagctaaat aattgttcttcctcaagaac 429gacctt acctcgtttt gttttccttg tctgagagaa acacattagc agtctcccat 4296ttttc cttttcctgt cacccaggac agagggcagt ggtgtgatca cagctctgca 43cgacttc cccaggttca ggtgatcctc ccacctcagc ctcccaagga gctgggacca 43gcacatg ccaccacgtccagcttaatt ttgtattttt ttggtagaga tcaggttttg 43tattgcc ccaagctgat cttgaattcc tgggctgaag caatctgcct gccctggcct 432aagtgt taggattaca ggtataagcc accgtgcagc cttatatttt gttttaaatt 4326ctgta tttttctctc tggcaaattg tttagggagt ttctttagtttatcagacta 4332caagg ctttccttcc aattttgaca tgtaaacagt ccctcatttc tgcttatcta 4338tattc ccaaatctgt gtttacagtc tagctgtctc tcctgagatt aagacttgtt 4344aacta cctgacggca gaatctcctc ttggaagtat caaggaggca gttcaaaact 435tgggca ttggctccactccttctcct tctctttact attaataccc tttctctcct 4356atgac cacactaagt cttatttagg catcgtttct tctgggagac ctttgtagaa 4362gaggt tatgttaaca tgctaaggtt ttcttgacat tctcagattg ggttaggtga 4368tagca acttatcttt ttactaaaaa gtcatccctc agtatctgtggggaattggt 4374gactc cctaaggata tcaaaatctg catgagcagc ccaggtgaga ccagcagaag 438ttacag tcacctacag gatcatgaca aataataaat catgtttaag ccacaaagtc 4386cataa aatggtatag tatttgcata taacctacac atcttcctgt atcctttaaa 4392tctag tttataatacctcatacgat gaaaatacta cgtaaatagt tgttatactg 4398tttag ggaataatga caaggaaaaa agtccacgcg tgttcagaat agatgctttt 44tctcgtc taatattatg gatccacagt tggttgaatc cacagatgtg gaatccatgg 44ccaagga acgactgtat gcattttgac aattatactt ctcatcttaccatgcattca 44aacagaa catgtaaagc ggtgataatg ctgtgatgaa aaataaagca ggggaagagg 4422tccat ctagtggaaa cgatgccctt ttcaatctgc acaaagagaa aaagctgctc 4428gttgg ggggtgggtg ggtcaggtat gtaaattggt caggaaggga tctgtaggca 4434agatt tgacgctaatgagatgggaa gccacaggaa ggttgtgaag aaaagacaag 444gatctg attcatgttt tgatctgata cactggttgc tagatggaga ataagctgca 4446gtgag aggaagcaga aacaatagga gggtaatgct ataatccagt ggtccataat 4452atccc cccaaggaac agttcggcaa tgtctggtga catttctggctgtcacaact 4458ggcgg agtgctactt gcatctagca ggtagaagct agggatgcta ctaaacatcc 4464tgcac aagacagccc ttcccccaac attgctggcc caaaacgttg atagtaccaa 447gagaaa ctctgttata atctgtccta gaatgtagct tggattgaga tggcagtggt 4476ctgga gaagtgcttagcttcccaat gtttttttgt ttgtttgttt ttgagacgga 4482gctct gtcgcccggg ctggagtgca gtggcgtgat ctcggctcac tgcaagctct 4488ctggg ttcacgccat tctcccacct cagcctcccg agtagctggg actacgggcg 4494cacca cacccagcta atttttttgt atttttagta cagacagggtttcaccatgt 45ccaggat ggtctccatc tcctgatccc gtgatccacc cacctcggcc tcccaaagtg 45ggattgc aggcgtgagc caccgcgccc ggcctgaatg tttttaaagt actggtgacc 45ttcgctg agggattaaa tgtaaggtat
gaggggaaaa taggaatcag acaccagggt 45ctgcctg agcaatgaga agaacgacgt tcctcatacg gagatgagga agaatgtgga 4524aggta aatagcatgt gcttgctttg tttggggctg tgcagaagag actgatggga 453cgtgct cagttctgga tatattaaac ttggaatgcc tatttggcaccaagtgaatg 4536ggtag gcagatggat aaatgagtct gaagttcagg ggagaggctg gggtggcaat 4542cttgg gagtctccac atctgaatag tatttaaagc tatacaacag gataaggtga 4548gaact aaacacaaat tgagacgaga tccgagccca gaggcactcc gatgtttaaa 4554ggagg aaccatcaaaagatactaag gagaagccaa gaagtaggag aactgagagt 456gagaat cattatactc atttgatcga ctgcaacaaa tgctgcttag aggtcaagca 4566aggac taagcaagga ccaccaggtc tggcaacatg gaggccaatg ccgacgtgga 4572gagtt ttggtgggaa gacaggaata aaagtctcac aggtctgaattcaagagaga 4578gcaga agaagggtag aggtggtagc cataaacaat gatacattct cttgaggcct 4584tgcaa agctcagtga agaaacatgg ttccagagag ggattttttt ttctctcatt 459atatgc aaacatataa aaaagctgaa agaattgttt gacaaccacc cttattctta 4596gattc aacatttaatgccatatgtt ttccctgtat gtactgtgta ttgtttgagg 46acttccc ctctaaatat acctcggatg tatctcctaa aataagtcca ttctcctaca 46ccatagt aaccatgaac acacctagga aaattaaaaa tatattctca aatatattat 46gctgggt atattacaat ttccccaata tgtgatttgc aaaccaggatcaagtcaaag 462tgcaca gcatttggtt gtcatgtgtc tttggtctct attaataatg atgactgttt 4626gacct gtcctataga ataaatttga ctgattatgt catgccattg aacttgtttt 4632tctag aaggatagtt ttttagggta gtgaatacat ttattactct tggcacaata 4638acatt tcccaatttccttatatctc tgccctttca ttttcagaaa atcaattatt 4644atttg tttttcattt atcatcactt attagctctg aagactcaac tgagcaactt 465ggttta tataccctat attcagaaaa aaactactac catctctcat ttaccctaag 4656atagg agagcatgtc ttaaagctga tcaataacca aaccaaacattttattgatc 4662acatt tggaaagcaa aatgaatttc ctaaaatttc ttccctgatt agcaaaatag 4668ccgaa cacttgaggg tgaaagttgt tgtcaaatat gcctacatga ctggaaatta 4674tccaa atgagttcac tgggtctgat aataatatgc tctacatgct tatgtctatg 468aaacag cttacatctggatgagaaaa ttgattatac aaatatttgg gcttctacaa 4686cactc atctgtaagt acttaaagca acttaaaatg caaactgacc taacaatgct 4692ttaga attccaaaga atgtttaggc attgtcaggt tatgttaaaa catcttctgc 4698tcttc aagtgattta tcttttctgt tgtgttgaat agctatagaagacaaatgaa 47tgcactc ctgaattcaa tgaacatttc aagtttcctc acttacactg taagattacg 47catattt taagaaataa attataatca ttttatttca cttattgaac ttcttttaag 47tggcatt agaattttaa tcaaagcact gccacttgct tacagtgatg gtttttaggc 4722gggcc tatggactatttcaatgacc ttcactagcc atctagtcca ccttatccta 4728tacca ctgcaaaaga aaccctcact tgaataaatc agtagatggg catgaggcac 4734aggag actataatta ttaactcata ctaaaatcaa aattgtagct attatcactc 474ggtttg gctctgtgtc tccacccaaa tctcatcttg aattgtaatccccacgtgtc 4746agaag cctggtgcga aaggactgga tcatgggggc ggccttcccc cttgctgttc 4752aaaga gttctccgat ggtttaaacg catgggactt cctcctactt gctcgctctc 4758ccacc atgtaagatg tgccttgctt cccctttgcc ttctgccatg attttaagtt 4764aggcc tccccagccatgcagaaatg tgagtcaatt aaacctcttt tctttgtaaa 477ccagtc tcaggtagtt ctttacagca gtgtgaaaat agactaatac aatcacctta 4776agtct gtctataaat cacctgaact ttcacagact atctagaaga acatgtaacc 4782agttc ttgatcatgc tatataaatt actgatacag aaatagagctagacaggaag 4788ggtag tagagaatca tcctctggac atattctcac agcctaatct ctagctagca 4794tataa tatatataaa aatacaatta tttcacaaaa ttaccatgaa acgattttat 48gatatta gacattactg aattacttgt tctgtgaggt atacagtgaa attaacatgt 48aaaattg tggtagccggcccccaagat ggcctccaat gaatccttca cctcttggta 48atacctt tgtgtaggta ggtctgtgta acccatagaa tacagcacag tgacagtagg 48cttccga ggttaggttg tgaaagacac tgtggtttct gcctctctct cagatcacgt 4824ggggg aaaagccagg tgtcattttg tgaagacact caagcagcctttagatgact 483ccacat aagaggctcc gaactggagc cactcagcta aaccactccc agattcctga 4836tatca tttcatacac aatgtatgaa atgacaaatg tctgttgttt taagctgttt 4842ataat ttgttacata acaaaatata actaatacaa taatacatac tgatttaact 4848tgtaa cttcataacttatttaggta ctaaaaatca cagcaacccg atgcaaagta 4854aaaaa aatccattaa tacctattga gtactgttga gggcatgagg aaagctcttt 486ctccac ataaaacttc cttaccgtaa tattcatggc tgacctctac tcttaactcc 4866aggat aggaggggct aactgatctg acagcaagtt tgggagaaaaaattctgagg 4872ccaac ttcctctctt ctttccattt gggatttggc tgactgaaga gggtcatttg 4878gcctg ctctcttaca cagtaaatgt agtgggacaa gctctattct tgttgataga 4884tcgaa ttttaaatct gcctagttct ttgcagctcg ttgttgctcc aaatctcagc 489ttttga aacaacttttttcagtaaac ttaatttcaa tcttcatgtg atttaactgg 4896aacac aggcagataa aaaaggtggg gcattactta tcaacctcta aactaagttt 49tttgtgc cctcatggag tttatagtat atttgaggtt taaactaaaa cacctggttt 49acagaaa ctataaaaaa cacgattaat aggtgaggcc gggcgcggcggctcacgcct 49atcccag cacttgggga ggccaaggcg ggtggatcac gaggtcagga gatcaagacc 492tggcta acacggtgtg aaaccccgtc tctactaaaa atacaaaaaa ttagcccggc 4926ggtgg gagcctgtag tcccagctac tcaggacgct gaggcaggag aatggcgtga 4932gaagg cggagcttgcagtgagccat tgcgccactg cactccagcc tgggtgacag 4938gactc cgtctcaaaa aaacaaacaa acaaaaaaca aataggtgaa aggccgtgat 4944gtaag cgtaagaaaa tctgagggag aaaaaaatat agatgcccag gccccatgcc 495tcatgg aatcatgcat gaaacccaag cagctgcagt tttaacaagttcccaatata 4956gaccc ctgaacaatg caggtttgaa ctgcctgggt ccacttataa aatggatttg 4962tttca ataaaagtta caccgagtgt gcctgcctct cctccctccc tccctacatg 4968gctct taagcctctg ccatgaggct taagacagca agaacaaccc gtcctgttta 4974atagt tttggggggtgcaggtggtt tttggttaca tggataagtt ctttagtggt 498tctgag attttagtgc aactgtcacc tgagcagtgt acactgtatc caacatgtag 4986taacc cccatccaac cttcttcccc aacccgaatc cccaaagtcc actgtatgat 4992tgcct ctgtgttttt atagcttagc tcccactttt aagtgagaacataccatttt 4998tccca ttcctgagct acttcactta gaatactggc ctccagctcc atccaaattg 5gcaaaaga tattatttcg ttcctttgta tggatgaata gtattccacg atgtacataa 5attttctt tatccactca gctcctcttc agtctactca atgtgaaggt gacaaggacg 5gatcttta tgatgatccatttccactta atgattagta aatatactta cttttcctta 5attttctt agtaactttt tttctctaac ttactttatt gtaagaatac agtatataac 5atatgaca tacaaaatac gttagtcaac aatatatgct atcagtaaac ttccagtcat 5gtgggcta ttagcagcta cgttttttgg gcagtcaaaa gcatggggaaggagagggtg 5ccctaacc cctgtgttgc tcaagggtca attgtaataa tacccattta agaatccatg 5atatatgg taagtgcaac aactctagaa gagagtgcta ggagttggaa aaggaaagag 5aacagaat ttaaagcaat ctgtaaagga catgcagggt ttagatgagg tggaagggtg 5ggaaaacc aacatctgctgtgagggcat attaactgcc agacattgtt ctatgtctta 5tcatttaa gagaatttca tttcacacat ggaaaaactg aagcccagag aggttaaata 5ttgcctga ggccaaaatt agttaaataa cagaagtggg attagtagat gttttcattt 5tcagtgaa actgagcctc agggaggtta aatattttgt atgaagtaacaaaactgaga 5aatatatg gccaagttta aatgagatct gtaaatctaa tgcctacact aaaacaaaaa 5aaaaagtg ggaagaaaag gtctatattg cttagcaaaa cagaggtagg gaagcaaaaa 5aacttaca aaatcagatt agaccaccaa aaaacagtcc ccattttaac ttatgtggtg 5aaccatat attaaagaccaccagtggct taaaaatctt tttaaaaaat gaatctgttt 5attattca ttagttttta tctaatgaat aatgtatctt aactgataca tttactaaac 5ttaccagc tccaattagc actcagttac aattcaatca ttaaactgac cctcaattta 5tgtcaacc tagtcaaaac agttaagtga ttttacggtc atcctcagttgcagaagtat 5tgtttatg gctggagtca ttttattttt aactaacatt ttttaaaaag attgctttgt 5caatgtgt tatgagtcct ttgtggtaaa tactgctttt tttttgagac gcagtctcgc 5tattgccc aggctggagt gcagtggtgc gatcttggat ctgaggctcc tgcctcagcc 5ctgagtag ctgggactacaggcatgcgc caacgtgccc agctaatttt ttgttttttt 5tagagatg gggtttcacc atgctggcca ggctggtctc gaactcctga cctcgtgatc 5cccacctc ggccttccaa agtgctggga ttacagctat tttaaggact ttttaaaaag 5aagctaaa catttattca tccctattcc tcatctatag ggacttgtgctctatttttc 5tgaagact gaagtaaaaa ttcacctttg tgagggtctt cctataatta aaattaatca 5ttttcctc catagcttct acaaaacatt gcctgtacaa ctctatttag cacttatttc 5cccgcctt gtatgaaaac tatttgttta caaacgtttc tacttctctt taggaataag 5ctatgcat tattcactgttgtattctcc ctgcatttat ggcagtcctt tgcacattaa 5acaagctt tttggctctg tgcatctctt catctggctg ttcatctgta ccctttaaaa 5tcctttat taaaaaaaca gtaaatgtaa aaaaaaaaaa aagccattga tgaaaaagtt 52agctttc tcaataagaa aagagtatca attatgcata cgtctgaactaacaaacatg 52gaaatag gctatttaat acattctgtt ttaaaagtag gtttggtcag ccatgtaaat 52aaattgg gagccaccaa gataactcat caacaaatat gcactatgta ctaggcacta 522gatgat ggtgaaccaa acagatgtaa tccttgctct tacagatctc acaacctact 5226gccaa aaatatatgtgtatgtgtgt gtgttataca tatatacaca cacatacatg 5232ataca tatacacata cacatatata catacgcaca catacacata tatacacaca 5238atatg ctatgaggaa aacaaacagg tggtgagaaa gaattagagt aggggtagag 5244agggc tcctcaaata gggtggacag cttgacacaa gacactcgagctaagactcc 525atgaga agacagttat gtaaagaaaa ggggactagc attgtcagca ggtagctaag 5256aaagc agacagtcat gtgctgcaat gccagcttca agcgaataca gttactaaag 5262ctaac cttctatgtg aatgtagtta ctaaagcata tcctccaact ttccattttt 5268gctat tgtttctaccacttctcctt ttctgttgac aattatttta aatttcctgg 5274ttaaa tgatggcatg aactctgggg aaagtaagac tacctatgtc caaataatcc 528ttcctt ctagtcctta tgactgatca attcaccctg aagtgacaac tatgtcccaa 5286aaaga gtgtttcttt atctgcactt aattttttga tttggaggcttcctgattgc 5292aacat gttgtgtgat tacttcaaca agtacttata gaacgttatt ttgtcactgg 5298cgttc tgctgctttc tgaactttag gttgctctag agtctaggaa gagtgactgt 53taaagca gttcctaatt actggacatt ctcagatctg ctagagctac atgtccaatt 53agaatat actggaaaaagccctggatt agaaatgaga ggatgtaggt tttagtacca 53cagccac cttgttaatg caaatttgag taaattgtta cttcttttag gccttgtttt 5322ttttg tttttctgac agtatggtct ctgtggtcca ggctggagtg cagaggcaca 5328aggtc cctgcagtct ctacctccca ggatcaagcc attttcatgcctcatcctcc 5334agctg ggattacagg catgtgccac cacaccctcg aactcctgac ctcaagtgat 534ttgcct cagcctccca aagtgctggg attagaggtg tgagccactg tgcctagcct 5346attgt tttcttactg gtaaagtggg aatatctaga agttgcatgc tacataaatt 5352atata ttattggcaaaaaattttaa agaaaaacat cagcttaaga gtactaattg 5358atgcc ttggaatgag catgagctgg aaagaacaaa cctgttgtta catcactcat 5364ttttc atatgctgct cattgtaaat cttgctcagt ggcatgattt tagtgtttaa 537ttattt gtttgtttgt ttaggacaaa gtctctacac ataatctacttgcttcatat 5376tactt atgcatatta tgtatgtaca tacatgctct cagggctcac atgaaaaaac 5382ttcag gtgatgtgat ttatctcata tgcttacttt agagtcaaca gggtgttgac 5388tatac aatactggca tggagaacac ataagtcaaa gtagacagga cccagccgta 5394ggcta gggcacaaatatattcacat atgtggagaa tgatgtacgt agaaaggtct 54ttgcaca atgctcttta ataaagatct ggaaaaaaaa aacacctaaa tgttcaaaag 54agggtag atgaaataat ggtacattat aaaatggaag attatgcagc cataaaaata 54aaatacc ttaaataata acagaacaac ttttaaggta agtgaacaaataaggtacat 54cactatg catagtatgt accatttaca tagaaaaagg gaagaaaaat aaaatatata 5424attta tttgttctta catgtgtaaa atttttctga aaaatatacc agaaactggt 543ctggtt gcttcctagg cagaaaatga ctgagtatcc ttttgtacct tttgaatttt 5436acgtg aatgaatgtgttacctatga acaaaatgac aagtttagat cagcaagaca 5442ttgag atgaaatggg attacaccct tagtaggaaa aactttttaa agcaggtggt 5448taaga gcaaatacct gcacatggaa tgttgaaact ataaggaact ctccttaaga 5454atcta ttccaaactt ctcattttat agatctgtaa actgagaccttaaaaattca 546cttgca taaggtcaca cagcagaaga gatgggatta gatgctagat attccaatat 5466ttaga ctattaaaaa ttcagtgact tgtgtaaggt cacacagcag aagagatggg 5472atgtc agatattcca gtatcaactt tagactatta tcacaccatc ttctcatttt 5478ggcaa aacagaaccaagtaagtttg ggctacatta cgagttgtca tgtttttgtt 5484ttttt tgagatggag tcttgctctg tcgctcaggc tggagtgcag tggtgtaatc 549ctcatt gcaatctctg acccccgggg ttcaagcaat tctccctgcc ttagcctccc 5496gctgg gtttacaggc gcctcccacc gcgcccggtt aatttttgtatttttttttt 55tttttag tagagacggg gtttcaccat cttggccagg ctggtcttga actcctgacc 55tgatcca cccacctcag cctcccaaag tgctgggatt acaggtgtga gccaccacgc 55gccgagt tgtcatgttt tatctaaatt ttagagtcta atgtataaat taaccttaag 552gaaact actaatttcttgtttggatc actatacggc tacacttaaa aatatgctgt 5526cctct atcattgcat gtatacaata tgatagatgc atgatatgac agacacacaa 5532tacac gtattttttt ctatcctaac acatctgaat ttactgaaat aactaaaatg 5538agtta cttttttaaa tatacacatg catagcacaa gcgtgttgccaaaaatatga 5544ggttt acaattcctt aactaaaacc caagggttgg atgtgtttta gaaataagaa 555atacaa tttttaagtg ttacagggta tataaaccat tatataacac ataccagggg 5556ggcag caccccataa tcaaacatat taatatagtt tcagcaaaac acatgggata 5562tatat acagcttctcaatagttcag gtcatatttt gctaccaaat gaattttgtt 5568gctta agaagttttt ggttttcacc gctttctgaa tgttagattg agatgtggga 5574gactg tactcataga gtgcttctag aaagcagtca gtcacttcaa ctctcatttt 558ttatga gactaaaaaa gaaatcatag caagtagctt ttatatcccaggtttgggcc 5586cttgt attgtggtta aggaatctaa cttagtagaa ggtgcacgag ctgacatcgt 5592gctaa aatgagagaa aaaaagagaa aatcctaatc atacagaagc actgaactac 5598ctgtt cgttagttat taatttaata aaagcttcct ccctttaaat catgtgagtt 56aactgga aataggtcaataaaatttct gtcccacact gctgacaagc gatggacgca 56agcttta atcccactgg aaggtactgc actctctctg ggaccaggat atgtagaaaa 56catttca aatatatagg aataaccaga aatgtataca gtattctcaa cttgggaccg 5622ctata atataaacga aaggggtttt ctagtcaatc tctgctgatctcctgtacca 5628cttcc ctttataagt cttgtactac cttttacaag aggaaaaagc tctagagcga 5634cagaa cacactaaaa tcccttcctt tctctttaca actcaagccc cgcctccatt 564ttctgt tactaatttt tcttctgaaa aaataccaaa tttacactga aagactaaaa 5646ctttg cagacaacgttttaaaaaat acaattcagt ttggtgatgt tgttttgcag 5652caatt ttagctacat tttaactgaa ccaattgttt tgttcaattt atgagttaat 5658gcaag tttgtttttt acaaatagtg tattccattc taaaaatgga agtagcagtg 5664caaga aaacaaccct ctgagttttg tctatttcag gaggaagtactactttctcc 567ttaatc acaattcata aaaaagaaaa acctaactag ctagatctta aatatacaaa 5676taaca atctagtaaa gcaacagaaa aaggtaaaca aactaaccag cctatttttg 5682agaaa ccccaacaaa ctgctggatt ccttggccat ttgcattcag aagtaccaaa 5688aaatc ctttttactaaataatttct tctacacgag acttgtttcc tccacaccac 5694ccaaa ttgtcagcat tattccagaa tataatcatt tagtttgaga ccactaaaaa 57ccgcagt ccaaaatacc aattgtggtt tttctgtaaa gaaatggtca gaaactacaa 57gttatcc taggacacag aaccaatcga ccaaaaggac ttctggaatatgctgccccc 57atttaga atgcacaggc agaaatagca tacgcggtca cgatgtccct taagccacat 57cttccta cgaaagcaaa ggcttaaact tatcaaatga gaactccccc tttctctgaa 5724aacaa ggcagggcag ctggaattag agcagcaggg acagatcggc tgttgactag 573aacggg tcgtggaatgcaaagtccct gcgctttcgc tgctcccctt accgtgagaa 5736gggag ggaggaaagg aggagaaaca ccccagaatc ctggtagaaa agcccctggc 5742agatg ggctctaggg agacagggag gggcagctcc gtgtgtgatg accctttgtg 5748gcact ctgtggcagc ttcagctcca ccgaggcttt gggagagcggactacggatg 5754cgcgg cccagctgtg aaggccgcgc cggcggagag ggtccatggc acccccgccg 576cggaag cccttccctc tcccacctcc gcgggtcacc ccaggaacca gcggctcccg 5766gctcg cgcggaccac ggaacagcga cgcgcaagca ggtctctttc gtcagcgtaa 5772ccgca gaaagccgcgcactagtttt aatcacgccc caccccctgg ccgctggcgc 5778ccgcc actcgggcgc tttccagcag cttccagaaa cgtcgcctcc ccaaacccag 5784cacac atggcgggct cagcagccac cggccccgcc cctcctcgtc gccgcagtcg 579tgcgtc tgcggccaca gggcggacag ccacgcctct gcggagggcgaccggaagtg 5796gtctt caccttcccc gccacgccac cgtcctttca ggcccagcgt gcagcaggaa 58ggactct tttgccgcgg actcaagccg gaagccgcct tcctagtgga gacgcgagtg 58gaggagc agtccgaggg gaacgtgggt tgaacgttgc aactagggtg gagatcaagc 58aacagga gttccgatcgacccggtacc aagaagggga gtgcccgcgg caggtaaggg 582gaggga ggggtttctt tccgctctcg aaattgggaa aagagacaga gctgggatga 5826ggggt agtcggcgcg ctgaaaggat gggctgggct gggacggggt tcaagtggga 5832tgatg attaaggtat agagttggac ttacagatcc gtttgggcgcagagaggtga 5838gaaga gaaaccagag tttgttttcg ttttccaagg agcgtggaga tgggcagggt 5844gaccc tgcgcctcct tcggcttctt agtttgggtg ttgaaactca cctcctttgg 585gttcgt ctctgattca agacagttgg gtttggtacc tgacagggct gggtgcagaa 5856accct gttcctcggcttccaggtcg gttgtggcct cgcttttgac agttcacgtg 5862cctac tcgctctcgg agggcgagct caaatgggtg ggtttaaggc cccctcttcg 5868ctgtt tccctgggtt tctccatttt gcacacagga gtgtgaatta agtttaattg 5874ttttt gcgattccca gggccacctt gacacgttca ttgtgctatctaactgggtt 588ctgggc taataattca cattaaggct tctggagtat aagtggttca cagaagtatg 5886gggat gttagaagaa agatgctggg ggtgaagtag agttgaggaa gacagaactg 5892ctagg ttggtttcac agtacaatga gctttaggtc ataatactac ctttaggtta 5898ggctg tttggacggagtttgctgta atcaggctag agtaaataga gaattttaaa 59agcattg acaggctcag acttgtagag gcatcatttt gacagtgata tggaagggaa 59ggtagag atttgagacc tttccaaaga actgtccaca gaatttggtg acttactgtg 59agaggga aataaagaat agggaacaac tcaagacttt ctagtctgtgtgtttggaag 5922agacg cccacattta agtgagatat gggaaggagg agcagattgt ttttgaaggg 5928gagca gttacttagg gtcaaattaa gttgtaaaat cccccccggg attttgtatg 5934caaag tgaattgtat ttggaagaag aactggggag cccacctctg gtattttttt 594tccctc atatggacaaataaacctct ggtattaaat gaattttctt ttgggggatt 5946tattc gggatttcaa ccaccaacct atctggtttt tcccgctgaa atgttgggtg 5952atcag gagagcagat ttggagactc tttatatttt ataattgaga gagacaaaga 5958ccgtt tgatttgaaa aagttttcta ggttccctca ggtagatggaaattttcatc 5964cagtt tattcaaggt acatagccta ctagtttccc atttgagagt accgcagaat 597cgacgt gtactgcttc tctacgcaga atgaagtata aaattagcac caaatagtaa 5976atttg tcaggtgcta aactttttac atgctttatc tcatttaatt cttagaagaa 5982tttta caagtaagtgtctggaccaa catctgcagg tacaaagcct gaaaagcgta 5988gactc ctacatagtt ctcttttgta agtagattat aaatagaacc agccaaaggt 5994gttgt ctgtgcctaa aaagaaagaa aaaagttagc atcagtagtt ctcaccagaa 6ggtgattt tgcttaccag gggacatttg gcaagtcagg aaacttttggctgttggatc 6gagggtaa aggtcagtga cgctgctaaa catcgtcagt gcatagaaca gccttcacaa 6aattattt ggtcaaagat atttgtagtg ctgcagttga gaaatttctg tcttatggtt 6ttcttcag gaataggaaa ttaagattcg
ccgatacttt ctttaaaaag cagttttatt 6tgaaatta ttccttggct tgaaaggttt gtgaagttta tatagccgaa ccagaatagc 6aattagat tttaaagtga attgtgagcc atcgattccc aggagatggg tgtcatagaa 6atggattc ttggatttgg gaaagactta tgcctagaat tattttacaacatttctgct 6gtggtaat tctcctctgc cctaaaggtc tcctgtattt gattttccta tcattgtgaa 6cacaatta aaatgctctt aattattttt tgcttacact gagctccggt ctcttgtaat 6ttactctg ttaaatgtgg ttctgcacca taggactgca ctcaaaacaa gcttgccaca 6tgtaattt gtactaggacagtgtttata tttttgttca gataacaaaa taagttaaat 6ggtgtaaa ttagatcatt tacaaataat aatttgttag cagcttttaa taagtagtat 6ttcccaac tggtgaagta ttaatgttgg tagttgaaaa caataggaat gtatggaata 6tggttcac tggttctttt gttcctgtca aatagtggca caatggatctggggtttttc 6agtataat gctggcatat ttgtttcaaa ttgtacatag actctaaaaa gttaggcttt 6aattctgg tcaatatagt ttgctttaaa tagtagctgc ctctactaca agttttattt 6tttgttga caaatgagtc tgctatgaaa accggtcctg ttgccagtca ctaccctctg 6cacaaatt tgctgggtttataaatatag gtatcatttt cacttcaaga ttataatttt 6aatatgtt tattctagga catatagccc tcaaaatctg cttactatat acgtcttata 6atagcatg gttctttttt atagtaaata gaatttttat ttaattgtct attgactttt 6tttccagg gttcattgaa aaaatcctta gtgatattga catgtctcaagtgacataaa 6agccaatg actcggaatg atggattctc cgaagattgg aaatggtttg ccagtgattg 6ccagggac tgatataggg atatcttcac tccacatggt ggggtatttg ggaaaagtta 6gaacttat tttttgcctg agtgcaaagt tttttttttt tctctatttt tgagacttaa 6tcaatttt gatgttaccagttaacttct aaaaaattgt gtcttccacg gaaatcttac 6taatggcg aaagattgtt ttaatgtgtt tacctttctg tgttttattg atacatgaaa 6ggaaataa aacatagacc ttatgattta ctgttctttg aaaatatggt acataaattc 6ccgggtaa ttgatgttac ttttttcctt gcaaataaaa ttgatactattcttaacaca 6aaatttaa tatttaaaac tataacataa ttctttttgg aataatagct gtatttaaag 6ttatatgc atttcttttg tttgccatgt ttaaaatacc ttgtcaggat acttgtaatt 6aaattata attttttctg gttacctttc catttaactt ttaatatttt gatatattct 6gaatgtct atattttaatttgctttatt tctcttttag aattttgatt cagctaaagt 6catcagat gagtattgcc ctgcttgtag agagaaggga aagttaaaag ccttaaagac 6accgaatt agttttcaag aatctatctt tttgtgtgag gatctgcagg taaagtatta 62ttatata gtatatataa gatttttctt ttttcttttg cttttttattaattgtttta 62gtttact cattttttgt tttttagact agatttttaa tatgtaatct cagtttgtaa 62tgtctgg tatacaatgt tatttttcca cctaccttta cttggttgcg taaagatgtt 6222ttatt gccatttgat ttgcgagagg agaaaataca tttcaaggtt tttttctttt 6228aacct tttggaggtccttgttagct attagcatat agtagttact ctctcatctc 6234tttat ctttgcaact gatgggaaaa gttatgaatt tctaatgtac ctggaagagt 624tggaaa ttggttagtc caaaaccagt atatatactc tgaactaaag agagtataga 6246gtaaa ttctaaaaga tccttttaga agctctaaat cgcttttagaattatagtaa 6252accga ctggtacggc ttttatatag cagctcatta aattctgtaa tactccacat 6258tgtat ttgacagttt atgagactgt ctcatacact tttaattctc agaactttgc 6264ttgta ttcctatttc atgaataaga aaataaattg atttcagagg gtttgggaac 627gatcct gatacagtggcagagctgtg gttggaatac agacttctaa tttcagatct 6276ttcca gcaaaaaatt agcagttcat cagaattacc tggagtgctt ttaataaatt 6282gtatc acccccagat gctgattcaa tagagttggc ccagaattct gtggttttgt 6288ttgag gatgagtctg atcatcatca gccaggtttg gaaaatactagactaaatca 6294ttgtt aatagatact tatgctgggt ataatttgaa gtaaagtaat cccaggcgtg 63acaaata taaatttctt tatgtttata ttcagtaatt ttttttatga gtgtcactgt 63gcactgt tgcagataca atgttaggat acaataataa aacaaaaatt tcttgccctt 63gaagtta tgtcatagagtgggaaagac agtgaacaag tatgtgtttt tctgtcaggt 63aaaaagt gctgtggaga aaaataaggc agtagggact ggaatgccaa agtaggggga 6324caatt ttaaatagga tggtgagggg aacgcttcaa tgaaaagtgc aattcgagca 633cctgaa agaggtgaag agcagtgagc tttctaggca ggggaagcaagttccaggaa 6336tgaga gaatggaggc tgcctgtcat gtttgtgcta ctgcaatgaa agcagcagag 6342gaagg tggatcagaa aaataatggg ggagctggac caagtagggt cttataagcc 6348aagct ttctggcttt tactatgggt gaaaccagga accatggcag agatgttggc 6354agtga cataagttgacttcagtgtt aaaagcatta ctgtggctgc actgttgaaa 636atgtaa tgggcaagac ctgaagcagg gagattagtt atagtataat atgaattata 6366tcctt gtctatggtt tccgttacag agctaaaagt cttggaattt cctgaatgat 6372tgtcc tgttattcag aatgagcctg tttgctaaca ccggggttcatactattgtg 6378ttagg atggagccgt agatagcctc agatggggca agtagctgga aagaccacat 6384gagaa ttaacgggtt agaactttta gccccacgta caggcctcca ggaaaggagt 639gggctg gagatcaagc tgtataaaaa tatcaagatt tggatttaat gagtgggttg 6396ggctg gtgccgtgtaggaggtggta tgcttagagg aagtggaagc ttcatacctc 64tgtccca taccttgccc tactcatttc ttcatctata ccctttataa tatcctttag 64aaaccaa taaacataag taagtgtttg tttgagttct gcgagctgtc cttgcaaact 64tatgccc aagaaggggg agtgggaacc tttgtagcca gtcagtcagatgtactggtg 642ggatgt gggattggca tctgaagtgg agggagtcat gggactgagc cctcaacctg 6426tctga catggtctct aggtagataa catccaaatg gaattggatt ataggatacc 6432ggtgt cctctggaga attgcttggt gtggggaaaa agcccccaca catctggtca 6438gtgtg ctgggaggatagaatatgtg aaaattgtca taatcaaaat ggagtcactt 6444aaaaa agaaaaaaaa atcctgactg gccaggcaca gtggctgaca actgtaatcc 645actttg ggaggctgag gcaggaggat tgcttgatcc caggaattgg agaccagccc 6456acata gtgtggcctt gtctctacaa aaaaaaaaat ttaaattagctgggcatggt 6462gagtc tgtagcccca gctacccggg agggggacta cgggtgcacg gcaccatgcc 6468ggtcc aggctgcagt gagctgtgat tgtgccactg cattccagtc aggatgacag 6474gagac cctgtctcta ttaaaagaaa aaaaaaagac aaatagatcc aggaaaggct 648agagag agctttcatgcataaatacc aaaatatctc aaaagactct gcaaaaacca 6486ttgca caaaggccat catgaaatac ttctgaaata cacagaaaat acatcatgaa 6492tacac agaaaatact tctgcaagga catctgccca gcaactgcct ggtccatctg 6498gggtg tcatccttgt tattgatcct tgtagccaag ggtaattatctcaaaacaag 65gtgatcc tccttatttt cctttaaaaa ccttttgtct tcccttacct ccctgaacac 65cagttta ctatggcatg tgtattccca ttggaatact ttattcctga ataaatgtca 65tcttttt agaagcttct cttttctttt tatttagatt gataagtaga aaggaaaaaa 6522ttttc cctttggactagttgaaggc agttgcagta ttctggggga gagggtggtg 6528ggtgt tgaggcatgg ttggagttta tttatacttt gaaggtaaag ccaacaggat 6534gaaag attgggatat ggggttggaa agaggaatca aggatagttc caagattttt 654tgaaaa attagaagaa tggaatcgtg aattactgag ctgggaagacttggaagagc 6546tttgg ggagaagatc aggactgtaa gaatagagaa gtccttgtcc ccaggagtta 6552ttggc tattaaagtt agatgtacta catagatttt tagttggttt tttgtttttt 6558ttttt tttttttttt tgagacggag tctcgctctg tcacgaggct ggagtgcagt 6564gatct cggctcaccgcaacctccga ctccctggtt caagggattc tcctgcctca 657cctcag taggtgagat tacaggcatg tgccacccag cccagctaat ttttgtattt 6576agaga cggggtttca ctatggccag gatgggcttg atttcctgac ctcaggtgat 6582cacct cggcctccca aaatgctggg gttacaggtg tgagccaccacgcccagccc 6588tttgg tttttgaagc attctttttc aagtgataaa gcaaaaaata tataatcaag 6594taagt atatactttg gaaatgttaa aaaggaacat gagtaattta ttattatttt 66aatttct agtcagcaat gagagcccag tgtactttat gaagtagatt ggtttacacc 66agtgagc agacattttgtatgatgcac aaacaaggaa tgattttttt gttttttaaa 66ttaggaa aatatcaaaa taaaaaatgc cagaaaaaat caaaagaagg gccaggtgca 66tttcaca cctgtaatcc cagcactttg ggaggccaag gtgggtggat tctcttgagg 6624agttc gagaccagcc tggccaacat ggtgaaaacc tgtctctactaaaaatacaa 663gccggg tgtggtggca tatgcctgta atcccagcta cttgggaggc tgaggcagga 6636gcttg aagccagtgg cagaagttgc agtgagccaa gatttgagcc actgcactcc 6642gggcg acagaggaga ctctatctca aaataaataa ataaataaat aaataaataa 6648tcaaa agaagaataccctttcataa tatgtgaaaa ttaaatgaaa ttcaaatttc 6654tcata aataaagttt taccggaaca tagccatgct caatcattta tgtattgttc 666cttctt ttgcatacaa caacagagtt gggtagttgt gacagactat gtagctcata 6666taaat atttattatc tagcccttta tcagtaaact ttgctgatccctgtataagt 6672gaatc aaattatttc caaagagttc cgttataaaa tttggagttt actctgctgt 6678gcaaa gaaccatttg gaaaacctct tttagtcagg tatttacatt aaaatgttcc 6684ttgta aacactaata ttcaagactg gtccaaaatt ataccaaatt gaaactctca 669ttttta aacagtaggaagttttaact tttttttttt cgtggagtag tctatcattc 6696ttact ttggaacatt taattagtct tttttaaaaa cccatgaaat ttataataaa 67tttaaat cattaatgtt gagtaatcaa agaaaacttt ttttgttttc tccatttgta 67tgagtac attattatta taatttgtct ttggccatac cttgttgataattacttata 67gtataag aagacatggt atgttttcct ttttcctatt tcacaagaat aagtacagga 672acttaa gctgctccaa aactcagtga aagagacagg attaggtttt tttcagcatt 6726ttaaa tgatactaga tggttgcgct gggctaaaat actaatgctt tgtgtatatt 6732gactt ttttgaagacagcttaaaag ctttattcta gttataaaaa tgatacatgt 6738gtaaa tagaaacaag tcaggtatac agagatacaa atatttagaa catgtggaaa 6744aacaa aattttataa aaagaaaaaa gataaaaatc tgaaatcatt aatttataag 675aaatca gggcaaggac aaattatatt acagattggc ctatggtgggagcacagatt 6756gagaa aagtcagtga agacacttgc gaagagtgtg ggtggaaatc actaagtttt 6762cccgg ggcctcttat ggtttattac tgttttgttc tttttttttt tttaatatgc 6768tttgg aaccaagggt ttattatgtt ttgaataaag tagaggtgta agtaggatgc 6774ccatg atcttgactacttgagattc acaaagggtt ttcgtctcag gatttttttt 678ttaaaa aaatttgtat taatttttaa attgtaaaaa aattcatcaa cttaaccatt 6786gtata gagttcagga gtattaggta tattcacttg tgcagcagat ctctagaact 6792catct tgcaaaactg aaactctgta cccattaaac aaccacttcccattttcctc 6798cagct tctggcaacc attctagttt ctgtttcttt tctttttttt tcttttgaga 68agtctct gtcgcccagg ctggagtgta gtggcatgat ctcggctcgc tgcaacttct 68tgcgggt tcaagcagtt ctcctccctc agcctcctga gtagctggga ctacaggggt 68ccaccat gcctggctaatttttttttt tttttttttt tttgtatttt tagtagagac 6822tttca ccatgttggc caggctggtc tcgaactcct gacctcaggt gttctgcctg 6828gcctc ccaaagtgct gggattacag gcttgagcca ctgtacccgg cctctagttt 6834tctat gaatcagact cagtacctca tataaacgga atcatacagtatttgccttt 684tgactg gcttatttca cttggcataa tggcctcaag attcatccat gttgtagcat 6846aatat acagttagga gttccttttc ttttttaagt cttaatctcc agtttatttc 6852attta tttattttat tatactttaa gttctgggat acatgtgcag aacgtgcagg 6858tacat aggtatacacgtgccatggt ggtttgttgc acctgtcagc ctgtcatcta 6864ggtat ttctcctaat gctatccctc ccctagcccc ctacccgccg acaggccccg 687gtgatg ttcccctctc tgtgtccgtg tgttctcatt gttcagctcc cacttacgag 6876acatg cggtgtttgg ttttctgttc ctgtgttagt ttgctgagaatgatggtttc 6882tcatc catgtctctg caaaggacat gaggagtttc ttacttttaa ggttgagtaa 6888cacat tatgtgtatg ccacattttc tttatccatt cacctatctg cagatgtttg 6894ctttc actttttggg aattgtgaat aatgctgcag tgaatgtggg tgtgcaggta 69tttcaag attctgcttttgagtttttt ttggatacgt acctttttat gatgctttaa 69catatat gctattttta aaggattctc agttttctga catatgatag gacttaggaa 69atctcaa agcatcatgt tgacaggttg ttagttgatg gtgactgcag ctagttggaa 69cagaaga atctagaact tgtccattta tactaaagaa tttcatagtaagtgcagtat 6924gtgta atgttcaatt ggtagaagag gctatctgag gggatttagt gcatttcagt 693tgttgg tgtgaaacga atcaccttga aacttagtcg ctcaaaaatt ttaatggtgg 6936catgg tggctcacat ctggaactcc agcactttgg gaggccgagg caggcagatt 6942aaccc aggagtttgagagcagcctg ggcaacgtgg tgaaaccttg tctctacaga 6948ccgtg gcaggcgcct ttagcaccag ctacttggga ggctaaggtt gtaggatctc 6954cccag gaggcagagg ttgcagtgag ctgggatcgt gccactatac tccagcctgg 696cagagc cagaccctgt ctcaaaaaaa aattttaatg gctccatttattatttcaca 6966atgtg agttgactag ggaattctta cacatcacac catgtcagct gggacagctg 6972tccac atggctggca gttggtacta gctgctagct ggaagttgag ttcaaatagt 6978agggg tctcagttat tttccatgag gttctctcca tgaggccagc tgggctcttc 6984gtgat agctgggactaagaaggagt gttccagaag aagggcttgt cctcttgagc 699gcttat caggcctcta tgtatatcat gtgtgctaat gttccatcaa agctagtcac 6996caagc caactctgta cagtgtaggg actggctgca ggagggcatg aattaccagg 7gtgtagtt ctctagttca tagggagggc catcaagata gtagtctaccatacttgtgt 7aagaaggc attaattaac tattattatt attattatta ttattttaga gacagggtct 7ctctgttg cccaggctgg agcagtagag tggggcaatc atagctcatt gcagcctcca 7tcctgggc ttaagcaatc ctcccatctc agcctcccaa gtagctggga atacgggagt 7actgccat gcccacctgaaaaagaaggc atattttaaa agcagacctt tagtgtagag 7ttcttgaa tttgttattt aaaatattct ggtagttttt aaacttagga aagacccact 7ttctttta gtgatatgtt tacattgttg ttatttggca taaattgtgt taatgcacag 7agatttca tgaagtcatt aaaattcagc cacttggact ctaaacccaataaagatgta 7acagcagt gctatgagat gcatattcag tttcaaaata taggaaacac agaaattact 7gtgcactt ttaatttgaa aatactttta aaatgtgtag tataatgtag tgtctgtccc 7aagagtaa cattcattat agtgtttctt tacgttgttg aaaattttaa attcacttaa 7ttagattt ttattaaagcaaaaatatgt tttccttatt agcttaccct tttgtaactc 7attaaacc cttgattgtt caaattaacc tgaaaaaaat tattcttttg gaggccaaac 7ttgattaa gtagttgttt gtctctaatt ttttcaaatt tatgtgtata aatataacct 7catcaaat caatgctaac attctataca tgtttttcat gatatgaaaactataaaaca 7aagttatt tgaatttgtg tagtttttat cattttattt ttactttcca gtgcatctat 7tttgggct ctaaatcact taataaccta atttctcctg atttggaaga atgtcacact 7acataagc ctcagaaaag gaagagctta gaaagcagct ataaggattc acttctttta 7aaattcca aaaagactagaaattatatt gctattgacg gtggaaaagt tttgaacagc 7acataatg gagaagtata tgacgaaacc tcgtcaaact tacctgatag tagtggtcaa 7gaatccaa ttaggacagc tgattccttg gagcggaatg agattttgga agctgatact 7tgacatgg ctactacaaa agatcctgct acagttgatg tctctggaactggcagacct 7ccctcaaa atgaaggatg tacatctaaa ctggaaatgc cactggagag caaatgtaca 7atttcccc aggctttatg tgtccagtgg aaaaatgctt atgctctctg ttggttagac 7tatcctgt cagctttggt gcactcggaa gagttaaaga acaccgtgac tggactgtgc 7gaaggagg aatctatattctggcggttg cttacaaaat ataatcaagc aaatacactt 7atatacca gtcaattgag tggtgttaaa ggttggtact aatattttat ttttatttac 7atttattc atctggagtc agggtctcat tctgtcaccc aggctggagt gcagtggcat 7tcatgtct ccttgcagcc ttgacttccc tggctcaggt gggcctcccacctcagtctc 7aagtagct ggaactacag tcgtgcacca ccatagccag ctaagatagt gagatggtgg 7ccactgtc ttgcccaggc tggactcgat ttcctgggtg caagcaccct tcccgcctca 7ctcccaaa gtgctgggat tacaggcatg agtcaccatt ccagcctact tgtctttaat 7ttaaaaat attaatgttgagttttgtct cccagcatgt gggaaagatg tcatccattg 72ctgtttc ctggaggcct gggagcaagg agcccaggaa cagtatcacg aagcttgaga 72taccagt tacattatcc tgactgccca aaaggcagtt tttttgtttt ttttttttat 72ttaagtt ctggggtaca tgtgcagaac gtgcagtttt gttacataggtatacgtgtg 72tggtggt ttgttgcacc catcaacccg tcacctatat taggtatttc tcctaatgct 7224tcccc aacccctcca ttccccatca ggccccagtg tgtgatgttc ccctccctgt 723atgtgt tctcattgtt caactgtcac ttatgagtga gaatatatgg tgtttggttt 7236tcttg tgttagtttgctgagaatga tggtttccag ctttatccat gtccctgcaa 7242atgaa ctcatccttt tttatggctg catagtattc tatggtgtat atgtgccaca 7248tttat ccagtctatc attgatgggc atttgggttg gttccaagtc tttgctattg 7254ttttt tttttttttt ttttttttaa gacagagcct cactctgttgcccaggctgg 726cgatgg catgatctca gctcactgca acctccgcct ctcaggttca agcaattctt 7266tcagc ctcccaagta gctgggacta caggcgccca ccaccaggcc cagctaattt 7272ttttt agtagagaca gggtttcacc atgttggtca ggctggtctt gaactccaga 7278tgatc tgcctgccttggcctcccaa agtgctgaaa ttacaggtgt gagccaccat 7284gccta ggcagtcttt ttcaaaactc taagactgtg cttgtgtctc agggtgtcag 729atagtg gttagtttta agtgtttaaa ctactgaaaa gcagaatgaa gaagtgagta 7296caccc ataatcacac aacctcctaa gatctcttgg cacaataagggatatgtttt 73ttttatt ctctgtaaaa taggatactt atgaacccac ctcccaacac aggaagaatt 73acattcc caataactta catttaccta tgcgtttcct cccatcccat tctctacctc 73cccataa gtaatcatta tctgaaatgt gtttcatcat tccatctttt cttagttttt 732catgtg tttatctaaacagtatacag tagtctcccc ttattgtagt tgtacttttc 7326ttcat ttaacccgag gtctgaaagt agatgagtat agtacagtaa tatattttga 7332aggga gaccacattc acataacttt cattacagca tattgttata attgttgtat 7338tatta gttttaatct tactatgcct aattataaaa cttgatcataggtatgtagt 7344gaaaa agcataatat ataaaatgtt tagttactat ccaaggtttt aggcatccac 735gtcttg gaaggtatcc ctctcagata atgggggatg gatggtactg aaccctgtat 7356atgtt tttccctata catacataat tatgatcaag tttaattaag agtaaattaa 7362ggcca ggtgcagtggctcacatctg taatcccagc actttaggaa gctgaagcgg 7368tctca tgaggtcaag agttcgagac cagcctggcc aacatggtga aaccccatct 7374aaaaa atacaaaaat tggctggcta tggtggcaca cgcctgtagt cacagctact 738gaggtt gaggcaggag aattgcttga acccaggagg tggaagttgaacaatcactt 7386tggga tcacgccact gcactccaac ctgcctgggt gatagaatga gactctgtct 7392aaaaa aaaaaaaaaa aaaaagtaaa gtaaatgtgg ctcaacatgt tgctgtcagt 7398cattt gtttctgatc gtgtcttcca cccacaaatt gaatgctttt tccatcttaa 74ttatcag gcactgtggccataacttga gcagttgaga tgcaacagca aaattagcac 74tttcttt ttctttcttc gcagtttcat ggataagaga tttgttctta gatctcagca 74tcagcat atgatttttt tctttaagtt gagaactttg acctttttac ttagagaagc 7422acagc ttctctttgg catatctgaa ttgccagcat tactatgctcgtgctttggg 7428tatta agtcaaataa gggttgcttg aacacaagca ctgcaatacc atggcaatag 7434atcac caagatggct gctaagtgaa ccacaggcag gagtgtagac agcatggaca 744agacga agggaagatt cacgttgcca gtggaacaca gcaggacagc aagagagttc 7446gctac tcagaatggcatgaaattta aagcttataa attgtttctg gaattttccg 7452tattt tcagaccacg gttgagttca ggtaactgaa accataggaa gcaaaacacg 7458agagg gaccacttcg tattgcctaa tttagtttgt tttgatcttc tgggaccttt 7464ttgtt gtaaaaattt atggggctgt ttatagttgt ggctcattgatttttcattg 747ataata cttccatttt gtaaatataa cagaatattc atctacctgt cagtggacag 7476ttttt ttgccattat aaatgctgct gctgtgacca tttggggggc aagtctcctg 7482cagta tgagtttccc ttctgtataa caaaggaatg gaaaattata gactttcgtg 7488attta caagataatgacaattgttt tccaaagtgg ttgtaccaag caattctccc 7494tagtg tatataagag gtcttcctga tccatatatt cttcttggtt tattttcaca 75ttgagat ttttgctatt tgagtggtat aaaatggtct gtgatcttga tttgccgttt 75cattttg aagaggttgt cggctctatg tgtatatatt gctcatatttgttccctctt 75tgaaatg ccttttgtat cttatcccta tttgttctgt tctgttgatt gtcacgtttt 75tgatttg tatgagtttg ttccttgtat cattgttgct agagttacat cagatgtgtt 7524atctg ctcccagttt gcagcttgtg
tttttacttt ttaaaaactg tcttgattta 753gaagtc tttatctttt catttggagc tagtaatgtt tgtggctttt taaagaaatt 7536tattc ccaaggtcag aaaatcattc acctatattt taactgaaaa gttataaagt 7542ttttg acattgaaat ttctcattca gttggaattc atattgatgtgtggtatgag 7548gatcc atttttttcc catttgcata gccagttttt gtagctccac tttattttct 7554gatct gccatgccac ctctagcatg tatcaacata tcatgtatgt gtgcagctgt 756taactc tcaattttat tctcttggtt actttgtcta acccagcact catacttttt 7566attat ggctaccttgtagggcaaga atcctcactt ttattcaact tcttttgaag 7572tgatg catatttttt ctgatcttac ttggccatat atattttggg gacagatgtg 7578atacc aagctttctt tgcttgacat tgtagatatt ttcttattca ttaatgtgct 7584ttttg agtttggtca tacagtcttt tatatggatc ttatacatcgtttccctctt 759accatt caggctgtta ctagtttttg ctgttgtgaa ttaacaccag gacaaatatc 7596atctt ttgaattaat tactgactag tttcctagga aagatattag aatatgaata 76aaggtct tgctgaatac agttttcaga atggttgtac caatatataa ttccattttc 76atgtaga aaaaatacctcagtgttttc taaccacctt tggttagaac attcaagacg 76tggtttt gttaggtaag aaatattttg tttcagtgta ggttttcttt gagactgaac 762ttgtgt gtgtcagtca tttacagttt tttgcaattt ttaaaattca gtttctcaca 7626tttgc ctttgacttt tcttctattt ctgctttctc taattacagaaaccccagtg 7632taggt gacagttcag ttgtttgctg cagaagagca gcagttcaat attggaatta 7638aattt tatgttttta atctgttact aattttttac agaataattg tagtttttat 7644ggtta attatatgtt tgagctgcat tactttgcaa tgtaagtttt tttttttggc 765tcaaat aacaaaaattctggttaatg cttatttcat attacaggag aatccagata 7656ttagg gaaacatata agcagagtgt gatcaggctg tatgaattat ttataagaga 7662gtgaa aagatctatt tgtagcttaa gagtaagtag agtcagatgc atgtagagtc 7668ttcaa aataattttc ttattaatct tggatagttt cttgtcacagtaattccatt 7674gataa taaatattac cataaagaag tgatcaaaaa catagatatg tgtgcccaaa 768tttatc acaatagtat ttataatagt gaaaaaagaa acaactaaaa tgtctggcaa 7686gaatg attaataaag cgatgtttca gctgaatata gtggcatgcg cctgtaagcc 7692actca ggaggttgaggctgcaagat ggcttgagcc caggagttaa tgaccagccc 7698acata gcaagaccct gtctccaaac acacaaacac acacacaagt gctatgtttc 77cactgta taataactag ccagattttt tgttgttgtt gttttgtttt tgtttttgtt 77tgagaga gcatctcact tgcccaggct ggagtgcagt agtacaatcacagctcactg 77cttgtag aaccctaacc ctcctgggct caaatgatcc tcccacctca gcctcctgag 7722gggac tacgggtggg taccaccata cccagctttt tttctaagag ataggggttt 7728tgttg cccaggctgg tcagttttta atgaagcaca tttgtgtaga caaagcagga 7734aaccg gataaacactatgttgccac tgaagacccc ttcaaacccc tcaaaaatga 774gaaggg aaatatgaga tattagtttg ggaaataatt gtaactttat taagactcct 7746attta tctgttccta tgacctggct aagttcaata aaagttacac agagtggaat 7752gttag acatcatttg tagtataagt aattgcacat aaggaggtaactttagctgt 7758agata gacatagtat ctgaaaggtt agttatttta ctagacctgt gattatttgg 7764aaagg ctttcactga gattttaccc attcagtaag tactaatgat attgtgctga 777atatat taagggaata tatggtatac cacagagaaa gaattaagga aattttgtgt 7776ttttt gtctgtttgcaaaacttact gactcagctt tcattcttgg gaatgtgtca 7782ctgtg ggaagatata cattgatgag gaattgataa tgttctctgt attttcttag 7788gattg taaaaaactt acctcagaaa tatttgcaga gatagagacc tgtctgaatg 7794agaga tgaaattttt attagccttc agccccagct tagatgcacattaggtaagt 78tggtaaa acttacttgt attatactca tctaccatat agaaatatgt acctcataag 78atataat actgtttgat taccttggat gatcatattc ttgggagaga gaatctgagt 78ttgactt aggaatctac cactgggtaa gttattgtag ggcagagctg ttccatataa 78tgtaggc tggtgttccacctcttgaga gtgggtgcag ttctcagaac caggagaatt 7824gggca tatcattagt tgcttctcta gtacgtttcc tagtagacag atctagcatt 783acctca attgtgcatt aaaaagcacc gagggaattt aaaagtaaat gccaatgctg 7836tttga attaggatct cagggatggg gctcaggaaa tcagtaatttttagaaaccc 7842gattg ttatatgtac ccagggttta gaatctcatc taaaccaacc atagtaattc 7848cccta ccagtgattg gtttaggaat gtccttgtgg tagagttttg gccagtggat 7854gagaa atatgctgat ggccttttgg gaaagcttcc tcgcctttag aaagggcaca 786tgggac ctctttgttctctgtgactt ggtttttggc ctgtgggagt ggcgtgcagc 7866agcta gagagtctgt ccaaaccttt ctaaattttt ttagtattgc gaaaaggagc 7872ggttt ttttgtttgt ttttgttttg aaagggcttt ttgttttatt tttcttgtat 7878tatta actcttctat taatgttata gtagcagaat atgatactccctattagtaa 7884catat tatgtaaaat atcagtgcct tctagttttt ctctcaatga gtgacattta 789atatta aaaaatgata tttatatttt ataataaaat cagttgttgc tactgatttg 7896catgt acaaaagaca ccatgcttcc agatcattat aaaatatgat attttataat 79tttacaa tatatttataacatatttat atacttagaa tatattttat aaggctgggc 79gtggctc atgcttgtaa tcccagcact ttgggaggcc aaggcaggcg tatcacaagg 79agagatt gagaccatcc tggccaacat ggtgaaaccc tgtctctact aaaaatacaa 792tagccg ggcgtggtag tgtgtgcctg tagttccagc tactcgggaggctgaggcag 7926tcgct tgaacttggg agacagaggt tgcagtgagc tgagatcacg ccattgcatt 7932ctggg gacagagcga gactccgtct caaaaaatgt atatatatat atatatatat 7938tgtat gtgtgtgtat gtgcgtgtgt atatatatat atcgggaagc atggcatctt 7944catgc tggacagcttttgacgtact tctttgactc atgcttctgc cccctaattt 795tttttt tcctacattt tattaaaatt aatatataat agttgtatat ctgctttatt 7956tggac ttatacatac atatttattc tgttcttata aaagtctgat ttttcgtatg 7962tttct gacatttcct cctctaggcc tgaagaactg ttgtaatttatgcatcagat 7968ctcag atggaatgaa tattcttttt tctttatatc aaggtgtaat ttacatatag 7974ccgtt tttaagtgtg tacagctctg taaccctcac tacaatcaag atataggact 798cactct aaaacttctc accaggttca tcacccccag ccactgatct gttgagcgaa 7986atttc aaaggagctttttccgtaag atccctagag tttagatgga agggctttcg 7992cattt agcagatacc atttcccttc tagactccct acttcagttc ccagttgaat 7998aatgg tttctccccc agcctgagtc actacccttc ttatccctga taattatttt 8gaacaaag ttacatcttt tgctccacct ccgccatggg cctggttttctatgtaacag 8ggaatttt taaattattg ttttgtgtaa tcataataat tgggcaagca tacagctctt 8cagtgcag gaggattcct ctcttgtttt actgcccatt caaggatagg tgctatattt 8gctgaaga tcttactaat gaaatgctct gtaatcatat aacttattta aagatgtgtt 8gagctctt tcataatattttaattcatg gagaacttta tgtattttag acctgaagat 8tatattgt cattatgaaa tgtaaattgt ttgctttttc agttaatata tagttacaat 8aatacgga tttaaaggct gataatgaat tacaaaattg tgctatatga catactgttt 8gcatacag tgttgcatat tttcatttct aggatattga tttgtatttctacttacaaa 8aacttttt aaaacttatt ttatggctgg gcccggtggc tcacacctgt aatcccagca 8ttgggagg ccgaggcggg tggatcacct gaggtcagga gttcaagatc agcctggcca 8atggtgaa accctgtctc tactaaaaat acaaaaaatt agccggacgt ggtgtaggtg 8tgtaatcc cagctactcgggaggctgag gcaggaaaat tgcttgaaac caggaggcag 8gttgcagc gagcagagat tgcgccattg cactccaacc tgagcaacaa gtgcgaaact 8ttctcaaa aagaaacaaa aaaacttttt ttaatgtttt tgttcaaaag tagcagtgag 8tatcccgc aaaggtgact actaaaatag cctttgtaac tactgatatttatagaatat 8ttagggtt agggtataac tcgcttgtat tatactcatc taccatgtag aaatatgtac 8cataagga aatataatac tgtttgatta ccttggatga tcatattctt gggagagaga 8ctgagtag tttgacttag gaatctacca ctgggtaagt tattgtaggg cagagctgtt 8atataaat atgtaggctggtgttccacc tcttgagagt gggtgcagtt ctcagaaccg 8agaatatt taggggacat attgttagtt gcttctctag tacttttccc agtagacaga 8tagcattt ttaacctcaa ttgtgcatta aaaagcaccg agggaattta aaagtaaata 8aatcatag ggacatttga attaggatct cagggaaggg gctcaggaaatcagtaattt 8agaaaccc cacatgattg ttattgctta ggtaataaca cctactgtct accttgtggt 8tgccaagg tgactgttcc tggccatgtt ccaggcaact gtagttccag gctaggggga 8actggacc atggaagtga ggctctgtcc agggtagggg aagggatgga aggtgactgt 8ctggccat gttccaggcaactgtagttc caggctaggg ggagaactgg accatggaag 8aggctctg tgcagggtag gggaagggat ggaaggactc agtctcttgg gccaaatcgg 8aggcagca tctaagctcc tctgagaata ggaaggagag caaccaattg gaaaaagaat 8gaaacatg tagattctcc tgcttacctt actttccagt ctcaaagctggaagccagca 8cactgttc agttattttc aatgacaaca agattcaaat cttcagttgt aaagttgtta 8ggaaagga ttagactgaa aagttaagaa gaacggtaga tgaagagtcc aaagagttga 8ctggtcat ttaaccattg tgtggccacg ccctctccac aggtggaaca agatgatcag 8tagaaatg gccaattctgatgtgtttct acagtgtttc actgattaca ttttttaaca 82gtagcaa accatttcca taattttttt tttttttttt agagacgagg tctcgctctg 82cccaggc tggtatgcag cggcatgatc atagctcact gcagcctcaa attcctgggc 82aatgagc ctcctgcctt agcctcctaa gtagcttgga ctacaggtgtgtagcaccac 822agctaa tttatttcat tttatttttt gtagagataa tgcctcgcta tattggccag 8226tctca aacgttcata gaaactggtt ttaggttcct agaggctggc agcaattctc 8232taacg caagcagtct tcctgccttg gcctcccagt gtgctgggat tacaaggtgt 8238accac acctcatcaatttttgtttt aatatactct aaggcttatc atagttccga 8244ttttt tttttcctga gaaatctaga aagatggaag acagtatggg tcttttgtgg 825tttgtc ctaagaaatt ttcataaatg tctgccaagg aaaaggaaag agatcaaagt 8256ttaaa tctttaggat ggacattttt agaaaaatgc tttataaacttcccctctcc 8262ctgag tgacttattg tgtcatactg tattaacaca tattcatgct gtaaatatag 8268aaaga caatagttca caattttggt ttagtttttg ccattattga ttatgagcag 8274cttcc ttttcttttt gaaggtgata tggaaagccc tgtgtttgca tttcccctgc 828aaaact agaaacccacattgaaaagc tcttcctata ttctttttct tgggactttg 8286tcgca gtgtggacac caatatcaaa acaggttagt ttcttttgtt ttttaaaatg 8292ttcta gtttctccac cactaaggtt aagagaacaa tttgagcacc agacactaca 8298cttgc ttctttaaac tggaagggtc aaaacctcat cgtttgatagactgctagta 83tatttcc taaggagttc ttcagtggga aatagggacg atgagaggaa taatacacct 83ttctcca gagtccttgc tgagtagaat acctctcaga atgccatgaa actgtaggca 83ttgttta ttcctctatt agaaatgagg ggttttgctt gtttacttta ggtttctaac 8322agaca ctagttttaggctcttggag gctagcagca attctcagag gtaatgcaag 8328ccatt tcttcccgta gtcctgtgaa agaccagcca cctccagaag cctacacatg 8334tctca gccatacttt ctgcttttcc taatgcctct cagcagcgta ttagaaaggc 834atcgat gtacctgtta ccttcaggct ttgcataagg tgtatatgaaacataatgaa 8346tgttt aggctcaggt cccatcccca ggttacctct ttatcttgga gacacttctg 8352ataca tttcagataa gagatattca acctgtaccc accacgtaag gagaggaata 8358tagaa gaggagtcag ggaggcaagg tattcccaga gggatattct cacttggtcc 8364tgaga aagttgctggctggcagtta ggaagatgac cagactggct caattgttcg 837ttcaaa ttattacaat agaaataact ctttccaccc ccccccgccc tttttttttt 8376gttgg agtctcgctc ccgtcacaca ggctggagtg cagcagcgtg atcccggctc 8382agcct ccacctcctg ggttaaagcg attctccttc ctcagcttcctgagtagctg 8388acagg tgtgtgccac cacgcccggc tgatttttgt atttttagta gagacagggt 8394catgt tggccaggct ggtcttgaac tcctgacctc aggtgatcca gccacctgag 84cccacag tgctgggatt acaggtgtga gccaccatgc ctagccacac ttttctttag 84aagtgct taagttagaaaacttgaagt ctctctaagt tactcaagta aaatgtgaga 84aaatatt acttttgaag gccgggcaca gtggctcaca tctgtaatcc cagcactttg 84ggccgag gcgggtggat cacgaggtca ggagtttgag accagcctgg ccaacatggt 8424gctgt ctctactgaa aatacaaaaa ttagccgggc atgatggcggacacctgtag 843agctac tcgggaggct gaggcaggag aataacttga aacccgaagg tggaggttgc 8436gctga gattgcacca ctgcactcca gcctggtcaa caagaatgac actccgtctc 8442aaatt aaaaaaaatt acttagatat tcattatcta aatatgaaat cctttttagg 8448aagga gtagtcaaggagagttcagt ctgggaggat gctccaggga atgcaggcaa 8454gtttt gttttttttt taactggtta actcagatct actagaacag ggtaagggag 846cagagt agacaccatg agcaaagcta accctcctga gttgaaaaaa ttatggacga 8466tatca ttgaaattaa ctgttggcag acatatccaa agaatatcgcaaggatttgg 8472ttatg catcctgaga cagatgaatg tgtggaatgg cagctggtgg gcaacagagc 8478tggca tggtggtgat acagggaaat agtttcatcg tgttaaaagc catggaacaa 8484cataa tggctgctct gcagaaaaat ccacgtcccc tctccaaagg gcctgtttta 849gatgta aaaattgggtcagataaatt ttcatattaa gctttttgtt gagtaaactt 8496atagt ccccaaaact cccactagaa cagggtgaga attaacgttt tattcatacc 85gacttaa ataatttagt gtaagcaagt gagtatgaga acacatctgt ttccagtctt 85tcattgc tttatataaa ttctctggtt ttctcctcac agtaactcagtgaggaagat 85agtgtcc tcatttggca cgtatggata tgacagcttg aaaggggtta gattgattcc 852atgaca cactgtaagt ggcagagtca ggagacacac ttaggctctt ctggcctcta 8526ttctt gctcactgtg gtatactcct taatcactac ctgggtttta aataatataa 8532cttgc tgattaaaatcagcttaatt gtagcttctc tggaatccat atcttagttg 8538cagtt ttcggttgag tgtcttctgt gtgttaggaa ctcaggcact ggaaatagtg 8544ttgcc aaatttacta attaggtaga gagataatac acgaacacat aatagaggtc 855gacttc gtaattaatc tgatctttgg gctgcttaac gttagctttgaatgcaagat 8556atgcg ttttagagat atatagcaca aactgtgaga gctcaaggga gggaagccac 8562gcttt tgtttgcttt tttgtttttt aaaaataatc ttactttgtt ctaaaaataa 8568gttat agagggaaag ctaaaatgaa gtgacgtttt cttaaatatg ttttaatatg 8574actta aaacttatttccacttaatc tgaaggagaa ctgtccagca aattcctttg 858tgtgaa gctgttttta gtgccagcat aagggctttt tactcaactt ggaaagtgta 8586gagtc agttaaaaac atagtcttca gaggcagatc tcaggtctgt tatttatcac 8592tctat gtgtcacttt ccccatctgt aaaatgggga taagaatagcacctgcctct 8598ttgtt tggaagatga gtgtccagtg ccatgccctt tgcacatagt ttaagtgttc 86aatgtca gatgtcatgt ggagaattaa cacttacttg ctgagacagt ctccttttta 86actaaac agtaggagcc tttacataac aattatcttt gaaaatttaa gaatttagca 86atcagtg catttgttgatatctttatg ttgctttgct tttaaaatgt taacctccct 8622ctgat gtttttaaca gacagtgctt cctcacaaga tttataagta tttgctattg 8628aaagg aagcttgtat ctcttaagta gctgctcttt aaattacaaa tatttttatt 8634ggatg cagttgaggt ttagtgtaca tctttaaagg tcatctttttagatggcgtt 864tcaagt attcagacta aagtgcaaat ttagaacttg tgtaacctgt gaaaacaaaa 8646tcaca attaatgctg tgtgtgtgtg tgtttttttt ttaaggatta aaaaaagtta 8652tatgt attcctgatt ttatgtttgg aaacatcccc ttttcatttt tggttgtctg 8658gctag ccagtttgagttatttgagt aaggggtgag ctcttaataa atttgacaac 8664aacag tggttcttca ctaagggcta ttttttcccc cttgggacat ttggcaacat 867agacaa ctggatgccg ttactggcat ctggtgagga gaggccaggg atgatgctta 8676ctaca gtgcacagga cagtgcttca cagcaaagac tctctggtgaaaaatgcagt 8682cattg aggaaccctg tctttttttc ttgcttcatc tcatagttga aagatatggg 8688aacat ggagcatctt cacagagctt ctttactaga ggtagggagg aacattgcca 8694acatg atttggggaa ataagaaagt atgaatcacg aaaaagggga ggaatacttt 87acattgg tttaaattaatgtaaatgca tttaacgtta atgaatttgt tatgtcattt 87tataggc atatgaagag tctggtcacc tttacaaatg tcatccctga gtggcaccca 87aatgctg cccattttgg tccatgtaac aattgcaaca gtaaatcaca aataagaaaa 87gtattag aaaagtgagt taaaattgtc ttataatttt tagtacaaaatgaaggtgga 8724atttt tcttaatgtg taggattgaa aatggtgaca acaacttacc tttctgaaat 873gttaac atatatttct gggttgccag ctgcctcgct ctatctggcc agtgagccca 8736acggt gaagccactg aaaagccaac ttaggctgac tctctggccc cactctccta 8742tttcc ttctttttgccttttttctc cctttaagga tatcaagctt cagtttttct 8748ctgcc aagtgtatgg agtttctaga attctgggat ttccttaatc agatttcaag 8754agatg attcaaagat aagccacagg ctcatctctc tgaatttcca tcttctccta 876tcagca tgctaattcc tcatcatctt gaaagctatc tagtggccttgagcagatat 8766cattg tattttgcca gcttttctgt ttgtcctcag ttggggaggt tggtcagcat 8772tttcc agtattacca gagaaccatc tgtttaaact cacaggtcag ttccatctca 8778tttcc ctctgtctca ttaatgcact cacacatgta cacaacctct ctactcttca 8784agtct aatcgtacattaaggaaatg ttttgaggtc taatttgatg taataaagaa 879gaacat taacctttat gcccttgaat gtgccagaaa cccttcagaa tctttcctaa 8796tattc tcattgaagt aataaatcct cagtttatca gtgcttacag gctcaaaagg 88aaagggc agtagtcccc tgttccctcc tccaggtatc tactttaaaccttcaaatta 88tagtatt tacttttact tttcaaattg atgtgcctat tctaccgtaa tgcagtctgt 88cctttta tagtaattga gactagggtt ctcacaccaa cacctgggcc ccatctctgt 882cctttc cctgtccttt caatgcaatt gcgtatttgg ctaactcagt actcggtgtt 8826tgtta ttaatatacatgtgttattc cctcttcagc caagcagtat atatagttag 8832acttt tacaattctt atttttccgg gaattgttat ttgccttgtt ttcatttgtt 8838atgta ctgtgagttt ttgccaaata ctttaaagac ttattaataa attttcaata 8844atgct tcacagtttt ttactctgtt cctctcccct ttttttcctggaactctttc 885cacctt tcactctttg ctgcagtctg cgctggttcc tctctgggcc tgcagcatag 8856tcttt attatgtaca cacttccagt cactatcgta gtttttagcc caaggcctca 8862acatt ctatcacatc tgttgcccat aaatatccag tcctttaggg gttctctggg 8868taagc tcttctttgtcatcaacata tgcactccgt agtactcatg tcttcacttt 8874ttctg ctgggtaagg tgccacttct ctgtttgctt tctgtcctct aaatatttga 888ttattt gcttattttc ctttctttgt ccttttggac tcatatcttt tttgcccctc 8886tattt gatagcattt gtgtaggagg gcgaagtggg aaggaagaggaggtgtctgt 8892tctga agattacaga agtctgtaat ctgtcttggc tgccaggtgt cagttttgag 8898aatgt tgatgatgag gtgaggagaa gagcagcaga gcatggggtc tgccatcctg 89tggacca tggcctgctt taggctgctt ggtgtatatg atttcatcta gctgttcata 89gcttttt cctgtgccccagcactgaac atagactcgt accattgttt tgtgtaatct 89aattggt tgcactgcag catatatatt ttttaactat acaaataagt tgcttccctt 8922ttcat gctctgatct ggaaatggat tcattaggta aaagtctttt aatggaaaat 8928ttgag ttccagtggg ccaatttatg agcagaattt ataatgtgggcatttcctgt 8934tcaaa agtaaattga actagtgtat gaagtttcac ttaaatttta aatgccaagg 894tatata agtcctttgt gtttttttaa ttttgaaatt tgtataactt gatttgtttg 8946aatgg aatttagaaa taaatttaat atagttttta gggctaacct aaaagtaatt 8952catca tggtgtcatatgtaattaaa acatatagaa tcctaaaaac taattaagtt 8958gacac cttatctcac ataacccaca tctctaatgt ctccccattg ggaaaagagt 8964gataa atcaggtgaa ttatgcctag cgggcccaaa tctgctactt ttctttaagt 897taggag ttacattcag accatggtga catggagcac caagaacttagaatcagatt 8976ttact tgacaaactc ttgaaaggtc actgccacag tctctcttga gtgcaaggct 8982tatgc tttgtagcac agggacgcga tatttctctg ctatctttgg gtagcagagg 8988acagc tcccttgtgc tttctttctc tcttttctat tttcttttct tttcctaagg 8994tcttt aaataggaggagtttaaccc catgttaggt gaattcaaat ggatcttagc 9gatgtctc ttgttctctt ttggttccag tttggttaat tcctttcatc caattttcca 9ggttgagg gagaacctaa cttgctctcc tcgactctga gcatcatcct tcactgacag 9caggcatt gtgggtagga agaagtctga gaacaaaacc tagggataaagtttagtaga 9tggggttt caccatgttg gccaggttgg tctcgaactc ccgacctcag gtaatccacc 9ccttggcc tcccaaagtg aggctggaaa taagacatgc tggaattgta agtaggacac 9gagtctag gggaatcaaa gaggaaaatg
aacagaaaag ggaaggggaa ggatattatt 9attgactc caagatgcta ctgtttgtaa gttttaccat tttaaaaata tgccattaag 9agaaatgc tggccgggca tggtggctta tgcctgtagt cccagcactt tgggaggctg 9gcggacag atcacctgag actaggaatt tgagaccatc ctggccaacgtggtgaaacc 9atctctac taaaaataca aaaatcagct ggatatggtg gcacatgcct attgtcccag 9actcagga ggctgagaca ttagtactgc ttgaactggg gaggcaaagg tttcagtgag 9gagattgt gccactgcac tccagcctgg gcaacagagt gagactgtct caaaaaaaaa 9aaaaaaga aagaaatgctgcttatttaa ctgtgttctg tcaatgttaa ggtgtatccc 9cttcagag atgttaacaa atgggaaaaa atttggaatt cattaggcat ttggaactta 9aagtttcg gccgggcata gtggctcatg cctgtaatca ctttgggagg ccaaggcggg 9gattacct aaggtcagga gttcgagacc aatctggcca acatggtgaaaccccatctc 9ctaaaaat acaaaaatta gctgggtgtg gtggcatgcg cctgtagtcc cagctactca 9aggctaag gcaggagaat cgcttgaacc cagggggcgg aggttgcaga gagctgagat 9tgccctgc actccaactt ggacaacaga gtgagacgcc atctcaaaaa caaacaaacc 9aaaaaaaa aaaaaatttcatagttacag aaagtagtat ggaggccata ccgagatttt 9acatggta gtaaaactct gcattatggc tctgttctgc atcatctctg ttctgcatcg 9tcactcca catcagaccc tggatagctt tggtgtactg gtcgatcttg tggcagtaag 9tagtgtaa ttaagaggat attttaaaac ttaacatata attgctctagttgttgtctc 9ttttgctg gttaagaaaa tcaaatttct atcctatctg aatctcatag cagactttgg 9atttctga caagtcattt cttactacct aggggaatgt acttgtactc agctagagtc 9agtatctt ctacatccag ggaattgggc tgagtgtgga ttttggtctt ggcagttttt 9ttttatta atttgcaaaagaatagaaga cttggaatgt acaagaagca taaaaatgtg 9aggtggtt ttacatgcgt tatttatcac gttaatatgt cttaagatat tttccacgtg 9aacttatg taaaggcagg aaactagtga gatttcatat tctagggatc aagagattgt 9tagtaact agcctcagaa agtatcttga aaggtattat ataaggtcaaggaactaaat 9tagtaaag agtcaggcca ggcgtggtgg cttatgcctg taatcccagc actttgggag 9caaggcag gcagatcact tgaagtcagc agttcgagac cagcctggcc aacatggtga 9ccctgtct ttactaaaaa tagtagtgtg tggtatggtg gcgcatgcct gtaatccagc 9ctcaggag gctgtggtgggagaatcact tgagcccagg aggcggagat tgcagtaagc 92gattgca ccactgcact ccaacctggg tgacagagct agtgtctgtc tcaaaaaaag 92aaaaaaa aggtcagata ggtgcctaaa gcctgtgtgt ctcgctatga gaatacatct 92gttttac tgtggttcat tgattcagac atgtagttca cattttaacctgtctgaaat 9222tatgt gaaattgatg tcatgatata gtttaattgg cagcatgttt tcatagtggt 9228ttata attagtgaaa tcttagattt gatgaaatag atatgatttt ttaaagtggg 9234ttagt gttatagaca gtttgcagga ctttttattt tgtaggtact taaattttga 924ttaatt attctctaataaagtgattg acaaggatta atgtataaat tataccttgt 9246tgaac aatctgcagt ttggacattg attcaaattc atttaggctg aataaatttt 9252actaa gtaagttttg acagctattt aaatattggg aaaggggata ttcaacattt 9258acatc ctgagagctt tgttaaattt agttatttga gacccattgggttctatttt 9264tcagc atgttgctgt aatggtaaaa tacaattttg aaattatagt tgtcttgaag 927taataa attgaccaat atgttgtatt tttttctcta cttagttaca aattgaactt 9276aagta gaacttttaa tttgacaggc cccctttgct tcctgaggta actgaaatag 9282attaa tgcttttttgaatatcttag gtttgttgct ttctttcaca tgttacctac 9288ttaac aaaagcaatt aatctcagca cttgatgcca aagaaaattc taaaaggtct 9294ttttc cttggatttt acaaagtagc tacaatggga cttttaagac aaagctgcat 93tgcttac agagcaattt ttgtttaatg gtctgtgtta gagtcatactgcatgatgac 93caactgt ctgggatacc attctgaaaa gggtttagtg ttacatactt cttagagaga 93ctccatt tctaattaag gcacacatct ggaggtgctc aagaaaaatt agtgcagtta 93ttggaag tgttatgtgt gactagttca cttcagacat cttttgtata atcagacaca 9324ttaaa tttatttaacttctcttgct tttctctccc acagagtatc tcccatattc 933tgcact ttgtagaagg cttaccacag aatgacttgc agcactatgc atttcatttt 9336ctgtc tttatcagat aacttctgta attcagtatc gagcaaataa tcattttata 9342gattt tagatgctga tggtaagtgt ttagaggttt tcttttaagataattggcat 9348ctaaa ttctagcatg tggggacttt ttggtttttg ttttataaaa aaagacaaac 9354cctga ctctttctct ctccattctc gcctttgcct tctgcccctc ctcgcatcta 936aagtga tggttttagt atcctgtctc attttttcct ttccttacat catgtattat 9366aacac atgcgcatgtgtgtatttct cttttagaca aaggatgaga ttactactgt 9372cagtt tttttttccc tacttaacat ctttgctttt attttttaga catatttcta 9378attaa acattagact tacgtagccc ttctgtcatt gtgaaataca tagtttacta 9384tacca tcaagataaa gcctttattt aaataattaa acttcttagtggaaagctaa 939gcacag tttatggatt ttgggaattt ttgccttgca tttgtctgat atggtaaaat 9396gtttg tttttctcat aatgttcact ttgtcttaga caagataact caatcccctt 94gggttgt atcaagccat tgataagggc tcactttgat ataaccattt tctgttattt 94cactctt tcacacttcctattttcctc ctggggatgg tttgaatgga tgacacaata 94tattata aaagcacttt acaaactgta acttatgtta taaatgtaat tattacctta 942tttacc ctgtttcaga tttgagtgga agtagttctt tacaatacaa aacaacttat 9426ctttt tttgcatttc aaagaatgat caatccactt caggtgcagcatggtttcca 9432gacag catggaagaa tcatttattt agcttctaaa aatgtgcagg ctgtacccta 9438gcctt ggggattagg cccaaatatc aatgttgggt gtttttggta ttggtttttg 9444cctac ccgcccttcc ttccttcgtt cctctctctc attctctctc tctctctctt 945tctctc cttctttgctccttcattcc ttctctctct ctcttttttt tttgagacag 9456cacta tattgcccag gctgttctca aactcctggg ctcaagtgat cctcctgcct 9462tcctg agtagctagg actacaggca catgctatgg caatactgtt ttaaacattg 9468aaggc tccccaggtg attccagtgt gggtcatgtg gtagagaaccactgacacag 9474caaag gatacataaa gttgtctatt taatgggtag gtgcaggtag tagataagag 948gccaca taaaccacat gcttagtgaa cggttttgtt ttgtgtgtat gtgagggatt 9486ctctg agtatatttt gttttccctt ttgaaactta tcagagaatt catatgtctg 9492tgact aatgctcacattaaaaaaag ttatgtgact ttttttaatt catatgtctt 9498ttcat ttattcattc atatgtctgt tatgtgacta atgctctcat aaaaaaagta 95ctcagtt tacttttttt atatcagatc atatatatat gttttttttt ttgagatgga 95ttgctct tgttgcccag gctggagtgt attggcgcag tcttgtctcaccaccacgtc 95ctcccgg gttcaagtga ttctcctgcc tcatcctcct gagtagccgg aatacacgca 9522tacca tgcccggcta attttgtatt tttagtagag acagggtttc tccatgttgg 9528ttggt cttgaactcc caacctcagg tgacccaccc gcctcggcct cccgaagtgc 9534ttaca ggcatgagccaccgcacccg gccatatctt atattttaat aaatatttta 954ggtctg taaatttttc tttttgggga atgtgtttta agtctgtgtt gagtcctaga 9546gttgt tctcagatag tcactagtga taccttaaca ttaaccagcc tgttggcaac 9552tggcc tgaagtgaca actaaggaaa ggtctctttc tcctttcttaatctttgcat 9558aagat tagttctttg taggaaggct ttgaagtctg gtggcaagta ccctttatcc 9564aatct taagataagg tctttctgag cattaaaaag tgactgtggg agatatgtca 957agtttt ctgtgtgtgc tctgagaaat ctttttttca aaaaaggata gatgtacttg 9576ggaaa agagaaactgagcgcacttt caatatttaa gtaagtgtct ctaacatgtt 9582acata aaatgatgac cactgtgttg gtcattactt ctctactgct aaaacaatgt 9588aaaat aatatactcc ttagaaaaaa atatagtgct ttgggtgtgc actgttgtaa 9594ggaat aggaaatgtt ttgtagtaag tgcgatggtg tttgacatcgtgatttatta 96tatcaca tttggtttca tagaaataga gtaagctacg tatttgctgt gccgcaatta 96tgacatt acacttgtat ctatttctgt ttcatagatg tgtagatatt gatatataca 96gaagtat ggattgtttt gataagtttc taatgaaagt acagatattt gttgattatt 96taagaaa ggttgttactcatccaagcc cgtggttagc ttttcccaaa ttatcatgtg 9624aagta aaatgtaaag aaatataccc tcccttaacc ccacaccacc tgttagcacc 963cacctt cctttacttc tcagccgtac tttttgtatt tttttgttgt agtggtaaaa 9636ataac ataaaattta ccattttaac atttgtaagt gtacaattcattggcattga 9642ttgtg tgcaaccacc atcaccatca ggactttttc atcaacccaa acagaaacta 9648taaac aataactccg catccttcca ccccaaagcc ctggtaacca ctattctact 9654tctct gtgaatctgt ctattctaga tacctcatag aagtggaatc gtacattatt 966cttttg tgtctggcttattttactca gcatattttc aagattcatt tgtgttgtgg 9666agcag aatgtcattc ctttctaagg ctgagtagca ttgtatgtat tatccattta 9672tacgg acatttgact attgtgaata atgctgttgt gaacattggt ggacaaggaa 9678agtcc ctgcttttca ttctttttgg cataaaccta caagaggaattgctgggtct 9684gtaat tctgtgttta atttttggac gaactgccag actgtttcca cagcagttgt 969ttttac atccccacca gcgttacaca aggattccaa tttctctaca tccttgccaa 9696gctat tttctatttt tttttaataa tatccatcct aatgggtgtc tttttttttt 97aaaggaa tggtttaaacaggttacctt cttactcctc attcatgctt tagttgacta 97aaggacc cctctcccta ttggcaccat tgaaattgtt caggcaaaaa taactgccag 97cacactg ctttaagtaa tggacttttc ccaagttttg tattaatatt tcagtatttg 972tgcatc ctactgctag tttttaaact cttcccttgt catctatcatctcattctct 9726caaat gtgaaaatgg aagctcagaa ataaaacaag aattaaaacg aatagtgatc 9732ggtaa caagcttcat ttatcatgaa aacatatatg tatgaaacat tctgttttct 9738tattg gataaattag gtgataacca aattctaagt tccaaaaatt aaatatactc 9744aagga ctttaacatggcagacaatg gtgacaaggt caagaacatg ttttagagtc 975cctttg gtcggtattc aatgatacaa cagttgaaaa ggccagaaga aagttaacct 9756ggtgg tttttgaata tctaactttc acttctttcc catcttccag gaagttggct 9762gtgat gacttaaaag gcccatgttc tgaaaggcac aagaaatttgaagttcctgc 9768agata catattgtta tttgggaaag aaaaatatcc caagtgacag ataaagaagc 9774gcctt ccacttaaaa agactaatga ccaacacgct ctcagtaatg agaaaccagt 978ttaaca tcgtgttctg tgggtgatgc tgcctcagct gaaacagcct cagtaactca 9786aagat atatcagttgcccctcgtac tctttcacag gacacagctg taactcatgg 9792attta ctttcaggtc caaaaggttt ggttgacaat attttacctc tgacacttga 9798ctatc cagaaaacag cctcagtttc acagttaaat tctgaagctt tcctgttaga 98taaacct gtagcagaaa atacaggaat tctcaaaacc aatactttgctatcacaaga 98actaatg gcttcttcag tatcagctcc atgtaatgaa aagcttattc aagaccaatt 98ggacata agttttccat cccaagttgt aaatacaaac atgcagtcag tacagctgaa 9822aagat actgtaaata ctaaatctgt gaataatact gatgctactg gtcttataca 9828tgaag tcagtagaaattgagaagga cgctcagtta aaacaattcc ttacaccaaa 9834aacaa ttaaaaccag aacgtgtcac atctcaggta tctaatttga agaaaaaaga 984acagca gattctcaaa ccacaacatc taagtcatta cagaatcagt ctctgaaaga 9846agaag aagccatttg tgggaagttg ggttaaaggc ttaataagcaggggtgcttc 9852tgcca ctctgtgttt cagctcataa tagaaacact ataactgatt tacaaccttc 9858aaggg gtaaataatt ttggtggctt taaaactaaa ggtataaacc agaaggccag 9864tatcc aagaaagctc gtaagagtgc aagtaagcct cctcccatca gtaagccacc 987ggccct ccatcgtctaatggcacagc tgcccaccca catgctcatg ctgcttcaga 9876tggaa aagtctggaa gcacctcatg tggagctcaa ctcaaccaca gttcttatgg 9882gtatt tcttcagcaa accatgaaga cttggtggaa ggtcagattc ataaacttcg 9888aactt cgtaaaaagc taaaggcaga aaagaagaaa ttagctgctcttatgtcttc 9894aaagc agaacagttc gaagtgaaaa tctagaacag gtgccccagg atgggtctcc 99tgattgt gaatcaatag aggacttgtt aaatgagcta ccatatccaa ttgatattgc 99tgagtct gcatgcacca ctgttcctgg tgtttccctg tacagtagtc aaactcatga 99aatttta gcggaattattgtctcctac acctgtttca acagagctgt cagaaaatgg 99aggtgac tttaggtatt tgggaatggg agatagtcat atcccaccac cagtaccaag 9924tcaat gatgtttccc agaacacaca tctgagacag gaccataatt attgtagccc 993aagaaa aatccatgtg aagttcagcc agactctctg acaaataatgcctgcgttag 9936taaac ttggagagtc cgatgaagac tgatattttc gatgagtttt tttcctcctc 9942taaat gctttagcaa atgacacatt agacctacct catttcgatg aatatctgtt 9948attat tgaattaatg cttgttaact tttttcatat aatatttatt attattagaa 9954tacaa tgtgttcaggtagtgtttat acactggact tgtgtaatta cttgtgtaat 996atgaac aaaatgcaag gtttaacctt tggttctgcc catgaagcat gtaatctttc 9966catta aaatcactga atgtgttctc ctttttggtt tcattttgtt cttgtgagag 9972ggatt tcaaaatgtt aaagatgaaa agtggcgtct agtttctgacagtttgtaca 9978atgca ttacattttt agatttgaag ttttggttat gttagtgtta tgagtgatct 9984gtggt tttcttcccc tggaaacctg ttgctcgtgg cgctttgccc acggtgcccg 999cttgtc ctgtgtccag atatgcagac aaatgaaggg tgaagaagaa gaagaggagc 9996ttagt gttagaacagctcagaagga gacccacagt gagcagctcc cctgtgtcgg cgggcaggtc gtccctcaag tgttcagctc tcagcagaga aaaggccctg gagagggtga ctcctctcag ctctcagcag agaagcagcc ctggagaagg tagcttctgt tcgcaggcag attgtccaga ggtcctgctg ctctcagacg gggccctgga gaggatagcttctatccata ggcaggttgt tctgccgtct ctacaggtct ctgaagctct tagcagagag ggtagctcct ccctgttgct ggtcgtccca ccctctgctc agttctggct gagcctgggg cattttacgg gcctcggggg aggaagtgca tacttactgg cctggaaaag gcaccagttc ccactcctac aggtgggactggcagcctgg ccctcagcct tcaggccctc cctgttcatg gcttccaggc ttacccccct gctttgatct gagagctggt gccaatagca gggagaagcc aagctgcaga ggcaagcact tccgagcctg caaaagcagg cccccaaaag tgcagggatg cctgagtctg cacccgcacc caggagggtg gagatcttgc ctgctccaaggctgcagccg gaatgatagc aggctgactg gagcacctgc caccatcatt agttcaagag tttatgcaga tttaagttgt atacggtata tgaatgtgtg acagttttcc ttatggttgt gtggccttct gtaagagcct acgcctgttt gttacaccgg tagagtgctg tggaatgtaa actttcccta tgtcacttat ctcctttatc tctccataca gaggagggca agaaaccttg ttacttgaac tttagtaatg ttaagtgatc aataaatcta taaataaatg atagcagaaa aaagttacct gtttttgtga tgatgtacaa actttacatg ttatcacaaa taccatcttt cttcccaaga catttacttc tgtaaccaaa gtgggacacc atctaacagttctgttttgg gagagagtaa taaccagtgc ttgtgaggct tgttagatgt tggttgtgat atatgagata gatgttattt catttagacc tcaacattcc tgtgcgtgag atacttttat cacatcttac agataaggag actgtactca ttcagttgtg gagctgagat tgagtagagt ggctattaca gcagttgagt gctgagcttatcaatatatg ttccactcct caggcttcat ttaaagtagg atgcccaaac agcaccactg ccgtagagat ttgagttaac agcagtactt actgaggttt aaggctggca gccagtgtcc ttgcagtaaa attatttgct agggactcag tacttcataa tctatttgtc agatttactc ctaagcttct gtgttgttttattttttttc tgacaaaagt agtgcatatt gtcaaggaaa aactaggaaa ataccaaaaa aaaagatttt tgaccatgca ttttaatact tagtgactac aaacattttc ctattttatg catatagatt ttaaataaac gtgagatcct attgtatctg ttttaatgga taaacattgt ttcactgttt taagattctg aggtgatttatactgtcttg ccattgttaa ttgcagcagt tagccttgtt gataaatttt tgcatggatc caagttttgt tttccaggag tggagttgct tggtcaaagg aaatgcacat ttaaggtttt ttggtgattg catgactgac ttccctgggc cctcgccaac actaggtagt agtattggga ggaagggggg aaccaatcctgggtgctcca agattactag tgagcctgaa cattttctat aactattgtc cacttgagtt gttgttttgt tttttttttg gtggaggcgg gggtgggttt aagaattgct tatcctttgc ttgtactaat tatcttttca acaaatattt ctagattact gctaaggacc aagcactgtt atcagcctga gataaggcag cacactagaaggaaatcctt gctccttttg agtttgcctt ccaaacatgg agatcaatat ataatgttag gtagtaatag gagatacatg cagttgattc atgtcatttg tagtagttat ggtcaataaa gttgccttga acactgaatt agtataaact gaaatactgt tcctagggga aataggttcc tgctagcctg tggtcatgag atttttgtca aacaatcact atataacctt ttctgtttct gtttaaagac atgttatttg atctatatgg ttgattcttt acattaacat ggccaacagc actgtaactc agcctgaacg aagcttatct gacacatggt gttctccata aggcacatca tagctttctg tgcttaggaa cactagacgg cacttcagca ctgcacttgaggacgtttta aacagtgaaa tcaacaaaaa gcacaaaaaa atgcaacaat aggctgggca aggtggctca cgcctgtaat cccatcactt agggaggccg aggcgggcgg atcacgaggt caggagatca agaccatcct ggctaacacg gtgaaacccc gtctctacta aaaatacaaa gaattagccg ggcgaggtgg caggcgcctgtagtcccagc tactcgggag gctgaggcaa gagaatggtg tgaacctggg aggcggagct tgaagtgagc cgagattgcg ccactgcact ccagcctggg cgacagagcg agactgcgtc tcaaaaaaaa aaaaaaagga acaataacaa agacactagt cccccaaaaa tacacttgtt tacagtgtga actgaaagaggaaggtggag tattgacttg tttgacctca gctggaaatg tgcacgtcct gtgactcaaa tttttctctg ttctgtgcat gcatgtccac gaataaccac aagaagcact gaaagcattg atttttaggg ttacaaatta attttagcaa gtaaatgaat tcacaaatac ggaatctgtg agtaatgagg actgattctt tttttttttggagatggagt ttcactcttg tagcctaggc tggagtgcaa tggcatgatc tcggctcact gcaacctccg cctcccgggt tcagcctcca cctcccgggt tcaagcgatt ctcctgcctc agcctcccga atagctggga ttacaggctt gcaccaccat gcccggctaa tttttgtatt tttagtacag acggggtttcaccatgttgg ccaggctagc ctcgaactcc tgacctcagg caatccaccc acctcagcct ctcaaagtgc tgggattaca ggcgtgagcc accgcgcccg gccgaggact gattcttatg tcagatggca ctaaatgcta tggagaagag gagtggatga gagggagaag tattttagac caggtagact tggaaggttt cttggaggtgggtgatgttt gagaagaggc ttcaataaag ttagggagct cgccatgtga ttgcaggaag agcgttccag gagaacaaaa gtcatgaaga gtgagtgcta ggcatgtgtc tggtctgttt gggctgctat aacaaaatac cttagactgg gtaaaatgta taaataatag aagtgtattg cttatagttc tagaagctgg gaagtccaag atcaaggtat cagcacattc tggtgaaagc tgctctgctt catggctggt tctctcactg tcctcacatg gcataagagg ggcacagagc cctcaaccgt ctctccagtg gccccatctc ttagtactgt tggattgggg atttagactt cactaatttt ggggggacac aaacattgag accacagcag catgactgaggataagcaag aggccagtgt ggttgagcag agtgatcagt gaaggagagt taggacatga gtaaagaggc tagcagacac cagatctcat atggctttgt aggccatagt gaggactttg tttaagctga gaataataga taacctcagg aaagtttcag gcaagagggt aacatgatct gatctgggtt ttaaaaggat cactgaagtggggagactgt ctacagatgg tctgaatagg agtcctagtc tattacaatc tccttggagt ttagggtggt aactggaggt gttcaagagt agttggatta ctgttggatt tcaaaagtag agccaacacg atatgtgcat tggctgtgag gtagaagagg agtcaaaatg aactccaggt tttattgact gagcaattgtgccatttcct gagatgggtc agatttggga aggaaagaat ttaaagggga taagataatc ccattaggag tgtgttaagt gtgagattcc tattagactt tcgagtggag atgatttaat aggaagatag atctgcaaca ctggagctca gcggagaggg acaccctgga gatagccgtt tgggaattag gaatgtgtgg atcatgttataggatggggt catttaggga cttaaaacag ctctgaagaa caaaaatggt gccttgatct tggacttcct ggtttataga actgtgagca atatatatat atttttttca agacagagtc ttgctccgtc atccaggctg gagtgcagtc gcaccatctc ggctcactgc aacctccact tcctggttca agcaattctggtgcctaagc ctcccaagtg gttgggacta taggtgtatg acaccatgcc cgactaattt ttgtattttt ttgtagagac agggttttgc catgttggcc aggctggtct caaactcctg acctcaagtg atctgcctgc cttggcctcc caaagtgctt ggattatagg cgtgagccac catgcccaga ctaaatttct aacatttataaattatccag tctaagatat tttgtgatag cagcccaagc agaccaaggc aaaggccaag cacacttgct cctcctgact tttgctcttc ctggaatgtt cttcctttag tcacatggtt gcctgcctag cttcattcaa taggagtgtg gtgccctgaa aatacaagga agaatgcttt tctttttttt aaaaggaagg gatgattatc tgtcagatgc tgctgaaaaa gagtaataga gtaattggcc actggctctg gcaataggga agttagctct gctaactcca catgaacagt ttcacatgaa caagtgtgag tgggctcaag agaagggatg gtgagaaagt ggagctatgg actcactctt gaaacatttt ctggtgcctc gtagggcaat gtgaggtcaaggtttttgtt actgttctga agatgggaga ggctgacaca tggatgttgt aggtgagaga
aggggcgctt gcgggggcaa acttctccag ggatgggatt ccagtgtcta agaggaggcg gtgtgaccct aagagctaga aaaattattt tattaatagg aaagacaaag tacttaggct cagatgctaa gagatttgct gataaaagaa tgagaacggt ctcttctgat tattttcttg gggaaataaa tagatcatcagctgagggtg tgaggggaga aggagttgaa catggaggaa gacaggtgtg aaatattggt ctcagaatgg agagcgaatt gaatagggac atgcagtggg cttgctaagc tgtgcggaga gcccgtggga agtttatggt catcaattta atggcgacca gccaagatgg tggtttattt ttctccagtt gtatttaactgctcaggtgc aggacagaga gactaagtgt gaagttaatt tcagccaacg tagaggaatt gtcaggcaga tgggacaagg agatagagga gaaaaggaat aaggcttcct gcaagggtaa tgattgtagg gatggataag taaggaacac aggaagtggc tgtctgctga gtggtggcag agctcagtgg gtcagagcaa ggttcaaagaatggcagaga ggcacttgtg gaggaagtaa gctggctaga aagtagtgtg cttgaaatta agcttctgga gatagcaagg ttacaggtga tgacaaagtc tgagtatgac aaggaaactg cagggccaga gttggcaaga attcatgaaa aatgaggaga aagaggcacc aagaggctgg gatagcacat ggattgtctc tgtgtgaggc aaagtcatct aaatggcagc agtggcccta gcagaaagaa atatacagtg agccggagca aaaatcctca aggacaggca gaacgccatg aaaacggcag atgacagcca aaggagcagg ggcaggggct cagtccaaag tgtttcagag tcactggagg gttgagtggg aaggggaggg agtggctgaa atggcaacaaggaagaacct ctctcatctc caggcccaaa agtatgtgga atgcgggaga taagacagcc accactggcc agggctgtaa agggacattc agcgaatatt caggttccat ttagcacgac agcagggaag ggactgttgg cagaaaaaaa ctggggcagt gggattaaag acagaccaca cattccaaaa ggcaccgtgg gagggtcagggggcgaggtt aggtctaggc ttcagtgtcc tgggagactc agtcttcaca gggtgacagc gatcaagagt gcagcttagg ctgggtgcag tggctcatgc ctgtagtccc agcactttgg gaggccgaga cgggaggatt gcttgaagcc aggagtttga gaccagtctg accaacatgg caaaacccca tctctactaaaaatacaaaa atcaactggg catggtggcg tgtgcctgta gtcccagcta cttgagaggc tgaggcaaga gaatcacttg aacctgggaa gcagaggttg cagtgagctg agatcgtgcc actgcactcc aacctgggca acagagtgag accctgtctc aaaaacaaca acaacaaaaa agaaaagagt acaacttatg aaggggtctcctggggagag ggtttttggg attctcctgc ctctcaaagt gctgggatta tgggcgtgag ccaccacacc cagccgaggg aggctgagtt ctaattgttg tatctctctt gggattggcc tcctgggcag tttaaaagac aaggcaagga atcttttgga gaaagagact gggggcaagg tgtgtctgaa caagaagtgtgagaagctct gtgggctccc ttcagacttc cagtcgttga attgggatct catttatatc agctctaggt gtaacgatat taaatcttct ctgtcatttg gcaattttgg tttatgcttg atcatcattt ttaatgtttc gacatgtaga agtttaacat tattttacat tcttttcctt ctggcatcat gttttagcaa gattgtttccaccaaaagaa tatatatatc ttctaatgaa actacgtttc tttttttttt ttcctttgct ttctcttttg gtatatgaat ctttgattat ttgtaatgta ttttgatgtg taacactgaa gtttctattt tgtactattt ttttccccaa acagtaaact tattgttcaa atacttattg aacaaccttc actattcttt aaccatttag aatacgccat tcacatatct ttcatactac atttaataac attttttaat taaaaaatat tctactgatt tgtttatttt gagaccaggt tatgaaactg gctaattttt gtatttttgt taaataccga aattcactgt gttgccaagg ctggtctcga actcctgggc tcaagcaatc tgcccacctt ggcgtctcaaagtgctggga ttacaggtgt gagccgctac acccggccac acccggccaa cacatattat ttgttattac atttaattcc cacagtacat tgaaattatc agggaaaagt tttcagtgaa acattattga acgccacatt aaaagtgtaa attacaaaga tttaatgcca atttttcaga agaaaaaaga ccaggaggaa ggtctatgaagttttagcca gtctctcatc cacctaccat ttcacgatca tgcactgtgt aagtcaggaa aagagtaaga aaagtgaaag atacaattga ttagagagtt ttgctggata ctatagatga aaagaacaca aaatggaaca gcctcttcaa gcttagagtc aacggctgta gtcccaaaga ctgtagtcag aggcggtagggccaaaagac atgacttatg gcattggagg aagaggatgc tttgggagtt catggtagaa gaggcggaaa aaatctggtg gattaaagaa agcatcccaa agtgacatta aactaatgac taaattctga gctgttttca ggggcaaagc ctgtttgggc acccctgcca cacttaaaga gtcacctagg tatggttcgt gggctctgaacaggcctgct cagtgaacat atttgtgact gtttctccgg cccttttagc tgtattgagt aaaatttaaa gagaccattg ttttggccta agctcctgcc ctaggcccaa agaacagacc aaacctgaat ggcttcactt gtcctaggtg ctgtgtactc aaactgaact ttgaaacagg tcggtttttc aaaaaaagcaaaagattcac agcaaccaat tagaagaggc ccggtcaacc tgagccagca tgatgaggct cttctgcttt aatcctacaa ggaaagaaac tttgaaatga ccaatctgct ttcattcttg gtttctgctt tctttggtct atttctgcct gtaaaaccta tctcctctgc tcagctcatt gaagtaccct tctatttata gatgggatgctgcccgactc atgtatcgct agtaaaagcc aattaaatta ttacactcga tttgttggaa ttttgctatt ttgacagctt ttcaaaaaca ccagtaggtt cacatcccta attccccagc cagtgttccc tcaaggaacc atggaagaag caaaggtggc tgaaaggcgc ctcaggatgc ttctaagcac ggcacatcca tgaaaaggca cttactaata tttgcaggat agcaaagcac tgcagtgacg ataaatctag tattggagaa gttcaaaata atcagtagat taacacagaa gccagagctt atagggagaa aaggaaccct atgaaatact tcaaatccga aaacgaacat gcatttcctg tttagttagt gcaggtacgt aaaagcttgg taaagtacccttcttgccag ctttctcttt cttacaagcc ttttcactgg gctgggaggc tgatattatc taaatatgct gaggaggttc aagtatctcc acaactcacc tcagagtgaa tgctcccctc ggccttaagg caatataaac cagccctgtt tagcaggata gcaaaatgtt tgcggttgta aactggtgtc ccattggctg tggcgcttgtggtgtaaaga atccctgtgc ttggtaatta atagagaaat tctatatttt aaacttcagt tgtatattgg ctcttatcca tggcagattt tcacgtatgt gttatttttt tatttattca gagccggagt ctcgctttgt cgcccaggct ggagtgcagt ggcgcgatct tggctcattg cagcctctgc ctcttgggctcaagcaattc ttctgcctca gcctccctag tagctgggac tacaggtgca tgccaccacg cccggctaat tttttgtatt ttagtagaga tggggtttca ccgtgttgct caggctggtc ttgaatttct gagctcaggc aatccgcccg cctcggcctc ccaaagtgct gggattatag gtgtgagcca tcatgctcgg ccctatgtgatatttattac aatgaattcc aatgatcaga cctatactca agtataagtg aatatatcat tcaatgaagt ataaatgatc attatgttca tattcacaca tacaataatg tactcaagtt tattgctaag gtaattcaga atctccttat tttgaagtgt gcatttgata tacctgtttg ggaataacta gtttcttatctttgacagaa aataattttg ttgttttgtt tttactaaaa aagcatggtg aaaaatggct ccatttctaa gagaggtaac taaaatatcg caatttgctg ggtgtcatta aagtaactca caagggaaaa aatgcaaatt ggtatctgct gatggagtaa atctccgcag aagtgatgac cctgaaagga tcaatatatt aaagcccctcccagctggtc attccagatt gcaacaataa agcattaagt gttaaaacct caaggcagct tttttttttt ttttttgtct caagtccttt attattaatt ttatagacct acttaattac taagccaaaa aaaatcaaac ttgtttctct ttgtgacttg tcaatagtat taaactattc tggtttttta tttttgtgtt accttaaagt ctccagttta gtaatttttc tgtacctaaa cacttcggat ttgacatgct ttgtggcctt tatcagtagt tagaatgtaa atccaataaa taaagtaaaa gccaggtctt caaaacctgg gggccaagaa ctctgtttta gagggcctgt gactctcttg gacactggac aaaatctcat ctctaaatat ggatattttagggagagggt ctttaggctg tcatttggat tttcacaggg ctccatgtat ccataaggta gtctcttggg aagtttgact tcaataaatg aagtttaact taaacctaaa atgaaattta actgaaaaac aaaatccaat gaaagatgct ttcttatgca aaaacaaaca aacaaaaaaa aaacaaaaaa accccaaaaa acccaaagccaaagattgtt tctgaaatta ggttctaggt tccagagcaa ctccatggtg gggaatcagc cacatgtaaa gtaagctaag agtttggaca atttgtaata tttattccta ggtttcttta agaccctttc agattttgaa ttcctattag tagcatcagc caggttctaa atgtaggcat caccatagac acttccccactgctgcagtc cccaacactt gcccaatttt cccttgaatt gcacccatgc tgccttctcc aggcctattt gaacccagaa cctcgttgtg cctcgtttga aatataattt cctcctaact agtctctgat ctactatttc ccctacattg ctgccacact aatcacctaa aatagatttc attctaccct gaaacagaaa tctctaataagttactccct tcccttacgg ggtaaagtta gccacatcct aggtattcaa ggaccttcca ggagctaaga acatttcccc tgcaccttct tgaagtacac ttgtcctatg tactggttat gttcatttct taccctcgct ctcgttttgt ctggaatttt ccttggcctt aaatgcctct cacctgcctg cccacatctctcagggttgt ttcaaatcct caatgaaggc tcacagcccc agtctatgtt ggccacttac ttcgtggcct gggaacattt ttctttggct gacttgctga cactccatca gatgcatttt tatctggttg tccatctgtg aaccataccc tgagaaggca gagagtgcct ctgcactgaa catgtgctag gggacaggtc tgtgctagaggggcaagcac tgggaatgaa gaactggtcc ctactcccaa ggagttcata tctcagtgga ggtgacaagc aactcactgt ttccgggggt tgtggtgact gctgggagaa ggggtgtcta tattagatcg aagcagcatc aggggaggtt ccctgagaag gtgatgcctc agcggatgtc tcccagctaa gtggggtgga ggtggagaag ggcagagcag ggagaggatc taggtggggc gtgtaagtct gcatgggtaa ctcagggaac ccttggtaac tgcatgtaac tgtgtgaagc tttcatgaag gaacatggta ggagactagg gtatggacta tagaagccct tttgctaagc tcaagaattt gaggccggga gcggtggctc acgcctgaaa tcccagcactttgggaggcc aaggcgggcg gatcacgagg tcaggagatc gagaccatcc tggctaacat ggtgaaaccc cgtctctact aaaaaaaaag tacaaaaaat tagcggggcg tggtggcggg cgcccgtagt cccagctact cagggagctg aggcaggaga atggcatgaa cccgggaggc ggagcttgca gtgggcggag actgtgccactgcactccag cctgggcaac agtgcaagac tccatctgaa aacaacaaca acaacaaaaa atttgaagtg tatcttgaag gaaatccctt ggagcctaaa aatgatcatt gataacagaa aatgatctct gctctcgcct agggtaatat attcagcttc aaagtggaag ggcatgtttt ccaagggcat gttttctaagtccctgtaat tgtagtgata gcaaatatat gccctgcatc ttgaaatgta agactaggtt tgaacagtat ataaattatc ttatgatcta atttcccctc attttgtggt ttctactata agctacccag aagtgtagac aggacgtttg gaatttgatg ggcatcggaa agattcctac ctaagaacat tttttttttt ttttttttttctgagaagga gccttgctct gtcacccagg ctggagtgca gtggcacgat ctcagcttac tgcaacctcc acctctcagg ttcaagtgat tctcctgcct cagcctcctg agtagctggg actacaggtg tgcaccatca tgcctagtta atttttatat ttttaataaa ggcaggattt cactatgtta gccaggctggtcttgaactc ctgaccccat gatctgccca ccttggcctc ccaaagtgct gggattacag gtgtgagcca ctgcgcccgg cctctaagaa aatttttgag agctacttgt tctgttgcct ggaattccac cgtaagtacg acgttgtgtc tccttctcca gggctactaa ctaaacaaca gagggtattg tgttatcgac aattatttgattgataacta tcagcaaaca tttgccaagg cattccttta aagatagcct agtgactcta ttaactactc cttcttccag gcttctaagt tctgttggag gtaagtagat cccagagata aagcacctac cataggacct gaatcttggt agaaataaat tatatcatca tgttatcata ttatcatgtg tttttctatc tttaaagtct tatgtgaata ttctgcttga aaaatatgtg tcctctgtta gaccagagtt gaaaatatgt tattcaagaa cttgtaacag gaacccgcac aatttctgct ggagtttaat ttcagggtta attctgtcag caatctaagg taaacattaa catttttccc tagattcaag tccgttgtcc aaaagctgta acagaacttaactgaataaa tagtttctta agatggtaag cttccatatg cttataatga ctcctctaca cgttttcatc tggaaggctg ctcatgcttt tggaagcaaa gaagacaatc ttaaataact acatttgctt tttggtggtg ccagattttt ctgagaaaca ccaatggaat ttataaattc accagtcaat gggcaattga gttgctgttttgctattacc actgccgttt gtgagcattg ttgggaaggt gtcttgaagc acacgtgcaa gtttcccttg gataagtagt aggaatagaa ttgccaaacc atggcttcca gtgcagacac agtctctccc ttgggcccag ccactaggca ccacacatta agaggatatt gtctgtccat gtcctagaaa cgttgtagcatcatgctcct attcgattaa aaatctcatt attaaaatga accatcgggt aaatgttgtc tcgggaaaag aagcactgac cgtccctggg tgggctcgaa ccaccaacct ttcggttaac agccgaacgc gctaaccgat tgcgccacag agacccagtt actcaggccg cgctgcggtg tgtacagatt tccgcggcgc cggcagccgctctagccacc ctgggcgtcg ccaccccagg cgttgccacc ccaggcacgg gctgagaagt cgcggggcgc gccgaggagg cagcggaagc ggccgaggtg cccagcggcc gccgcggggg gagaggctgt gccccggcgc gcgggagggg gcgggcgagg ccgcgtgact ccgggcttct ctggggacga agcgcgcccctcgtggcggc agcggccagt ggtccgcagt cggcccggac tcggggtagg aaagatcctc tcagcaatgg ctgcgcgcca tgcgtgctct gcggcgggga ccgtgccggc cgggcgcgcc accagtaacc agggacccag gggagaacct gccaagggga ataggtcgca cggagagaat acgacacgct tggagggaag aaccacgtgctgtacaggtt taaaggatgg agagtcacgt gcgcttaggt cccaaactta agggacctaa ccctttttct gggttgccgc tattgcccct tctccttaga cagtttttca tctcatcacc tctcaccccg taaaatgcaa cgaacataga taggctgtgt atcaatgtag actgtatgta tatctgtgct tcgtacataa aaagaatatg atttttgcca ccttctaaga accaatttgc accccatttt gaggcatatg gcctctgttg agattgcata gtttagggga catcaaaaaa gccttataga gggactggca attaagatag cctttcagtt tgaaatggcc attgaaggct tctccctttc cctgacttct gaattttttt tttttttttt tttttttttttttgagatgg agtcttgccc tgttgctgga gtgcaatggc gcgatctcgg ctcactgcaa cctccgcctc ccgggttcaa gcgattcctg cctcagcctc ccgagtagct gggaatacag gcgcctgcca ccacgcccag ctaacttttg tatttttagt agaggcgggg tttcgccatg ctggccaggc tggtctggta ctcctgacctcgtgatccgc ccgcctccgc ctcccaaagt gctgggatga cattacaggc gtgagccacc gtgcccggcc aattttttta ggcgcactgt tcagtggcac taagtacatt cacattgtta tgcaactatc accgccatcc atttccagaa ccttttcatc ttccgaaaca gaagctccct acccattaca cggtaactcacgattcccct cctctagtcg gaacaatcac cattctactt tctgtccctt tgaatttgac tactcttaga gacctcatgt aaatggagtc atacggtgtt tgcctgtggc tggcttattt cacttaccat atgtcttcaa ggtccatcca cgttgtagcc tgtgtcagga tttccttcct ggataaggct gaataagctg cactgtatgcaggtatcgca ttttgctttt ccattcatct ctccgtgaac attagggttg cttccacctg cagctatgaa catgggtcta caaataactg attccctgct ttcaattctt ttgggaatat acccagagat ggagtagctg gatcacatgg tttgctattg gctgtaccat tttacattcg caccaacagt gtacaagagtccctatttct cctcatctat ttttttttta aataatgggc atcctaatgg gtatgaagta tcatctcatt gtggttttgc tctgcatttc tctaacgatt agtggtgttg ggcatctttt ccagacacca ccaatctgaa ttctatggcc cttcgtttac tcacttcctc ccagcaagag ccatttctgc ttcagcaagg aggaagctgcgactgataga gggaaagggc ccagggggct tgcagagtgg ggcctgtgcc atgcaaggag aggagaagaa ggtggatctt tgagtaggac tatctggaga tcctgctttc acaaggtcct tgcttgtgtg ctgggcagct tttggagcta gttatcttta ttttagccct tgagggatat ttaggcatgt ggtgcttgtg agcagccaat ccatgaagaa ggaactgatg gtctccacct tggaaatatt ggaagagata atgccgtcca aattgcagtt ttagaagtta acttaaaatt atgctatttt aatggaattt tgggtgcatt tccattttct tcttaagaat tgctggaatt tcttaagtgt ttaggtgatg atctcttttt gtgattcctt ttttaaaaaacaacaacaaa atctttcaaa tacataagaa ataggccggg cacggtggcg taatcccacc actttgggag gccgaggagg gcggatcatg aggtcaggag atcaagacca tcccggctaa cacggtgaaa ccccgtctct actaaaaaat acaaaaaatt agccgggcgt ggtggcgggc gcctgtagtc ccagctactc gggaggctgaggcaggagaa tggcatgaac ccgggaggcg aagcttgcag tgagcctaga tcgcaccact gtactttagc ctgggcgatg gagcaagact gtctcaaaaa aaaaaaaaag aaaaaaaaag aaagaaatag acctttattt ttctgtaact ccacaaaatt tctattttga ttccctatta ttttgctatt gtcaacacagtctcagtcaa ttcaagatcc tgtttgtgcc tttccctgga gtcatttcca agtgctaagg ctttggtcca tgagtcgcat gtgcacactc atggctgtag agggagtttt gctcccggtg aaggtcttgg tggctcttct ataccttgat tgagggaaag gaatcttatg tgaagttagc tttgttgtat cagatattcc ataaagccatttctgggaca gtcccctctg tttatcggac cacaagcttc tctgtcctca tcaagcccac ctttatactt catttctcca gacttcatgt ccagactgtg ggatgaacaa gtggttataa ggttttagag gctcctgtag gactagatgg aaggcaaaaa aaggaaataa cctttaagca tgctctcgat tccttaaatcccatctgaaa gtcttaagga tgtcttctca gtcatactta tttgacaata ttacctaatt ttctccatta gcccaagctc aggggtcttt cttcttccat attcacatgg gtgcaatggt tttctgaaag gaaaacagca ttactagggc agtaacattt aattaatcac aggtacttat caaactacaa aacaggcatt ccaggaactgggtgtttctg tttgtaaaat tacactctcg tgtacatgct cccactaaaa tgtaagttcg ctgaggatgg aggttttggt ctctttgctc tgtgctgtaa ccccaacact gcagcagggc ctggcacata gcaggcatgc agggactatg cactgaatca atgaggaaat gaaaaccagg accatgaagt aaactggaca aaataaaatg tgatagaaaa tctaaattcc taatacataa ggagcactta tcaattgata tttacaaaat ctttttacaa ttcaattaaa gacaacataa aacaaataag aatggggaca ggaacagaaa attcccccaa agaaaaaaat atatatacat ggtacagcca ttgtggaaag cagtatggag ttctcaaaaa tattaaaatagaactatcat ataatccagc aatcccatcc ctgggtatat atctaaagga aatgaaatca gtaccccaaa gaggtgtctg cactcccatg tttattgcag cattagttac aacagccaag atatggaatc aacccatcag cagatgaaag gataaaggac atgtgataca tatacacaat ggagtagtat tcagccttaa aaaagaagaaaatcctgtca tttgcaacaa catggatgag cctagagaac atactaaatg aaataagcca ggcatagaaa gacaaatgct gcatagtctc acttaggtgt ggaatctaaa aaagtcaaat taaaaaaaaa tgtcaagcag agaatagaat ggtagttgcc agggactctg ggaagtagca ggggtggggg tggaggggaggggatgggca gaagttggtc aaaaggtaca aagtttcagg tagacaggtg taagttctgg ggatctattg tacagcgtgg tgactgtagt taatactgta ttgtgtactt aaaaattgct caccaaaaat gttctcacca aaaaaatgat gtttggatat gttaaacagt ttgatttaat cattttgacg tgtgtgtgtg tgtgtgtgtgtgtgtgtgtg tgtatacatc aaaacatcac attatatacc atatacaatt aatatataca atttttgtca aagaaaaaat gcacatgacc aatatgataa aagtttagtc tcactagtaa taaaaatcaa aattaaatga aataaaaatt tctttcccca aatcgcaaaa gagaaagaaa ggtaatacta aaacacagtcacggtgtagt gagagggctg ctctcacaca ggactgatga gaataaaatt ggagagcagt gtggtaatat acatattaaa caatgtatat accctctcat tttagaaatt ctatattaga aatccatcct aagaaaataa ccagggatgt gatcaaaatt ttgaatgcag cagcacagta ttatttataa tagttataaa taagaaacaacctgaatgtc cagcaacagg caaaaatgat aaataaattg tggcatattt aagctggtgg ctcatgcctg taatcccagc actttgggag gctgaggcag gaggatctct tgaggccagg agtttgaaac ctgtctgggc aacataacga gacccagtct ctacaacata ttttttaaaa ttaggtgggg catggtaact catgcctgta atcccagcac tttgggaggc tgaggtgagc agatcacctg aggtgaggag tttgaaacta gcctggccaa catggtgtaa caccatctct acaaaaaata caaaaattag ccagggtggg gtgcgttcct gtagtcccag ctactcggca gactgaggta ggagaatcac ttgaacccgg gattcggagg ttgcattgagctgatatcat gccactgcac tccagcctgg gtgagaccct gtctcaaaaa aaaaaaaaaa agaaaaagaa aaaattagct gggcgtggtg ctgtacgcct gtagtcccag ctattccgga agctgaagcg gggggattgc ttgagcccag gaatttaagg ctgcagtgag ctatgattgt gccactccgc tccagcctga gtgagaaagcaagactctgt ctcttaaaaa aaaaaaagtg atatattttt aaaatagagt atattactta tatagacatc aaaaacaata ttttcaaggg atatttaaaa acataggatc atgacaaaat gtaaagttca aaggtaagat ggagaatgga gaactgtggg gaactgtata atctgacaat tcgtagttgc atacatctttctgtgtgctg gtgctgttag aacactttgt acgcatcacc tcatttaagt tcagcatccc taggtggcag atactattat tatattccag ttttgtttca cgttgtatat gcggtgtgag ccccaatatg ggatgtgtgt gtgcacatgt gcagtatttg gaaagttcta tgaaatatta ttagtggtta tctctgggag gtgatttttattccttttcc agtatgttct caagcatttg ctgcaagcag tcttttgcgg ggccagggtt gagaggcagc agcagtttcc ctaaattaca gatagaggga ggtaggtggt tatgcttggc cagatctctg tctaggggta gaggagtgcc tgtgtgtggg tagggacacc ggcggggggc tttgccaaac acagtggaactgtcacgctg gtctctcttc tcaactcttt cactcacctg agaaaagggt gtctatggac catgcacact tctgtgggga attttacaag atgtgaatca tcagtgatga agatgctttc atttaaaaag aattggagta cctgagatta gagataactt ctaccctttt aaaatatttt taaaaatttc tttgcactga ttttttttcttcgtttttat gagttgtttt catttgggtg ggataactca atctacagga
gaatattaag actttttaaa ttttaaaaaa tatactttca aatacttaat acattttgtg ttaaatgaca gccagcagat attgactgaa ttgggctaga tgcttcaggg atctcccttc catttaagac tctccgagag gccattcctg actgcaggtc actgtattat ttttaatttt aaaattttta cttacttattttatttaatt ttattttttg agacagagtc tcactctgtc gcccaggttg gagtgcagtg gcacaatctc agctcactgc aacctccacc tcccgggctc aagcgattct cctgcctcag cctcctgact agctggggtt acaggtgcag gccaccacac cccgttaatt tttgtatatt tagtggagtc agggattcgccatgttggcc aggctagtct caaactcctg acctcaagcg atccttccac ctcagcctcc caaaatgctg ggattacagg cctgagccac cccactcggc ctactttatt aatccacttg cagaaacagg atatacacaa aaacgtttca aggctgtaag tgccactgca tggcaccaat ggtaaacgtt ttacaaattt gagtcaggaacaatcattag tgtcactagc aacaaaaatc aaaattaaat gaaataaaaa atttctttcc ccaaatggca aaggagaaag aaaggtaata ctaacacgca gtcagggtgt agtgagaggg ccgctctcac acaggactgg taagtacaga gccatggagt aagcaggtct tgagctgaca ctggagagga tccttttttt tttttatttt tattttttta gagtcagggt cttgcttttt tacccaggct ggagtacagt ggtgccatca tagctcactg cagcttcaaa ctcctgggct caagagatcc tcctgcctca gcatccccag tagcagggac cacaagtgag aggatccttt agtgttgtca aggagaagga acagaggtgt ggatgggtgg gcacagacacaggagcacag ctgaagcaga ggattacaaa gggtggagcc tgatgtaaag aaacctaata ggtgacagag catggaggct cttgaatacc aggctggaaa ctgcattagg aacggtgctc ataattgcag aaaattttac atggcctaga tagtcatcaa aggatgatgt acaaacaact atggcatatt tatacaatgt gccgacaggatgcactgaac attttgaaca acaaagagac ttgataatgg cgaggttttg aggaggtgaa tcaggatgca aaaaaagcaa acaactaata aagttgattg atgacaaaca ctatcaaaag gcagccagga gaaaagctac tggttacctc cagggagctg gtgagggagg ctgggtggga ggatctaccc ttctgaattctgagggcacc tccagtgtgg ccctcagaaa gcaggagctt ccaggctaga atcagatccc gacatccctg ttaattccac ggattccaca ccgagtcaga tttatgattt actatagggt tttaaaaacc aaattgcagg gatgctagcc tatcacagct tatctcagac attgtccact aaggtataca gagtgctgcc tgttcctttggtaccctaat caggaaaccc catcagatct gctccttcct atggggtagt gagtaacacg aaggcttacc atctcacaca gataactggt cataggtcca gcagaagttt aaaacagaaa atgaggaaag ccatgtgatt aactgctgcc agactgtttg tgttacaaac agcagttcct taggcattgc ctgggacatgcaataatttc tgttacacaa tctgtggtag ttaaaatgct gcacgatgaa agctatctga tttggattca ttattaggtg agccatctcg tctgcaattt ggttccacca ttttcattta acaaatgtaa aaaagtttat taagctctta caaagttatg ctgggcaaat atgcaaaagt ccagatcacc taccgcagga actaatctagcctcctctct gggcaccctg ttgtttgggg ctgggcagtt ctttcctgtg tagaaccatc tagggctgaa taggtcattc tgacacctgg gcacctctgc ctgctcgtaa atgggacaat cagaaagggc ccttatgttt ccaaactttc tttaaagtag ctgttctgaa aacatggtcc agggacccct gattgtccct gagacctttg aggggatctt caaggttaaa attaatgtca taataatact aatatgttat ctgtcttttt tcactctcac tttctcacac gtgaacagtg gcattttcca ggtgacagag tgtgtgataa tgaacctaac tgaatgcaga agcaaacatg agaacctagt tttttcaatc aaaccagacg tgaaagagat ttgcaaaaatgaaaaaacaa tgctatcctc ctcacaatat ttttgtttta gaaaataaag ttatttttcc tagaaatgtt tttgagttta tcagtcatag gtttattatt ataattaaaa aatgaaatat acatacacag acatattttt taaagttctc agttttaatc tctttttttt tttttttttt tttgagacgg agtctcgctc tgtcgcccaggttggagtgc agtggtgcga tctcagctca ctgcaagctc cgcctccctg gttcgcgcca ttctcctgcc tcagcctccc gagtagctgg gactacaggc acccgccacc gcgcccggct aattttttgt atttttagta gagacggtgt ttcaccatgt tagccaggat ggtctcgatc tcctgacctc gtgatctgcccacctcggcc tcccaaagtg ctgggattac aggcgtgaac caccacgccc ggtctcagtt ttaatttcta atacagtaag tattgatcag tgtgccccac attagtaaaa gctcttgggg tcctcagtac ttctttttaa gagttgtcaa ggagtcctgt gaccaaaaat aggagagcca ctgccctaga aggacagccc cagcccgggtcaggaacaac tgggacagaa cctactgctc ctagtggatt gtaatatgat aggatttaac cttcaaggtt tcaactcttg gcaagagtcc atgaggggcc atggtttgtc ctgagcattg cttactgtta acaggagcaa gttccttagg ctggtgagcc aagccagcct gacgctggcc atggacatct tagtgggctgcttgttctag tgtgggtttt cattttatgg gaaatgtcat ctgctctaag gctcttctca tttggggaaa tcacaagttc tcagaatgtt tgtctctctt ggttggggcc tctataatta aattataaaa cagaggtaat ggttaagtaa tgcaagattt gacagaaacc acagaggatt tagggtttaa tttgagtgag gcaaaggggggatgaagatg agcggtcctg gagacaagaa aaagattgga tgaagctggg cacggtggct cacgcctgta atcccagtac tttgggaggc caaggtgggc agatcacttg aggccaggag tttgagacca gcctggctaa cataatgcaa ccccgtctct actaaaaata caaaaattag ccaggcgtgt tggtgtgtgc ctgtagtcac agctacttgg gaggctgagg catgagaatc gcttgaatcc gggaggcaga ggttgcagtg agcagagatc atgccactgc actccagcct aggcaacagg gtgagactct gtcttctttt tttttgagac ggagtctgtc gcccaggctg gagtgcagtg gcatgatctc tgctcactgc aagctccgcc tcccagcttcaagcgagtct cctgcctcag cctcccgagt agctgggatt acaggcatgt gccaccacac ccagctaatt tttatatttt tagtagagac ggggtttcac catgttggtc aggctggtct caaactcctg acctcgtgat ctgcccgccg cggcctccca aagtgctggg attacaggtg tgagccacca tacctggctg agactctgtctttaaaaaaa aaagagagag agggagagaa agattggatg aaacaacaga gtggggagga cctgtgagct tggtagcttg gtgaaggcag ggctttattg ggggccttag aggggatcca ataaaggttc ccagtcatgg tagtgaccta aagaaaatag cattttaaca tctttcattt cataatagac agtcacagtttacaagaccc tttccataca ttccttatga catccatact acagcccaga ggcaagttgt gcactctctc ctctcacaaa tacaaaaact cagcctctag aggccagcga cctgctcagg gtgatgtgca attcagggat gacagagtcg aggctcccag cccagtggtt atccctcaca ggcacgttgc ctgtcagtgt gcagtataaaactttgtaca agaaatcaag ttgcattagt cagtcggatt ccccaaatga tcacattgta gatggtgtat gctgtgggca gagcaagggc tgctgtttct tgggcaaaac aatcagtccc cctccccccc aaaataaatg aatgccaatg gtgtgacttt attttattta ttttattttt attattattt gtgagacagagtctcactct ttcacccagg ctggagtgca atggcatggt ctcggctcac tgcaacctct gcctcctggg ttcaagcgat tctcccgcct caccctcccg agtagctggg actacaagtg catgccactg cacccggcta atttttgtat tttttttaag tagagacagg gtttcactat gttggtcagg ctggtcttga actcctgacctcatgatcca cctgcctcag cctcccaaag tgctgggatt acaggcatga gccaccgcgc ccagcaatgt gactttataa ttacagaatg taggactcag ctcccactat tgttatgact caatattctc ttagataatg tttggggcac tagcttacag gcagcattgc ccggtggtta atgttgtagc tttgcaggca gactgaccat attaaaattc gatcacacca tttgctaagc ctgtggactc gggcacgctt ctttctctgc gttagtttcc tcctctgtaa aacacggatg atgctataaa cacacccaag tcctagaatt gttatatgag ttagaaaaga taggcaaata caactctcac aagacagcct ggcctccagt aagtgccact gagtgtttgctcttattgta cagtggctcc aagtgcttct gtcttggatt atttctgacc aggtggctat gtctcctagt aacttaccaa tcctgttgag tcttaataag cacgtctttg atgcctacag tgcgactgaa tttccaggcc tcattactgg agacacaatc atcctatatg cttttttcca tttgttttta ataaagtggt acatgtgtatggcaccagat caaacagtac agaacaagtt acaatggaag agaatggcct cccagctttc ctgaaatcct caactcagag acaacttttt tttttctgac ggtttcttta tacagccctt tttgtggtta ccttcctaac tctagaaaaa ctattcttac ctctgtttat ttacttagaa acattagacg ttacctttcaactcctcagt atgaagcttt agttttcagc accccaggcc accaccctct ttccaggact tactacttat actggtggta ggtggaattt taaaattcat cagcattctt ttgtgattct ctgtgtgttc cagttttaca gcaacccgta cttgttgcat gagtacagta gaactgggag gctcataact tagcctgcag gacttttcacttaaagcctg gccctcaggg tgatgtcacc cacctcattg tgcctggctc aggagtttag tccctcagtt gcctggttgt atagtttgga tgttcagcac ctccaaatct cacattgaaa tgtgatctcc aatgttggat gtggggcctg gtgggaggtg tctgggtcat caggtgggtc cctcttgaat ggcttggtgccttccccatc gtaacgagtg agttcttgct ctggcagttc acacaagagc tggcttttta aaggagcctg gcaccttccg ctctttctct tgctcttcct cttcccttcc tttgtcacta aaagcttcct gagccctcac cagaagcggt gcagatgctg gtgccatgct tggacctcct gtagaactgt gagccaaata aactctttcctataaattac ccagtttcag gtattccttt atacaatgca aaacagactc acacatctgg taaaccccag ttgtttgctt ctaggtaaga cgggaggagt ggggagctgg tgagggtttc cactgcattg tctattttca ggcaaggtgt ctccactgag taggcttcac attcagagct ctgggtaagg tgggcaggaa gagggttgca ggctgcccaa aggagggaga gaagaaggct gaatccttca gtgacaacct gtgaaccaga gtcttagctc tctttgaata ttttgttcag tatctttggg ttttgtttta ttttgcctag gggtaaatgc tgactgcctg ttctctggac aggaatggag aagatggtgc tagcagggtt gctgttcata tgtagacattcatgcagtca ctctcttttc agcacacttc ttacttctgc cctgggttca gttgctgact ctgagcccag aaaccttcta gggttctgtt aggtagattg gcttccaccg tctttgcgac aaccacagaa aattctagac tgttttctct tcgggcttca ttagtcaact tgcttcagtc tgtcttgcat cttctaaata tttatagatctctctctttt gttggagtgg cagaaaatgc tagttgacca cccaatattc aaattatcct gcctccttaa taacagaata tcattggatg tggtgggtaa ataatatacc ctaactttcc ttgcagagag gggtggccaa tgagatggaa atgaaagtca ttgggaaaga ctcccaagac atctctttaa acaagacagactgaagcaag ttgactaatg aagcccaaag ctagcagttg tttttgttta tctttgcctc tttcttcttc ttcctgtggg gacaaagggc agtgatatct ggagctgcag cagccatttt ggcataatgt tggaaaagcc aagagactct cagagaccgc agctccagca gttttttatt ttttccaaat atttgctcca ctgcaggaggatgagatatt cgtgtttgtt gccttgtgac tgtaggagga ctgcacttcc ctgccttgtt gtcaagtttc cccatgtggt ctgctttggc cagtaaaaca tgagtgggag aagcttggtg aaccattgca tgtctaccag cttttttgct ctcttccctt tggcattaga aaggcatgtc caggatggag ttgttccttcagcctagatt gggttatgag aagctagctg ggggagtcca gtaacatata aagcgagtta gaaataaaac tttgttgttg taagctatat atatatatat atatatatat atatatatat atatatatat aatatgtatg taatatataa atacatatta tactttaagt tctagggtac atttgcacaa tgtgcaggtt tattacataggtatacatgt gccatgttgg tttgctgcac ccatcaactg ctcatttaca ttaggtattt ctcctaatgc tatccctccc cagcccccca cccctcaaca agccctagtg tgtgatgttc cccttcctgt gtccaagtgt tctcattgtt caattcccac ctatgagtga gaacatgtgg tgtttggttt tctgtccttg tgatagtttg ctgagaataa tggtttccag cttcattcgt gtccctgcaa aggacatgaa ctcatccttt tttatggctg catggtattc catggtgtat atgtgccaca ttttcttaat ctagtctatc attgatggac atttgggttg gttccaagta tttgctattg tgaatagtgc cgcaataaac atatgtgtgc atgtgtctttatagtagcat gatttataat tctttggata tatacccagt aatgggatca ctgggttaag tggtatttca agttctagat ccttgaggag tcgccacact gtcttccaca gtggttgaac taatttacac tcccaccatc agtgtaaaag cattcctatt cctatgtctc cacatcctct ccagaatctg ttgtttcctg actttttaatgattgccatt ctaattggcc tgagatggta cctcattatg gttttgattt gcatttctct gatgaccagt gatgatgagc attttttcat gtgtctgttg gctgcataaa tgtcttcttt tgagtagtgt ctgttcatat tgtttgccca ttttttgatg gggttgtttg ttttttttct tgtaaatttg tttcagttctttgtagattc tggatattag ccctttgtca gatgggtagg ttgcaaaaat tatctcccat tctgtaggtt gcctgttcac tctgatgata gtttcttttg ctgtgcagaa gctctttagt ttaattagat cccatttatc tattttggct tttgttgcca ttgcttttgg tgttttagac atgaagtcct tgcccatacc tatgtcctgaatggtatcgc ctaggttttc ttctagggtt tttatggttt ttaggtctaa catttaagtc tttaatccat cttgaattaa tttttgtata aggtgtaagg atggtttcca gtttcagctt tctacatatg gctggccagt tttcccagca ccatttatta aatagggaat cgtttcccca tttcttgagc tacagatattttgagtttgg ttaccacagt attatctagt ggaagttgac ttatacagta tgtaatagga taaatatagg tgtgtaacag aatattaagt gttcgtgttt caaagctgag gggaaaatgt taaaagtgtt cacacactct aaaaagagat tagctaaaac tgcttcatta accacacttt ggggaaacca gttctgagat tcttctccattactctgaca ggttggaccc tctggggagc agatctcaag atcaagttat gagtgcaaga ggtgtgttgg gaagcgatgg ttgtaaaaga atcctgcagt agcaccaggc acaagtctgt ccagggagag gaggacttct actctctacc agcatctctc ctaagtcccc ttaggggacg ggggcaagga agtgctggga agggcagggc atggttcctg gctaggactc cacccccctg gggcctgtac ccacggacct aggtgaagac aggcactcct gccttctcgc ccaacggttg cgtttcccaa gatcatcctg gcctgccacg cccccatcta cctattaaac tcccccacct tccccaaacc ctagcaggca gacacacatc ggtggaagaa gacaggagcggctggacatt gaaaggacgt cgagaggagc acacctgcac accatcgacc agcggaacga ggcagagtgt ggctggagca gtcggaggga agcctgggcc gctgactcca ggggaaaacc atctcctttc tggctccccc ctctgctggg agatactttc actgaataaa accttgcact cattctccaa gcccacctgt gatccgattcttcctgtaca ccaaggcaag aacctgggat acagaaagcc ctctgtcctt gtgataaggt agagggtcta actgagctgg ttaacacaag ctgcctatag acagcgaaac tgaaagagca cacaatagca cacactcatt ggggcttcag gagctgtaaa tatccacccc tagacgctgc catggggcgg gagccccacagcctgcccgt ctagaggttt gagcagcggg acactgaaga agagagccac accctcatcg cacgtcctgc gagggagaca agggaacttt tccggtttca cttctgcttg gcttgagctg gcactgaagc acccttttcc ctcctcactg agggagcaga ggggaaaagc ggtagaacta acaggctaac aatgctcctc cgaaaatatatcgtattttt ggatccctag agataggtga tcacggcagc cgcggagtgc atttgggtct cctttcaaga aagaacttgc tgctcagcgt tgaagaatgc agttggccaa cagcctccag ctgctctgtc ttcagcatct gccatggcat ctgagctgag gtcatgttct tcctgggagg tccccagcag aaggatcacgtggaagctcc acaagctcca cagatgttcc aggagaggaa taggcagcat ttggaagaca tatcctgcca taacagaggg catttgctag tagagacaac aaacagcaac agccaagtaa acaaacacac aagcacaaag cactttctcc catttcccct cattgatcct gtccgggtag aagctgggga ggaagtagaa tagggtgaggcggggtgggg ctggggggcc tacaccttct tccttccccc gcaggtcctg tccctgggcc aggcttgaac taggggaatg ggaaaagctg tgaagtgaat gagaattagg agtttttatt tagactggac ttgaattttt tttttttttt tttttttttt gagacagagc ctcgctctgt cacccaggct ggagtcccgt ggcgccatct tggctcacta cagcctctgc ctcccgggtt caagcgatcc tcccaccaca gtctcctgag tagccgggat tacaggtgcc tgccaccatg cccagctatt tttttttttt tttgtatttt tagtagagac agggcgtcac cgtgttggcc aggctggtct cgaactcctg gcctcaagtg atctgtccgc ctcggcctccccaagtgcta ggattatagg agtgagccac cacgcctggc ctggacttga atttttaatt cctaaaaatg aactaccagt taaaatttaa aaatgaccaa aaaagctatg ggatatgctg atgttttgct ttggggataa ggaaaagata tctggttgag cggcattgaa aacagtgtag ggagagaaaa actcattcct ggctcacccttttgagtccc actatctcaa taatctgatg ttatatgaca cacacacaca cacacggagg aatcctggaa gactccatat caaggtggtg atgaaggtga ccagtgggtg ataggattat aggtgtgtgt ttatttattt attttaatta ccttttttta gagacagggt ctctgtcatc caggctgcag tgcagtggtgtgatcatggc tcactgcagt cttgcactcc agggctcaat cctcctgcct cagtctcctg agtagctgga gctgcagtca tgcaccaacg tgcccaacta atttacttta ttttattttt tattttttgt taagatggaa tctcacttta ttgcctaggc tggtcttaaa ctcctggttt caagcattcc tcctacctca gcctctcaaagtgctggaat tactgcactt ggccctatta tatttttaaa aaatttcaat agttttaggg gtaaaagtgg ctttggttac atagatgaat tgtatagtga tgaagtctgg atttttagtg tacccatcac ccaaatagtg tacattgtac ccaatgagta gtttttcatt cctcaccccc acactgtccc cacttctgagtctcctgatg tccattatag caccctgctt ttgcgcactt agagcttacc tcccacttag aagtgagaac atgtggtagt tggttttccc ttcctgagtt acttcactta ggtcagtggc ctccaatttc atctgagttg ctgcacataa catgatttca ttcttttttt gactgagtag tagtccatct ctctctctca cacacacacatacacacaca cacacacaca cacacacaca cacatttatc cactcatcca ttgatgggca cttaggttgc ttctatatct ttgcaattgt gaattgtgct ccaataaaca tacatgtgca agtgctgttt tttctccctt ttatccttct tttcttccct atgcttccat aggtactgag aaagagtctt ttttatataa ttatttcttt tcctttggga agatacccag tagtgggatg gcttgatcca atggtagatc tgtttttagt tctttgagaa atctccatat tatctccata ttgttttcca tagagattgt actaatttac attcccacca acaatgtatg tgttccattt tcactgcatc ggcaccaaca acggttgttt tttgactttt taataatggccattctggct ggggtaaggt ggtatctcac tgtggtttta acttgtattt ccctgataat tagtgatgtt gagcatttaa gaaatatatt tgttggccat ttgtatatct tcttttaaga aatatctctt gaagttgttt gcccactttt taatgtgatt atttgttttt ttttcttgct gatttgtttg agttccttgt agcttctgaatattagtcct ttgtcagagg tatagtttgc aaatactttc tcccattctg taggttgtct ctttactctg ttggttattt cttttgctat gcagaagctt tttagaataa ttaggtccca tttacttatt tctgttattt tgttgcattt gtttttgggg tgttagtcac aaattctttg cctagaccaa tgtccagaagagtttttcct aggttttctt ctagaatttt tatggtttca ggtcttagat ttatgtcttt aatccatctt gaattaattt ttgtatatgg tgagagatag gaacccggtt tcattctttt acactacatg tggctatcca attttcccag cactgtttat tgaataggat ttcctttccc cagtgtatgt ttttgtttgt ttggctgaagatcagttggt tgtaggtatt tggttttatt tctgggttct ctatgctatt ctacttttat accggttcca tgctgttttg attacaatag cctcgtagta taatttgaag ttgggtaatg tgatgcctcc agatttgctc tttttttgct taggattgct ttggctattt ggacccctct ttggtctcat ataaattttaggattggttt ttctaattct gtgaaaaatg acattggtat tttgataagg gttgcactga atctgtggat tgctttgggt agtatagtca tttttacaat attgattctt ctaatccata agcatggtat gtttctccat ttgcttgtgt catctattat ttctttcatt agtgttttgt aattctcctt gtaggggtct ttcacctccttggttaagta tattcctatg tattttattt ttattttttg cagctattgt aaatgggatt gagttcttga tttgattttg agcttggcca tcattggtgt atagcagtgc tagtgatttg tgtacattga ttttgtaacc taacactact aaattcactt atcaaatctg ggagattttt gaggattcct taggattttc taggtatgag atcatatcat tggtagaggt agtttgagtt tctcttttcc agtttggatg ccctttattt ctttctcttg cctgattgct ctgactaggg cttctagtac tatgttgaat agaaatggtg aaaagtgggc atccttgtct cattctaatt tttaggggga aatgctttca acttttcccc attcattttg atgttggctgtgagtttgtc atagatgatt cttactattt tgagatatat tcatttgatg cctagtttgt tgagggattt tatcataaaa ggaggctgga ttttattgaa tgctttttct gcatctatta aaatgattac gtttttcatt tttaattctg tttatgtcat gaatcacatt tattgactta tgtttatttg ttgcttacat ctactttctaattttactat aataaacatg tataattttg ttatcagaaa agtaaatgta aaagtgagtt ttaattttaa aacttgggcc taagtcttcc tgcctcccaa gcccattccc ttcctgatat ctggggcttc cctcctcaag cctgctctgc aggataaggg gatacagtcc acatgcctgc tgctggtttg gcccatgataacctccatgg gcaatgtctg agcctctgct gttgagtttt gctttacaca ctcctggcaa ggaaaggatg gccaacatgg cttggacatg ggttgctgat aattggtgat gtctcatgac tggttctgcc tggagggctt gctgtaagtc cctgatagga ggaacatgga cctgcacaag agcagaactt atctgacact gaagaggacacttcaagaac agattatcaa agtctagctc agggagaaat atactttaga gcagaatgag gaatggcgag gcagctgagc ttagacacaa gcagaaggaa atccatggtg agggcacagg caaggaaagg ggctgagaga gcattagtgg gggcagtcag gggcagtggt caggatgctc ggatgccagc gtgaacaatcgcatcaagat taaacaccat gaggatcgtt agacttcctg tcatatgtct ccaggtggtg ctccaaatat cctaaaccag atgacagcac ccctccaccc tctgctgtat aagcacatct gctctcctat aatcattccc acatagcaat ttatcatttt tattgatttt tcttcattta atacacgtat aagtgtgtct tttatttttaaaaatttgca ttcctttaat tgctttggag attgtgcatt tttctctctg
ttgatttact ctgccaataa acatgtaatc ctaccataag catgttttac ttgtgtaatc aaccaaaata aaaaatttaa aaaggaatca ctgactatga attagacatg tggataggca ccagggttgc agacatggcc cacgttcttg cattaacttg cactgtggct ggggcattgg atgggtacat taaaaggattaaagtaatat aaggcagtat ttattaagtg ttgagtgagc actacagaac ccaagtgctg agggagtttc atgcaggaag agatcaagag taacacagag aagaagaata gatcaattta gcgcattcat ttaaaaattc accttttgca taaggggatg tgtcttttgt ggggaggagg ggagttccga ttggcagtttgttctcaggg agcttgaaga agagatcttg gagaggagac gcagagaaaa caaatgaaga aaatgtcaaa atggaagggg ttggcccggc tatgcatacc ttagttagct taggtagagt ctaaactttt acaagtggtt tcaataggtg tgtttggtct gggttctttg ggaggtatca taggagaatg aaggcaggga ggacgcttccagcaccaaaa ttcaaaggga aatgtatttt acatgcatag cattgtttta ctctctttcc atttggagca tatcttaaaa attccatttg gagcatatct taaaaaaccc atttctctga caatggttct aaaaggggga aacatccttt gcaacagaat cattcattct ctcattcatc aaccactgat tgtgtactaa gtgtcagacc tgatctccat cctgcctggt atggcactag cttctgtctt gagacaagca ttgtgataaa ccatgaccaa aaaaagggca gttttataaa cacaagtctg ccaggctttc agcaattcta aatttccttt tgcaagtcag gctggagtta atggctcttt cctgcagcgg cggagatgac agggctctcc cacagtgctgagcaggcagt ttgaaagccc cacttcctgt ctctgcatgg gcgagtgtcc actggaagcc actgagagga aggagggaaa cctcagaaac cggcccctgc ctggctgctt caccctagaa agcccaggca gaggagggaa aggtgaagtg ctgaaaaaga ataaaaaagg gggaacatga aaaagagcaa gagcaggaag gaggcagggacgggaaagga ggggaagcac ggaaacagcc aatgtcaagg agaagaaaag atggctggtg gaaaggagct tccaggaatt gggacacagc cctgtcttat tgcaaaagat ggaaaccctg aaggagaaca ggaaggaaaa agaaaacaag tccgtctgag ctggcagggt ccactttctc attctacaga tgaggaaacagaggcacaga gaggaagtgg cttgcccaag ggggcagatt cttgaaagga tcatctgcac tctctctccc ttaatgcatt cttacctctt ctttactcgt gagtcagtcc tgaaggacaa gctgcctgaa gtcccacaca gatgggcctg gggcaagcat caaacatcct gggggccctg ggtgaggttt gcttttaaat tccaggtcagggaaaggaag gtctttaagt tgtctgctct aagcttagta atccccctca gagttatggg tgcggtgtct ggggtagccg ttgcgtctct gggcaaatac cctggagaat gcagtgttgg ttgtctgagc tggggacaga gtgacagcat agttgcatgc agagctggag gctcctgcag ctgtacaggt aaggtgctgaaattctccac caacccttcc tctttgcccc cagcaccacg aagataaccc tctttgaata tgtggaagtc tgttctccaa actttctaac attctcatgt cagtcttaat agattcagct cagttactgc ctcctccagg aagtcctcct tgtctgcaaa tcggctgccc accatgccgg ctcactcata gttttaactc tgtatctttctaatatgcct tagcccactc tgtcaggatt ccagtcagct tccttctcct agactaggag ttgcctcagg ccaggaggac cagccttgtt catatctgta ccctgcaaac ctgtcaatgc ccaaacctgc tcagtgcttt ggagtatgga accagccgtc aatgcaggaa tgttacactc taagagttcc caaaggtaga gagatgaggg attggtgctg gaagtgggag gttattctaa ggatgggtat ggcaggaaac acaattatag ttcagggagt ggagtgtcca ggagtgggag gagaggaact gggagaaaga gcagagagtg aaagtgagag cgggcacaaa gaaagggaaa aagagtcagg gatcaaccaa agtgcatgct tccttttcag ccctgccaggatgtgcaggg cggctgctgt ggacgcgtca aggctcagcc tcaaacatgt cttcttcctt gacttttgtc tatcattcta aagctaggtc atttaaaaag ttcttttgtt ttctttccac cgatactctg atttctgaca ttcgccaaaa agaggtcaag accctggcat accgccctac taagattaaa ataaatatta tccattgaaactgttatttt ttccttaact gttatttgta gagttaaaga ttcccatgat cgcgctggct ctaacatcat ttttggctct tttgagatca aatttgcaat ttgatgcaaa aatagctgtg acgcatatgt gtctgtatgt gtgtggttag gagatttttt atcattacat cttcttttgc cctgcctttc tgcctttctgtccttttaat ttgcgggctt ttggcaacca cagcacgggt ctggtttcct aggagtttct tttgtaggat caaaccgcta gttggctctt ggccctgtga tagggccctg ggctaactta ttgggaaaat gttgctgtaa cccctgccca gaggtgcctg tgacatgggc cgccatcttc tcctcttccc ttggcttcag ccccacctagaaacctgaac aaacattttc cttgacattt cataaagtgt cagtggctcc tcatttagca aaatacatcc cagggaagtt caaaagtgaa aaaaggccgt aacttcttct tcttctcagg gacctacaga aaatatgtgg cacctcggca gcctggcctg cagcactccc ctccccatcg gtgagtcctg ctacagtgggtccaggtgtc tggacgcccg gcacgcacgg ctctctgcag acctctggac agtaccatgg gagccgcaca gtccctgcct gttctgtccg gcagttcttg tttcccagca ccctgtctca ggtgagaggt tccctcttct gctgggcttc tcctccctgc tgtgaacccc aaatatctga ggcaggtcaa tttaggaacc ttattttgccaaagttgagg atgtacccat gacacggcct caggaggtcc tgaagacaag tgcccgaggt gatcgcggca cagcttggtt ttatacattt atacagacat cagtcaatat atgtaagata aacattggtt cggtcccgaa aggccggaca actccaagtg gagagggggc ttccagttca caggtagata agagacaaaa tgttgcattc ttttgagttt ctgattagct tttccaaagg aggcaatcag atatgcattt atctcagtga gcagaggggt gacttggaat ggaatggaag gcagttctca gtttaaattt tccctttagc ttagtgattt tggggtccca agatttattt tccattcact ctgcagacag gggcttctgt gcatccaggg agcccctcctcacagaagga agcaggccat taatgagacc caatccagct tcaaccacct ggtaacaatt aggacatcac ttctctgagc aagagctcct gcctgtccat gagttatcaa gacattccaa ttgttcctcc acatctttga catgaagact tgagggggtc agattttcca gggggcttga tggcatgttc tcttcactgt tccctgccctggtcatccaa gtgacccttg gcagggaaga ggccccgagt tgcagaatct ctgttctcac aagccattgc caacccggag agtggctttg ccactattcc tagcatgttg ttggctattt caggaatggg agtatttgac ttttcccttt gcagtgattg ctgcaaggag aggaattgag agactcaagt ccctgagataaatatttatc aactattact gaaagggagt atgtcaaaga aaaaatgtgg agaaacttca gcttgaacac atagtttaaa tccagcttgg gtgtactcca gtgggcatgg atgtattact gttttgcagt gcattcttct atgatcaata cacagaagca aacaggccac gtgggtaaac agtaattttc atttaccagg gtgaatatggaagtcctctt gtttccatgt catgatgaag gaaagcaagg accatctttt gccaaggaac agtggctgtg ggggaactga ggagatggaa ggacaaggca gtcaaaagct ttggaacaac tctttttttg agatggagtt ttgctcttgt tgtccaggct ggagtgcaat ggcacgacct cggctcacca caaccgctgcctcccaggtt caagtgattc tcctgcctca gcctcccgag tagctgggat tgcaggtatg ctccaccatg cctggctaat tttgtatttt taatagagac gggatttctc cacgttggtc agctggtctt gaactcccga cctcaggtga tccacctgcc tcggcctccc aaagtgctgg gattacaggc atgagccacc atacccggcccttttttgga ataattttat aggttttcaa actattacac ttaccttttt atataagaga caggacatag tcactgaaca atcactccag attttaagta agtccaggat gggatgacaa tggaacaacc atgaaatgaa aggaagaatg tgtcactggt atgtccacac gtctccaaat ctctcacctc tgtcagctgc aaacagagcc tgaaataaat gtttcctctg tgcacagcct ccacaacttc ctccctccac gtttctcact cactcctctc cagcacttct ctccgggttc tgcttacaaa cttgaaaccg gctatgcaaa aattataact gtggaaatta tgacagtgaa agagatcaga cctaaccgac tccatcttgc ttctaacctt taagctgtccttgttcattt ttgggctgaa ctaactttgg gaaggaattc agttcatggt agaactctga aacaaaattg ataatagccc tttcctgaaa agaccccctt cttgcctggg gacaagtctg ccattgtagg actaacaaat taactacaag attagaaatt aaggtttagg gttcatgcag cctccagttc caagagtcta aacctccccaaattgctcct ggggataaca tcactgttgt aaaagctaag accagtgctt gagatatttt gtagaccctg ctctggatgg atcagctgac accatccaga ctggtaattt ggctcaacca gctctgccat cccacccagg aacagaaaaa tactcacttc atcaccccat gagtccatct ctaacctgac caatcagcactccctacttc ccaggcccct actcgccaaa tctgcctttg gaggcagata acaacttatc tttaaaaact ctgatccctg aatgctcagg agactgattt gagtaataat aaaactccgg ctctgcatga attactcctt ttccattgca attctcttgt cttgataaat tggttctgtc taggcagcca gcaaggcgaa ccctttgggcggttacaaac tcatcctctg tggaagagta ggagttcatg gagaaattgg ttgcaaatta caaaatttta ttgtaaggtc aacttgtccc agtgtccgtc tgtgcagcga agggcccctg catggtttag tgattgcaag ttgagcctct agggtcaggt tgtctaggtt tccatcccag ctcattcact tattatctgtgtgttcttga gcaagctcct taatcaattg aggctttgtc cttctgtttg tataatgatg agaataataa cctccacaat aacctcatca taaggttgtt gtgaagatgg atcagataat atatatgtag agtgcttata acagtgcctg gcacataaaa aatgctcaaa aatcttaagt gttattaata ataaactgac atatatttcttgagcagggt ggtggtaaat gggtgttctt tttattaagc tttaaagtgt gcatagatca tattaattct ttttatgcat atgatatatt gcacatgcat gaaaatacat gcattaaaaa taaatgagca tttatgagat ttagtttagc agtcacatgt cccaggatta caagccagca ataatgggtt ggaaaacatt ccaacccatt ccaaccattg gaaaacattc caacccatca ctggacccat gtgccaaaca atggaaccgc ccacaggttc tcattcttgg ttaaaaaaat atgattatta cgggaataat actgattccc taagaattaa tatctgagca agtttctttt ttttcctgtc ttcttggaag atcagcaggt tctagattca atggagtcactaggattgag ccaccagtat acgccagtcc tctccagaac ggccacctgg tggtgggcac taaggcagtc tcagatgagg actgattgac ttttgtgtga actcaaactg ccaaagtccc tccctcacct tgcaaacttc aaagcacaac tttcaaagca ctactttctt tcttggctct caattctctg cctagaaaaa gggaggtgttggcaaggatg tttgtttagt tctgggcatc agtcaatggt acccagatct tgctgaacag aaaagacaca gatttgtttc tctgaggcag ttggtagtgc ttattgctta ttgctctcag gggcttctgc agcagtagaa gggccctctt cccctgccat gccacactga gaggagcatc cttggagtca tggttggaatctgtttttgt tatgctagtc ctcttccgca tgctagctgt tgcattgcag ggatatgtgt acctgtttat cttctccact aggctctaag aagccaggtt tcttaaagga aggaagctga tcttgtttat cttgaagtcc tcacagtgac attgctcagt caatgttgag tgtatgaatg aataaacggg aaccatcacg aaaaagccgaaaatacagtg gaaagactgg atcataaaat cttctaagca aatttttttt cctcttacac tccatttcca aatagataaa gtatttttta aaatcctatc agaatattct aacacactga gttgacagaa tagagatttt taaatgcagt gtcatttggc cagccatttg tgagaattta taaatgtttc agtaggttgaaaacactata aaagcaagga ctatgttcat acccaacagc tggcacttag tatgaatgct aaatgaaaca ttctcttctc tttcaagagt cagtccaacc agtgaccctg acaagaagga aggcacattt aactcaattt aatgaactct tatagagcat ctccttctcc aagtgctttg ctaaggatgg ggtaaaaaca tgaataagtcttggattctg tccttcagga attttcagtc tttggaggca gatacatttg cacccaacta ttatcctagg cagagtgtga taagtacgat aatagcagta aaagctctaa gttaggcagg agaggaggag ctcgttaaag cttatggggc ctgggaggct ttcggcggag taaactccag ggggacagct aggcatctgg ctgctggaat tgggaggagg atcattttaa gtggctacaa ctctgggtgc acaggactag agggtgaggg ccaagatggg aaattgtggc agccatcttc cacactgggc gcccgccgac ccttgcttcc tggtattcat attattgtgt agtgtccccc aacattgtat cagggttggc ctgtgtgacc aattgcatat ggtgggaatgatggtgtgtg acttctaaga ccagttcata gaagatgtgg ccaattccct tactgtcttt ttttttggca ggggagtgcc gagtttcacc cttgtcgccc aggctggagt gcaatggtgc gatctctgct cactgcaacc tctgcctccc aggttcaagt gattctcctg cctcagcctc ccaactagct gtgattacag gtatgcgccaccatgcctgg ctaattttgt atttttagta gagacggggt gagatcaatg aggcagtcaa ttggccagcc tggttttgaa ctcctgacct caggtgatcc acccgcctcg gcctcccaaa gtgctgggat tacaggcatg cgccaaccgc gcctggccct tactgtcctt tggatcagct gctctggggc taggtcaatccttcatgtga ctgcagcccc agccaacatc tggactgaaa cccatgagac accctgagcc aaaaaagccc agctaagact tcctgcattt ctgacccaca gaaactgaga aaagaaatgt tttgttgttg ctttaagcca ctgacttctg gggtcatttg ttttgcagaa atagatagca gatacagaaa agcaggctgg tggaacagtgtgggaaacac cttgattttc agggagttgc actttgttta tgtgcaatgg tgcactgttt ttagaaagac acaaagatga taatactggt gatgggcata atacgggttg tcaagaggag tgactgaggc ggggataatt taagaggcca cagcagtagt gtggcaagag gtaatgaggg aattgaactt ggtgggaatgggtgagatca acgaggcagt caatatgggc agtgagtgtg aaggagctgc gaaggatgat tctttggttt tgagcttagg aacatgagag aaccaagatc tcatttatcc aaagaggaaa cacagaagtg agcccctgtt tgggggcagg gctgggtagg aggaaaagag tggagacgtc tatctcccca ggaagagagc cccctgcttccagatcccag tggatggcag ggcactcggc tcattcacag actgggctcg ttgagaaacc tttccctgga gggcagggct gctctgtttc acagcccata tccctcatgg ccaagtgttc ctcgagtgac agtctctgcc atcaatattt ttagcatgtg gtctttcaga gactaaagag tggcatccat ctcctgaaac tccttcccca gctgacagct ggtgacccgt ggaggaggga gcttcaggga gcctgatggg cgagagtctg ttccaatgcc aatccattgg aagagatgaa gtcagacccg agtttgatag aaagcctact tcctcccttg tatccagctg tggagaccta ccaacatcaa tgcaaaccag aagctaacac ccagttcata tatcccaagtggaaggaagc ttctcgtgga attgtcttac atgacagtaa cataaatcct gaaggtaata cttggccagg taatgttaga aaagaacccg aacataggca ttgctattat agatcctagg ataggcctga gcaaaaactg tctgggattc ataacatgct tcgttgcaat ctgatagagg gagtgagatc cactccaaat ggagtctgatttggggcaaa gcaaagagta tggaaggaaa cttgagaaag ggggacagct tctcaaatgg agtctggcca cagctggggc tggaaaagag acatgactgc gcttgcagag tggtgagaat ttgctgctag aatttttaag ttgtgtgttt tcatttttat gataatgtaa actgagataa gcatattctc tgctatcccaatgagcccct cctctaggag gactaccttg ccaccttatc cataaatgtg tttataaatt attttgatgc cagctggtat tttttaaaaa gtggttttgg actcacaaaa aaaaccatga tggatttaat acataacaaa gcatttgtgt caagtgaagg ccaagtaaca tcttagcgtc ctgtgtgagc gaaggtgtcg tggcagttcaaacaagaatg ccgatgaagc tgcccaggat ggccaaggcc accttggtgt gtttgagggg aattagagtt tagaaaaaaa aaaaaaggca cctgacactc tgaactaatg tggttacctg gaattttggg gttttgaagc tttgcattta atttgcagct tatggcctga aggaaaagac aggtgaaatg catatcctgggatgagtcac ctggaggaga gggctgggaa ggggctgagc tgcacatgct cagatcttct cccaggctta tcgacccagt gagtcaagtc ttcttccaac gggatagagt gtgagagaga gcagggaaca gaagccagag tctctgttaa atttctcggt acatttctgt tagagaatgg aagtttctct atcgtaggag accttgagagcctgggatag aaattacccc tttgtcatgt attttcctcc cagaaatagc atggccactg tcactgctaa gctggagtat catgagcaca atttctctca ctttctatac ccatgccttt ctaggagatt ggtggctcca tcaaaaagga gttaaaaaga agcagcacta ttttgtggaa tacaatcatc accattatca ccatcagcac caccaaccag caccaccatt atcaaaagca ttcacctggt gtctgcctta caaactgcaa actgcagtag gtatttgtaa tagaatgttt cctttccccc ttgggatctg cagaaaagct ggagaatgtt ttggtatcaa cacactaggt tgcattgcta atcatgtgat ggccccatga cagtctctgt tggctggtgtagttcaggtg gacgactgca ggattttgtt cttggagcct cagttctgac tgggcttggg gtgtaaaagg tttgggagcc agatgacaag agtatttgat gggtagaata atgggttcat ccaaaagatc accagaatgg ttattaaata gtacaaagga ggaatttact ggtaatacca gtttgcaaac agagaagaga gtctccaatgtggactgaaa gtgctctctc tttgaagagg ggaaggacag attgggtttt atgcctcaca ggactggtac catacatatt cagcaggttt ttggggaaaa tctatacata tttataaggt gagctgatgc ctgcataata gataaacata tatgtaacat acttttcata ttcattttgg gactgggttt tggcactaaaatttgtggaa tttggctctt tatgttaaaa ggtgaactag aggacacaaa gacggtttgt gtgcaccctc tataaactgg ctgaaactgg cttaaggtct gcaactgctt atccaaaaag aatgtttgta aggccaggcc tctgtccagt cagagttgta gtggtccagg ttgtaaatca aagtttatag ctctttttgt tagagagttcagctgtagga atttagaaat ttgccatgcc tgccaggccc tgaacctttg acccataggt aactttattt ccttaacctt agggtcagtc ttagttgata tggggcatct attctggtat ctcagatcct atggtcaaga gaaaagatcc tccacaagag ggtcctatgt ggctgcaaaa actgctctga gctaaatccactcaaaatca ctgcaggatg tcactactag aaaatagggc agggataggg atccccttcc catgctgcca gaaaatgcct gatagcttac ctcccccggc ccttgaggct cccttggaat aggcacatgc aatcccatct ccacccaata gagcttgtcc tagagctcag ttttttccca tagttttccc acccacttgc accagaaaatctaataaagt catgtgatta atacaattca ttttatcacg cttctgaaga tttaagagag agcggtcaca ttggattcca cagtaccgac cttctgacga ttcttcattt cacctttatc tatttttatt tttattttat ttttttttcg agacggggtc tcactctgtc acccaggctg gagtgcagtg gggcaattac ggctcactgc aacctctgcc ttctgtgctc aagcaatcct cccacctcag cctcccaagt agctgggatc ataggtgcac atcaccaagc ctggctaatt ttttgtattt ttggtagaga tggggtttca ccatgttgcc caggctggtc ttgaacttct gagctcaagt gatctgccca ccatagcctc ccaaagtgct gggattactcacgtgagcca cctcgcctgg tccctttcac ctttattatc tttgccttta actctagtgc ttcctccctg aatcagttaa ggattgcatt tggctgcatt aacagaaacc tgactgcaga agcttaacca aatagggtag tttttaaaga gagattgctt acatcacgca aattgcacaa attttaagtg catagttcaa tgagttttgacaaatgtaga ataacatagc tatataaaac cattccatca aaaaaatttt atcaccatag gaaattgtgt cctgtccctt tcttgtcaat cccaactcct ccccacaagg caaccttcat tctcatttct ctcaccatag cttagtttta catgtttcta taatacagca tcatataaat ggaataatac agaatgcaatcttttgtatg aagcttcctt tggctcaatg taatgtttat gagattcatc catgttattg aatgtatcag tagtgttttc atttatattt cctagtgttc tattgaataa atatactaca atttgtttat ccacttattt gttgatgaac atttggaccg ttggcaattt ttgcctatta tgcataaagc tgttaaaaaa cattcttgtacaagtctttc atttcatatg tttttctttt tctgaggtaa ataactacaa gtagaattgt tgggtaataa ataggcatcc atctaatatt ataagcaact gcacaacagt ttttcaacgt ggctgtacta tttcactctc ccaatagcaa cgtatgtgtt ttccagctac tccacatgct cactggcatt tcctgttgccagtttaaaca tttcagccat tccagtggat atgaaatctc tctggctata ataattgtat ttctctgatg actaattatg tcaagcccct tttcaaatgc ttatcagcca cttctatact gtcctctgtg acatgtccgt tcaatctttt tgctcattct ttaaaaacat tgggttgttt gtctttttct tagtttgtct tttgcttttcatttatagga gtacatatct tcggaataca agtcctttgt cagataaatg tattgtgaat aattttctcc tagtttgtgg tttgcctttt cacattctta atatcttttg atgagtggaa actaactttc aaattatgtt cagtagatta acttgttttt gttttgtttt gttttgtttt ttgtttttaa cactgggtct cacttgttgc ccaggctgga gtgtagtggt gccatcatgg ctcactgcaa cctctgcctc ctggactcaa gggatcctcc tgcctcagcc tcccaagtag ctgggaccac aagcacgcac cactacactt ggctactttt ttatattttt ggtagacaca ggatttcgcc atgttgctca ggctggtctg gagctcctga gctcaagcgattcacccacc tcagcctacc aaagtgctgg gattacaggc gtgagccacc acgcccagtc gagtagatca agttttaatt ttatggccag tagagatcta tttcaaggct ctctattttg ttctgttgct ctatttatct acctttatgc caattttctt ctcttttgat tcagataggg ttataataat aattattttt tccagggattagatggacca gggctggtga agttgttcaa gggagtgatc aagagcctgg ctcctttcat ccttctgttc catctccttt ggctcatgga ttttgttttc caagtggcaa gatggcgcct ccacctttgg tatcctattt tagttcctgg cagaaagaaa ggaacaggct aatggccctg atgagtctac ccccttttaacaggagaaaa tttaaaaaac aaaaaccatg aaaccctttc ccagaggcaa caaccagaat tccatttatc tttcattgac cagaacagac cacatggtca ctggtggtgg caatggagac tggggagatg aatattttta aggtggcata ttccagaaga acactgtgca ctgattgcat taatgaaccc attaatgtgc caaggggaggtttacctatg agcatgggca aattagaacc cactcttgga gctgcaggtg agccaatccc acctaaacag tgtggatgct acaagatggg gaagtaaatt gattctattc cataccctaa cctctctcca agatgtattc ttaaaataga agagggaaga cagaagaaaa catccagaat atatttttat tgtcttttacttcttcagtg cattttagat cagtgcttct caatctggca aggggcatgc aggaggatgt gagttttatc aggaaaacta cacaaccccc caaccacaat gctaccccca ctcctgtgga ccttctttaa gagagactca ctattataga tggagttgat acgattttaa gagaggccat atattatttg ctttctgtct tgaaaaacttgtgatttttc tgtattgtgc tactgccaaa gagaatagaa acctgactga
ggtgtcaatg tttatgtaac tgatttcatg tactttctgt agttctacca tttctgatgg ttaaaaattt cttgtgtgtg tgcagttggg gagtgtgtcc tcctccttct gctcttatac cacacattag cacatcaaaa tgctctaatc tttgtatgat tatgtggcat gtggtgatgc agcctcacag tggaaaaacttctcttgggc cattgcaaat gtaacatttc tttcaatcag atagtgccat taaggatttc attatggccg tcacatcctg tgacatctct aaacatgcag cattagggcc taagtgcagc cctgcaggta gagttgccag gtttaacaaa taaaaattac acgctggcca ggcggggtgg ctcatgcctg taatcccagcactttgggag gctgaggcag gtggatcatt tgaggtcagg agttcgaaac cagcctggcc aacatggtga aaccccatct ctactaaaaa tacaaaaatt agctgggcat ggtggcaaat gcctgtaatc ctagctactt gcgaggctga ggcaggagaa tcacttgagc cctggaggcg ggggttgcag tgagcagaga tcacaccattgcactccagc ctgggtggca gagcgagatt ctgtctaaaa aacaacaccg tatttggggc atgctgatac taaaaaatta ttcattgttt gtctgaaatt aaaatttaaa ttgggggccc tgtattttac tgggcaaccc atttgcaata tcagcaacaa tctcttattc agaccactga ttaagtgtgc aaaatttgaa tctctgaaca gtacctatgt ccttgatatc ttaaattaat gagtgtctta gacactcaaa gcaggaggaa gcattatggc agatgtttga gccccagaga tgtccatgag cacagcatag agctcagagc cttctttatt atttgcttca cgacagagca aaggactgca gcaggttgac tgatataaaa gttttaccat gtctcacagcaggcctttgc tcaagtttcc agtaaggata ttgtatcatt tcttgcctgc agtacttgta aatccactta cactgcctgc tgttgagtca tttgtttcgt cttgagtagc atgtcatcct tgttcctaga agatagtgag tttagagaca gtagccaagc aacagcagag cagcctcaac caaaacgatt ttccattttg gtgggatgaattgaaacaca agcatcttct atccagggga gatttgggga tcataaagaa tcaatctgag ctggtaccac catattggct gctgcatttt ctagagttgc cgtaactagt ctcacaagct gggaggcttt acacaacaga catgtattgt ctcatagttc tggatgctag aaatctggaa tcaaggctcc aggggagaagctgctccatg gttttctctt agcttctggt gttgccagca atccctggtg ttccttggcc cgcaggcgga tcactcccat ctctgcctcc attgtcacac ggcattttcc cagtgtgcct gactctgtgt ttcttctcat aagaacatcg gtcatattgg attacaggcc cgtgctactc cattatgacc tcatcttaac ttaaacaattacatctgcag tgatcctgtt tgcaaataag gtcacattct gaggttccag gaattagaac atagacatat cttttgggaa caaaattcca gtgataacag tttcggagac agactagtcc tggagtttgt aaggtgagcc aggaccaagg tgccaggatt ctcattttgt aaggtccagg aacaaagtga tgttaatagaaagaacatgt ttttgtttgt ttatttgttt ttgagacagt ctcactccat cacccaggct ggaatgcagt ggtacaatct cggctcactg ccgctgccat ctcccaggtt caagcgattc tcctgcctca gcctcctaag tagctggaat tacaggtgtg tcccaccatg cccagctaat ttttgtatat ttgtgtgtgt gtgtgtgtgtatatatatac acacacacat acatacatat atatacatac atatatatat acacacacac acatatatat atatataaaa tatatatttc ttttagtaga gactgggttt caccatgttg cccaggctgg tctcgaactc ctgcgctcaa gtgatccacc tgtcttggac tccctaagtg gtgggactac aggcacaaac caccacgccc agacagaagg aatatgtttc cttccagtct cacttgactg gctgcttccc tagataacaa cagaggatgt ctgttgcagt tctcattgct ggggagtcta aactggaata aaacacccac tatctccatc aggcttgcac tagagcccag ctctagctgg agagaaagaa gctaacccgc acagacacag gactgtaggcagggagcatc cgggggtatt tgggtcctgg ctctgatgtg cctaaggcca acttctctct ggccatgctg gcgtgcatga gctcactaat cttccttttt gccttccatt ttctccaatc ctgacttagc aaaggttggg caaaagagac tctgtgtgag ttcgagcaaa gcctgagatg ctggattttc caagatacga gaaggggctgggggctgggt gaactggtgg tggaggaggg aaggattaat ttcccaagga ggggaagggg ccaggacatc aggccccggg gactttgaag agagggtcgt gggtaggagg tagatcaagt ggagtgacac aaaggtcagg aaagaggaag tgtccacact gtccttcgac agacttgagt ctatgggact tcctccctgcacggtacaag gaaatgagta agtgagataa tgttgtaact tctggccctc tgacattgca ctgccccgat gtcacagttg gaaactgtac ctgcccccat ccttgtctgg ggtgtgtttg gtctggggag ggctggtgaa gcaagaggta ctcagaaaaa ggacagaaat tgcttcctat tatctgggca tttggaggtg aaggggtcacagctctggca aagatggggt tgaaagggcc cggactccag ggaggggcag ctctgcatgg cctgattcct gcaccccacc tttgccccct cacacctcct ctcatctccc gtttttgaag aggaggaccc tgtcacatct ggacaattct gcaagaactc tgtagaactg acttcactgt gaaccaggct ccagaagtcaacagaaacaa aaatgctcac atttaatcac gatgctccct ggcatacaca gaagactctg aaaacttctg aatttgggaa atcctttggc accttggggc acattgggaa cataagccat cagtgctggt gtgtgtgtgt gtgcgcgcac acgcgcatgt gtgtgcatct tctaccatgc ctcctacaaa tttgacctgg gcccagggccatgttcggtg gtttttaaga accgaggctc ccagaagcag tattgggcag ctagagtggc cccaggatct atatcaaact ctacctgttt ctgaaccaaa tttcttctag aattttattc cataaatctg aattatggtg tcagactcct agcatacact aaaggaactc tctgccttgc attaaataac aggagttacc cctggaggta actcctagcc ctggctcttt agagaacaga tgccgaatag gcattagggg atgtgatgga tgtgctaact ttcaaaaaaa aaaaaaaaaa aaggcctgag ctgagtgctc agagattcac aaaaagctga cagcatctct ctgttccatt ggaagctggg tgatcctttc tactctttcc tgagaaaggc agttgggcaggaaaaagctg tatctctgtc ctcactgaga gggtttccca gtctgagggt gaaggatcag gagagggaga cctgacgggt cgatgtgggg catcatccac ttgagtgaga accagaggga tcccgtcatt gcccagggca gatgctccat tttggggggc atcattcatt ctttcctgtt ctccctgcat tcctctggct cctgcccaggagaggtggcc gctggcaaga gagcttggtg gaggtgggag gtgggaggtg gggggtgggg ggtggggagt tcttgagcca ggacctagcg catagtctcc agcctgctga tggctgtctt ggatgcttca aaggggagaa gatcctagat gtgggaaaca ttggtgggcg ttctgctggg gcatctgtag cctctgagaaggctaccagt ctctcctaag cttacgccgt cacaccctgg gcacttgttg aatgacttta cttagcttac agcctctggt tcctgttggg aaacttaggg cttgccacag tgttcatttt cctttgcggg caactccgtt cctggcactt atcatattac ccactgtact ccccgcttag agctgtgtca aggttctgag aatctatcccttggcttgga aggggtcatc tctctggcca gatcatttcc tgataggtcc tgaggcacca caacacatag gaggcttgtc ctctctctgg ggttcactgc cttgctcctt ctccaggtca atatgtgacc ttggaccggt tgcttgagtc ccctggtcat tcagaaacaa ttgggtttcc ctggctttgg agcctggcagcctggctttg agaaccgggc tttaacttgt cacatgacta tggccaagtt cctggggctc tccaagcttc acttcctctg taaaaagggc aataatataa tacctgtctt attgggtttt gtccatgtta gatgagacat tgggtacaaa gcacttggtc ccgtgcctgg cacatttact gcacttaatg tatgatagtt ttcttattattctaataaac aatatggctt tgggagtata gttctgccac attgcagtgg ccagagtgaa ggtggtgagt gccttctggg gccctgggag tcaaggttat ccgcatgccc tttcttgctt gctcctcagt gtggctgcct ctatgtccac accatgcaga tgcaacaggt agtttgaacc tctgaggccc acagtgggat ggggaggcag ggacatcact tatggggtgg gaagtcaccc attccccagg aaatggcccc agctgccttt tccatgactc ctcttgaaac cctgtggagg ccacattcgt gttggggcgg tctttcccat gaggatatgt tcagatgccg aggcattttg aaaagccctc catagagttt cctttcataa cacatgatca tccccttgggcttctggttt tttttctttc aggaccttat tttcaggcaa gtggcctttg acctctaagg ctgtcctttc ctagctaccg aatccagcat tcaaagtgat ggaaatatgt atatatagta atagtaaaat atcagcactt aatggcctga taagaatgtc actgcaatgc tgagtttgga ccaacatttg cctgctcctg ccattgagcccgggctcccc tccagagctg agctgctgca agggatctga gtaactaggg ctgtgtcaga gtggcgatga cagccaccac atgctaagga agagatcccc aaggacaagg agaatcccac gtggagctac ttgcttcttt gtcagtcttg tttttcttat ttcacaacct tctaaaacac aatctctcaa cctctattgttagcttgcat ttttcaatca tgagcacagc tttacctggc tccatgcttt gattgactct acctgccaac actgcaacaa cagggaaagg gacaccggcc tcataccatt agatggtgtg tagcctgggc atgaggataa ttaaaaactc ccaaggggat tttaacatgt aacacagttt ggaaaccatt gatgtaagat cttcttactcaacatgtgct ccaaggagct gttgtatcag cttatcagaa atgtagatca ggccgcactt ggacctgtag aatcagaatc tgcattttat cagattccga cattatttgt atgaacatta gcttttgaga agtgttgctt taagagacta agggggtcaa tctacctcac tttgcagctc tgtgttcctt agtcattggctaaaatatca gcccccctgc aatgagccat cctcccttgt atagtcagtg atggcctgtg aacctttagc caactggaag tgggagggga cacagtccac aaaacactat cctgactttt gacaccaact acaagtcaag gggttcccca aaccaccctg agttgtgata attcgctggg agatctgaca gaactcactg aaggttgttatactcatggt tgtgatctct tatagggagg gaatacagat taaaatcagc caaaggaaga agcacacagc acagagtcca ggacagtgcc tgacatggag cccctacggt cctctcccgt ggagtcacgg acagcgccac tctcctggca ttgatgtgtg acaacacaca gggagtgttc cccaccaggg aagccttggt gtccagggtc tttactgtgg ctctgtcaca tgagcacagc tgactgccca tgcggccgat ctgttcccag actctccacc gctacacatc actcacagtc cctgctctaa atcacacacc atgacccaat gtccccgggc aaatgaaaac acctctagca ggcaggacgt tccaaagcct tagagatcac ctctcagaag ctgagggcagaagccagacc tctttttggg cagggttaaa ttctttatta ctgtttttga aaaaactccc aaattgagtt tttcctcttc acttacagca gcataacaac aatcatcaat gcagaagact tctgcgagca aaggtgtggg ggaaaacccc aagcagtgga cactagctgg tgtcctccaa tttgattctg atgctgtcta ctgggagatagtgtcagatc ctcaagccta aaccctcctt ctcccagtca gagggctggc ctttggaact tctgaccaat ccacttcaag ttgaggttcc aaccactccg ctctttgggt ttggttgatt tgctagagtg gctcacagaa ctcagggaaa cacagctacc agtttattgc gaaggacatt ttaaaggata aaagtaggcagataaagaga tgcatagggc gaggtgtgga aaggtcccta gtgcaggagc ttctgtccat gtggagcggg ggtgcaccac cctctcagta catgaatgag ttctccttca cctgcctatc agcctctaca tgttcagctc cccaacccag tcctcttggg tttttatgga agcttcaaga cacccacatt ctttccccag agtatagggcaagaccttct ctggggaggg ttttaagacc cacagtcaga aaggtggggt ggggtcaaga ttagagtcct gccttgacgg gcaggtgaaa ggggtagggg gagtaggtga gaaaaattct gtttattttt tctttttttt tttgagacgg agtttcactc ttgttgccca gggtggagtg caatggcaca atctcagctcactgcaacct ccgcctccca ggtttaagcg attctcctgc ctcagcctcc cgagtagctg ggattacagg cgtgtgccac catgcctggc taattttgta tttttaatag agacagggtt tctccatgtt ggtcaggctg gtctcaaact cctgacctca ggtgatccac ttgcctcagc ctcccaaagt gctgggatca caggtgtgagccactgcatc tggccaaaag attctgtttt tgaggcctgc ctctgaggtc taacacactc aacattataa caagactgta gtaagggcta tgggagttat gagccaggaa ctgtggatga aaacctatca cagatatgca tatatatata tatatatata tatgcatatc tataataact ccacaactac acactgcctt attgctcagt tcttctctcc atgtctctga cccacccttg cccccttcct ccatcctttt ctccattgca tacccatcca ctgtgccctt tggaatgctc acaccatgaa ctgcaaactc tcgtgtggct tcagcctctt ctctgaaagt tcctctcacc tattactttc tctggaacct gccatccctg ccaccttctc aaaaaaggccttttattctc ttcattccac aaagctcagt gtcaaaacat ggggtttaca ctggaagctg aggtcacatc agtagccggg atcagggtcg ccctagctgc ccaatgcagc tcccaggcct cctgtaaaac cttgaccttt gaggtcatga cagccctctc ctgctatgct catagctgac cactgaactc ctggacactc cctcccccaagttcacagag aatgtgggca catgccttac agtcttccct tgatccaaac tactgccttc atcttgagtg acagcagcat cttttggatg tcttggcctg tctagcttta tttttttgtg ttctgccatc aagttgctac ttctgttgcc atcgtgcctg tcagcgcagt gcaggctgtg gtgaaatccc acgaactcaggcatcacact gaccgggtct gagtcctgtc tcagttgtca gctagttgtg caatgaaggg aaagggacct acactttcca agcctcaatt cactcatcta tggcatggtg acaataatgg aggttgattt aaagtccttt gtaagaatta agagttataa tagacataaa gtgctgtatc tggtatacct agaaaacatt ccataaaagttagtaattgt tggtcatgta atgatgactc tctaggctag gatttcagct tcattgcatg cacatggtgc actcacaggg cgtgacctct ctctgtctca gtaacctcat ctgaggaccg ggataatcat accgcttcaa agggatgtca taaagattaa ataatatgtg taaggctgct tgcatttagc tgcattcaacaaatatttct gtatctttct cctcatttct ccttactttc ttgcttatta tctgctctag gtatagattt cagagaacta agcttgttac aatccttcat aaaataacca ggttggttag ggcatttcca agagtcaata ctgtttagtg actattctct gtttaatcta ttttgattgt ccagggtcat cttttgctat gtcataggttgttggcttct tctagagaag tgagacgatg gacaagttcc aagtgagtga ggcgactggt caggatattc cgctgaaaaa ctcatgtcag ttctaattcg tgattgtaat tcaatcacag cctgagaaca gtaggactgt agttcaaatg ctctgttccc tttttttttt cccagaggat aatttttttt tttctttgag atggagtctt gctctgtcac taggctggag tgcagtggcg tgatctcggc tcactgcaac ctccgcctcc tgggttcaag caattctcct gcctcagcct cccaagtagc tgggactaca ggcacatgcc accacgccca gataattttc gtatttttag tagagacggg gtttcccctt gttggccagg gtggtcttga tctcttgacctcatgatccg cccacctcgg cctcccaaag tgctgggatt acaggcgtga gccaccgcgc ccggcctcta gaggataatt tttaaatgtg cttttgcatt tggaaaatgt gattggcatt tttttctaat tttctaatat gatacgctgt cggatgctat ggattactta aaccctctgg ctacctagaa agatctttaa gtggttctcaacaagcttca tacgcaatgt aaattgtatt atctctcagg atgtgtgaga acatctgttt ttcttctaat gcagtaaaca tataagggtc tcttgggata tcttttaaat agacttaata caacattcag gaatgataac aaaatataat cacagttgta agggaatgtg agcatttcat attaataaca ttggaaccttatgtttaata cagtgttaaa agttgacaaa catgtaggag tcagaaaatt caattaaaat tatcacagta atatgaattt agccacatcc tgtgttagtt atgaaatcca tttaacacca caaacagtaa tatttttagc cagtttattc aaaaggaaaa caggaactaa accactttca tgcaatatat actctgttaa tgtggtcaggctaattttgc tgggggaagg aacttaactt ttgaatattt gaatgcccag tcatttaatc tgaatatcct atttccttgc atgttgcaaa atttttgtca ataaaaggca gaaaaagaaa tctcttctcc atgctcatcc ctaagagaat gggttgtctg taccctgaga gcattttatg gaggggacaa ccacttttctaattttcctt cccacttctc tgtgggcaca aatgctcttt ggttgaaaga gttgtaattc agtcccaaga tgaggtgtgg ttactgcatc cctaacctat atctggggac cccacagcca cacacatggg ggaaatggag cttgtcattc agttctccag ccattgcaca gggttcatgg actcttcgtt gatcccaccc cacgcttcttctctctgcta gccgaacaca cttctctctt ctttatcagg aggccatagg agaagggcat tcatttttaa tacacataca tctgcatcaa gtctaatttt gccatgtctc aatccaactg tcaaatgggt tgtttggggg ctatggtgct tatcaaacat ttactcaaga atagccaaaa ttagccaagc aaggagaact tcagcaacgt tcccaaatgg ccccaaccaa gtactgtaag actgaggata gctaaagggt cttgagaggg acttctcagg cagtggcccc gacatttatc tgttttttta agtgagaaat ctgagtacca ttcttgactc ctcttcctta cccccaaccc ctcactaagc cttgtgctac tatttagtaa acagaccctc aatgcacaaacttctgtcta aggccatggc caccacccta gtctaatcca ccatctcttc tctggaacag accccagctg ctctccctgt ctctgtgctg gtctctcaat ccatgctcca cactgcagcc agagtgctct acaatgcaaa tccatttgtg agactcctcc tcttaaaatc ctcaagtggc ttctctttgc ccccaggatc attttgaaactccttaatgg aagaggcatg gccctttggg atgtggttcc ccaacccctc ccacatcatc ttttcaatca gatttcccac taaatggaaa ttttttcagg tcctcaactt tatggtgact ttctcttgct caggatcttt gaacatactg tttcttcttt ccttttgtat ttgccaagac aacacttcct ctggtaagattttcctgaca tcctctataa aaaaagattg agatagttga ctacccaaaa tgtttcccat tcattccaag ctctattcaa ggcagtaaag tgcccggctg acagattgca ttcctcatct tttctgaagc tagcaatggc catgcaacag cattctggcc aataagatag aagtcgaagt tgaagggtgg gatttccaag aaagctcgttgaagacataa ttcctcattt cacttcttac tctttctctt tcctgcttcc taaaatgcgg tgcagatggc agacacttca aagctgtctc aggcaatcag gtgatgttaa ggcagaaacc agctttatga tgggtagaac aggaagaaag aaggcaccta tgttcttgtt caccttgaac cacaccagca ctgccttgcctacccctgga attcctttaa tgagaggcaa atgagagctt acgtgtttaa gccattgcta ttttattttt ttttgtttat atgcaaaaga acttaatcct aactgatatt aacactaact gggtctattg cttggtacca agccaatgca tgacacatgg tatatatgct cagtaagtat ttgttgaatg agtgaggcaa tgaaagaacatagaggatat atataacagt cctcctgccc agatgtcatc tgatcctctt taggatctgg gcccataaaa ctgtatctga tatagtttga atatttgttc cctacaaatc tcatgttgac attttatccc taatattgga ggcagggcct agtaggaggt gttttggtca tagtgataaa tggcttggtg ccgttctcac agtaacgagt gagtttttat tctagtggtt cctgcaagaa ctgattgtta aaagagcttg gatccttcca cccctctctc actcttgctt cctctctctc accttgtaat ctctacaagc tcttcacctc cccttctcct tttgccataa gtggaagatt tctgaggcct caccagaagc agatgttggt tccatgcttc ttgtacagcctgcagaacca tgagccaaat caacttcttt tctttataat tatccagtct caggtattcc tttatagcaa cacaaatgga ctaagacagt ttctaatgct atggttcctt tagtaggtca gtgtaaaacc ctggatcact cctgtaacaa attacttgga actcttctca ccatacatat ttaaaaatag ttgccatgtt gaaaatcctataagatcata ttttatttca aatccaacaa ctcattgcta aggagataca agaagcagaa aatacagaga gactaatgtg ttgatgattt ttgtgaggga cataaggtct gtgtctagat tcattttttt gcatgtggat gtccagttgt tccagcacca tttgttgaaa agactatctt tgctccactg tattgctttttctcctttgt catagatatc tggtcacctt accttagagt cacagatgaa tggtcctatt acttaactac tgaaaataca ggccaaagca aacagaggaa taagggatat ataataaagt atttgtgtac ttgacttggc tctaaaggaa gcattgcgtg tctgtgtaaa aagaatgggt gagagttttc caccattcaa tatttctaatctttctgaaa tacaaagcca ggacatcctc taatccatac attccatagt ttggttaata taaattcctt tattaaatcc ttattaaata aagttattta tgtttctatg aaactcattt taactcctaa gtgaaaaata ctactgagct aactaaacat caaacatttt taatttttta aattttttta gagacagggtcttgctatgt tgcccaggct ggctttgaac tcctgtgctc aagcgatcct ccaaactcag cctcccgagt agctgggact acaggtgcat gccactgtgc tcagctaaac atttttttga aatgctcttt taaaatcaat tttattgaag tataagttac ataccataaa agtactcatt ttgagtgtac agattgacaa gttctgacaaatgtgaacaa ccatgtaacc atcaccaaaa ataaagatat gagacatttc cattacccca aaaagttccc gtgtccctct ccagtcaata tccagcccta gccccagctc caggcaacca ccaatctgct ttctgttgct ataaattgta cttatctttt ctagtgtttc atacaaatgg aatcatacag catttactct tttgtgtctg tcttcttctg ctcagtgtaa tgtttttgag attcatctat gttctgtgcc tcagtagttt gttcttttta ttactggata attccattat aagaatatac cacaatttgt ttatccattt actgcctgat gggcatttgg ttgtttccag ctttgaacta ttttgaatcc taaaagactg ccagttttga atgagaccccagaacaatga atgtaggctc tgtatacaag ttcaggctgc tgggcaactt aggccttaag acacaactct gccacttagg ccttaagaca caactgacat gatggtgctt aaagtggctg tgatggaaaa ggaggctgtt tggagccttt ggagtgcctt tataggtgaa ccccagcata gcacctaatg atttggagca aagctgtgtcattccccaaa gataactatt cgccttttga gaaacatctt ctagctacta tcaataataa acacagaatg catcaccatg ggccaccgtg ttgtcttttg acctgagttt ccattgtgaa caagagtcat ttgatccaag gcagaaagtt gggtgcacac agcagtgttc catcatcaaa tggaatatga gattgggcccaagtaggtcc tgcagacaca aataagttgc aagagcaagt agtacaggcg cttggcctgg ccagtactgt tgccaagttg actgcttccc ctcagtctgc atctgtggct tcatggggag tttcctatga ccacttgatg gaggaaaaaa caaattggag catagtttat agtgctggta ctacccaaag tggctagctg aggcactacatctccactct ggggtgcccg tgaaggacag tgccaaagga aaaccccctc agtgagcaga acttggagca atacaagtgg gtgttcattt tacctagaag agaagatgtc cgtgagttac agatctacac aaaatcacag agagtggtta atcgtttagt ctgatggtca gggacttcca agagacatga ttagaaaactggtgacaagg agtcctgggg aagaggcata tggatacctc tgaacacaca caaaacatga gaatatgtat cccatatgaa tgttaaccaa agagcagcca caacagaaga ggattttaaa atcagctgaa taagatgatt cattctgaca gcatcagcta gtctctttcc ccagccactg ttgcccagtg ggcttacata tatcatggccatgggggcag ggctatgtat ggacacagca acatgaattt ccactcatca
aggccaattt ggctccagcc attgctgagt gctcagcctg ccaagataga aatctacgcc aatatggcac cattccctgg gctagaaaac caactggtgg aaggttgatt acattggacc atttccatca tggaaggggc agtgctttgt cttccctgga atagacattt actctggata tggatgtgcc ttccctgactactacaatgc tctgccaaac ctaccatcca tgggcttaat tttatttgtt ataaaatttc aaccaccatt gcttctgacc aaggaagtaa tcttacagca aaggaagtac agatatgagc ttctgatcat gggcttcact ggcctcacag tgaagcaggt ggccagatta gaacagtgga atggatttta aaggctcagttacagcacca gctgggtagc aacaccctgc tggcctgggg ttatgtcctg caggatgctt taagtcagtg accaatatat gatgctattt ctcccattgt caggattcat gggtccaaga atcatggggt caaaatggga gtggcttttc tcactatcac cctggtgttc gggtagtaat ttttccttcc cattcctgta actttgggctctgctattgc agaaatctta gctcctgtgg ggggaatgct tccatcaggg aatacaatgg tggttccact aaactgacag ctgagtttgc catctcctcg tgccagtgaa tacacaagca aggaaggggg ttcctttctc acctagggtg actgatccta attaccaagg agaaattgga ctgccacttc acaatgaggg tgaggagtat gtactctatg tgtctgtgat taatgtcaat agaaagtgac accaacctag tacacagagg actgatcatg gtccaggccc ttcaggaatg aagatttgag tcaccaggca aggaacttgg actcactgag gagggcatat tccaaggaga atattttatc tatgtccatc tatgtccatc tatattccat ctgtgttccccttggaattc ctattcatga acatggggaa ttccaagggg aatatagaat gagtagtgga aggtagttat aaatgtaagt caaaaaccac acaaccaatt tgagaaatga ggaaggtaat agtgttgaat atgtcttctt tatcttgata taaatgtatt tgtgcatata ttaaccagtt tatttattta ttattatttt ttgagatgagctctcgccat gttgcccagg ctggtcttga actcctgggc tcaactgatt ctaccattta gtcctccgag tagctgggac tacaggcatg caccaccata cccagctgac cagttttttc ctattcctct acttaatttc tctactatac aacataatat gtgttaatgg tagttaactt tatatctcag tattaagtcacaagatatca aaaagggaat gcgacttagt tacaagcaga atgaatatca ctcaaagatg aataaagaga agagggttag tgcattttct gttggatgag agaaagtttc attgttaggc agaagcatga ttttgccttt tttttttttt tccaaggtct cactctgtgg cccaggctgc agtgcagtgg tgcgatcttg gctcactacaacctctgcct cccgggttca agtgattctc cagcctcagc ctccagagta gctgggatta taggtgcgcc aggttaattt ttgtattttt agtagagaag gtgtttctcc atgttggcca ggctggtctt gaactcctgg cctcaagtga cccacctgct ttgacctccc aaagtgctag gattacaggt gtgagccactgtgcacagtc accacggtct ttttgggagg caactttagc atggttaaga ggtgcgaatg gatgttaagc taacaccagg taagccctgg tagatgtgta ttgtgtcagt gggcctacgc tggagccatg tttccccaaa ttcacttttc ctatgtacct ctggattagt gtgggccact ggagacattt cacatgagat gaggaaggtgggagtgaagg agcagcatct ttttacacta agcaggtcgg ggagggcatg tggctctgtc tcacattgtt gggaatctgt ccatcatctg gttggcttag gtcagtgggt gagttcacag ctgttccagc ttctgctgga aactccttcg gtttctctga ctgctccgtg atgagggcat cagattctcc tgcagaaagc cccagtgttg aagttggggc ttcatgttgg tgagtgatag ttacgggttc tagcccaacc tgtggtttct tgcaaatttc agtgtcagct cagtcttgcg ggttttgggt tgtccttgct tcccacactt catgcctttc tttccctcct gacagtctgc cctttagatt ttaggattca gcaccagcca cagaaacagc aacctcactgttaagggttg aattgtatct ccccaaaagg taggttgagg ccctacctgc caggacttca gaatgtaacc tcatctggga atagcatcat tgcaaatata attaattaag atgagggcat actggctcag gatgggctcc taattcaata caactaatgt ccttctatga cagccacagg aagacagaaa cgccaaggga gaacaccatatgctgatgga ggcagtggca gctgccagcc aaggattata accagaagtc aggaaaaagc aagaaggaat cctcccttag tgattttaca gggagcatag ccctgctgac accttgattt tggactttta ttccccaaaa ctgtaaaaca atacacttct gttgttttaa gccactcagt ttgtgctact ttgttatggcaactccagaa aacaaaaata cactcagact gtttaatcaa cctccataat tgcataaggt ctaatcccta taataaatcc cttaaaaatg tctgtgtata tatatttaaa aatataaaat atcttctagt ggttctgcat ctctggtcaa tccctgactg atacagaata tgtattttca tttctaatga tgaaatacct gaatgaaatttctaggacat atggtaagtg tatgtttagc ttttaagaaa ctgccaactt gggggaattg cttgaggcca ggagttcaaa cagcctgggt aacagtgata ccctgtctgt acaaaataaa aaatattagc agcgtgtggt ggtgtgtgtc tgtagtccca gctactcagg aggctgaggt gggagattca cctgagcccagatctttgaa gttatagtga gctatgatca cgccactgca ctctagcctg ggtgacagag tgagaaagct ggtctctaaa aaacaaacaa acaaaaaaga aactgtcaaa ctcttcccaa catgttgcca tttttacatt taccatttta cattcttacc agcaatgatt gatagttcca gttgctccat acccttgctg accattccaatagatgtatt gtgttatctc attgtagttc taatttgtat ttccctagtg attaatgatg tttaacatct tttcatgcac ctattggcta tatgtatatc ttctttagca aaatatatgt tgttatttga agagcggaag ttttacattt tgatgaagtc taatttattg attttttttt tcttagatgg ctcatgcttt ttgtgttatc taaaaaaaat ttgccttctt catggtcaca aagactttct cctatgtttt cttttggaag ctttatattt ttagttttta tgtttatgtt taagacccat ttctagttac aatttgtgtg attttttgga agggtcaagg ttcattttct tttccataag aatgtacagt tgttctagca cccttgttaa aaagactttcctttccccat tgaactactt tgtcaaaaat caactgagca tatatgggca tcatgaattt taatcctgtt agaactgaat gttcccaagg caggccatgc ccatgactga cctcctttcc ttggattgcc tacaaaacag ataaagctaa gtctggagca aagaaatcca tgtctaacct gtattttttt tttttttttt ttagatggggtctcgctctg tcacccaggc tggagtgcag tggcgtgatc ccagctcact gcaatctctg cctcctgggt tcaagtgatt ctcctgcctc agcctcccga ggggctggga ttgtaggcgt gcaccactat gcccatctaa tttttgtatt tttagtagag atagggtttt gccattttgg ccagactgtc ttgaactcctgacctcaggt gatctgcctg cctcggcctc ccacagtttt gtgattatag gcatgagcca ccgtgcccgg ccttaacctt tgttttctta cacaacacac tacgtgatgt tttccacatg catgggtcat ttgcttcatt tacgtacaaa tgcataagca atatactgtg tggtgtgagt ttgtgatggg aaaaggaaga agttttgcggatactacact ggcttcctgc tatctgtctg tgtgaatggc tatggacttt gtcttctatt tgttcgctta gcgcagatat gatcagctta caacttaaga ttctagagaa agagggtcat atctgtaaag cactctgagc atgtgtgaag tttaatcaat agcatatgag gttacagcaa attcactatc tttgtttcttcagctataga atggcatgag gattcatctc aatttagttc aattctgttc agaaccatga gctagctgtt catggaagga aagcccacct gattgtggcc agggaaggag aaacaacact ttaaccaggt tgatttggtt ctcacagaca ccattggcat gtgacatctg gaacagacca tgcctggtct ctgttcgtat cacttactattcagctcaat attggtctga atattcttta gactgactga aatgaaaagg aactgttgtg taaccatcca taattccagc ctgtagacct gggctgtatc tctatgccct gcctggcaca gaccccacct cctgctcctt ctccctcacc accagtcaat ccttgtccta atgaacaggg agggcaaccc tgaatgggga gtggagggaa gagatgtcat gagatggcaa cgtgcaccct gaagtgagga tgaaggctat gtgaatgttg taggctgaca gccgggcata gtggccccgt tgccatggcg atggaggcat gttgatgcga agtgtctgca cagctcctag gatttttaac agcagctggg cagagcctcg gcgtccctga attgttgccc ccctgagtcactgcttggcc ccagctgtcc tgatctctgt tgacaaatgg ttgtccttca cagtcaaact actaacagta ctctaattaa tgaatgtgct aattattctt gcctactccc agcatatttg tctaactaac ctgtcacaca cagatcagtg cagcatatgc ataattacgg agagcgctgg gagcagggga tgggtgggag aggggtgggctcgcagccct gtcgctgtgg gatatttctt gtaaagttac ctttgctaac ggtcagatgt cgtggggata tgttatttcc cgtgaagtgt atatgtcttc ctttctttcc tttctaagaa tctctcttca gggctgaggg gccattgctc agtgctttag cctgtgaggg gattgccagg tacaaatgca gaaggaccagggagcccagg ttctgaagac gattccggta gcagcacgta gggtgattaa aactccagac tttaaagcca gaccggcctg ggcttgaacc cttgttctgc tccttgctat gtgggtcttt gccttgacca catttttttt ttttttttaa gacaggatct ccctctcttg cccaggctgt aatgcagtgt tgcgatcaca gctcactgaagcctccatct ctacagcctc aagcgatcct cctgcctcag ccccgagtag ctgggactac aggtctgtgc caccacgtcc agctaattta cttttgtaga gttgggggtc ttgctatgtt gcccaggctg ttctccaact cctggactca agccatcctc tagcctcggc cttccaaagt gctgggacta taggcgtgagccacggtgcc aggcccttga ccacattttt aacccctctg aacctcagtt tcactttctg ggcaatggga ggggggtaat ttgtccctca gagggttgca ctgaggggca aatgtgaggc tctgggtaca atgcccagta cagactaggt ccccacgaca cagccgctca gcggctccgg attctgggct gctctggact gcggccaggcggtcttctgc gggaatccgg gcaggcaggg cgggctgcgc tcccctcccc ggctctcccg gtgccccttg tctttttgtt ctgtctcagc agctctctat taagatgaat ggcatttcca aaggcttcac ctctgataag tgttcctctg cagctgcagc cagaatctta atgtgcgcgc tgtaatttaa tggccgtctc ggctattaac acgctcttct cgggtgaagt ggactccctc catccccggg cctctgcacg tgctctgcgc gctggctggg ggtgactcca aggagctcag agcggggtgc ccggcacctc tcgccaggcg cctttcgacc ttctaaagcg cgaatggctg gacttttctc ccatgtgtgg ggccccagaa ggtgtggggc cccagaaggtgtggggtccc tgcgttccac ggagcccgga aggtttccag tgatggtggg ggctgaccac gttggtcccc gtgggtgctg ttttcatgtg ccggcagatt gggatgagtt taaaagacag aagcgtgtag gatagagaaa cttctttaaa aactggaaat tttaatctgg ggattataac tattggacag tcaagtgcaa gagtgaatacacttctcact ccctcctccc aatttttatt tgcgggatta gtcagtcccc ctctgccaca tgataattgt gagaactacc agggtcttca ttctcctgcc atctggttga cctctccaag aatggacacc cgggcagcct gggccaatga ggctgtccta agagtttaga tgagagaagt cagtctttga caggtgatggaagctgtaaa atgtaaaact ccacagttgg tgaagatgtc tccaggaaac aggtctgcag agagaatacg tttgacatgc taagagaagc tgagagagag cgagaggaga gattggaaga aagacagaga cagaggtaga gagaagggaa agagagagag aaagggacag aagagagaga aaaaagaggg ggccgggcgc ggtggctcacgcctgtaatc tcagcacttt gggaggccga ggcgggcaga tcacgaggtc aggagatcga gaccatcccg gctaacacgg tgaaaccccc gtctctacta aaaaatataa aaaaaattag ccaggcgtgg tggtgggtgc ctgtagtccc agctactgag gaggctgaga caggagaatg gcgtgaaccc gggaggcagagcttgcagtg agctgagatc gcgccactgc actccagcct gggcaacaga gcaagactcc gtctcaaaaa aaaaaaaaaa aaagagagga agggcgggag agagagagag agaaagctct ctagctccaa ggcctaacca catctctgtt cttttcaact tcagctgtca gatttttaga ctctttgagt gaataaattc tcctttttgcttaaactagt ttgagctaag tttctattgc ttgcaactgg aatactttgt aagaggactg gccttcattt ctgatgcatt gtcactaaga tgtaagtgtt agaagagcta acgctttatg gggttcaaac tccttggcta ccaaaaccta aacatcccct gaaacttacc aaactgcagg tatgaattgg atctcactaa ggtgaatata caaatcttgc aagtgctgag ccctaaccaa tcttgtaata actctgtggt agttaatttt atgtcaaatt gattgagcta aaaaatgccc aggtagctgg taaaatgttt ttttctgggt gtgttaggga gggtgtttct gaaagagatc agcactggaa tcagcggact aagtaaagaa ttcccaccct caccaatatggtgggtgtca tcaatccact gagggcctga atagaacaaa aagcgggcag aagggcaaat tccctcttct tcttgagctg ggccatccat cttctcctgc ccttggacac tggagcccct tgttctccag cttttggatt cagactgggt cttgcaccat tgccctccat cttctcctgc ccttggacac tggagcccct tgttctccagcttttggatt cagactgggt cttgcaccat tgccctcctt gatgctcagg cctttgaatg cagactggtc tccaccagca gcttttctga gtctccagct tgcagatggc aaaccatgaa acttcatggt gtccatgagc atgtgaacca atttctatta taaatctgca atatatatat atgaggagac ttatttatatattggttcag tttctctgga gagccttggc taatataaag tctatactct acaaagtgcc ctaggtactc agggagtacc caagtgtgtc atgaccagcc cgacagccct ggctgctggc ttccccgcac acaactctgc acgctgcctt catcagcctt tctctctcag ctgaaccgag ggcattgaag cgggcctctg gcactgtacctatgagggag caatatcttc ccctacactg acctcttccg tgccgagatg cagccctccc tgctgccact agttacagtg gtccatgttc cctttcaaag tgaagttttg ataaaagcac ctcttaacca atgccaaata gctaagtctg ggacaaagat tgcaggtatt ttgcattttc catgtaacct cagagggattgccattcaca ctgatctgag ctgcagaata ccaggcagcc acctcaccca cccagcaggt ccactcttat actttctcag aaagcacagc cactctactc ttattcagtt gaaaagaatt tccaggaagg tgtttctgcg attgcctcag aaaagtcagt tccctttggg aatttccctt agggatcatc tgtaactcca tttctgccttttacctgaat tctttggttt ggtttgaatt ctttggttta atttatgaat tccctttatt acttttctct gaagaaatgg agatatcagc tgtccctccc cactgccatt tattccttcc ttcattcaaa ccttatgtgg ctgctactta ccgtgtgtta agtgttcact ttttttcttg gaattcaaaa aaagaaggac agtatttggg gcacagatct tttggtgttc tatacatttt tttaaagttt cattttacat ttgtgtgtgc gtgtgtgtgt gtgtgtgaga cagtcttgct ctgttgccca ggctggagtg cagtggcata atcattggct cactgtagcc tcaaagtcct gggcccaagc aatcttccca cctcagccac ccaaaatgct ggggttacaggtttatgcca ctctgtctga cctgaaagtt ttgggtttac tttcccttct ttctctttgc tgaagtcaga gatgatggca gcttccagat tctctggtgc ctgtgctggg ctcgtgctgg tcatggtctt gggtccagga ttcattctgg agactctcag ggaagtttcc catgacaagg aaatgtagga gagtgtgctg gctttgcgtgctcctctgcc aagccctgct tctcctggtg ggacacactg aaccacagcc agggcatttt ggtggttagt taaaaaaaaa aaaaaaaaaa aaaaaaggaa gaagaaggca ctgtgtaatt gtgccgggga tcttcagaaa ttgtaatgat gaaagagtgc aagctctcac ttccccttcc tgtacagggc aggttgtgcagctggaggca gagcagtcct ctctggggag cctgaagcaa acatggatca agaaactgta ggcaatgttg tcctgttggc catcgtcacc ctcatcagcg tggtccagaa tggtaaggaa agcccttcac tcagggaaga acagaagggg agattttctt tgatggttgt ttggaagtca ggcttaaaca attgtgtctg tgtgtgcgcatgcacaaaca cttttacctt atctttattt tcttcttttt atttgaatgt atagggttgt gtgtatttct gtgtaaattt ggggttttcc tcctcttagt ctttcacttt tgtggtgatt accagtccca tttttagagc cagggctgca acttgaaggt tttgctaaaa ccctcaccga agtgtctatg atcagcattttaactattaa ttaatgtggc caggcaaggg gtggaaggtg agaagactag aaagggaaca tgatatacac atttactcag atactgggct tttctaacat ctgcagtgca attgaagtta ccagtcatct gcagtctaaa aagaaagtga ttttgggagg tgcgtagaaa aaatcatctt attatttttc ctctatatta cttttttctttttttctcct gaagaaactt ttttttttgg tgataccttc tttttctcta gcacgtataa ttttggaagc atttttcata tgcagtgtat acttcagaaa gagagagaga gagaggaaaa ttgtcctgtt cagcgtttgc atttccatta ttcctgctat tagttaaaaa caacaacaac aacaaaaaac aagcaggata cctagatctg gaaaagggag aattgtgtag agctgtcttc ctaaagttct gagttagggc tgcctcagac cactttcata actatctcca gtggctttgt gttttatatt tattaagata gagaaaaaaa gagtaattac taagggcagc tgctgtagct ttatggtgat tactgaacat tgacatgctg tcacgttttt ggaactttgagtatttaatc actttgggat attctatttt cccccatctt gagtgtggac agatgctggt gatgtagcct tctgggcaca gagcaagcct ccccctcagc ctctgcacca gaaaggctca gcttcacaca ctccaagtat gttttctaca agaactacac tttgtggctt tctgacccaa acatttttat actaaattac acacaacaaagttgtagctc agagagggaa caaatggctt atttaggcca ccattttctt gagccattat gatttcacac agggctccct tggccctgta aattggcaag gattccatta ttcaacccgc atacatgtac agagaccctg ctctggccca gatagtattc tgggtacagg cggatagagc aggaaacaaa acagctacagtgatggacag gtcagcctgc agcaatgcct gcagtctctg caaaggtagc tgtatgggtg ggcaggtggc tagcacttat tcagctctgg aaggatctcc cctctggcct ctcccctgac acccatcaat aaaactgagg agcatcggtg gacaggggac cttgtgcccc ctccctgcct gtgcagttgg ggctgaaccc agctacgaagtttgagctca ctctctccag ctccctctca attcagagct gaactgtggg aagcttcaga gctctctgtt tcaaggacag gttctcctca cctctcctaa tggaggtgca ccagggaact ggccctgctc tgcccagggc tttctcctgg actttgccat catggtctag caaaccctgt tcagattgag gtgagtggtgagatttcgaa ttctttttga cagataggat taagtcttct tctgtgggac aagtgggagg tagaggtaag attaaagatg gccaaatgtc tgagtcctga cagccacaat atggagatct agacttttta cagaccacag ggcacagggg cctcactaac agagttcccg gaagtgatga gtgtgctggg ggcttcctgg ttgaagagacactagaatgg accagctggg agctaatttt ttgggctgga gtgtgatggc ctgcacatca ctgcctctgt ccctccattg tcacagctgc cccttaggag ccagctgagg caatttgtgg tcagagtgac tttgcacagt tgtcctgcct gtgttcagga agggagtttc tgtggtccct ttgaaaccac agaagagccc ctcgtatagc tctcaatgga gggggcaaaa cattcaaata actcaggaga taacacaact atttgttttt aactgtgagt ttttaggcaa tcacaaagat ccagatgtat gtccaagcct ctctttgcaa ttctaattaa cctcaatgtt gcaaccatag acctacctta cagagttcaa aaaaatatgc aaaaaccctg cctttcttcttcctcatacc ccaaaatgcc attctgaaca tttcctgtta gttaaaaaaa gatttccatg gtgttaccag gcactgtaca cagtctgtgt cccaagacaa ggaggtacag ttccacatgc gcccatgact gggttgggct ctgcactctc tctatacttt gagagcctga ttttctgtga ttgggcagag ctggcccacc tggtgcaatgtcctcctctg cctttcaaac atgttttagt catcaagatc ttcaaatttg taaccctttc cagcttgatc cagcagaatg cagatttgga aaaacagaac gagtttaaaa tacatgattc taagaaacct ggaccagaac tatcaaaact tggtttccca gagaatatag caaatgggct cattggccaa tactatgacattggcttttg agaaaagaaa ggctttattg caaggctggc cagcaaggag acaggagttg ggctcaaatc tgtctcccca gtttggggct tagggcaagt tttaattaca cagacgcatt tcttatgagt agcaggcaga gagcctccaa cttcttctgc ctaggtacca gcagcttaga catgatgcaa acctgggaag cacatactgtatttggagaa agtgattggg aagaaatgtg agctgagggg aggggctcag tgcccctgag ctacacttag tgatggcaga ggaaggatgt cctcccgcag gaggctgttc cacatctgct ctggttgtag ggggagctgg caggcattag cagcggcctc tttcccccaa gagaggcagc ctcctccaag ttttggcgacattatggccc tgcaatcata agggtttgtg agcatagtgc taaggaggga aatggagctg ctgttactag ttccacccca acacacacac acacactcac aagaaacctc acaagcaccg tattggaaga ctttgccatc caacctggga tttgacaggc tctagaagca gaatcataga ctcatgaagt tcccccaaag caggaatcttccttacagta acccccaacc acccccctcc accgcctcca ccggctgctt cttcctgaac actgcagtgt ttggaaaact cacaaacttc caagcttgcc tttcctattg ttgcatggat tgaaagcttg cgttgtgtga agaatggcgc ttcctgctgt gcttagtttt atctcatata atctttgcac catttaatcc ttgcactcac ccactcatgc aactgccttt gcagagactg gaggggccgc tgtaggctga cctttccttc actgtaccta ttttgttccc tgctttattc ccctgcaccc aggacactgc ctggcacaaa gacaggtctt tataagtgta tgcaagtgaa taaagatata tatattatta ttgttatttt tgagacagtt tcactctgtcacccaggctg gagtgcagta gcgcaatctc agctgactgc aacctctgcc tcccaggctc aagtgattct catgtctcag cctcctgagt agctaggact acaagcatgt gccaccacgc ccagctaatt tttgtatttt tagtaaggac agggtttcac catgttggcc aggttggcct ccaactcctg acctcaagtc atcctcctgcctcgacctcc caaagtgctg ggattacagg catgaaacca gcctagaaat acatactatt atttattctt gttttacaga taagcaaagt gagtcatgga gaatttggtt gaaagtccca aggtcaggag tcgtgaagct gggattaaaa cctaatcatc tgactttaga gagtagacac ttgctccatg catattgcctccaattcatt cattcaagca ctccctgctc aagaagttct ttcttatgtt gagctgaaat ctgcagccct atgcgtttta cccagcagtc ctggtgctgt tccctaaaat cacttagact gtgcctgctc tttctgtgtt tacagtgtca gctgtaatat ccccctcttc ggcctaacgt ttctgaagtc ccttgccact gggtctcctctcctcttcct gtgttctttc taagaacacc tatgcagata ggtgtcttct gtacagggaa gctgttcctg agatccgggc atcgactctg ttagaataat ctacgtatga gttatttttt tgagaactat gtgtcattgc tgactcatat taactctgtg gttaactaaa atctcaagat ctctttatgt ttgttgagaaacttatttaa cttctctggc cctccgtttc cttcactgag cagtggagtg attgataacc tccacctgtg gttgctgaag gtcttgcaca agatgatata gttaaagtag ctagcagtgc ccacgtacgg cggatgcctc acaacggttt gcagccatct ctctatctgt gtctttgtct ctctctcaca ctggttttgg cttactgttagcagctagcc gagataagtg tgtttatggt ctttgcatgt attgtttctg
tagcatactg gaggattaca agaggttggg gagtgagggg gcggtgagga gtagacaaag gcagccaact cttccaagtt tagcttagaa ggaaggagcg gtaaacccta gttgaatgtt ggactgaagc aggtttgttt ttgttttgtt taaaggatag ggaagatctg tgcgtgtttc caggataaag aaaaggagagaatatgatat taaagattct ggaagtggga gaaggagcaa tgaaatacag acttgaagtc agtggcatgg acagggtcaa gatcacagtt agaggatgca gccttagaga aaaggaaggg gctcggttct ctgagcaagg agggaaagaa gagaggcaga tgcagagaag tacggcacat cgtgctgctg gttgtagaaataacctctga cttttaataa agtcatccct cggtatccct gggggattag ttctatgacc tccctcggat gccaaaattc gtggatgctc aagtccctga tataaaatgg catagtattt gcatttaacc tacacacatc ctccatatcc tttttttttt tttttttttt tttttttttt tttttgtgag atggagtctt gctctgtcgccctggctgga gtacagtggc tcgatcttgg ctcactgcaa gctccgcctc ccgggttcat gccattctcc tgcctcagcc tacaggtgcc tgccaccacg cccagctaat tttttttttg tattttttag tagagacagg gtttcaccat gttagccagg atggtctcga cacatcctcc atatacttta agtaacctct agataatctc tagattactt gttttgtctt tttttttttt ttttcttttt gagatggagt ttcactcttg tcacccaggc tggagtgcaa tggtgcaatc tcagttcact gcaacctccg cctcctgggt tcaagcaatt ctcctgtctc agcctcctgt gtagctagga ttacaggccc ctccccaccc ccacccccca acaactggctaatttttgta tttttagtag agatggggtg tcaccacgtt ggcctggctg gtcttgaact cctgacctca ggtgatctac ccgcttcagc ctcccaaagt gatgggatta taggcatgag ccactgtgtg tggcctagat tacttataat acctgataga atgtaaatgc tatgtaaaca gttgttatac tgtattgtta aaagacagtaacaagaaaaa aaatctgtac atgttcagtc cagacaaatg gttttctgtt tttttttttt ttttttaata tttttggtca gtggttggtt gactccagga atgcagaacc cgcagatata gaaggttgat tatgcgttca gaggcaggga ataccatctt gggttccaga aagaaaatga tcagcatttt ctgtcatactctggtaaaaa cagatctttt gaatggacag gtgtattaaa ccctgtggag ctggctgggc ctggcggctc acgcctgtaa tcccagcact ttgggaggct gaggcaggtg gatcacgagg tcaggagttc gagaccagcc tggccaatat ggtgaaaccc caactctact aaaaatacaa aaattagccg ggcgtgatga cgcatgcctgtagtcccagc tactcgggag gctgaggcag aagaatcgct tgaaccctgg aggtggaggt tgcagtgagc cgagatcacg ccactgcact ccagcctggg caacagagtg agactccgta tctaaaaaaa aaaaacaaaa acctgtggag ctgatgaaat cctgcaggga gcttcacggt gacagcaaga ggagaaacacatccccatat gccccgcaga gtttgaagtc ccggctgcac ctctccccag cagcaggttg actctggaaa gttgcagcgt tcttacctac agagtgggaa cagtactacc cattgcacag agtgggtgca aagctctgtg acggaataca tggcaagtgc ccaccacatt gcctgggatg aggtgggccc ttcctttacg taagagagccctacagatac actcaaagtg ggcacattcc tacagaagga gtgttatttg tgtagaaaag aaaaacatga aaggctttta ttcctataca caataaagca cccctttaat gtctttttga ggaggataat atgaaattga tgaaaaggaa ccctgtggtt ggatccctga caatcacatg tatccctttt ttcactcttg aaaaaggagt aaaggaataa aatagaaggg gagagggggc agagagacct tcaccgcccc ccccccaccc cccatcatcc aatctatagt caaaccctcc agactgtgtc tccttggcat ctctgacacc cccaccgcca ccaccccagt caattcctat cttatccccc tatcctggat ctgattctgc taagttcctg ccacactaaagacagggtgg ctttctgatg acaacattcc tctgcttaaa cctgtcagta attccttgtt gctctcagac ggaactaagt tctgaatttc ttcacacggc tctcagcaag gtcacagtca ccctgctagg ccccaggggc aaatctcaat ggtcatcttc ttgaagacct ggctcagtta tttctttctc attgaggctc acgaccccaccttcttgcat gcctcaaacg gccccttacc atgctcttct ttcgcccata gctcagcaca ccatatcatt ttaatttatg tattttgctt aatgtggatg atctgtctcc tcctctgctg tcctcaccag agcatcagtt cctcaaacca aggctctttg ttttgttctt ggatgcaagc taaatgtctg gcatgtggcaaatggtcata gatacatgtc attgaaagaa tgattcatca cctccctctt tggccttgtc tgtggttcta ccaaatccca ttccctcccc agtgccctcc attccccctc cttggctgaa cattctgaac cacagacagt tctttaccct gaacctttgc atattttgtt ctcttagctt agagcggccc ctctccctcc gtctgcttggctaatttcta cttgttcttc agattttatc ttagatgtca ttccctcaag gaatccttct gtgactcaac atggaattaa gttgcctcct ttgaccctga aagcaccatg tactcaatct catcttggca tgactcactt tgctgtgtgg aatgtctgct ttccttgttt gtctattcct ttagactgta agatcctagaaagtgggggc cgtgccttgc tcatgactgt gtttctaaca ccaaacacag tgttcagtag agagcagctg ctgagtacgt ttctgctaaa tgacagttga tggaggacat ttagggttgc ttggaggtca agtcaaggag gcatttaaca ttctagtaaa acaaggaagt aacaggctcc tgaacatgcc cacaatgaac cagatgcaaaccttttccct tggcaggatt ctttgcccat aaagtggagc acgaaagcag gacccagaat gggaggagct tccagaggac cggaacactt gcctttgagc gggtctacac tgccaagtga gtcctaaccc tgatgttgct aataagtggg ggcatgggca ggggggcctc cttctaggag tgatgaccac ccttaatacc acatgtctgt ctgagccaag tttctgagcg ccagggaggt gaggaaggtt ggacttcacc agagaggctt tgtggacacc ctttatcatc ttagtgagtg ctagtgtcaa aacaaaggga gtggggatat ggggcacatt ggtggaggga ggtgtgatct ctgcagcttc agaaagatct gaaagagtca tttggttaga gaagttgacctatttcctgt ggggttagac cagggttgct actgtgaaca ccagccatga ctcaccagtc accttcagaa gccacaggca ggacatgctg acgacagcct tcaactcacc caccccttgc tcccctgcgg gtggaagtct ggaggtgaca ccactgcatt ttctaacacg ggggctcctt gagcaactag aacaagaaca gaaagaatggggacattagc aggtgctttc cccctctctc attcttttct ttgaataaaa aggttgtttg aaaacacctg agcggctcct aaagatgggt gcaatctatt cgggatgcaa atccgaatga atgttattca aatgctcctc tcttctttat gcagagtgta tttcaaggct cagccagtgg caggcatgct ggggactatggactacggac taggggcctg tcacagagga aggcctcatg ctagagagct aagggaggag ctggccttca gttccatccc aggagcaact ttgatgttcc cagagatcct tccaaagggg gagtcatggt cacccaagaa aaatgtattc agaatgccaa gaatggtgca aactcaggac aaagattcac actgcagggt tggagtccctgggcttgctg ctggcaccat gggagggagg gtccccttca ggggtaccgt tggtttcctg tgaattaaac tggcttcaag ggatctcgac tgaacaggcc tatatcacac tcactgatat actctctctt cagtccttct cctcatctag gtatttttaa ttgtttcagt gaggtgtagg catgagggga ttggagggggcatctcctcc attgcagttt ttcattggct gctttgctcc ctcagctccg aaatcgctgg gccactctcg aacgcattag tacggtagtc acaggttgat tgcctggccc cttgccctct gtgggcattt tccctttcag acagcccctg agtactcaca gtgctgctac agtgggccac ctagatctcc ctctttctcc atgctcccacgtgctctggg ctccactccc ttctcccaag cacttctgtc cagggctatt ccagcagtct gacctcaagg aaatcctttg ctaaactgat tatagagagg tttctatttt aacatttagg tcttccatgt attaattctc agaatcaatt taagatgttt aaaggtgtga tttaagacat tttaaaacca tttggaggag agtacagaaa ttatgtcact tgctgtcagc ctctttgcac catctgcaga gaaagatact agagtcccgc cttggacaca tccacatgca agaggtgcaa agaaggtgtc tttgatgagg caaggtcaaa acttctcccc agacgaaatc caaagaaagc attcctacta tgctatatca gtttggaaag aaaaacttct gccaggtgactgcattctca ctggtcacat tgtgttccta tggactcctc agctcaacca atttggagaa gttatggtgc aatttcacca tatctggtta gaagttaagt ttccaatttg ctggcaatga agaagaaatg gagcaggcca ggctgtgtag tttctgccac gtgcccccgg gagtgaacag ctctgtttgt aagaagccat ggtgcttagacctgggctcg ctagttgcca gcctccaaat tgcagaagtg ccctttggtt ggtggctatg ctgtgtcact tgggaaggtc gtttggaagt tccacagtcg ttgtggggtg ccagagatta aaaagcgtaa gaggagagtg gaaagtgatt gttgctgctt gggcatcccc accgtgtggg tgctgcagcc cagctctcaaaacccatggg tctgtacact caacctccat gagagggaag gagaaggatg agggagggga gagatagcca tggaaaggta ggaactaagc aggcagggtg gagagttttc tgtaagacaa aaactgtctg gacactgctg cggttctgtt acaaagacca cttcctccct gggccagcaa catatctgtg tgcctgtctg ggttgtaaaaagggtcaaag atcaatgcag caggcagcta catgctggca aaagccagag gcagctggtc tgtttgcctg tgccaggaaa ccactgggaa tggggttgtg tgttattcta ggagaaagtc gtcccagcag cagcttctcc aggggcatcc aagagcactg aaaagggttg caagatgacc catgaggctg caggaagaaaagaacatgca tttaatcttg ctatctgaaa agtaagacat gaagctttcc tcatttttaa tatacacatg gacagtagta tgtgtatata gtttatatgc aaatatactt gttataaggt tgcatgctca aaatttttgg ttcatggggt gtgggatcat aaatgtttag ggaccatggc tatcaaggaa aaacagcatg aaggataaatgatactggtg gattaaaaag acagatgcat gtatttttag cataaaacac aactgctgac tgatacagat agctcaagat tctggggcag ctgctgaaca gatacactag ccagtgtggc tcatcggctc agacttggcc ttaattaatg ggctgtccct ccacccatct cccatgaggg cagagctgag ccagggtttg agagctaaaa ggaattggac ctggactctg ttcacgtgta tattttaatt ctaattaatt cattcttttg aaagacagag tcacactctg ttgcctaggc tggagtgcag tggcacgatc ttggctcact gcaacctcgg cctcccaggt tcaagttatt ctcctgcttc agcctcctga gtagctggga ttataggcac atgcccccatgcctgactaa tttttgtatt tttagtagag acggggtttc accatgtcag gctggtcttg aactcctgac ctcaggttat ccacccgcct tggcccctca aagtgttgga attacaggtg tgagccaccg tgcctggcct gttcacatgt ataaaacaca gtttaatgtc ctattcccag ccaatgagca tggctagagc agccttggtcaaagtttggt ttttggagaa aaatccttgt tagctgacct aagattcctc tttgtgagtg taagtaagca caggttgcag agaggagaag ggtctctgga gaggtgtaat tttctaaatg gattacaagt tcatggactt ttaacaggtg ttacagggga taacaagttc tttatagaca gacttttgag gacgtttaagggtattctga ttcttggttt tctaagaggg gaatgtatta tttaactaca gacaccccta ccgcccactt tttgcagagt gtatcaaaac atgtttttgg aataccaccc tcatgtcgct tctccctgca tctcttatct cttggtgtcc attctagact cactttcttt ctgtttttta tttttatttt tttttgagat ggagcttcactctgtcacca ggctggagtg cagtggtgca atcttggctg actgcaacct ctgccttccg ggcttaagca atttttgtgc ctcagcctcc tgagtagctg ggattacagc atgcaccacc atgtccggct aatttttgta tctttagtag agacagggtt tcactatgct ggccagcctg gtctcaaact ccttacctcaggtgatctgc ccgcctcggc ctcccagagt gctcagatta cagacgtgag ccactggtgc ctggcctaga ctcactttca agtggcatag acttgtaaaa ttatttaaag gtgataggtc tacaatgatc ctgtcaatta gtattgacac tattattaat aaactgttat taattatatt tacttacttt aaattaatcc aaactaattaacggaacact aaagagtttc tatgttttat tcccagaggt ggagaaaaat gaaagggaat atagcaacga attcttttct ccataaaaac atgaatagtg cagcacatca agttgaacat accacagcaa attgttgcaa gatctgctga gtagctccta tttagacctc aaggaatgag actcaaaatg ggttcatcag ttctgttttg cagaaaaaat agcgcaaaat ttctcaaaag aaaatccaga ataataataa tttgtcaata ggaaagacat ttccactggg ggttaagaag gaagacattg gaacaatgat agccaccact tattgaatgc ttactgtgag ccaggtggca cttcaccttg tttcattctc acaacagtct agggaagtaa ttactaatgtctccatccac ctcttgtaga tgagcaaact gaggctcatt gaggctagga aatgcaccca cactcacata gcccataaga ggcagccatg gcattgggcc cagaccatgt gaacttcaaa gactacacga gcagccactg ggcagctgtc atggctaaag ccacttgaat tcagcccagc agcaaccccc tctccaggag gggcacataagcttgcagct ttgggtagaa gctgcacttg aagtcctgga tggcgagagg gactggcttg agccagagcc aggaacaagg ctctgagaat attctggaaa tccacaggag gaacccattt tcttacagct gggagaattt cattcaactc caggctgacc atgttttatt aggaacgaag gtgacttgaa ctaatagtcaggaatggttg aatacggacc caatgtcaaa tcactaggca gttcacattt ctaatgagca aatcccttag acaattaaga atttttttcc ttttgcataa cccagacaaa atcgctactt aaaaacaaac caaagacccg aaacatgaga aagagaagga agcaggggaa atctttggta ctaataagtt tttaaacaat aagagcaccagatattttac cccatcagac acagaatgtt attcgaataa ccaaaaaagg aattttttct ctaagtttct tgaactggaa aatgaatcat attttctcag tcctgaggct gcaattttgt gcctctagta acatataaga atagatgtga tgccagtgcc cagtagctgc tgcaattgtt acttggggac ctgtttattcactaagcact tcaccccagt gataaatttg taggggcctc ctgccctttg gagctcctac cgtgtccatt agatcagtgg aaattctggg attcagagca ctttgcaagg tcagcagggg tctgctcttt ctgtcctgtt cctggttttt ggttgtgcct ggattccagg gtaggtttct catctgttac cttcatagac ttctccagaaaaggatcttt tgaccatcag aggaccacga agattccatt ggtgaggcgc agataacctg atctctctgg gttctctgca gggcacagat gaagggctgg ccattcccaa gttctcagtg gtaccactga ggcatgagac cctaatggtt tgcatgagca gtttgaaaat tgcatctttg tttttaccta tataatcaca tgaaacccgt ggttctcaaa cgtcagcagg catcagcatc acatggaggg cttgttaaaa cagatttctg ggccccaaca cagagtttta aattctgaag gcctgaggtg ggtgtgaaca tttgcatttc taacatgttc tcgatgctgc tgccgcctct ggtcccgaga gcatgcctgg agaactgcca ccttcgacca tggactgtgagaattcacat ggacctcaga attataatca gtctctcagt tttacagata aggaaactaa atccagagag attgttttgc caatggtgaa cagctggtta aagtcaggat ggagacttta atcctagtca agtgaccttt cctctgtatt tatttccctc cctttttatg cctctcaagt ctagttacac tgtttttcat ggatgggcatatttattgtc ctgatctgga ctgcagactt ctcaggagga cacctatgat ttaatttagt atagttgaag agttaacaga catggctttg gagacagact gattatggtg tgaatcccgg ctttgccact ccctagctgg atgaccctga gcaagttatt cagcttctcc aagcctgagt tccttattgg aaacatgagagcaattgtga taggcagaat aatggccccc tcaccaatca tgcccacatc ctaatcctag gaacctgtga atatgttatg ttacatggca aggggaaatt caggcagcta gccagttggc cttaaaataa agagattatc ctggatgatc tgggtaggac ctgatgtaac cacaagggtc tttttaatgt ggaagaagga ggcataagagtagatgtcag agtcattcaa aataagaaag atttgatggg ccatccctga ctttcaggtt ggaaggaggt tctgagtcaa ggaatacagg tgacctctag aagctggaga aggcaaggaa atggtttctc ccctagaagt tccagaagga ttgcagccct gctaatatct tgactttata gccctttgag atttattttggatttctgac atcctgaacc atagtaaaag ggtgtttttt gtttttttga gacagagtct tgctctgttg cctgggctgg agtgcagtgg tgtgatcttg gctcgctgca acctccgcct cccaggttca agtgattctc ctgcctcagc ctcctgagta gctgggatta caggtgcttg ccaccacacc tggctatttt ttgtgtttttagtagagaca gggtttcacc atgttggcca ggctggtctt gaactcctga ccttgtgatc tgcctgcctc agcctcccaa attgctggga ttacaaggcg tgttgtttta agccactcag tttgtggcca cttgttacag cagcaagagg aaactcatac agttatcatg tgaactcaca ggaatatggt gagttaaaaa gagaggaagg gtgcaaaaca tccacggtag agtgagaact ctccagggag tgaggactgt gcccagcata cagtgatcac cctcttagta agctaagttt ctgagcacca gcttttttga gttgactttg ttgtctttaa catttgaaga tcacccttct ttgctcagcc tggcttgcag acctgggctg atttgtggat ctgatagaaaagtttcctta gttgggctct tctccccgac cacccccatg ccagtgtggc cacatcctct gtctgcattg ctcactcttc aattccaaga agcgcagggg caccgccagg aacaggaacc ctgccagagg aatacatcaa gaaaccaagt ctcccttacg catcaccgta ggaacagagt taatggatta tgaacatgtg tttgctttataccattgttt gtttcccagg tggcagctgg ctgccccatc ttattgggta gatgtaagtg gaattacgaa tgggatttat gtttcatgca cgatggtgat tattaacttc aactttcagg taattttcag accacattgc actaacttgg tctctgattg tttttctcct tgtttgttta ttctgcagcc agaactgtgtagatgcgtac cccactttcc tcgctgtgct ctggtctgcg gggctacttt gcagccaagg taactcagac ttccctttgt tcattctcct tctataaagt gcatctcaag gaggttcaaa gggcaggctt tttgttgaaa ggactttgcc tgacctctgg ctcccatctg tgaagccctg gagaggtgag agccctcggg aggccgtgtttcaggcatgc tctgcacccg tgcagagcgc gtgtgataat gcattgctaa tgcttgctcc ctggtggctg gctgagagct gctgtgctga caagggtggt ttaaggctaa atgtgactca gaatccttaa gcagtgttag ttcagataca agggcattat aaatgagagt gcctgaggga tctattttgg gaccgctgtcacttggctct tctgctaata agcttccagt gtggtggccc tccttcaggc atgtttccac tgagccacgg gctggatgcc acatccccgg ccttcccaca gttatcagca gcccacaggc ttgacttgag caagttggaa agacaaatca acttccagag ttgatttaac attgagtgga aatcagtcat acttttggtc ccctttcggggccacgcctg gcactgtgcc tggtggcaga tcggcatgaa ctggccagct tctgtggccc tggagggcac aggcagaaag gccacactca gtcccatgat gaactgttta agacttattg ttgtctcccc gctctgtaaa gtagatagag tggattttat gtcccttatt acctttcagg atactttgac tcagggagat aaagtaactt gggtacagct actcagctgg tgaagaacac aggcagaatg agtgcctggg tcttttgact taaaattctg gatttttcac aaagatcctc ttactttatt catttacata ataaatatat attgaagagc tactctgtgc caagccctgt gcctagatat acagtgataa ataaagagta gcttctagag gtcacctggcggtgaggcac aggccagctg gcaagatgga ccacagaagt cagtgaatga agacaatgac aagggtggga agcgccatat gggaagagaa ccaagttcag tgatagagag cagaggtgag gcggcagcag aaaccactta agggacacca cgtggcactc cttctgtgct gagaaggctg tcagtaagct caccatttat ttcctattttctctcctgag ttaaatagga aacatgtctc gcattacttg aaaaatcaag tcaaactatg ctcttactag gagttatggt tctttttatg tcttagatga tgcttgatct agatgaatgc ggacttgctg tagctagata aatacaatgg gagtttgaag gtgtttcgta gccctggaaa taggtatttc ctgtcaaaacaagctttgtc attgccagca gacaaaagca tcagtaacct tggttgataa tcgtcatttc ttaggaataa agtagactgt agaatttttt ttagcagaaa ggaaacccaa agataattct agtgcaaatc cctcacttta tagagcagaa gctcaagtcc cagaggaaca agtggcttga acgaacatca gaattttagg ggctggatttgtaccctcct ggtgccagca gcccacttcc ctgcaggagg cactcacctt ccttgcacag gggtatgagt gtggccattt tccacccata atctctgtta gctcatgttc aattgggttc ccattgaaag aaaaatggac cagtaagttg gagcagaatc attcagatgg tataacataa ggaaaaactt tgcccaaggcaaatcgtgat tgtgacagct ttgtgatttt tagagaatag catgggccag gcacagtggc tcatgcctgt aatcccagca ctttgggagg ccgaggcagg caggtcactt gaggttggga gttcgacaac agcctgacca acatggagaa accctgtctc tactaaaaat acaaaattag ctgggcgtgg tggtgcatgc ctgtaatgccagctactcgg gaggctgagg caggagaatc acttaaacct gggaggcgga ggttgcggtg aaccaagata gcaccattgc actccagcct gggcaacaag agtgaaactc cgtctcaaaa agagttcaca gtttctcttt tgctttgatt ttcttatctg ccggataaca atagtatttt ggaaggcagg aggaattgtg gaaagaaatg ggttttgggg agtggctgat tggaggcaaa tccaaggaca ctcattgctg gtgtgtgact ccaggcagtt actcagcttt tccaagcctc agtttcctta ttgtaaaaca ggaccatggt ctagctagta gcattcctat ggtgagtgaa ataatatgta taaagctcct gacacagtgc ttggcatata tcagattgagccatgtaaaa ctgccaatat ctggctattt atgacctaca aaaatagcat ttcatatgat tccacctaac atctgaagcg caataaatgt tattattgat aatgcaggtg gtggtgataa agttttgaaa tcagaaagac ctggcttcaa attccacgcc ttcactggcc tgacttattt tcattcattt gacaaatatt attttgaacacccctatgtg ccaggcacta tgccaggctc agagatgatc taggaaaaag acagatgtcc tcatctgtct taggctcttg tggcctaagc ctaaatttcc tcgtctgtca aatggtgaca gtaacacact ccttaccaga gagctgggag gattggagac tcaagttccc aaaacgccag gagcactgcg gcaggtgaaaagtattccct caatggcgga agtgtttaaa ttgcttttat atctgtagct ctagataaca ctagttccag cttagttaac tcccagctcc aagccttcag gacttcatag agttattggg gtgctgctct tggcagtttc ccaaaaagct agaatgcaga gggaatctcc ttcccaaaaa gctagaatgc agagggaatc tccttcccaaaaggctagaa cgcagaggga atctccttcc caaaaggcta gaacgcagag ggaatctcct tcccaaaagg ctagaatgca gagggaatgt ccttctcttc taaatggtag ctgttagttc aagaaaggtt aaacattgtg ctgtggggag gctcaggggt gaagggtgta cttttaagag aaccagtttc agagctgggtttggggttta agccctaccc tctgccccct tttacgagct gacagcctta tgcaagcctg gttgaccacc tgaacccacg tttccacatc tggaaataga aatgtgggta ctagttatgt tgaaaggact caggttagat gatagatatg caaatacctt ggaaaccagg agtgtccagt cttttgggtt ccctgagcca cactggaagaagagttgtct tgggccacac atagaataca ctaaccctat caatagctga
tgagctaaag aaaaaacgtt gcaaaaaaaa tctcatattt ttaagaaagt ttatgaattt gtgttgggct gtattcaaag ccatcctggg ccacgtgcga cccgcaggct ccgggttgga caagtttgtt gtaaacaatg ccatgatgcc ggcataaggt cgttaccagt attaggaagg ttctcaggtt tcctctagcccttgggctct tttcctgaag tgcgtgtgtc ttctgctaga ttttgtgacc aatgttgatt gcctaattgg gctaacagca tgttttggtg gctacgaaac tgacacaggt gttttcattt ctccacttag ttcctgctgc gtttgctgga ctgatgtact tgtttgtgag gcaaaagtac tttgtcggtt acctaggagagagaacgcag aggtaggtaa ctgggactac taaagaactg tggagcgatt cctgattttt gagcaggaag agtgacaatt caaaacagta tttgactaga ttcacggctc cgtagcatcc ccttgggtgg gagggggaag gctgactagg acctctgatt cttctttccc tgagctttga aggctctgaa aatacagctg gggggacttgcccagttttc ttattaagca attcctccgc atggtgctgg ctttcaaagg gtgcttcagt gctgtttgct gcacgtgcct tgcagcccca caccctgcac tcccgccctg cagagtctgg cgctggaatg acattttagg tctgggttcc caggcctcct gagagtgaaa tgtttcattg tttgtctaga gaaatgagaa ctaaagcttg caccttgtga taagttgtcc tgaggaacat atctttcagg gaccagaaga aagaatgttg ggaaaataag atgcagtaag atgcagacat gacagcaggg tgcagcggct cacgcctata atcccagcac tttgggaggc tgaggtgggt ggatcacctg aggtcaggag tttgagacca gcctggccaa catggtgaaaccccgtctct actaaaaaat atacaaaaca ttagccaggc atggtggtgg gcgcctgtaa tcccagctac tccataggct gaggctggag aatcgcttga acccaggagg cagaggttgc agtgagccga gattgcgcca ctgcactcca gcctgggcaa caaaagcaaa actccatctc aaaaaaaaaa aaaaaaaaaa aaaaaaagatgcagacacga gactgtgaaa ctgactagca tcaccattgc attgtttata gatgttgcca gacagaaagc cccaaagcag cacagtacct tcctgacatc tggactagga aatctagatt ttagtaaaat acatgctaat acttacagaa gaaatgtcgg cgttagagta tgccgtcagt tccttagaga ttgcaattcctaatgcacta gtatggtttc aggtgccagg aacacgttct gtgaggctgc tgccccaggt gctgacccca gccttccaca ccattttcct tccttgtgtt cacagccgct ctgtctttta caatagcacc cctctctagt ggctaatggg ctctatgatt agatagcatc cttcagtagt gataaaggca gtgacatcct agggaggtcagcgggtgaaa gcgctatatc tggaaaacct gagagcctgt gaagctcaag gacttgacgg ggttagaccg tgagccgggc tgcagctgga aaaagaatga ctgttctttc agcagatcct tccctgtgcc atctctttct tcattcctct ctagtggcat tcttatttat cctctaaaac cacaattcca ttatctctcctattcttatc aacactgccc taaatgatat tctttattct cttttgccct ggaaaacctc tatcatgcct tttcccatgt gattacctcg ttaagagtgg gggtggaatg tctagcaatg aaataagagg gtcttctctt ttgcctggct ccctatgcag ccctatctta ccccctgcaa agtcccaggg atgtggctca gtcactgctcctctcttcat ctgtcaccac ttgcttgaga tcctacagct gctttaattc cgagaccatc tgcagaacat gacaaaattt gtccacctac ccacatgtcc ttttaacttt aaaggcttta ctaactgatt cctattaggg aatgaacaga ggtggcaaaa ataaacaata ggagattgat ttacaagaaa tctttaaaat agtagatttc ttcggacctc attgaaatat aaatggcctg ccttcttgtg tccctccctg gtctccctct ttaggtgata agaagaagat cctgccagcc ccataacccg ccatctgcgc gggttctaga cccccttctc ctcccctctg gccgtggtag gcattactga tgaatcatgg tgctctttct tccagagacc aaacctggcctcggaatcct tcttaacaca gatactgctt aacacaacca ctctgagcag ctgtcataag tagaagtaat agatactaga agaaatgtct aagcctaatc tagaccaaaa tacggcctga tatagatgca agccagaggg gctttatggt taaatgcaag gagattttca accctgccgt ctagaagcta cttgctgaga tcttcttcagttgggcccat ctcctcccca ggcctctctt ctgttcctgg gctatgtcac acttggactc tgcagacacc taatgctctt gggacctgct ttagttcttg acctcaccaa ccgaggagga attgctagat gagatccttc ccccggaatt tctctcttga accccagatg gtccgttgcc cctttccaga agttgctccagccctgtccg cttaggaagt tcagtgtcat ccttgatcca gtgggtaggg aagacattcc ataatgaatg ccccagtctg agcttcttcc ttcaggcttc aggctgccct gcgaggattt tgcagctccc tttttaatgc cctctagaag tttctggctc ttattttcag cccttcatcc tactctctct gaccccttcc tctatcctgtttagttcacc tgtagcagtt actacccagc agtgaaggat gaatcttggt ttcgtttctt ttctcttctt ttcttttttc tcttctcttt tccccttccc ttcccttccc tcccttcaca tcacctcatc tcacctcacc ttacatagtc ttgctctgtc acccaaactg gagtgcagtg gcctgatctt ggctcactgcaacctccacc tcttcccagg ttcaagtgat tcttatacct cagcctcttg agtagctgag actacaggtg tgcactacca cacccagcta attttttgta tttttagtag agatagggtt tagctatgtt ggccaggctg gtctcgaact gctgaactca agcaatctgc catccccggc ctcccaaagt actgggagta taggcataagccacccatga tgcccagcct gaatcttggt ttcttcccca ttcatttaag ctattacctg ggcctgaact caatggcacc tggcaccaac tggcaactga ctcttggtct tttattacct accttcccta gcaggcactg ggttgctccc tcttcctatc ccatggagtc ctgtcctctg ttggggctcc tactgatcct cttggcaata tgaagttctc agctcaatgg tgggtgggca atgactgcca actcttgagg ccaatgaact caggttaccc cactcctcct cctcctgagt tgctcactca ctcctcattc actcaacatt gattcagtag atatttgcta cctgctctgt gccaggtacc aggtcagttg ctgaaggagt aacagtgaac atgacggagtctttgtcccc aaggagaccc aaggtgtctc ctagagccag gggcacattg caagaccaaa tatattcaac ttaccaaaat aatcatagac ctagttctca aaaagcaaga agactgattc ctcgttgtca tttctcctcc tcagcatcaa tgttttagag tctgtgggcc cctccaagtg tggagtatgg tgttacttca ccagagtttgaggagaaaca ttcttctttt ggaaggccgg ggagcataga tggatatcaa ggctgctgtt tctaaaagcg aaacccacca aacaacagta ttagaatcat ctgtggtgct tattaaagat acagattcct gggccccatc ccagacttat gaatcagaat ctctgccaga ggaagcctga 2aatttgcat tctcagatgattctgcattc tcagataaca cattctttag gtgattctta 2acacactgg agtttgggaa tcgctgaagg ctgttcactt ctcttttctg agaaatgatt 2attcatttc agaaatattt gcagaggtcc ttatttattg gagatttgtg ggtgggcaga 2gagaaatat cttgtcctca cagagcttac aatttttatt ttctttagaggtcaccaggc 2taaaatgac acttccctaa attctgaaaa gaacagattt ttaaaacaag aagggactgt 2atgttttct gttcctacct cgtattttgt tcacattaag aacctggggt gggaagtgga 2gaggggggg tgactggcgg ggggccacag agagctgagc tggggtggtc tcgaactcct 2aactcaagcaatctgccag cctcagtctc ccaaagtgct gggattatag gcatgagcca 2ccacgatgc ctgggtggaa ctcagggctc tggatgcctg ggcgccccca tctcccacac 2acggcgcct catcctagaa gtggttagca cctttgagat gggaattatt tagcaggatg 2ttttgtgtt ttcatgtaag ttttatgctg cctgtggagggcacagctgt ttcaaaacta 2taaccaaat cctggtctcc gaagtctgaa ggcatccttt gccctgcagt gcaaagcacg 2gattctggc ctcacacagg caggtctgaa ctcctgtgtt gcctcttgct ggctgtggga 2ctgaggcaa atcatgcaac ctctcttttc tgtttgccta gatggaaaat aggtttacaa 2acgccccca taggatggct gtgagaatta aaggaagtca tgggtgtaca atacctggcc 2cgaaagatg cttaataatt taattctgac cttcctcact catttaggat tatgtaccaa 2ttttagaaa caatgaaaga ttagtgagtc ttctgtggtt ggtataaaaa aaaaatagaa 2catgaaaga gatgtcctcc ttgttcaagggctaatgacc ctggtgtgcg ctgtctaggc 2cccaaggtc ttccttccct gctcacagca tttcaggttc tccgcagctt tgctgagcct 2ggtcaggtt cggtatctgc ccaccatgct cacttgccac agctgtggcc ccatttccaa 2cttcagaga cttaaaggtg cagctaatga tgtgcccggc ctggggtcac attccctgag2cctgcagac aagggagcag gaggctgagc tcttatcttc cacaccctgt gcacagcctg 2gaagagtta aagcacccta gtcctatgct gcgagggcca catgccctga gaccttggaa 2aaatcctac ctgaattgaa gagcatcact atttcatcag gaggcgctgc catttcattt 2tcacttcgg ttttatcttgagtgtaaaac agcttcgcaa atcacttttt cttgtttctg 2aatgagcat atggtggcct cattcgtgtg ataaatctga gccaccacga tatttgactt 2tcacaattt aatttatctg aaccctctat tctctggcta aaaaatatcc cttacttgga 2ttctttatt ttattttcaa ttcccttacc agcactagca ggggactctgtactcatctg 2tggcgctgc cataacaaag cactgcagcc tggggggctc aaaccacaga atttattctc 2cacagtcct agaggctaga agtccaagat caaagtgtgg gcagggtcgg tttctcctgc 2gcctctctc cttggcttat agagtgccac cttctacctg tgtcttcaca tcatcacctc 2ctgagcatgtctgtgtcca aatctcccct tcttataaga ccccagtcat actggatgag 2atccaccca tatgagttca ttttacctta attatctctt taaacaccct gtctccaaat 2cagtcccat tctgaggaac tgagagtaaa gattcaacat atgaattttg gaagggacct 2attcagccc acaacaccct cttttgggat gtttattttcccccttaagg agctagttag 2atgtcttat ctcatgaaca tgactgtgaa caggaaaaca gggagagaat gaagctggcc 2aggaacagg gctggtgtca gctagcagtg cttttctgat gtgagtgggt cccacaggga 2cttgttaaa atgcagattc tgattcatta ggttccagag ggacctgaga tttcccattt 2tgacaagtt tccagtgtgg gggctgatgc tgctggtcca cggaccatac tttgagtagc 2aggagcttg atacataatg gctgagtgac tttcagactc ctgctgtaga aaaattatga 2ttggctggg cgtggtggct cacgcctgta atcccagcac tttgggaggc cgaggtgggc 2gatcacctg aggtcaggag ttcgagaccagcctggccaa catggtgaaa caccatctct 2ccaaaaata caaaaattag ccaggtgtgg tggcaggtgc ctgtaatccc agctactcag 2aggctgagg caggagaatc gcttgaaccc gggaggcaga ggttgcagtg atctgagatc 2tgccactgc actccagctg ggcaatagag cttgactcag tctcaaaaaa aaaaaaagaa2agaaaaaga aaaattatga gttatattat cagcatatgg ggtgcctttc aaattgataa 2atttctaat attaaacctg tggatgccaa atgctgctct ctgattatgg caggaaacgg 2acttggcag tacgaagtta gctgttgggc tgagctggct catcttgttg tgcggtcctg 2ttgcctaaa gatgccttcccaggatcttt actaacaatc ctcctgagtc atttggactt 2cccaacctg ttatcacctc tcagatgggc cagccatgga ggcagtcaga ggagggctct 2cagagggag ggcagaaaca gggtggcctc tgcatgccat taggaggtca catctcactg 2gggatgcag tttaggattt agtgccttgg agagaaggat agagtatattaaaacatgtc 2ccgctaggc atggtggttt acgcctataa tcccagcact ttgggaggcc gaggtgagtg 2attgcctga gctcaggagt tcaagaccag cctggctaac atgacgaaac ctcatctcta 2taaaataca aaaagttagc tgggagtggt ggcgtgcgcc tgtagttgca gctacttggg 2ggctgaggcatgagaatca cttaagccca gaagactgag gttgcagtga gccgagattg 2accactgca ctccagcttg ggctacagag tgagactcta tctcaaaaac aaagaaacaa 2caacaacaa taacaacaaa aaccaagtct ctccctccac tcaaaaatgc aagggcctgt 2tcccattgc tgggtgccca ggtctcatga atgtagatatgaattattcc agtcagcctc 2ggagaatag aatgagccct cagatgccga agcacctttc agattccacc ggttttatcg 2ctcatttaa acttcacttc taacacagtc ctgcattaca cacgtgtctg tcgttatggg 2agctgcaga gagggtctta atggtcctaa tgctcagtga ggatgcccaa tggtcaacag 2acctgccat cttcaggcca tcaaggagct ctggagttaa ggaaatcatg agagcacaga 2gggcgggta cagcagagcc ctcgtggtaa tgggttttga ggtctaggct ctcttcactt 2ggtttgaaa taagttcaat gactagtaat agctgagaca cttctaccct tcaaatgaag 2aaatgggaa aatggagcat tgttgagtccagggagctat aatttaaacc ccatatatct 2aaaggggta acatttttgt gtgtgtgaaa ttggtgtcat tcgcactgca tctacagttt 2ctttttcct tctcttccag cacccctggc tacatatttg ggaaacgcat catactcttc 2tgttcctca tgtccgttgc tggcatattc aactattacc tcatcttctt tttcggaagt2actttgaaa actacataaa gacgatctcc accaccatct cccctctact tctcattccc 2aactctctg ctgaatatgg ggttggtgtt ctcatctaat caatacctac aagtcatcat 2attcagctc ttgagagcat tctgctcttc tttagatggc tgtaaatcta ttggccatct 2ggcttcaca gcttgagttaaccttgcttt tccgggaaca aaatgatgtc atgtcagctc 2gccccttga acatgaccgt ggccccaaat ttgctattcc catgcatttt gtttgtttct 2cacttatcc tgttctctga agatgttttg tgaccaggtt tgtgttttct taaaataaaa 2gcagagaca tgttttaagc tgatagttga ggggttttgt taatggcttttgggggattt 2tctctatac ccacaaacga ctagtttgtt ttcctcaaac taaatgataa tattaaaaat 2cacatcctg gccaggtgtg gtggctcata cctgtaatcc cagcactttg ggaggccgag 2caggtggat cacttgaggt caggaattaa gaccagcctg gccaatatgg tgaaagcctg 2ctgtactaaaaatacaaaa attagccagg tatgctggtg gatgcttata atcccagcta 2ttgggaggt tgaggcagga gaattgcttg aacccgggag gtagaggttg cagtgagcca 2gatcatgcc actgcactcc agcttgggca acagagtgag actccatctc aaattaaaaa 2aatacacat ctggcttctg gaaaaattac ttgaagatcttttatgacat ccatccctct 2cacacagcc atgtgaatta ggttggtatc ttcatatact agcatcgtgc ccagcacttc 2atgttatac agtttaaaat gttctgtaat tccctgtggg aacctaagat aatgcgagga 2cgtcatacg tgcccccaaa tattggcaaa ccaatgaata aatgaatgaa tgagtttatg 2atcgctaac tggctgtatt taatgaagta tgtgtgttga gccatttccc acagtgtgga 2agatttgtc ccacaatatg ggcctcttcc caaaggccct accacctaat gccatcacac 2ggggatttg atttcaacat gtgaatttgg ggagagtgca aacactcaga ccatagcacc 2tctcagtaa atgtcccact ggtcactcagttcatagtga cagtgatcca gccactgtca 2gacaggtgc cacttggcag aaacagcaca gcttggaaga tggcggggtg tagtcaagat 2ccaggatcc ccaacagaga agccagctct tataggggag ccattcatca ggattgaact 2tcaatcgag ctggacagta ataggtgggt ctgtgttatt ccccagatga gtatcatgac2gtcacaatc ctaggaagga tgtgaagcct cccccagctc tcctccagtt gcctgcttgg 2cagcagaga tgatggaatg tggagtctgg cgtggtctga ggcctgaatc catgtgcctc 2tgtatgatg ctcaggcaag aggatctctc aattcaaggg agagggcctg aatgagcctt 2ctttccagg cctgtctgatggtccaggct gaagcccctc ctggcttgca ctgccagacc 2catccagca ggagctcctt ggcattgact gcttcaggat agttgcttct gctctgagtg 2tctctaaag agcagtgctc taccatccaa gctgggcttt tcttttcttc ttgctgatag 2gaaggcatg ggacattgca ggatggaagt ggcccccagg ccttctcatgcctgggcttg 2tttggaagg tggtcaggtg atcaataatc ctgattggcc tggcattgag gagttttcct 2ggatgtggt cctttcggtt ttttaaaaat tatttttatt gatacacata tttgtaggta 2ttgtggggt gcatgtgata ctttattatg tgtgtggatt gtgtaatgat gaagtcaggg 2atttagggtcttcatcacc ttgattatca tttctatgtg ttgagaacat ttcaagttct 2agttccagc tattttgaaa tagacagtcc attttgttag ctacagtcac ccaacccggc 2gtcagacat tggaacttac tcctattgaa ctgtgtattt gtacccattc accaaactct 2tttgggctt tcagttttac aactgggatg atcctgggaaaactaaagta aatcagacac 2cgacgtgtg agctaggtta taatatgccc agtggaccct ggggacatct tagctttcag 2ggtcatgct gtccaagctg actgtggggc ttccagaagg tggggagagg aaatgatgca 2tggcccatc agaggcacta cttggggcct ggggccagag tgcatgtcta aggcattaag 2ggaggggag agcagccttc ataattatga agaggagtct caggtgcaca gcttctgatg 2gggacagct tctaattgaa gacagcattg tgtaatgctc aaactccctg tcttcagagt 2cctgctgta tcccaccatc agttctgtga cttctcccta agcctcaatt ttgcatgtgt 2acattggga taataatagt gccaaactcatggggttgtg aggaataatg aggtaaagca 2ttgaaaagg tttagcacaa tataagtgct caataaaagc cattattatt attttattac 2ctagttttc aattcctgca tagcaaattc ttgcaaatgt agggactcaa aacaatataa 2tttattatc tgacagtttt tctgggtcag aggtcttact aggctgtaat cagagggcaa2caaagctgt gatctcagct gaagctcagg attctcttcc aagctcactg gttgttggca 2aattcagtt ctttccagtt ggaagactaa agcctacagt cttcagtctc tagaagcctt 2tctctggca caggtttctc tacaacatgg ccatttatgt ctttaaggcc aataggagaa 2atgattagc atattttttttaagtgaact ttagaccctt ttttaaaggc ctatctgatt 2ggccaggcc caagtgagct ttaagtcaac tgattagaga tcttaattac atctgcaaag 2cccttcatg tttaccgtat aacataactt agtgaaagga gtgaaattgc aaccaggttc 2gcctgcact ccacggaagg ggattctgca gaagtgtggg tcacgggggggttattttgg 2attctgcct acgtcactga gtcaaaagaa gctgaatggt tgtgatgctg aggtttttgg 2cagcagcag tgtgtgtgtg tgagtgaatt catacgtatg accacctggg aagaaaggag 2ctgtggttt cctccacctc ctggcagaca gagaaatttc tttttttttt tgagacaggg 2ctggctctgttacccaggc tggagtgcag tggcttgatc tctgctcact ggctcactgc 2gcctctgcc tcccaggttc aagtaattct tgtgcctcaa ctccaagtag ctgggattac 2gacacacac tgccacgcct ggctaatttt tgtattttta gtagagacga ggttttgcca 2gttggccag gctggtcttg aactcctgac ctcaagtgatccgcccacct cagcctccca 2agtgctggg attacagacg tgagccacca ttaaccattt ttctatctcc tgtgggaaag 2gcacagtga aagaacagat gaagctgaga catacaagtg aactcctccc tcctctccat 2tagactaaa ataggattat tcatactgag attctccctg gttgcaaaga gataatctgt 2caactgggt ttttacaatt atccctaccc tatgctttcc tcatctgtct tcctcgtagt 2agctcaggc tgctataaca aaacaccata actgggggct tttgaacaac aaaactttac 2tctcacagt tctagaggct ggaaatccaa gatcaagttt ctggcagatt cggtgtctaa 2gaggtcctg ctttccagtt tatagacagtgccttatcgc taccgcctta cacagtggaa 2gagaggacg agaagctcct tgggcttttt tttgtttctt tctttctctc tctctctctt 2ttttttttt ttaataaggt cactatctta gtccattttg tgttgctaaa aggaacatct 2aggttgagt aatttatttt attttaaaaa gtggccaggc atggaggctt atcctgtaac2ctaatcctt taggaggcca aaacagcagg attgtttgag gccaggagtt caagaccagc 2taggcaaga tagtgagacc ccatctaccc catctctact aaaattttaa aaaattagct 2tgtgttgta aagtgtgctt gtagtcccgg ccacttgaga ggctgaggtg ggtggagttc 2aggctgcag tgagttatgattgagccact gcactccaac ccgggtaacg gggcaagacc 2tgtctctat ttaaaaaaaa aaaatcttta tgtggctcac tattctgggt ggctggaaag 2tcaagattg ggcatctgca tctggtgaca gcctcatgtc gcttccagtc atgggggaag 2cgaaggaga gctggcacgt gcagatatca cgtgttgagg gcagaagcgagagagagagg 2gagagatgc caggctcttt ttaacaacca gcactgggga aactaataga gtgagagctc 2ctgactcct gagggaggac attaatctat tgatgagcga cctgcctcca tgacccaaac 2cctccaacg ataccccacc tccaacactg ccacactagg gattaacttt caacttgaga 2ttagaggggggaaacttac aaactatcgc aggcactaat accactcatg agggctccac 2ttcatgacc taatcacttc ctaaaggcct tacctcttaa tctcatcaca ttgaggattc 2atttcaact tgaattttgg ggggacacca acattcaggc catagcatca tctcaataac 2gtcccattg gtggtcactc aggccccaaa caaaggaaccttcctccatt cctttccgcc 2tcccaccca cagtcaatca tccccaagct ccatcagctc cacctttaac ggccaaccca 2ctctgccac atctcaccat ctccactgct atccctgtca cctgggccca ccattctctc 2cctggacag tctccatagc cacctctgtc agatttattt tattttttta tttttttttt 2gagacaggt tcctgctctg ttgcccagac tggagtgcca tggcatgatc acatctcact 2cggcctcca tcacctgggc tcaagcaatc ctcccatctc agcctcccaa gtagctggga 2tactggcac caccatacct ggctaatttt ttgttgttgt tgtttaattt ttaatacaga 2gaagcctca ctatgttgcc caggctgctcttgaactcct gggctcaagt gatcctccgg 2cttggcctc ccaaagtgct gggattacag gcatgagcca ccgtgcccag cccatcagat 2ttaatgcta cacgcacttg cttaaaatcc cccagataat tctcgctgct cttggaataa 2tcccacaca ccttggcgtg gccatgcagg ctctgtgcca tcggatatgt ccctgccccc2ctcccaact cctcctttcg cttgctcgtt cactcagttc cagccacatt gccctgggag 2tgctcccac catggggctt cctaatgcac tggtctctct catgcagtgg ggcctctccc 2ccttttact cagtgtctcc cagcacccac ctcctccaga gccttccctg accaccacac 2tacacctag gcccttcctcctccacgctc cctcctccac cccggcctcc tacccacgtg 2cacttcttt atactcgctg ccacctgaaa ttagatcatt tatttacccc tttatttgtt 2agtttgcct tgtccgttag aatataagct tccaaagggc aggagctttg cctatattgt 2aggccgggc atacaatgag cactcaaaaa aatatttgat gagtgtatgaaagaacagac 2gggttatgt aattgtgcct acttacctat atgaccgtgt ggtggggttt atggtgggtg 2ggtggtgat ggctataggg ctataagcaa atttgggaca gggagtctaa gaaatgttct 2aaattttag taagcaaagc atcctctaca gaacctgtct taaaacatga aagttcctta 2tgctacccccagaggtatg atttggtagg tcaaggatag ggcctggaaa ttcacattct 2gttaagatg ttcttcatcc ggggtttgtt gaccaccttt tcagaagatt tttgctctgt 2gctgtacta cccaatgcag tagttcgtag tcagtgtggc tcctgagccc ttgaagtgta 2ctcctctga actgagacgt gctgtaaatg taaattgcacaccggagttt gaagagttaa 2acaaagaaa aaggaatgca aaacatctca
ttaataatgc tttacactga ttacatattg 2aatggtaat cttgtagata tagtgcgtta aataaaatat actgttaggc ttaatttcac 2tctttatac ttttaatgtg gctactagaa aaatttaaat aacatattca gctcacatta 2actcctatt gaacagagct gatctataag ttccatggaa gatggcaagtcttcgcagct 2aaataaagg ctggatccca ttctacgggc tcatctttag caatgatttc ttgcagacga 2attgaaaaa tgtggcaatg aaagttacca caagcatcaa accagtcctg cctaaatctg 2aaaatagtt atctgaggct gttagcatat gatcatgaga gcgtttcacc atggatttct 2atcacagatgtggcacatt attaaaatat cacttttaca gtcaccctag aggctagggt 2atctgaata tggagaaaga aacagcttgt ggagctgttg tataaatgaa attactagaa 2gtaatgcac tcaattgcat attggctcgg ggggttattc ttattaaaat gtttagagag 2actttctgt tcatttctgc agaattgctc ttcaaattaagaatttgctt gacacgctaa 2agaccacag tcccaagaga agtttatcct tttttcttct tatccttgct aagcacttag 2tgctctgct gataggtagc atatattgtc tatatgaagc ttttgtgtta acattgacta 2tcctgcaag ttggcacact cttacttggc ctaaaagaaa tcagcaccag gctttaagaa 2atcagatga tctacctaaa ggaacacaac tctgtctctc ttttgacaat tgttgtaaac 2aattttaat ggaaatttgc cttaattgtg aagaagttgc tgctaaaatg gacttgccat 2aatggactg gaacccattg cataagcaga atgaaatata agccttctca ggattcacac 2tataaaaaa ccattcagcc aatcaacaagagggcaaaag aacaaacatt tgatgtgtaa 2tacttaatt tagtgcatat gcatttgggt cctcaatgtc agcactatgg caaccagaac 2tggccacaa taactgtctg gaaatgtcta ttcttacctg gacccagcag gccatgcccc 2ctgattata taatctccct ctctccttgt tacggtctga atgcttgcat ccctcaaaaa2tcatgtgtt gaaatcctaa cccccaaggt gatgatatta ggaggtcggc cttttgagag 2taattaggt catgaagaca gcatcctcat gaatgggatt agtgtcctta taaaataggc 2caagggagc tcattcactt tgtccaccat gtgagaacac agcgagaggg caccatttat 2caccaggaa atgggccttttccagacaat ctgtcggtgc ctggatcttg gacttcacag 2ctctagaac tgtgagaaat taatttgttt tttataagcc accaaatcta tggttttttt 2atagaaacc gtaatggact aaaacactcc ctaattatat ttaaacttat cagtgcactg 2gcagtgaca tattaaaaga atgctggcca acgtaattga caccataaggctggatgatt 2ttgtaattt tcagcctcag aaaaaggctg gggagaggag tcaggggaaa ggaggtggtg 2gtgtgtgtg tgtgtgtgtg tgtgtgtgtg tgtgtggtac ggtggatgcc tgctgagaga 2aaagagcta taataacatt ctgtggttca gctgacacat cctttctgca tcccctccaa 2cacctgggttaatggggac ctcgctaatg tctgaacctc atctcatttt aaccttttgt 2tcaaagcct ctcttttcat gacttccccg ccttcatttt tcccatatgg tggggttatt 2ttaagacat taaatgagag tggacaggta ggcaaaggag gtgggttgca ggggagttga 2ggttgcctg tgtacttttc tagactgttc cacttcacatcagtgaaata ttcccaattg 2tactatcat gaaacaaagc aaatgaaatg ctgagcacgg agcttcgtct tgatgaaatg 2tgaaagaaa agaaaggaaa aataaagtag ccattatttt tgcccttcct cccaccccca 2gtttactac tcttatttct cttttgtatt gttgtgttgg aagcacagca tcagaaaaac 2cccagtttt gagagataac tcagtgttta gttcacttaa acctgagaaa ggagaagagg 2tgccaccgt gaggtccagg acgtaaagag gaaaaaaaca gacaaaaaaa tccatatgaa 2tgaaaatgt gaaagaggcg ctttcgagca gatgagtgtt gtagattaca gtgttgagag 2tgtttgtgt ccagagctgc ttgctgcacctggcgggata aacactggtc taacagagga 2ccttgtttc aaggaggctg ccttttattt ggggggacaa aattgttctt gaaagctgct 2agtggttca agctacagca tggtggacta gcagaatgga ctccagggcc tccgaggaga 2agtgactgc tgccagaaat agtcaaggat agaaaggaag gacttcactg aggcctggga2aagattatg gaatgggact gacagcagtg acggggagta aaagggggtg tctgggggaa 2tgtgcccca tggtgagagc tagagggttc acaaagactt aacccgacgc atctctctca 2cctggagat tgggcccgtt caatctaact ggatggctat aatttaaaag gtttaggtat 2atgacaaac atggatatattaggtgatag caatgcaaaa tgcatatggc ttcttgatat 2aaacacaag acttgaaagc agcatctttg gctgggtact acagccaccc tcctctgtca 2taagggagg ctttggtgga aagggctgag agcctctaga ctgtgaacaa aagtaggcac 2gaagaacag ttggagataa taagtaaacc atcttgacag gaatgaagaatttcctgaaa 2gaaggtccc tgagttaggt tgttggatgc tttcagtagt gagttattga aagtgtttgg 2gggtgtgtg tgtgtgtgtg tatgtgcagt atgtgtgtgt 2 Homo sapiens 2 Met Asp Gln Glu Thr Val Gly Asn Val Val Leu Leu Ala Ile Val Thr Ile SerVal Val Gln Asn Gly Phe Phe Ala His Lys Val Glu His 2 Glu Ser Arg Thr Gln Asn Gly Arg Ser Phe Gln Arg Thr Gly Thr Leu 35 4a Phe Glu Arg Val Tyr Thr Ala Asn Gln Asn Cys Val Asp Ala Tyr 5 Pro Thr Phe Leu Ala Val Leu Trp Ser Ala Gly LeuLeu Cys Ser Gln 65 7 Val Pro Ala Ala Phe Ala Gly Leu Met Tyr Leu Phe Val Arg Gln Lys 85 9r Phe Val Gly Tyr Leu Gly Glu Arg Thr Gln Ser Thr Pro Gly Tyr Phe Gly Lys Arg Ile Ile Leu Phe Leu Phe Leu Met Ser Val Ala Ile Phe Asn Tyr Tyr Leu Ile Phe Phe Phe Gly Ser Asp Phe Glu Tyr Ile Lys Thr Ile Ser Thr Thr Ile Ser Pro Leu Leu Leu Ile Pro 3 873 DNA/RNA Homo sapiens 3 acttcccctt cctgtacagg gcaggttgtg cagctggagg cagagcagtc ctctctgggg6gaagc aaacatggat caagaaactg taggcaatgt tgtcctgttg gccatcgtca tcatcag cgtggtccag aatggattct ttgcccataa agtggagcac gaaagcagga agaatgg gaggagcttc cagaggaccg gaacacttgc ctttgagcgg gtctacactg 24cagaa ctgtgtagat gcgtaccccactttcctcgc tgtgctctgg tctgcggggc 3ttgcag ccaagttcct gctgcgtttg ctggactgat gtacttgttt gtgaggcaaa 36tttgt cggttaccta ggagagagaa cgcagagcac ccctggctac atatttggga 42atcat actcttcctg ttcctcatgt ccgttgctgg catattcaac tattacctca 48ttttt cggaagtgac tttgaaaact acataaagac gatctccacc accatctccc 54cttct cattccctaa ctctctgctg aatatggggt tggtgttctc atctaatcaa 6tacaag tcatcataat tcagctcttg agagcattct gctcttcttt agatggctgt 66tattg gccatctggg cttcacagct tgagttaaccttgcttttcc gggaacaaaa 72tcatg tcagctccgc cccttgaaca tgaccgtggc cccaaatttg ctattcccat 78ttgtt tgtttcttca cttatcctgt tctctgaaga tgttttgtga ccaggtttgt 84cttaa aataaaatgc agagacatgt ttt 873 4 24 DNA Homo sapiens 4 cctttgcttt gttcctatttcttt 24 5 2omo sapiens 5 tcccattgcc cagagttaat 2DNA Homo sapiens 6 tcctcatgtc ttcacctaga agc 23 7 2omo sapiens 7 ccactcatga gggagctgtt 2DNA Homo sapiens 8 tgtcacaggc acacactctc t 2DNA Homo sapiens 9 gagtatggctgctgctcctc 2 DNA Homo sapiens ctcaca ctggcctaaa 2 DNA Homo sapiens cagacc aataatagtg cag 23 NA Homo sapiens caccct ttaaacagca 2 DNA Homo sapiens aggaag caactccact 2 DNA Homo sapiens tgaatt ccctggcata 2 DNA Homo sapiens ccctag tcccactctc c 2 DNA Homo sapiens aggcct gcataaggaa 2 DNA Homo sapiens tgccgg tggcttaaat 2 DNA Homo sapiens tgttcc cgtctgtctg 2 DNA Homo sapienstcctct gccaaattcc 2 DNA Homo sapiens 2gtatt cactgcctga 2 DNA Homo sapiens 2cattc ttcttcctct tac 23 22 2omo sapiens 22 tatgtgttca gcccagacct c 2 DNA Homo sapiens 23 ccctgccatg tgcatttac omosapiens 24 catttcggaa ggcaaagaaa 2 DNA Homo sapiens 25 ttgcaatgag gaatgaagca 2 DNA Homo sapiens 26 tccattatcc atctgttcat tca 23 27 25 DNA Homo sapiens 27 gaagaattaa ttgtaggagg caaga 25 28 2omo sapiens 28 ctgacatcac cacattgatc g 2 DNA Homo sapiens 29 catacacagc catgtggaat ta 22 3A Homo sapiens 3gatga cgcctacatt 2 DNA Homo sapiens 3tggac caattaccta gaa 23 32 25 DNA Homo sapiens 32 aaattacttc atcttgacga taaca 25 33 2omo sapiens 33 ctattggggactgcagagag 2 DNA Homo sapiens 34 agccagtgtc cacaaggaag 2 DNA Homo sapiens 35 gagggtgaga cacatctctg g 2 DNA Homo sapiens 36 aatcgtgcct cagttccatc 2 DNA Homo sapiens 37 ccaccaggaa caacacacac 2 DNA Homo sapiens 38ttgctctcca gcctgggc 8 DNA Homo sapiens 39 ttcctctggc tgcctgcg omo sapiens 4catga gaaggaactg 2 DNA Homo sapiens 4ttcac tgtggctctt 2 DNA Homo sapiens 42 tttgattccg tggtccatta 2 DNA Homo sapiens 43ttatttggtc ggtgcacctt t 2 DNA Homo sapiens 44 ggtgcaccga ccaaataagt 2 DNA Homo sapiens 45 ccagcttatt ctctctgcct tc 22 46 22 DNA Homo sapiens 46 ggtaggttga aatgggctaa ca 22 47 2omo sapiens 47 tcatgacaag gtgttggatt t 2 DNA Homosapiens 48 cctcctctgc catgaagcta 2 DNA Homo sapiens 49 ctatttggtc tgcgggttgt 2 DNA Homo sapiens 5ggtta tcgcctgacc 2 DNA Homo sapiens 5ggacc tcttggacat 2 DNA Homo sapiens 52 tttcggcaca gtcctcaata 2 DNA Homosapiens 53 cagctgggtg tggtgacat omo sapiens 54 cagagaggaa caggcagagg 2 DNA Homo sapiens 55 agtggctggg aagccttatt 2 DNA Homo sapiens 56 aggtgagaga acaaacctgt ctt 23 57 2omo sapiens 57 gccttccttc taaggccaac 2 DNAHomo sapiens 58 ctgtagactt tatccctgac ttactg 26 59 24 DNA Homo sapiens 59 caatgaatga tgaagattcc actc 24 6A Homo sapiens 6ccatg tcttactgtt tgc 23 6A Homo sapiens 6tacaa tgagaaccaa atctc 25 62 2omo sapiens 62 caggatcatcagccaggttt 2 DNA Homo sapiens 63 gctgcatgtc actaggcatt 2 DNA Homo sapiens 64 ccacagaatg ctccaaaggt 2 DNA Homo sapiens 65 gagttcaagt gatggatgac ga 22 66 24 DNA Homo sapiens 66 cagatagatg aataggtgga tgga 24 67 2omo sapiens 67cactgttcca agtgctttgc 2 DNA Homo sapiens 68 tatgcgttgt gtgtgctgtg 2 DNA Homo sapiens 69 gggccttaga ttcttgtagt gg 22 7A Homo sapiens 7agact gcctcctaca 2 DNA Homo sapiens 7cacct ggttcacaat 2 DNA Homo sapiens72 tttgcgagtc cttgtggagt 2 DNA Homo sapiens 73 acagtccgct ccctcctaat 2 DNA Homo sapiens 74 atgcttggcc ctcagttt omo sapiens 75 ttggcaaccc aagctaatat g 2 DNA Homo sapiens 76 ctccacagtg acagtgagg 7 DNA Homo sapiens77 gagaggttcc caatccc omo sapiens 78 cagctcctgg ccatatttct 2 DNA Homo sapiens 79 gagccatttc tctgggtctg 2 DNA Homo sapiens 8gtgtc aacccttaga 2 DNA Homo sapiens 8tgatg ggagggaaa omo sapiens 82cgggaaatga cagtgagacc 2 DNA Homo sapiens 83 tgcctagatt ctcccgtaag 2 DNA Homo sapiens 84 gtgcccagcc agattc 6 DNA Homo sapiens 85 gcccccagtc aggttt omo sapiens 86 tttctctctc cacggaatga a 2 DNA Homo sapiens 87aacccattct cacagggtgt a 2 DNA Homo sapiens 88 aggagtgtgg cagctttgag 2 DNA Homo sapiens 89 tggattcccg tgagtaccag 2 DNA Homo sapiens 9gggat cacaggc 9 DNA Homo sapiens 9ggtgg acttttgct omo sapiens 92agcatttcca atggtgcttt 2 DNA Homo sapiens 93 catgttgata tgcctgaagg a 2 DNA Homo sapiens 94 cactgtctgc tgccactcat 2 DNA Homo sapiens 95 agagattatg tgatgtaccc tctctat 27 96 2omo sapiens 96 tgatgaagat ctgggcgtta 2 DNA Homosapiens 97 tgcctgtgct cactcactct 2 DNA Homo sapiens 98 atgacctaga aatgatactg gc 22 99 2omo sapiens 99 cagacaccac aacacacatt 2omo sapiens tttaaaa acctcatgcc 25 DNA Homo sapiens ccaaact ctgtacttat gtagg 25DNA Homo sapiens tggctgt tgtgactggt 2omo sapiens tcaggtg ggaggatcac 2omo sapiens tttgcca gtagccttga 2omo sapiens ggaaagt taacccagag a 2omo sapiens gggaagagccatgagac 2omo sapiens tgggcat tggaggatta 2omo sapiens agacaag tcaggtgagg 26 DNA Homo sapiens agtatgg agtcttcatc attatc 26 DNA Homo sapiens tactaga tttgaccaac ca 22 DNA Homosapiens ttgtaaa ggatttagtg atttcg 26 DNA Homo sapiens gaaggcc tctctctgtg 2omo sapiens ttcttga gggaaagcat 2omo sapiens tcagagg atttcccttt c 2omo sapiens gtttgac tccagcttca2omo sapiens ggcacgg aatagacact 29 DNA Homo sapiens ctccttt gctctgaag 2omo sapiens ccctgtg gctgattaag a 2omo sapiens agttcca gcccgttcta 22 DNA Homo sapiens caaaggaatatccaagt gc 22 DNA Homo sapiens cgtacca tataaacagt tctc 24 DNA Homo sapiens >
ttcaatgaag gtgccgaagt 2omo sapiens ctatccc aaagctgcaa 2omo sapiens cagtcca agttcatgct c 2omo sapiens gattggg ttctggatac 22 DNA Homo sapiens actttcc atctcctcct tg 22 DNA Homo sapiens agtaagt tggagaattg ttga 24 DNA Homo sapiens agactct gttgaagaag aaga 24 DNA Homo sapiens ctctgtt tgagtttctc g 2omo sapiens tgggcag tcagagaaac 2omo sapiens gtgaagt ctgagaggtg 29 DNA Homo sapiens cacagtc gctcatgtc 24 DNA Homo sapiens ctttagc taatggtggt caaa 24 DNA Homo sapiens catgtgt gactttcata ttcag 25 DNA Homo sapiens ggctatt cattgctaca gg 22 DNA Homo sapiens ctggatg ctggtttcta 27 DNA Homo sapiens gagagag agaaagagaa agaaaga 27 DNA Homo sapiens gtggatg cagttgaggt tt 22 DNA Homo sapiens agccatt acagacaacc aa 22 DNA Homo sapiens ggctcca tgtatccata a 2omo sapiens tctttgg ctttgggttt 26 DNA Homo sapiens gttgagc ggcatt Homo sapiens agcctgg atgaca 22 DNA Homo sapiens atggaag catagggaag aa 22 DNA Homosapiens acttctg agtctcctga t 2omo sapiens aaatgga gctgctgtta 2omo sapiens tgggtga gtgcaaggat 27 DNA Homo sapiens tcagcag gcatcca Homo sapiens aacgtaa ttgacacca 2omo sapiens aaggaag gtccctgagt t 2omo sapiens tgctttg cacaagttat c 2omo sapiens atgaggc tgtatgtgga 2omo sapiens gcaggaa tgagaagtcg 28 DNA Homo sapiens taggccccataatct 2omo sapiens attcctc aattgcaaaa t 2omo sapiens cattcag ggagccattc 25 DNA Homo sapiens ttatatt tcaccaagag gctgc 25 DNA Homo sapiens caaggct gacagggaag 2omosapiens ctcagcc ctcaatgtgt 2omo sapiens tgggttc ctctcccaat 2omo sapiens aactctt gctgctggtg 2omo sapiens ctggtca tctacccatt 2omo sapiens actgcag cgctgatctt 2omo sapiens ttccaga aggtttgcat 23 DNA Homo sapiens aaagttg ttcaagagag aca 23 DNA Homo sapiens caggaag atggacaggt 2omo sapiens actgcat cacacatacc c 28 DNA Homo sapiens gccagtatgcctgct Homo sapiens acatcag tccatttgc 23 DNA Homo sapiens ttatgtc tgtgtgtgtg tgc 23 DNA Homo sapiens gggatgt cagagaaata tgc 23 DNA Homo sapiens tgaaatt gcctagtgat gc 22 DNA Homosapiens tccaatc gtacgctacc 2omo sapiens taaacac cacggactgg 22 DNA Homo sapiens gtatcga cattcttcca aa 22 DNA Homo sapiens gatctag ggaattattt gtcttc 26 DNA Homo sapiens gccactaaggtccagat 2omo sapiens ttgaggc tggatctgtt 23 DNA Homo sapiens ccttatc attcattccc tca 23 DNA Homo sapiens tattgtc tccgttccat ga 22 DNA Homo sapiens agatata aggacctggc ta 22 DNA Homosapiens aagccct gtggaatgta ttt 23 DNA Homo sapiens attgcag gtcaagtagg g 2omo sapiens ataaggc tggagacaga 29 DNA Homo sapiens agcagat gggagcaaa 2omo sapiens cagttgt ctttcatcct g23 DNA Homo sapiens ctgtgct tgtatattct gtg 23 DNA Homo sapiens catgtgc ataccagacc 2omo sapiens aagatga cctctggaaa 22 DNA Homo sapiens gtgttcc aggtgagaat tg 22 DNA Homo sapiens ccatatc ccaaggcact 22 DNA Homo sapiens ttcccac attcattcta ca 22 DNA Homo sapiens aactcgt ggcaaagacg 28 DNA Homo sapiens catgcct ggctcttt 22 DNA Homo sapiens ttctcca gttgtgtggt tg 22 DNAHomo sapiens accattg acactctcag 26 DNA Homo sapiens ggccatc cattct 25 DNA Homo sapiens gtgtgta ttgtgtactc ctctg 25 DNA Homo sapiens cacaatt tgaaccaatc ct 22 2NA Homo sapiens 2agatatgaaggccaaa 22 DNA Homo sapiens 2cagcta gaacaatgtg aa 22 2NA Homo sapiens 2catgtc agcagcagaa g 2omo sapiens 2acaggt gagggcatgg 2omo sapiens 2catagc tgtagccctg t 2omosapiens 2atgggc atctttaggc 22 DNA Homo sapiens 2caaaca aacaagcaaa cc 22 2NA Homo sapiens 2cgtttc tttcagtgag g 23 DNA Homo sapiens 2aactta ccagcatgtg agc 23 2NA Homo sapiens 2ctcacc taaggatctgc 23 DNA Homo sapiens 2gcaaat ctctcaactt cca 23 2NA Homo sapiens 2ctccat gctgcttcct 2omo sapiens 2caattg cccaatagag 22 DNA Homo sapiens 2gcttgt ctacctagtt ca 22 2NA Homo sapiens 2cacgta tttgttggtg 2omo sapiens 2agcaga aatgggaacc 2omo sapiens 2gggcta tcaatttctg 2omo sapiens 2tgcaat ctggtttcca a 2omo sapiens 2agactg aggaggtcaa 2omosapiens 2acggag aggaaagaga 2omo sapiens 22aagca agcaatcaca 2omo sapiens 22gatgc accatgttta 2omo sapiens 222 tgagaagcct gggcattaag 2omo sapiens 223 acaagctcat ccagggaaag 29 DNA Homo sapiens 224 agagctgatc tggccgaag 2omo sapiens 225 ggtggacaca gaatccacac t 28 DNA Homo sapiens 226 ggcctgaaag gtatcctc Homo sapiens 227 tcccaccata agcacaag 22 DNA Homo sapiens 228 tcaacctagg attggcattaca 22 229 2omo sapiens 229 tctaggattt gtgcctttcc a 2omo sapiens 23tgcag ctgtttctgc 22 DNA Homo sapiens 23acatt gtaaatggag ga 22 232 2omo sapiens 232 ggtgggaatg tgtgactgaa 22 DNA Homo sapiens 233ccaggtacaa cattctcctg at 22 234 Homo sapiens 234 tgcaggtggg agtcaa 24 DNA Homo sapiens 235 aaataacaag aagtgacctt ccta 24 236 2omo sapiens 236 aaaggatgca ttcggttaga g 2omo sapiens 237 actgtcctgt gcctgtgctt 2omo sapiens 238 gtccacctaa tggctcattc 2omo sapiens 239 caagaagcac tcatgtttgt g 29 DNA Homo sapiens 24gtgat tggctgaga 2omo sapiens 24acagc tgcctccttt 2omo sapiens 242 cccacagagc actttgttag a2omo sapiens 243 gcctccctta agctgttatg c 23 DNA Homo sapiens 244 cactctttac tgccaatcac tcc 23 245 Homo sapiens 245 gccgtgtggg tgtatgaat 22 DNA Homo sapiens 246 ttgtaccagg aaccaaagac aa 22 247 2omo sapiens 247cacagacaga ggcacattga 2omo sapiens 248 gctctggtca ctcctgctgt 29 DNA Homo sapiens 249 catgcctggc tgattgttt Homo sapiens 25atcgg gaactg 2omo sapiens 25tcttt aagtccatgt c 2omosapiens 252 cagcaactga caactcatcc a 2omo sapiens 253 cctcaatcct cagctccaac 2omo sapiens 254 tgattggttc tgttgttgct g 29 DNA Homo sapiens 255 agcccaaggc tcttgtgag 2omo sapiens 256 tccttcacag cttcaaactc a 22 DNA Homo sapiens 257 agtgagaagc ttccatactg gt 22 258 2omo sapiens 258 gccaaccgtt agacaaatga 2omo sapiens 259 ctacatgtgc accacaacac c 29 DNA Homo sapiens 26attgc cgccgagag Homo sapiens 26ccacattcacaagc 2omo sapiens 262 cgattgccat gtctctttga 2omo sapiens 263 gagatctggc ctggatttgt 23 DNA Homo sapiens 264 tcattgtcag cacagaatga act 23 265 2omo sapiens 265 ggagggaggg aagaaagaga 22 DNA Homo sapiens266 gggaagagga gattgacttg tt 22 267 2omo sapiens 267 ggaacaccat cattccaacc 2omo sapiens 268 tacaagctcc accgtccttc 2omo sapiens 269 tgagttgctg cctcttcaaa 2omo sapiens 27atggg ccaaggaata 23 DNAHomo sapiens 27atgtc ctcatgaata gcc 23 272 2omo sapiens 272 tgtcctgcag acagatggtc 2omo sapiens 273 cctccggagt agctggatta 2omo sapiens 274 gagactggcc ctcattcttg 25 DNA Homo sapiens 275 aagaagccag agacaaagaaataca 25 276 24 DNA Homo sapiens 276 catctatctt tggattcagt ggtg 24 277 2omo sapiens 277 tgctcccaac atcttaccag 23 DNA Homo sapiens 278 tgtcctctgg tcatttctat ggt 23 279 23 DNA Homo sapiens 279 catgaatgag aagtgatgaa tgg 23 28A Homosapiens 28actgt aaactggctt cg 22 28A Homo sapiens 28attgc tatcagcgta 2omo sapiens 282 atgtgctgtg gtccagattt 25 DNA Homo sapiens 283 cctactactg caattactcc ctacc 25 284 2omo sapiens 284 tgtcataggc ttgcggtattt 2omo sapiens 285 ttggtagggt cctttccttt 2omo sapiens 286 gcctgctcac tgttgtttga 2omo sapiens 287 cggttatcag agactggtgg t 2omo sapiens 288 ggcttatttc atgtacggct a 26 DNA Homo sapiens 289ggttaaactc tacttagtcc tgatgc 26 29A Homo sapiens 29ctgca ggcacctctt 2omo sapiens 29agcgc ttgtactgaa 2omo sapiens 292 ttggcttctc gctctttctt 2omo sapiens 293 agccatcagt cacatgcaaa 2omo sapiens 294 agatctccag ggcagaggac 2omo sapiens 295 ccttcctccc tccttctctc 22 DNA Homo sapiens 296 cagtcaaatg tctcaacctt cc 22 297 2omo sapiens 297 ctagcaacat ggccaagaaa 2omo sapiens 298 cgtcattgat cccaatcatct 2omo sapiens 299 ggctgatagc ctcccttgta 2omo sapiens 3ttcaag cttccggttt 2omo sapiens 3atccgt
ccatctatcc 23 DNA Homo sapiens 3agtcac ttgtctgtgg tca 23 3NA Homo sapiens 3taggaa tcaagtcaaa taatgta 27 3NA Homo sapiens 3cggaag cttgagccta 2omo sapiens 3agacca ctgccatatt 22DNA Homo sapiens 3aggttt gggtatattg ga 22 3NA Homo sapiens 3taatgt agtggcagca 2omo sapiens 3gccttt gtgaattcct 2omo sapiens 3aatgag gtgggcatta 22 DNA Homo sapiens 3gaataaatcaggtgtt ga 22 3NA Homo sapiens 3cagctc agcatttctc 2omo sapiens 3ttaatc ctccagccat t 2omo sapiens 3cacctt gttaccctga 2omo sapiens 3ccctgg aatctggact 22 DNA Homo sapiens3gaaagg aaaggaaaga aa 22 3NA Homo sapiens 3aagact gaaacttcat cag 23 3NA Homo sapiens 3cttgct ttgggaggta 2omo sapiens 3ttagag cccatccaag 2omo sapiens 3tcagct tcatccacat 2omo sapiens 32aatat gcaaaattgc 23 DNA Homo sapiens 32ctgtt tcttgactta aca 23 322 2omo sapiens 322 gggaacaggt cacaggtcat 2omo sapiens 323 ggaagactgg gtggtcacag 2omo sapiens 324 ttccttctgcttgtgagctg 2omo sapiens 325 taccctcacc ttcctcatgc 2omo sapiens 326 gaagacattg gcaggtctgg 2omo sapiens 327 gagccctcat gttgggataa 22 DNA Homo sapiens 328 ttgttgattc tcccattctg tg 22 329 25 DNA Homo sapiens329 tcacctacct catctcatac tcaaa 25 33A Homo sapiens 33cggac aagtttccaa 2omo sapiens 33cattc tggacattca 2omo sapiens 332 gcaaatgagg ctggtaaggt 2omo sapiens 333 tgcactgtgg tagagggaaa 27DNA Homo sapiens 334 caacatactc ctatgcctag aaagaaa 27 335 2omo sapiens 335 ctcaccaggc agaaacaggt 29 DNA Homo sapiens 336 cccaatggca tgcttcact Homo sapiens 337 ggttctccca gcattggtt 2omo sapiens 338 aaggcctctgggtaggtagg 2omo sapiens 339 aagcaatcct tatgggctct 2omo sapiens 34taatc agaagcctca 2omo sapiens 34ttaaa tccagccatc 2omo sapiens 342 cagggactgc agtgtctcaa 2omo sapiens 343atgccacatt tgcctctctc 25 DNA Homo sapiens 344 ccaccttcca cttaatacaa acttc 25 345 2omo sapiens 345 gaagcaatcc attccaagaa a 2omo sapiens 346 gtcctgaggg tgtccaggta 22 DNA Homo sapiens 347 gctggagaac tcctattctg ct 22 348 2omo sapiens 348 tggagctatt gcggttctct 23 DNA Homo sapiens 349 tcaaatctct ctttcctcct cct 23 35A Homo sapiens 35ccagc tacgggagaa 2omo sapiens 35tttag gcaagtctca 2omo sapiens 352 aagcacacacagatgctagg 2omo sapiens 353 cctcagcctc cataatctca 2omo sapiens 354 gtacagagcc caccttctgg 2omo sapiens 355 tcactatgct gcaaggcaag 23 DNA Homo sapiens 356 ggtgcttgct gtaaatataa ttg 23 357 2omo sapiens357 cactacagca gattgcacca 2omo sapiens 358 gatttgaaaa tgagcagtcc 2omo sapiens 359 gtcgggcact acgtttatct 2omo sapiens 36gaaga tgctacctga 2omo sapiens 36cttcc tttccctctc 2omo sapiens 362 tgccaggtct gagttgtaag c 2omo sapiens 363 cagcatgaga ccctgtcaaa 27 DNA Homo sapiens 364 gaaagaaaga aagaaagaag aaagaaa 27 365 2omo sapiens 365 aatcaccaaa cctggaagca 27 DNA Homo sapiens 366 gaaagaaagaaagaaagaag aaagaaa 27 367 2omo sapiens 367 aatcaccaaa cctggaagca 25 DNA Homo sapiens 368 tctgagttaa acacttgagt tgctg 25 369 2omo sapiens 369 ccagtaaatg gcagtgtggt t 27 DNA Homo sapiens 37tggat atttctacat aaaccaa 27 37A Homo sapiens 37atggt tattgcttcc ttc 23 372 2omo sapiens 372 cgctttgttt ggtttggttt 2omo sapiens 373 atgcagttgt cccacatgct 2omo sapiens 374 tcctgcactc caaaggaaac 25 DNA Homo sapiens 375 aactctggtttaattcagct ttgtc 25 376 2omo sapiens 376 ttcttgaggg cataaagctg a 2omo sapiens 377 cacactcacc aggcactctg 23 DNA Homo sapiens 378 caggtttgat gaaggaaata tgc 23 379 22 DNA Homo sapiens 379 gggatcctct gcatttctct aa 22 38AHomo sapiens 38caaat caaccttcag 2omo sapiens 38ttcac acctctgacc 2omo sapiens 382 actcacacac aaccaccaca 2omo sapiens 383 gctactggtg ggtcgtaagc 28 DNA Homo sapiens 384 ttcagagacc atcacggc 25 DNA Homo sapiens 385 ctggaaaaat cagttgaatc ctagc 25 386 2omo sapiens 386 aggaaagccg agaaagcata 2omo sapiens 387 catgtatcca catgcccaga 2omo sapiens 388 ccttcagcgc agctacatct 2omo sapiens 389agaactgcga ggtccaagtg 22 DNA Homo sapiens 39aaaga gaggtaggaa gg 22 39A Homo sapiens 39aagtt agcagcatcc 27 DNA Homo sapiens 392 ttctagagga gtctatttct ttactgg 27 393 2omo sapiens 393 ggagctgtca cttgagcttt g 2omo sapiens 394 ccgtgaccta cagggaacat 2omo sapiens 395 ggcatcgggt gtttctattc 2omo sapiens 396 agacctgcct gtgttctggt 23 DNA Homo sapiens 397 ggagtgaaat aagtggaact gga 23 398 26 DNA Homo sapiens 398 cattaaatgagtcataaagg tcatgg 26 399 2omo sapiens 399 aacattgttg ctttgctgga 2omo sapiens 4ttagct cagtttctgg 2omo sapiens 4aagaca tttgcggata 29 DNA Homo sapiens 4catttg tgtacgtgt 23 DNA Homosapiens 4gccgtg gtagtatatt ttt 23 4NA Homo sapiens 4ccagtc atttgggtgt 2omo sapiens 4tgctcc ctcgtccaag 26 DNA Homo sapiens 4ttaagg tctattattt cctttc 26 4NA Homo sapiens 4atgcaggaagactcaa 2omo sapiens 4tgaaag gacacacatg c 23 DNA Homo sapiens 4ttaact atgcagcttg aaa 23 4NA Homo sapiens 4tgcaat cccgagag 2omo sapiens 4tcctgc tggctcttct 2omo sapiens4tgtggt caggaaatga 24 DNA Homo sapiens 4taaaca catgtgagtg agag 24 4NA Homo sapiens 4accatg ctttctcttt ga 22 4NA Homo sapiens 4gatgac tccctgctgt 2omo sapiens 4cattga aaggcaggta 2omo sapiens 4ctttcc ggcttctatt 2omo sapiens 4tgggaa ccattctcct 22 DNA Homo sapiens 4agaagg gatttactcc ag 22 42A Homo sapiens 42acatg gagcaagctg 2omo sapiens 42atcatgctgtaagga g 2omo sapiens 422 cacaggctct cacattctcg 2omo sapiens 423 tgacactcat ccctctgctg 27 DNA Homo sapiens 424 tgagtttcat aagtttacta cctgctg 27 425 2omo sapiens 425 ggcagggaga aaggacaaat 22 DNA Homosapiens 426 tcccttatgt gggattagtt ga 22 427 23 DNA Homo sapiens 427 cagacatgga actgagattt ttt 23 428 22 DNA Homo sapiens 428 tgttccatct ctctacccat gt 22 429 24 DNA Homo sapiens 429 tcaatgttct tattgagtgg gaaa 24 43A Homo sapiens 43cacccacccacacat 2omo sapiens 43ctgag ggcagagacc 29 DNA Homo sapiens 432 ccgtccttcc tccactgat 2omo sapiens 433 agagcactga gggagcaaat 2omo sapiens 434 agctacagca cgaggcagtt 2omo sapiens 435tttgaattga gttgctgttc g 2omo sapiens 436 tgtacaccac caaccattct g 2omo sapiens 437 gggaagaaag gcaaatagca 2omo sapiens 438 ggattggcaa ttagcaggtc 22 DNA Homo sapiens 439 gcctggtcaa agataacaga cg 22 44AHomo sapiens 44ttaag ctggcctttg 2omo sapiens 44tctgg gaccctcatc 2omo sapiens 442 gctttgcttc cttcttggtg 2omo sapiens 443 caacattacg gccagtctca 2omo sapiens 444 ggtgcatctg ataagccaaa 2omo sapiens 445 gctgtcttgg acacagtgga 2omo sapiens 446 caccatcatc atctggttgg 2omo sapiens 447 gagctcattg aaaggcagga 25 DNA Homo sapiens 448 ccatccatct atccatttat ctctg 25 449 2omo sapiens 449ggatttatcc ttgccctgct 23 DNA Homo sapiens 45atcca tccatcctat ttg 23 45A Homo sapiens 45gcagc tacctggaaa 2omo sapiens misc_feature 8 n = A,T,C or G 452 aggactanag atgaatgctc 2omo sapiens 453gacatgactc catgtttggt 2omo sapiens 454 cctcaccttg caatttcctg 2omo sapiens 455 ctgacttgcc tgttggcata 2omo sapiens 456 tttgggatct tgaagacctt t 29 DNA Homo sapiens 457 ttgtggcatg tccttggtt 23 DNA Homosapiens 458 tgtacactgc aaacattgct aaa 23 459 24 DNA Homo sapiens 459 ttgtcctttc attatgacgt gtct 24 46A Homo sapiens 46tgaaa ggatacacac aaa 23 46A Homo sapiens 46tccca gactttccag 2omo sapiens 462 ggtgaatcccaccctcatac 24 DNA Homo sapiens 463 ttggtatgtt tcctattgtt gcat 24 464 2omo sapiens 464 gaaccagtga gtttttatta c 2omo sapiens 465 agacacagca tataatacat g 2omo sapiens 466 tgaagctttg tggcttgttg 2omosapiens 467 gactgagtcc acagcccatt 25 DNA Homo sapiens 468 cctggcctgt tagtttttat tgtta 25 469 22 DNA Homo sapiens 469 cccagtcttg ggtatgtttt ta 22 47A Homo sapiens 47atgca agaacagatg 2omo sapiens 47gcact tggctgtctt24 DNA Homo sapiens 472 ttgcatgaag taaagtatcc ctgt 24 473 2omo sapiens 473 cacaaaccac aagatgattg g 2omo sapiens 474 gggcatcatg tctacaactc a 2omo sapiens 475 accaagggca cttgctgata 2omo sapiens 476aggatgaaga gggaggaagg 26 DNA Homo sapiens 477 ccagactgat cttccttaat tagttg 26 478 2omo sapiens 478 cctcctcttt ctgctgctgt 2omo sapiens 479 agccaaagaa cccaaagaaa c
2omo sapiens 48acttt gcctcagaaa 2omo sapiens 48tcatg ccagcctcta 22 DNA Homo sapiens 482 aactgtgtta atgatgggca aa 22 483 2omo sapiens 483 aacgagcgca tgaaacctat 2omo sapiens 484cctggtcaat tgaacccaaa 23 DNA Homo sapiens 485 tgaaggaaga taaagcaggg taa 23 486 2omo sapiens 486 ctctctctgg ccctctcttg 23 DNA Homo sapiens 487 ggtaacttgc cattcttcta cca 23 488 2omo sapiens 488 actccacctg aagggagaaa 2omo sapiens 489 tggaagccac taattggaga a 23 DNA Homo sapiens 49atgga tacctcctta tca 23 49A Homo sapiens 49tgtgg ctttctgtgc 2omo sapiens 492 gtacccacac ctcaccaagc 2omo sapiens 493 cgtagctcacattcccaaca 2omo sapiens 494 ggcgagtgaa agagaggaca 2omo sapiens 495 gggtggtaat tcccagatga 2omo sapiens 496 tctgcaacag ccagaatcaa 22 DNA Homo sapiens 497 tgtctgttgg caactttctg tc 22 498 2omo sapiens498 aggtgaaccc agtccagcta 2omo sapiens 499 tcttaggcaa aggagccagt 29 DNA Homo sapiens 5gagcac tggtgactg 2omo sapiens 5tcaaat gttttaagca 2omo sapiens 5gggtgt tcgctattcc 2omo sapiens 5ctgtcc agtcctgacc 22 DNA Homo sapiens 5tgcagg tctaggtcac ac 22 5NA Homo sapiens 5tagctt gagcccg 396 DNA Homo sapiens 5atatcc cacctaccac tgcagctcca ggatccagct tcacaaacat ttgttgaatg 6ataag aaaagaggac acccccaaag aggctgcaag ggaaaaagct acaaagacag caccagg aaaaagtagg gtcatgtaag tcaaagcagg aaaaaagttc catggtgggg tcagcag tgtctaatrc cacgaaggca caaagtagga taaaggttaa aaatcagcct 24tttgg caaatatgaa gcttatcggt agccttagcgagaacaattc catcagggag 3agctaa ctgcagtggg ttgagtcatc aagcaggcat aaggaagtag ggatacccca 36agcta ctctttcaag aagctcaaat ctgaag 396 5DNA Homo sapiens 5aaatta ccatcatatg ctgtcatgca tgtctgccag tctatttatc atattattta 6caaacatttattgaa gatttatcat gtgctcagca ctgccaaaga ggaaataaag ataatat ctattcttag aaaataacat taacacaaat agaaaacaag aaaccataat aaaaata ttacatagya acacagaaag acaatgtata attatacata cgcactaaag 24ataac ataatttata aattatgagg tacagaatag ttagattctgaaaattaaaa 3caggaa aaacttcatg aagatgagat ctgggctgga tcccaaagga taggcaggtg 36tgtag aacaggggaa aggagttcct gatcgg 396 5DNA Homo sapiens 5aaagaa agccacaaaa gttcacctca atgccaagac atttcttgat ttttgaaaac 6tgtcg aaccacccatctatagaaac ttgaaagact aaaaactatc ttactctaaa tttctag gaagttgatt ctacaacaca ttttggtttt ccaatttggc ttctaataat ttcaaag tttctgtgrc ctaaattttg ttttacattg atcctttgaa tggactactg 24acatt ttagaacatt taaaaagata tctacaaccc gagtctaatc ataaaaaaaa3acagat ccaaaatgtg gaacattcca ctaaaaaagg agtggggaga ggtctttatt 36aaaaa tatcaatgcc ataaaagaca aagacg 396 5DNA Homo sapiens 5ttcaac cccagcccag ctgctaactg actacagcca catgaacaga accaggtgag 6aggaa acttccagtc acctaccagatcatgacaaa taataaacga tgttttttaa acaaaga tttggagcag catttgttac acaaaattag acaactatta cagttcgact aacatgt tcatttacra tactaaatta gaagtgtaag aatgggagaa aaacttcata 24aaagt cattttttcc tccaaaaact tccaactttg aaaaactgat ttttataatg 3aaaatt aaaataacct tagaatttat atgagtagca tagccagctg gctttattat 36gtact caacacttca ataatcactg atgttt 396 5DNA Homo sapiens 5ccttac ctcgttttgt tttccttgtc tgagagaaac acattagcag tctcccatct 6ttcct tttcctgtca cccaggacagagggcagtgg tgtgatcaca gctctgcagc acttccc caggttcagg tgatcctccc acctcagcct cccaaggagc tgggaccaca acatgcc accacgtcsa gcttaatttt gtattttttt ggtagagatc aggttttgcc 24gcccc aagctgatct tgaattcctg ggctgaagca atctgcctgc cctggcctct 3gtgtta ggattacagg tataagccac cgtgcagcct tatattttgt tttaaatttt 36gtatt tttctctctg gcaaattgtt taggga 396 5DNA Homo sapiens 5ttggta gagatcaggt tttgccttat tgccccaagc tgatcttgaa ttcctgggct 6aatct gcctgccctg gcctctccaagtgttaggat tacaggtata agccaccgtg ccttata ttttgtttta aattttcctc tgtatttttc tctctggcaa attgtttagg tttcttt agtttatcrg actaaatttc aaggctttcc ttccaatttt gacatgtaaa 24cctca tttctgctta tctagtgatt attcccaaat ctgtgtttac agtctagctg 3tcctga gattaagact tgtttctcta actacctgac ggcagaatct cctcttggaa 36aagga ggcagttcaa aactgaactg ggcatt 396 5DNA Homo sapiens 5atcttg aattcctggg ctgaagcaat ctgcctgccc tggcctctcc aagtgttagg 6aggta taagccaccg tgcagccttatattttgttt taaattttcc tctgtatttt ctctggc aaattgttta gggagtttct ttagtttatc agactaaatt tcaaggcttt tccaatt ttgacatgya aacagtccct catttctgct tatctagtga ttattcccaa 24tgttt acagtctagc tgtctctcct gagattaaga cttgtttctc taactacctg 3cagaat ctcctcttgg aagtatcaag gaggcagttc aaaactgaac tgggcattgg 36ctcct tctccttctc tttactatta ataccc 396 5DNA Homo sapiens 5tcttat ttaggcatcg tttcttctgg gagacctttg tagaatctct gaggttatgt 6tgcta aggttttctt gacattctcagattgggtta ggtgaacttt tagcaactta ttttact aaaaagtcat ccctcagtat ctgtggggaa ttggttctag gactccctaa tatcaaa atctgcatra gcagcccagg tgagaccagc agaagcactt tacagtcacc 24gatca tgacaaataa taaatcatgt ttaagccaca aagtccttta cataaaatgg 3gtattt gcatataacc tacacatctt cctgtatcct ttaaatcatc tctagtttat 36ctcat acgatgaaaa tactacgtaa atagtt 396 5DNA Homo sapiens 5agttcc taattactgg acattctcag atctgctaga gctacatgtc caattacgag 6actgg aaaaagccct ggattagaaatgagaggatg taggttttag taccaggtca accttgt taatgcaaat ttgagtaaat tgttacttct tttaggcctt gtttttgctg tgttttt ctgacagtmt ggtctctgtg gtccaggctg gagtgcagag gcacaatatc 24cctgc agtctctacc tcccaggatc aagccatttt catgcctcat cctcctgagt 3gggatt acaggcatgt gccaccacac cctcgaactc ctgacctcaa gtgatctgct 36cagcc tcccaaagtg ctgggattag aggtgt 396 5DNA Homo sapiens 5atactg gaaaaagccc tggattagaa atgagaggat gtaggtttta gtaccaggtc 6ccttg ttaatgcaaa tttgagtaaattgttacttc ttttaggcct tgtttttgct ttgtttt tctgacagta tggtctctgt ggtccaggct ggagtgcaga ggcacaatat gtccctg cagtctctrc ctcccaggat caagccattt tcatgcctca tcctcctgag 24gggat tacaggcatg tgccaccaca ccctcgaact cctgacctca agtgatctgc 3ctcagc ctcccaaagt gctgggatta gaggtgtgag ccactgtgcc tagccttaca 36ttttc ttactggtaa agtgggaata tctaga 396 5DNA Homo sapiens 5tgtttt tctgacagta tggtctctgt ggtccaggct ggagtgcaga ggcacaatat 6ccctg cagtctctac ctcccaggatcaagccattt tcatgcctca tcctcctgag ctgggat tacaggcatg tgccaccaca ccctcgaact cctgacctca agtgatctgc cctcagc ctcccaaakt gctgggatta gaggtgtgag ccactgtgcc tagccttaca 24ttttc ttactggtaa agtgggaata tctagaagtt gcatgctaca taaattcaac 3tattat tggcaaaaaa ttttaaagaa aaacatcagc ttaagagtac taattgagta 36cttgg aatgagcatg agctggaaag aacaaa 396 5DNA Homo sapiens 5aaaaat tttaaagaaa aacatcagct taagagtact aattgagtac atgccttgga 6catga gctggaaaga acaaacctgttgttacatca ctcattgctg ttttcatatg ctcattg taaatcttgc tcagtggcat gattttagtg tttaaagatt tatttgtttg gtttagg acaaagtcyc tacacataat ctacttgctt catatataca tacttatgca 24tgtat gtacatacat gctctcaggg ctcacatgaa aaaacagcca ttcaggtgat 3tttatc tcatatgctt actttagagt caacagggtg ttgactccac tatacaatac 36tggag aacacataag tcaaagtaga caggac 396 5DNA Homo sapiens 5tttgtt tgtttgttta ggacaaagtc tctacacata atctacttgc ttcatatata 6ttatg catattatgt atgtacatacatgctctcag ggctcacatg aaaaaacagc tcaggtg atgtgattta tctcatatgc ttactttaga gtcaacaggg tgttgactcc atacaat actggcatrg agaacacata agtcaaagta gacaggaccc agccgtacca 24taggg cacaaatata ttcacatatg tggagaatga tgtacgtaga aaggtcttca 3acaatg ctctttaata aagatctgga aaaaaaaaac acctaaatgt tcaaaaggat 36agatg aaataatggt acattataaa atggaa 396 5DNA Homo sapiens 5tcaccc aggctggagt gcagtggcat gatcatgtct ccttgcagcc ttgacttccc 6caggt gggcctccca cctcagtctcccaagtagct ggaactacag tcgtgcacca tagccag ctaagatagt gagatggtgg ccccactgtc ttgcccaggc tggactcgat ctgggtg caagcaccst tcccgcctca gcctcccaaa gtgctgggat tacaggcatg 24ccatt ccagcctact tgtctttaat tcttaaaaat attaatgttg agttttgtct 3gcatgt gggaaagatg tcatccattg cttctgtttc ctggaggcct gggagcaagg 36aggaa cagtatcacg aagcttgaga taatac 396 52NA Homo sapiens 52tgatg ggcatttggg ttggttccaa gtctttgcta ttgtgatttt tttttttttt 6ttttt taagacagag cctcactctgttgcccaggc tggagtgcga tggcatgatc gctcact gcaacctccg cctctcaggt tcaagcaatt cttctgcctc agcctcccaa gctggga ctacaggcrc ccaccaccag gcccagctaa tttttgtatt tttagtagag 24gtttc accatgttgg tcaggctggt cttgaactcc agacctcatg atctgcctgc 3gcctcc caaagtgctg aaattacagg tgtgagccac catacctggc ctaggcagtc 36caaaa ctctaagact gtgcttgtgt ctcagg 396 52NA Homo sapiens 52gaggt aaggatccat ttttttccca tttgcatagc cagtttttgt agctccactt 6tctca cttgatctgc catgccacctctagcatgta tcaacatatc atgtatgtgt gctgttc cttaactctc aattttattc tcttggttac tttgtctaac ccagcactca tttttaa attattaygg ctaccttgta gggcaagaat cctcactttt attcaacttc 24aagtg tcttgatgca tattttttct gatcttactt ggccatatat attttgggga 3tgtgac atcataccaa gctttctttg cttgacattg tagatatttt cttattcatt 36gctaa aaattttgag tttggtcata cagtc 395 522 396 DNA Homo sapiens 522 gtttctaaca ttatagacac tagttttagg ctcttggagg ctagcagcaa ttctcagagg 6caagc ttccccattt cttcccgtag tcctgtgaaagaccagccac ctccagaagc cacatga gtcttctcag ccatactttc tgcttttcct aatgcctctc agcagcgtat aaaggcc atgatcgayg tacctgttac cttcaggctt tgcataaggt gtatatgaaa 24tgaat ttcgtgttta ggctcaggtc ccatccccag gttacctctt tatcttggag 3ttctggtcccatacat ttcagataag agatattcaa cctgtaccca ccacgtaagg 36aatag gttttagaag aggagtcagg gaggca 396 523 396 DNA Homo sapiens 523 gcatctatta aaagtgatgg ttttagtatc ctgtctcatt ttttcctttc cttacatcat 6atagg taaacacatg cgcatgtgtg tatttctcttttagacaaag gatgagatta ctgttag ctcagttttt ttttccctac ttaacatctt tgcttttatt ttttagacat tctaaga ctattaaaya ttagacttac gtagcccttc tgtcattgtg aaatacatag 24taaca gctaccatca agataaagcc tttatttaaa taattaaact tcttagtgga 3taagtaagcacagttt atggattttg ggaatttttg ccttgcattt gtctgatatg 36atatt gagtttgttt ttctcataat gttcac 396 524 396 DNA Homo sapiens 524 gataactcaa tccccttaaa gggttgtatc aagccattga taagggctca ctttgatata 6tttct gttatttaga cactctttca cacttcctattttcctcctg gggatggttt tggatga cacaatacca tattataaaa gcactttaca aactgtaact tatgttataa taattat taccttaarg ttttaccctg tttcagattt gagtggaagt agttctttac 24aaaac aacttatttt aacttttttt gcatttcaaa gaatgatcaa tccacttcag 3agcatggtttccaacc ctgacagcat ggaagaatca tttatttagc ttctaaaaat 36ggctg taccctagac cagccttggg gattag 396 525 396 DNA Homo sapiens 525 tcctctctct cattctctct ctctctctct ttctctctct ccttctttgc tccttcattc 6ctctc tctctttttt ttttgagaca gcatctcactatattgccca ggctgttctc ctcctgg gctcaagtga tcctcctgcc tcagcttcct gagtagctag gactacaggc tgctatg gcaatactrt tttaaacatt gttttcaagg ctccccaggt gattccagtg 24catgt ggtagagaac cactgacaca ggcaaacaaa ggatacataa agttgtctat 3tgggtaggtgcaggta gtagataaga gtgtagccac ataaaccaca tgcttagtga 36tttgt tttgtgtgta tgtgagggat tagcat 396 526 396 DNA Homo sapiens 526 ttcaggttcc atttagcacg acagcaggga agggactgtt ggcagaaaaa aactggggca 6attaa agacagacca cacattccaa aaggcaccgtgggagggtca gggggcgagg ggtctag gcttcagtgt cctgggagac tcagtcttca cagggtgaca gcgatcaaga cagctta ggctgggtrc agtggctcat gcctgtagtc ccagcacttt gggaggccga 24gagga ttgcttgaag ccaggagttt gagaccagtc tgaccaacat ggcaaaaccc 3tctactaaaaatacaa aaatcaactg ggcatggtgg cgtgtgcctg tagtcccagc 36gagag gctgaggcaa gagaatcact tgaacc 396 527 396 DNA Homo sapiens 527 taaatgatca ttatgttcat attcacacat acaataatgt actcaagttt attgctaagg 6cagaa tctccttatt ttgaagtgtg catttgatatacctgtttgg gaataactag cttatct ttgacagaaa ataattttgt tgttttgttt ttactaaaaa agcatggtga atggctc catttctawg agaggtaact aaaatatcgc aatttgctgg gtgtcattaa 24ctcac aagggaaaaa atgcaaattg gtatctgctg atggagtaaa tctccgcaga 3atgaccctgaaaggat caatatatta aagcccctcc cagctggtca ttccagattg 36ataaa gcattaagtg ttaaaacctc aaggca 396 528 396 DNA Homo sapiens 528 ctcatcaagc ccacctttat acttcatttc tccagacttc atgtccagac tgtgggatga 6tggtt ataaggtttt agaggctcct gtaggactagatggaaggca aaaaaaggaa accttta agcatgctct cgattcctta aatcccatct gaaagtctta aggatgtctt agtcata cttatttgrc aatattacct aattttctcc attagcccaa gctcaggggt 24ttctt ccatattcac atgggtgcaa tggttttctg aaaggaaaac agcattacta 3agtaacatttaattaa tcacaggtac ttatcaaact acaaaacagg cattccagga 36gtgtt tctgtttgta aaattacact ctcgtg 396 529 396 DNA Homo sapiens 529 taggactaga tggaaggcaa aaaaaggaaa taacctttaa gcatgctctc gattccttaa 6atctg aaagtcttaa ggatgtcttc tcagtcatacttatttgaca atattaccta ttctcca ttagcccaag ctcaggggtc tttcttcttc catattcaca tgggtgcaat tttctga aaggaaaaya gcattactag ggcagtaaca tttaattaat cacaggtact 24aacta caaaacaggc attccaggaa ctgggtgttt ctgtttgtaa aattacactc 3gtacatgctcccacta aaatgtaagt tcgctgagga tggaggtttt ggtctctttg 36tgctg taaccccaac actgcagcag ggcctg 396 53NA Homo sapiens 53atagt ctcacttagg tgtggaatct aaaaaagtca aattaaaaaa aaatgtcaag 6aatag aatggtagtt gccagggact ctgggaagtagcaggggtgg gggtggaggg gggatgg gcagaagttg gtcaaaaggt acaaagtttc aggtagacag gtgtaagttc ggatcta ttgtacagmg tggtgactgt agttaatact gtattgtgta cttaaaaatt 24ccaaa aatgttctca ccaaaaaaat gatgtttgga tatgttaaac agtttgattt 3attttgacgtgtgtgt gtgtgtgtgt gtgtgtgtgt gtgtgtatac atcaaaacat 36tatat accatataca attaatatat acaatt 396 53NA Homo sapiens 53aaatg ctgactgcct gttctctgga caggaatgga gaagatggtg ctagcagggt 6ttcat atgtagacat tcatgcagtc actctcttttcagcacactt cttacttctg tgggttc agttgctgac tctgagccca gaaaccttct agggttctgt taggtagatt ttccacc gtctttgcra caaccacaga aaattctaga ctgttttctc ttcgggcttc 24tcaac ttgcttcagt ctgtcttgca tcttctaaat atttatagat ctctctcttt 3ggagtggcagaaaatg ctagttgacc acccaatatt caaattatcc tgcctcctta 36agaat atcattggat gtggtgggta aataat 396 532 396 DNA Homo sapiens 532 atggagaaga tggtgctagc agggttgctg ttcatatgta gacattcatg cagtcactct 6cagca cacttcttac ttctgccctg ggttcagttgctgactctga gcccagaaac ctagggt tctgttaggt agattggctt ccaccgtctt tgcgacaacc acagaaaatt gactgtt ttctcttcrg gcttcattag tcaacttgct tcagtctgtc ttgcatcttc 24attta tagatctctc tcttttgttg gagtggcaga aaatgctagt tgaccaccca 3tcaaattatcctgcct ccttaataac agaatatcat tggatgtggt gggtaaataa 36cctaa ctttccttgc agagaggggt ggccaa 396 533 396 DNA Homo sapiens 533 cagggttgct gttcatatgt agacattcat gcagtcactc tcttttcagc acacttctta 6gccct gggttcagtt gctgactctg agcccagaaaccttctaggg ttctgttagg attggct tccaccgtct ttgcgacaac cacagaaaat tctagactgt tttctcttcg ttcatta gtcaacttkc ttcagtctgt cttgcatctt ctaaatattt atagatctct 24ttgtt ggagtggcag aaaatgctag ttgaccaccc aatattcaaa ttatcctgcc 3taataacagaatatca ttggatgtgg tgggtaaata atatacccta actttccttg 36agggg tggccaatga gatggaaatg aaagtc 396 534 396 DNA Homo sapiens 534 tgggattgag ttcttgattt gattttgagc ttggccatca ttggtgtata gcagtgctag 6tgtgt acattgattt tgtaacctaa cactactaaattcacttatc aaatctggga ttttgag gattccttag gattttctag gtatgagatc atatcattgg tagaggtagt agtttct cttttccart ttggatgccc tttatttctt tctcttgcct gattgctctg 24ggctt ctagtactat
gttgaataga aatggtgaaa agtgggcatc cttgtctcat 3attttt agggggaaat gctttcaact tttccccatt cattttgatg ttggctgtga 36tcata gatgattctt actattttga gatata 396 535 396 DNA Homo sapiens 535 tcttttgccc tgcctttctg cctttctgtc cttttaattt gcgggcttttggcaaccaca 6ggtct ggtttcctag gagtttcttt tgtaggatca aaccgctagt tggctcttgg tgtgata gggccctggg ctaacttatt gggaaaatgt tgctgtaacc cctgcccaga gcctgtg acatgggcyg ccatcttctc ctcttccctt ggcttcagcc ccacctagaa 24aacaa acattttccttgacatttca taaagtgtca gtggctcctc atttagcaaa 3atccca gggaagttca aaagtgaaaa aaggccgtaa cttcttcttc ttctcaggga 36agaaa atatgtggca cctcggcagc ctggcc 396 536 396 DNA Homo sapiens 536 catggatttt gttttccaag tggcaagatg gcgcctccac ctttggtatcctattttagt 6gcaga aagaaaggaa caggctaatg gccctgatga gtctaccccc ttttaacagg aaattta aaaaacaaaa accatgaaac cctttcccag aggcaacaac cagaattcca atctttc attgaccara acagaccaca tggtcactgg tggtggcaat ggagactggg 24gaata tttttaaggtggcatattcc agaagaacac tgtgcactga ttgcattaat 3ccatta atgtgccaag gggaggttta cctatgagca tgggcaaatt agaacccact 36agctg caggtgagcc aatcccacct aaacag 396 537 396 DNA Homo sapiens 537 tggtggtggc aatggagact ggggagatga atatttttaa ggtggcatattccagaagaa 6tgcac tgattgcatt aatgaaccca ttaatgtgcc aaggggaggt ttacctatga tgggcaa attagaaccc actcttggag ctgcaggtga gccaatccca cctaaacagt gatgcta caagatggrg aagtaaattg attctattcc ataccctaac ctctctccaa 24attct taaaatagaagagggaagac agaagaaaac atccagaata tatttttatt 3tttact tcttcagtgc attttagatc agtgcttctc aatctggcaa ggggcatgca 36atgtg agttttatca ggaaaactac acaacc 396 538 396 DNA Homo sapiens 538 tgagccaatc ccacctaaac agtgtggatg ctacaagatg gggaagtaaattgattctat 6accct aacctctctc caagatgtat tcttaaaata gaagagggaa gacagaagaa atccaga atatattttt attgtctttt acttcttcag tgcattttag atcagtgctt aatctgg caaggggcrt gcaggaggat gtgagtttta tcaggaaaac tacacaaccc 24ccaca atgctacccccactcctgtg gaccttcttt aagagagact cactattata 3gagttg atacgatttt aagagaggcc atatattatt tgctttctgt cttgaaaaac 36atttt tctgtattgt gctactgcca aagaga 396 539 396 DNA Homo sapiens 539 gggttgcagt gagcagagat cacaccattg cactccagcc tgggtggcagagcgagattc 6aaaaa acaacaccgt atttggggca tgctgatact aaaaaattat tcattgtttg gaaatta aaatttaaat tgggggccct gtattttact gggcaaccca tttgcaatat caacaat ctcttattsa gaccactgat taagtgtgca aaatttgaat ctctgaacag 24atgtc cttgatatcttaaattaatg agtgtcttag acactcaaag caggaggaag 3atggca gatgtttgag ccccagagat gtccatgagc acagcataga gctcagagcc 36tatta tttgcttcac gacagagcaa aggact 396 54NA Homo sapiens 54gcaat atcagcaaca atctcttatt cagaccactg attaagtgtgcaaaatttga 6tgaac agtacctatg tccttgatat cttaaattaa tgagtgtctt agacactcaa aggagga agcattatgg cagatgtttg agccccagag atgtccatga gcacagcata ctcagag ccttctttrt tatttgcttc acgacagagc aaaggactgc agcaggttga 24ataaa agttttaccatgtctcacag caggcctttg ctcaagtttc cagtaaggat 3tatcat ttcttgcctg cagtacttgt aaatccactt acactgcctg ctgttgagtc 36tttcg tcttgagtag catgtcatcc ttgttc 396 54NA Homo sapiens 54gttct cattgctggg gagtctaaac tggaataaaa cacccactatctccatcagg 6actag agcccagctc tagctggaga gaaagaagct aacccgcaca gacacaggac aggcagg gagcatccgg gggtatttgg gtcctggctc tgatgtgcct aaggccaact ctctggc catgctggyg tgcatgagct cactaatctt cctttttgcc ttccattttc 24tcctg acttagcaaaggttgggcaa aagagactct gtgtgagttc gagcaaagcc 3atgctg gattttccaa gatacgagaa ggggctgggg gctgggtgaa ctggtggtgg 36ggaag gattaatttc ccaaggaggg gaaggg 396 542 396 DNA Homo sapiens 542 gagaaagaag ctaacccgca cagacacagg actgtaggca gggagcatccgggggtattt 6ctggc tctgatgtgc ctaaggccaa cttctctctg gccatgctgg cgtgcatgag actaatc ttcctttttg ccttccattt tctccaatcc tgacttagca aaggttgggc agagact ctgtgtgart tcgagcaaag cctgagatgc tggattttcc aagatacgag 24gctgg gggctgggtgaactggtggt ggaggaggga aggattaatt tcccaaggag 3aggggc caggacatca ggccccgggg actttgaaga gagggtcgtg ggtaggaggt 36aagtg gagtgacaca aaggtcagga aagagg 396 543 396 DNA Homo sapiens 543 catgcctcct acaaatttga cctgggccca gggccatgtt cggtggtttttaagaaccga 6ccaga agcagtattg ggcagctaga gtggccccag gatctatatc aaactctacc ttctgaa ccaaatttct tctagaattt tattccataa atctgaatta tggtgtcaga ctagcat acactaaakg aactctctgc cttgcattaa ataacaggag ttacccctgg 24actcc tagccctggctctttagaga acagatgccg aataggcatt aggggatgtg 3atgtgc taactttcaa aaaaaaaaaa aaaaaaaggc ctgagctgag tgctcagaga 36aaaaa gctgacagca tctctctgtt ccattg 396 544 396 DNA Homo sapiens 544 ctttggagcc tggcagcctg gctttgagaa ccgggcttta acttgtcacatgactatggc 6tcctg gggctctcca agcttcactt cctctgtaaa aagggcaata atataatacc cttattg ggttttgtcc atgttagatg agacattggg tacaaagcac ttggtcccgt tggcaca tttactgcrc ttaatgtatg atagttttct tattattcta ataaacaata 24ttggg agtatagttctgccacattg cagtggccag agtgaaggtg gtgagtgcct 3gggccc tgggagtcaa ggttatccgc atgccctttc ttgcttgctc ctcagtgtgg 36tctat gtccacacca tgcagatgca acaggt 396 545 396 DNA Homo sapiens 545 acatgatcat ccccttgggc ttctggtttt ttttctttca ggaccttattttcaggcaag 6tttga cctctaaggc tgtcctttcc tagctaccga atccagcatt caaagtgatg atatgta tatatagtaa tagtaaaata tcagcactta atggcctgat aagaatgtca caatgct gagtttggrc caacatttgc ctgctcctgc cattgagccc gggctcccct 24gctga gctgctgcaagggatctgag taactagggc tgtgtcagag tggcgatgac 3accaca tgctaaggaa gagatcccca aggacaagga gaatcccacg tggagctact 36ctttg tcagtcttgt ttttcttatt tcacaa 396 546 396 DNA Homo sapiens 546 ccgaatccag cattcaaagt gatggaaata tgtatatata gtaatagtaaaatatcagca 6tggcc tgataagaat gtcactgcaa tgctgagttt ggaccaacat ttgcctgctc ccattga gcccgggctc ccctccagag ctgagctgct gcaagggatc tgagtaacta ctgtgtc agagtggcra tgacagccac cacatgctaa ggaagagatc cccaaggaca 24aatcc cacgtggagctacttgcttc tttgtcagtc ttgtttttct tatttcacaa 3ctaaaa cacaatctct caacctctat tgttagcttg catttttcaa tcatgagcac 36tacct ggctccatgc tttgattgac tctacc 396 547 396 DNA Homo sapiens 547 tcttatttca caaccttcta aaacacaatc tctcaacctc tattgttagcttgcattttt 6atgag cacagcttta cctggctcca tgctttgatt gactctacct gccaacactg caacagg gaaagggaca ccggcctcat accattagat ggtgtgtagc ctgggcatga taattaa aaactcccwa ggggatttta acatgtaaca cagtttggaa accattgatg 24tcttc ttactcaacatgtgctccaa ggagctgttg tatcagctta tcagaaatgt 3caggcc gcacttggac ctgtagaatc agaatctgca ttttatcaga ttccgacatt 36tatga acattagctt ttgagaagtg ttgctt 396 548 396 DNA Homo sapiens 548 cttttgacac caactacaag tcaaggggtt ccccaaacca ccctgagttgtgataattcg 6agatc tgacagaact cactgaaggt tgttatactc atggttgtga tctcttatag gggaata cagattaaaa tcagccaaag gaagaagcac acagcacaga gtccaggaca cctgaca tggagcccyt acggtcctct cccgtggagt cacggacagc gccactctcc 24ttgat gtgtgacaacacacagggag tgttccccac cagggaagcc ttggtgtcca 3ctttac tgtggctctg tcacatgagc acagctgact gcccatgcgg ccgatctgtt 36actct ccaccgctac acatcactca cagtcc 396 549 396 DNA Homo sapiens 549 gtggctcaca gaactcaggg aaacacagct accagtttat tgcgaaggacattttaaagg 6agtag gcagataaag agatgcatag ggcgaggtgt ggaaaggtcc ctagtgcagg ttctgtc catgtggagc gggggtgcac caccctctca gtacatgaat gagttctcct cctgcct atcagcctyt acatgttcag ctccccaacc cagtcctctt gggtttttat 24cttca agacacccacattctttccc cagagtatag ggcaagacct tctctgggga 3tttaag acccacagtc agaaaggtgg ggtggggtca agattagagt cctgccttga 36aggtg aaaggggtag ggggagtagg tgagaa 396 55NA Homo sapiens 55gtgca ccaccctctc agtacatgaa tgagttctcc ttcacctgcctatcagcctc 6gttca gctccccaac ccagtcctct tgggttttta tggaagcttc aagacaccca tctttcc ccagagtata gggcaagacc ttctctgggg agggttttaa gacccacagt aaaggtg gggtggggkc aagattagag tcctgccttg acgggcaggt gaaaggggta 24agtag gtgagaaaaattctgtttat tttttctttt tttttttgag acggagtttc 3ttgttg cccagggtgg agtgcaatgg cacaatctca gctcactgca acctccgcct 36gttta agcgattctc ctgcctcagc ctcccg 396 55NA Homo sapiens 55ttctc cttcacctgc ctatcagcct ctacatgttc agctccccaacccagtcctc 6ttttt atggaagctt caagacaccc acattctttc cccagagtat agggcaagac ctctggg gagggtttta agacccacag tcagaaaggt ggggtggggt caagattaga ctgcctt gacgggcarg tgaaaggggt agggggagta ggtgagaaaa attctgttta 24tcttt ttttttttgagacggagttt cactcttgtt gcccagggtg gagtgcaatg 3aatctc agctcactgc aacctccgcc tcccaggttt aagcgattct cctgcctcag 36cgagt agctgggatt acaggcgtgt gccacc 396 552 396 DNA Homo sapiens 552 tcttcattcc acaaagctca gtgtcaaaac atggggttta cactggaagctgaggtcaca 6agccg ggatcagggt cgccctagct gcccaatgca gctcccaggc ctcctgtaaa ttgacct ttgaggtcat gacagccctc tcctgctatg ctcatagctg accactgaac tggacac tccctcccsc aagttcacag agaatgtggg cacatgcctt acagtcttcc 24tccaa actactgccttcatcttgag tgacagcagc atcttttgga tgtcttggcc 3tagctt tatttttttg tgttctgcca tcaagttgct acttctgttg ccatcgtgcc 36gcgca gtgcaggctg tggtgaaatc ccacga 396 553 396 DNA Homo sapiens 553 tatttttttg tgttctgcca tcaagttgct acttctgttg ccatcgtgcctgtcagcgca 6ggctg tggtgaaatc ccacgaactc aggcatcaca ctgaccgggt ctgagtcctg cagttgt cagctagttg tgcaatgaag ggaaagggac ctacactttc caagcctcaa actcatc tatggcatkg tgacaataat ggaggttgat ttaaagtcct ttgtaagaat 24gttat aatagacataaagtgctgta tctggtatac ctagaaaaca ttccataaaa 3gtaatt gttggtcatg taatgatgac tctctaggct aggatttcag cttcattgca 36atggt gcactcacag ggcgtgacct ctctct 396 554 396 DNA Homo sapiens 554 ggtataccta gaaaacattc cataaaagtt agtaattgtt ggtcatgtaatgatgactct 6ctagg atttcagctt cattgcatgc acatggtgca ctcacagggc gtgacctctc gtctcag taacctcatc tgaggaccgg gataatcata ccgcttcaaa gggatgtcat gattaaa taatatgtrt aaggctgctt gcatttagct gcattcaaca aatatttctg 24ttctc ctcatttctccttactttct tgcttattat ctgctctagg tatagatttc 3aactaa gcttgttaca atccttcata aaataaccag gttggttagg gcatttccaa 36aatac tgtttagtga ctattctctg tttaat 396 555 396 DNA Homo sapiens 555 aaggctgctt gcatttagct gcattcaaca aatatttctg tatctttctcctcatttctc 6tttct tgcttattat ctgctctagg tatagatttc agagaactaa gcttgttaca cttcata aaataaccag gttggttagg gcatttccaa gagtcaatac tgtttagtga ttctctg tttaatctmt tttgattgtc cagggtcatc ttttgctatg tcataggttg 24ttctt ctagagaagtgagacgatgg acaagttcca agtgagtgag gcgactggtc 3tattcc gctgaaaaac tcatgtcagt tctaattcgt gattgtaatt caatcacagc 36aacag taggactgta gttcaaatgc tctgtt 396 556 396 DNA Homo sapiens 556 cctgggttca agcaattctc ctgcctcagc ctcccaagta gctgggactacaggcacatg 6acgcc cagataattt tcgtattttt agtagagacg gggtttcccc ttgttggcca tggtctt gatctcttga cctcatgatc cgcccacctc ggcctcccaa agtgctggga caggcgt gagccaccrc gcccggcctc tagaggataa tttttaaatg tgcttttgca 24aaaat gtgattggcatttttttcta attttctaat atgatacgct gtcggatgct 3attact taaaccctct ggctacctag aaagatcttt aagtggttct caacaagctt 36gcaat gtaaattgta ttatctctca ggatgt 396 557 396 DNA Homo sapiens 557 tgtgattggc atttttttct aattttctaa tatgatacgc tgtcggatgctatggattac 6ccctc tggctaccta gaaagatctt taagtggttc tcaacaagct tcatacgcaa aaattgt attatctctc aggatgtgtg agaacatctg tttttcttct aatgcagtaa tataagg gtctcttgrg atatctttta aatagactta atacaacatt caggaatgat 24aatat aatcacagttgtaagggaat gtgagcattt catattaata acattggaac 3tgttta atacagtgtt aaaagttgac aaacatgtag gagtcagaaa attcaattaa 36tcaca gtaatatgaa tttagccaca tcctgt 396 558 396 DNA Homo sapiens 558 acttaaaccc tctggctacc tagaaagatc tttaagtggt tctcaacaagcttcatacgc 6aaatt gtattatctc tcaggatgtg tgagaacatc tgtttttctt ctaatgcagt catataa gggtctcttg ggatatcttt taaatagact taatacaaca ttcaggaatg acaaaat ataatcacrg ttgtaaggga atgtgagcat ttcatattaa taacattgga 24atgtt taatacagtgttaaaagttg acaaacatgt aggagtcaga aaattcaatt 3ttatca cagtaatatg aatttagcca catcctgtgt tagttatgaa atccatttaa 36caaac agtaatattt ttagccagtt tattca 396 559 396 DNA Homo sapiens 559 catttaacac cacaaacagt aatattttta gccagtttat tcaaaaggaaaacaggaact 6acttt catgcaatat atactctgtt aatgtggtca ggctaatttt gctgggggaa acttaac ttttgaatat ttgaatgccc agtcatttaa tctgaatatc ctatttcctt tgttgca aaatttttkt caataaaagg cagaaaaaga aatctcttct ccatgctcat 24agaga atgggttgtctgtaccctga gagcatttta tggaggggac aaccactttt 3ttttcc ttcccacttc tctgtgggca caaatgctct ttggttgaaa gagttgtaat 36cccaa gatgaggtgt ggttactgca tcccta 396 56NA Homo sapiens 56ccatg ctccacactg cagccagagt gctctacaat gcaaatccatttgtgagact 6tctta aaatcctcaa gtggcttctc tttgccccca ggatcatttt gaaactcctt ggaagag gcatggccct ttgggatgtg gttccccaac ccctcccaca tcatcttttc cagattt cccactaart ggaaattttt tcaggtcctc aactttatgg tgactttctc 24cagga tctttgaacatactgtttct tctttccttt tgtatttgcc aagacaacac 3tctggt aagattttcc tgacatcctc tataaaaaaa gattgagata gttgactacc 36tgttt cccattcatt ccaagctcta ttcaag 396 56NA Homo sapiens 56ttcct ctggtaagat tttcctgaca tcctctataa aaaaagattgagatagttga 6caaaa tgtttcccat tcattccaag ctctattcaa ggcagtaaag tgcccggctg gattgca ttcctcatct tttctgaagc tagcaatggc catgcaacag cattctggcc aagatag aagtcgaart tgaagggtgg gatttccaag aaagctcgtt gaagacataa 24cattt cacttcttactctttctctt tcctgcttcc taaaatgcgg tgcagatggc 3acttca aagctgtctc aggcaatcag gtgatgttaa ggcagaaacc agctttatga 36agaac aggaagaaag aaggcaccta tgttct 396 562 396 DNA Homo sapiens 562 cctacaaatc tcatgttgac attttatccc taatattgga ggcagggcctagtaggaggt 6ggtca tagtgataaa tggcttggtg ccgttctcac agtaacgagt gagtttttat agtggtt cctgcaagaa ctgattgtta aaagagcttg gatccttcca cccctctctc cttgctt cctctctcwc accttgtaat ctctacaagc tcttcacctc cccttctcct 24cataa gtggaagatttctgaggcct caccagaagc agatgttggt tccatgcttc 3acagcc tgcagaacca tgagccaaat caacttcttt tctttataat tatccagtct 36attcc tttatagcaa cacaaatgga ctaaga 396 563 396 DNA Homo sapiens 563 gttgtttcca gctttgaact attttgaatc ctaaaagact gccagttttgaatgagaccc 6caatg aatgtaggct ctgtatacaa gttcaggctg ctgggcaact taggccttaa acaactc tgccacttag gccttaagac acaactgaca tgatggtgct taaagtggct atggaaa aggaggctrt ttggagcctt tggagtgcct ttataggtga accccagcat 24ctaat gatttggagcaaagctgtgt cattccccaa agataactat tcgccttttg 3acatct tctagctact atcaataata aacacagaat gcatcaccat gggccaccgt 36ctttt gacctgagtt tccattgtga acaaga 396 564 396 DNA Homo sapiens 564 aactctgcca cttaggcctt aagacacaac tgacatgatg gtgcttaaagtggctgtgat 6aggag gctgtttgga gcctttggag tgcctttata ggtgaacccc agcatagcac atgattt ggagcaaagc tgtgtcattc cccaaagata actattcgcc ttttgagaaa cttctag ctactatcra taataaacac agaatgcatc accatgggcc accgtgttgt 24gacct gagtttccattgtgaacaag agtcatttga tccaaggcag aaagttgggt 3acagca gtgttccatc atcaaatgga atatgagatt gggcccaagt aggtcctgca 36aaata agttgcaaga gcaagtagta caggcg 396 565 396 DNA Homo sapiens 565 gaaaaggagg ctgtttggag cctttggagt gcctttatag gtgaaccccagcatagcacc 6atttg gagcaaagct gtgtcattcc ccaaagataa ctattcgcct tttgagaaac ttctagc tactatcaat aataaacaca gaatgcatca ccatgggcca ccgtgttgtc tgacctg agtttccayt gtgaacaaga gtcatttgat ccaaggcaga aagttgggtg 24agcag tgttccatcatcaaatggaa tatgagattg ggcccaagta ggtcctgcag 3aaataa gttgcaagag caagtagtac aggcgcttgg cctggccagt actgttgcca 36actgc ttcccctcag tctgcatctg tggctt 396 566 396 DNA Homo sapiens 566 ccccaaagat aactattcgc cttttgagaa acatcttcta gctactatcaataataaaca 6tgcat caccatgggc caccgtgttg tcttttgacc tgagtttcca ttgtgaacaa tcatttg atccaaggca gaaagttggg tgcacacagc agtgttccat catcaaatgg atgagat tgggcccarg taggtcctgc agacacaaat aagttgcaag agcaagtagt 24cgctt ggcctggccagtactgttgc caagttgact gcttcccctc agtctgcatc 3gcttca tggggagttt cctatgacca cttgatggag gaaaaaacaa attggagcat 36atagt gctggtacta cccaaagtgg ctagct 396 567 396 DNA Homo sapiens 567 gtccgtgagt tacagatcta cacaaaatca cagagagtgg ttaatcgtttagtctgatgg 6gactt ccaagagaca tgattagaaa actggtgaca aggagtcctg gggaagaggc tggatac ctctgaacac acacaaaaca tgagaatatg tatcccatat gaatgttaac agagcag ccacaacasa agaggatttt aaaatcagct gaataagatg attcattctg 24atcag ctagtctctttccccagcca ctgttgccca gtgggcttac atatatcatg 3tggggg cagggctatg tatggacaca gcaacatgaa tttccactca tcaaggccaa 36ctcca gccattgctg agtgctcagc ctgcca 396 568 396 DNA Homo sapiens 568 acatgattag aaaactggtg
acaaggagtc ctggggaaga ggcatatgga tacctctgaa 6acaaa acatgagaat atgtatccca tatgaatgtt aaccaaagag cagccacaac agaggat tttaaaatca gctgaataag atgattcatt ctgacagcat cagctagtct tccccag ccactgttrc ccagtgggct tacatatatc atggccatgggggcagggct 24tggac acagcaacat gaatttccac tcatcaaggc caatttggct ccagccattg 3gtgctc agcctgccaa gatagaaatc tacgccaata tggcaccatt ccctgggcta 36ccaac tggtggaagg ttgattacat tggacc 396 569 396 DNA Homo sapiens 569 gggaatacaa tggtggttccactaaactga cagctgagtt tgccatctcc tcgtgccagt 6cacaa gcaaggaagg gggttccttt ctcacctagg gtgactgatc ctaattacca agaaatt ggactgccac ttcacaatga gggtgaggag tatgtactct atgtgtctgt taatgtc aatagaaart gacaccaacc tagtacacag aggactgatc atggtccagg24cagga atgaagattt gagtcaccag gcaaggaact tggactcact gaggagggca 3ccaagg agaatatttt atctatgtcc atctatgtcc atctatattc catctgtgtt 36tggaa ttcctattca tgaacatggg gaattc 396 57NA Homo sapiens 57aatga gtagtggaag gtagttataaatgtaagtca aaaaccacac aaccaatttg 6tgagg aaggtaatag tgttgaatat gtcttcttta tcttgatata aatgtatttg atatatt aaccagttta tttatttatt attatttttt gagatgagct ctcgccatgt ccaggct ggtcttgamc tcctgggctc aactgattct accatttagt cctccgagta 24gacta caggcatgca ccaccatacc cagctgacca gttttttcct attcctctac 3tttctc tactatacaa cataatatgt gttaatggta gttaacttta tatctcagta 36tcaca agatatcaaa aagggaatgc gactta 396 57NA Homo sapiens 57ttctt tatcttgata taaatgtatttgtgcatata ttaaccagtt tatttattta 6atttt ttgagatgag ctctcgccat gttgcccagg ctggtcttga actcctgggc actgatt ctaccattta gtcctccgag tagctgggac tacaggcatg caccaccata agctgac cagtttttyc ctattcctct acttaatttc tctactatac aacataatat 24aatgg tagttaactt tatatctcag tattaagtca caagatatca aaaagggaat 3cttagt tacaagcaga atgaatatca ctcaaagatg aataaagaga agagggttag 36tttct gttggatgag agaaagtttc attgtt 396 572 396 DNA Homo sapiens 572 gcagtggcgt gatcccagct cactgcaatctctgcctcct gggttcaagt gattctcctg 6gcctc ccgaggggct gggattgtag gcgtgcacca ctatgcccat ctaatttttg ttttagt agagataggg ttttgccatt ttggccagac tgtcttgaac tcctgacctc tgatctg cctgcctcrg cctcccacag ttttgtgatt ataggcatga gccaccgtgc 24cttaa cctttgtttt cttacacaac acactacgtg atgttttcca catgcatggg 3ttgctt catttacgta caaatgcata agcaatatac tgtgtggtgt gagtttgtga 36aaagg aagaagtttt gcggatacta cactgg 396 573 396 DNA Homo sapiens 573 gcccaggctg ttctccaact cctggactcaagccatcctc tagcctcggc cttccaaagt 6gacta taggcgtgag ccacggtgcc aggcccttga ccacattttt aacccctctg ctcagtt tcactttctg ggcaatggga ggggggtaat ttgtccctca gagggttgca aggggca aatgtgagsc tctgggtaca atgcccagta cagactaggt ccccacgaca 24gctca gcggctccgg attctgggct gctctggact gcggccaggc ggtcttctgc 3atccgg gcaggcaggg cgggctgcgc tcccctcccc ggctctcccg gtgccccttg 36ttgtt ctgtctcagc agctctctat taagat 396 574 396 DNA Homo sapiens 574 tttttgttct gtctcagcag ctctctattaagatgaatgg catttccaaa ggcttcacct 6aagtg ttcctctgca gctgcagcca gaatcttaat gtgcgcgctg taatttaatg gtctcgg ctattaacac gctcttctcg ggtgaagtgg actccctcca tccccgggcc gcacgtg ctctgcgcrc tggctggggg tgactccaag gagctcagag cggggtgccc 24ctctc gccaggcgcc tttcgacctt ctaaagcgcg aatggctgga cttttctccc 3gtgggg ccccagaagg tgtggggccc cagaaggtgt ggggtccctg cgttccacgg 36ggaag gtttccagtg atggtggggg ctgacc 396 575 396 DNA Homo sapiens 575 ggagcccgga aggtttccag tgatggtgggggctgaccac gttggtcccc gtgggtgctg 6atgtg ccggcagatt gggatgagtt taaaagacag aagcgtgtag gatagagaaa ctttaaa aactggaaat tttaatctgg ggattataac tattggacag tcaagtgcaa tgaatac acttctcast ccctcctccc aatttttatt tgcgggatta gtcagtcccc 24ccaca tgataattgt gagaactacc agggtcttca ttctcctgcc atctggttga 3tccaag aatggacacc cgggcagcct gggccaatga ggctgtccta agagtttaga 36gaagt cagtctttga caggtgatgg aagctg 396 576 396 DNA Homo sapiens 576 cagtgatggt gggggctgac cacgttggtccccgtgggtg ctgttttcat gtgccggcag 6gatga gtttaaaaga cagaagcgtg taggatagag aaacttcttt aaaaactgga tttaatc tggggattat aactattgga cagtcaagtg caagagtgaa tacacttctc ccctcct cccaatttyt atttgcggga ttagtcagtc cccctctgcc acatgataat 24gaact accagggtct tcattctcct gccatctggt tgacctctcc aagaatggac 3gggcag cctgggccaa tgaggctgtc ctaagagttt agatgagaga agtcagtctt 36ggtga tggaagctgt aaaatgtaaa actcca 396 577 396 DNA Homo sapiens 577 taagagaagc tgagagagag cgagaggagagattggaaga aagacagaga cagaggtaga 6gggaa agagagagag aaagggacag aagagagaga aaaaagaggg ggccgggcgc ggctcac gcctgtaatc tcagcacttt gggaggccga ggcgggcaga tcacgaggtc agatcga gaccatccyg gctaacacgg tgaaaccccc gtctctacta aaaaatataa 24attag ccaggcgtgg tggtgggtgc ctgtagtccc agctactgag gaggctgaga 3agaatg gcgtgaaccc gggaggcaga gcttgcagtg agctgagatc gcgccactgc 36agcct gggcaacaga gcaagactcc gtctca 396 578 396 DNA Homo sapiens 578 tccaccagca gcttttctga gtctccagcttgcagatggc aaaccatgaa acttcatggt 6tgagc atgtgaacca atttctatta taaatctgca atatatatat atgaggagac tttatat attggttcag tttctctgga gagccttggc taatataaag tctatactct aagtgcc ctaggtackc agggagtacc caagtgtgtc atgaccagcc cgacagccct 24ctggc ttccccgcac acaactctgc acgctgcctt catcagcctt tctctctcag 3accgag ggcattgaag cgggcctctg gcactgtacc tatgagggag caatatcttc 36cactg acctcttccg tgccgagatg cagccc 396 579 396 DNA Homo sapiens 579 gcctctggca ctgtacctat gagggagcaatatcttcccc tacactgacc tcttccgtgc 6tgcag ccctccctgc tgccactagt tacagtggtc catgttccct ttcaaagtga tttgata aaagcacctc ttaaccaatg ccaaatagct aagtctggga caaagattgc tattttg cattttccwt gtaacctcag agggattgcc attcacactg atctgagctg 24tacca ggcagccacc tcacccaccc agcaggtcca ctcttatact ttctcagaaa 3agccac tctactctta ttcagttgaa aagaatttcc aggaaggtgt ttctgcgatt 36agaaa agtcagttcc ctttgggaat ttccct 396 58NA Homo sapiens 58ttctc tgaagaaatg gagatatcagctgtccctcc ccactgccat ttattccttc 6ttcaa accttatgtg gctgctactt accgtgtgtt aagtgttcac tttttttctt attcaaa aaaagaagga cagtatttgg ggcacagatc ttttggtgtt ctatacattt taaagtt tcattttaya tttgtgtgtg cgtgtgtgtg tgtgtgtgag acagtcttgc 24tgccc aggctggagt gcagtggcat aatcattggc tcactgtagc ctcaaagtcc 3cccaag caatcttccc acctcagcca cccaaaatgc tggggttaca ggtttatgcc 36gtctg acctgaaagt tttgggttta ctttcc 396 58NA Homo sapiens 58atcat tggctcactg tagcctcaaagtcctgggcc caagcaatct tcccacctca 6ccaaa atgctggggt tacaggttta tgccactctg tctgacctga aagttttggg actttcc cttctttctc tttgctgaag tcagagatga tggcagcttc cagattctct gcctgtg ctgggctcrt gctggtcatg gtcttgggtc caggattcat tctggagact 24ggaag tttcccatga caaggaaatg taggagagtg tgctggcttt gcgtgctcct 3caagcc ctgcttctcc tggtgggaca cactgaacca cagccagggc attttggtgg 36taaaa aaaaaaaaaa aaaaaaaaaa aggaag 396 582 396 DNA Homo sapiens 582 cttcagaaat tgtaatgatg aaagagtgcaagctctcact tccccttcct gtacagggca 6tgcag ctggaggcag agcagtcctc tctggggagc ctgaagcaaa catggatcaa actgtag gcaatgttgt cctgttggcc atcgtcaccc tcatcagcgt ggtccagaat aaggaaa gcccttcamt cagggaagaa cagaagggga gattttcttt gatggttgtt 24gtcag gcttaaacaa ttgtgtctgt gtgtgcgcat gcacaaacac ttttacctta 3tatttt cttcttttta tttgaatgta tagggttgtg tgtatttctg tgtaaatttg 36ttcct cctcttagtc tttcactttt gtggtg 396 583 396 DNA Homo sapiens 583 ttttctaaca tctgcagtgc aattgaagttaccagtcatc tgcagtctaa aaagaaagtg 6gggag gtgcgtagaa aaaatcatct tattattttt cctctatatt acttttttct tttctcc tgaagaaact tttttttttg gtgatacctt ctttttctct agcacgtata ttggaag catttttcrt atgcagtgta tacttcagaa agagagagag agagaggaaa 24cctgt tcagcgtttg catttccatt attcctgcta ttagttaaaa acaacaacaa 3aaaaaa caagcaggat acctagatct ggaaaaggga gaattgtgta gagctgtctt 36agttc tgagttaggg ctgcctcaga ccactt 396 584 396 DNA Homo sapiens 584 ttttggaagc atttttcata tgcagtgtatacttcagaaa gagagagaga gagaggaaaa 6ctgtt cagcgtttgc atttccatta ttcctgctat tagttaaaaa caacaacaac aaaaaac aagcaggata cctagatctg gaaaagggag aattgtgtag agctgtcttc aagttct gagttaggrc tgcctcagac cactttcata actatctcca gtggctttgt 24atatt tattaagata gagaaaaaaa gagtaattac taagggcagc tgctgtagct 3ggtgat tactgaacat tgacatgctg tcacgttttt ggaactttga gtatttaatc 36gggat attctatttt cccccatctt gagtgt 396 585 396 DNA Homo sapiens 585 ggaactttga gtatttaatc actttgggatattctatttt cccccatctt gagtgtggac 6ctggt gatgtagcct tctgggcaca gagcaagcct ccccctcagc ctctgcacca aggctca gcttcacaca ctccaagtat gttttctaca agaactacac tttgtggctt gacccaa acatttttrt actaaattac acacaacaaa gttgtagctc agagagggaa 24ggctt atttaggcca ccattttctt gagccattat gatttcacac agggctccct 3cctgta aattggcaag gattccatta ttcaacccgc atacatgtac agagaccctg 36gccca gatagtattc tgggtacagg cggata 396 586 396 DNA Homo sapiens 586 tgtggacaga tgctggtgat gtagccttctgggcacagag caagcctccc cctcagcctc 6cagaa aggctcagct tcacacactc caagtatgtt ttctacaaga actacacttt gctttct gacccaaaca tttttatact aaattacaca caacaaagtt gtagctcaga ggaacaa atggcttayt taggccacca ttttcttgag ccattatgat ttcacacagg 24cttgg ccctgtaaat tggcaaggat tccattattc aacccgcata catgtacaga 3ctgctc tggcccagat agtattctgg gtacaggcgg atagagcagg aaacaaaaca 36agtga tggacaggtc agcctgcagc aatgcc 396 587 396 DNA Homo sapiens 587 tttttatact aaattacaca caacaaagttgtagctcaga gagggaacaa atggcttatt 6cacca ttttcttgag ccattatgat ttcacacagg gctcccttgg ccctgtaaat caaggat tccattattc aacccgcata catgtacaga gaccctgctc tggcccagat attctgg gtacaggcrg atagagcagg aaacaaaaca gctacagtga tggacaggtc 24gcagc aatgcctgca gtctctgcaa aggtagctgt atgggtgggc aggtggctag 3tattca gctctggaag gatctcccct ctggcctctc ccctgacacc catcaataaa 36ggagc atcggtggac aggggacctt gtgccc 396 588 396 DNA Homo sapiens 588 ttttcttgag ccattatgat ttcacacagggctcccttgg ccctgtaaat tggcaaggat 6tattc aacccgcata catgtacaga gaccctgctc tggcccagat agtattctgg caggcgg atagagcagg aaacaaaaca gctacagtga tggacaggtc agcctgcagc gcctgca gtctctgcra aggtagctgt atgggtgggc aggtggctag cacttattca 24ggaag gatctcccct ctggcctctc ccctgacacc catcaataaa actgaggagc 3gtggac aggggacctt gtgccccctc cctgcctgtg cagttggggc tgaacccagc 36agttt gagctcactc tctccagctc cctctc 396 589 396 DNA Homo sapiens 589 gacaggtcag cctgcagcaa tgcctgcagtctctgcaaag gtagctgtat gggtgggcag 6tagca cttattcagc tctggaagga tctcccctct ggcctctccc ctgacaccca ataaaac tgaggagcat cggtggacag gggaccttgt gccccctccc tgcctgtgca ggggctg aacccagcya cgaagtttga gctcactctc tccagctccc tctcaattca 24gaact gtgggaagct tcagagctct ctgtttcaag gacaggttct cctcacctct 3atggag gtgcaccagg gaactggccc tgctctgccc agggctttct cctggacttt 36catgg tctagcaaac cctgttcaga ttgagg 396 59NA Homo sapiens 59tctcc agctccctct caattcagagctgaactgtg ggaagcttca gagctctctg 6aggac aggttctcct cacctctcct aatggaggtg caccagggaa ctggccctgc gcccagg gctttctcct ggactttgcc atcatggtct agcaaaccct gttcagattg tgagtgg tgagatttyg aattcttttt gacagatagg attaagtctt cttctgtggg 24tggga ggtagaggta agattaaaga tggccaaatg tctgagtcct gacagccaca 3ggagat ctagactttt tacagaccac agggcacagg ggcctcacta acagagttcc 36gtgat gagtgtgctg ggggcttcct ggttga 396 59NA Homo sapiens 59ttaag tcttcttctg tgggacaagtgggaggtaga ggtaagatta aagatggcca 6ctgag tcctgacagc cacaatatgg agatctagac tttttacaga ccacagggca gggcctc actaacagag ttcccggaag tgatgagtgt gctgggggct tcctggttga gacacta gaatggacsa gctgggagct aattttttgg gctggagtgt gatggcctgc 24actgc ctctgtccct ccattgtcac agctgcccct taggagccag ctgaggcaat 3ggtcag agtgactttg cacagttgtc ctgcctgtgt tcaggaaggg agtttctgtg 36tttga aaccacagaa gagcccctcg tatagc 396 592 396 DNA Homo sapiens 592 agttgtcctg cctgtgttca ggaagggagtttctgtggtc cctttgaaac cacagaagag 6cgtat agctctcaat ggagggggca aaacattcaa ataactcagg agataacaca atttgtt tttaactgtg agtttttagg caatcacaaa gatccagatg tatgtccaag ctctttg caattctawt taacctcaat gttgcaacca tagacctacc ttacagagtt 24aaata tgcaaaaacc ctgcctttct tcttcctcat accccaaaat gccattctga 3ttcctg ttagttaaaa aaagatttcc atggtgttac caggcactgt acacagtctg 36caaga caaggaggta cagttccaca tgcgcc 396 593 396 DNA Homo sapiens 593 agggggcaaa acattcaaat aactcaggagataacacaac tatttgtttt taactgtgag 6aggca atcacaaaga tccagatgta tgtccaagcc tctctttgca attctaatta tcaatgt tgcaaccata gacctacctt acagagttca aaaaaatatg caaaaaccct tttcttc ttcctcatwc cccaaaatgc cattctgaac atttcctgtt agttaaaaaa 24tccat ggtgttacca ggcactgtac acagtctgtg tcccaagaca aggaggtaca 3cacatg cgcccatgac tgggttgggc tctgcactct ctctatactt tgagagcctg 36ctgtg attgggcaga gctggcccac ctggtg 396 594 396 DNA Homo sapiens 594 tctgcactct ctctatactt tgagagcctgattttctgtg attgggcaga gctggcccac 6gcaat gtcctcctct gcctttcaaa catgttttag tcatcaagat cttcaaattt acccttt ccagcttgat ccagcagaat gcagatttgg aaaaacagaa cgagtttaaa catgatt ctaagaaayc tggaccagaa ctatcaaaac ttggtttccc agagaatata 24tgggc tcattggcca atactatgac attggctttt gagaaaagaa aggctttatt 3ggctgg ccagcaagga gacaggagtt gggctcaaat ctgtctcccc agtttggggc 36gcaag ttttaattac acagacgcat ttctta 396 595 396 DNA Homo sapiens 595 aaccctttcc agcttgatcc agcagaatgcagatttggaa aaacagaacg agtttaaaat 6attct aagaaacctg gaccagaact atcaaaactt ggtttcccag agaatatagc tgggctc attggccaat actatgacat tggcttttga gaaaagaaag gctttattgc gctggcc agcaaggara caggagttgg gctcaaatct gtctccccag tttggggctt 24aagtt ttaattacac agacgcattt cttatgagta gcaggcagag agcctccaac 3tctgcc taggtaccag cagcttagac atgatgcaaa cctgggaagc acatactgta 36agaaa gtgattggga agaaatgtga gctgag 396 596 396 DNA Homo sapiens 596 tacatgattc taagaaacct ggaccagaactatcaaaact tggtttccca gagaatatag 6gggct cattggccaa tactatgaca ttggcttttg agaaaagaaa ggctttattg ggctggc cagcaaggag acaggagttg ggctcaaatc tgtctcccca gtttggggct ggcaagt tttaattaya cagacgcatt tcttatgagt agcaggcaga gagcctccaa 24tctgc ctaggtacca gcagcttaga catgatgcaa acctgggaag cacatactgt 3ggagaa agtgattggg aagaaatgtg agctgagggg aggggctcag tgcccctgag 36cttag tgatggcaga ggaaggatgt cctccc 396 597 396 DNA Homo sapiens 597 tggggcttag ggcaagtttt aattacacagacgcatttct tatgagtagc aggcagagag 6aactt cttctgccta ggtaccagca gcttagacat gatgcaaacc tgggaagcac ctgtatt tggagaaagt gattgggaag aaatgtgagc tgaggggagg ggctcagtgc tgagcta cacttagtra tggcagagga aggatgtcct cccgcaggag gctgttccac 24ctctg gttgtagggg gagctggcag gcattagcag cggcctcttt cccccaagag 3agcctc ctccaagttt tggcgacatt atggccctgc aatcataagg gtttgtgagc 36gctaa ggagggaaat ggagctgctg ttacta 396 598 396 DNA Homo sapiens 598 cctcctgagt agctaggact acaagcatgtgccaccacgc ccagctaatt tttgtatttt 6aggac agggtttcac catgttggcc aggttggcct ccaactcctg acctcaagtc ctcctgc ctcgacctcc caaagtgctg ggattacagg catgaaacca gcctagaaat tactatt atttattcyt gttttacaga taagcaaagt gagtcatgga gaatttggtt 24tccca aggtcaggag tcgtgaagct gggattaaaa cctaatcatc tgactttaga 3agacac ttgctccatg catattgcct ccaattcatt cattcaagca ctccctgctc 36gttct ttcttatgtt gagctgaaat ctgcag 396 599 396 DNA Homo sapiens 599 tcatctgact ttagagagta gacacttgctccatgcatat tgcctccaat tcattcattc 6ctccc tgctcaagaa gttctttctt atgttgagct gaaatctgca gccctatgcg tacccag cagtcctggt gctgttccct aaaatcactt agactgtgcc tgctctttct tttacag tgtcagctrt aatatccccc tcttcggcct aacgtttctg aagtcccttg 24gggtc tcctctcctc ttcctgtgtt ctttctaaga acacctatgc agataggtgt 3tgtaca gggaagctgt tcctgagatc cgggcatcga ctctgttaga ataatctacg 36gttat ttttttgaga actatgtgtc attgct 396 6DNA Homo sapiens 6tgagct gaaatctgca gccctatgcgttttacccag cagtcctggt gctgttccct 6cactt agactgtgcc tgctctttct gtgtttacag tgtcagctgt aatatccccc tcggcct aacgtttctg aagtcccttg ccactgggtc tcctctcctc ttcctgtgtt tctaaga acacctatrc agataggtgt cttctgtaca gggaagctgt tcctgagatc 24atcga ctctgttaga ataatctacg tatgagttat ttttttgaga actatgtgtc 3ctgact catattaact ctgtggttaa ctaaaatctc aagatctctt tatgtttgtt 36actta tttaacttct ctggccctcc gtttcc 396 6DNA Homo sapiens 6tggtgc tgttccctaa aatcacttagactgtgcctg ctctttctgt gtttacagtg 6tgtaa tatccccctc ttcggcctaa cgtttctgaa gtcccttgcc actgggtctc tcctctt cctgtgttct ttctaagaac acctatgcag ataggtgtct tctgtacagg gctgttc ctgagatcyg ggcatcgact ctgttagaat aatctacgta
tgagttattt 24agaac tatgtgtcat tgctgactca tattaactct gtggttaact aaaatctcaa 3tcttta tgtttgttga gaaacttatt taacttctct ggccctccgt ttccttcact 36gtgga gtgattgata acctccacct gtggtt 396 6DNA Homo sapiens 6tatgcagataggtgtc ttctgtacag ggaagctgtt cctgagatcc gggcatcgac 6tagaa taatctacgt atgagttatt tttttgagaa ctatgtgtca ttgctgactc ttaactc tgtggttaac taaaatctca agatctcttt atgtttgttg agaaacttat acttctc tggccctcmg tttccttcac tgagcagtgg agtgattgataacctccacc 24ttgct gaaggtcttg cacaagatga tatagttaaa gtagctagca gtgcccacgt 3cggatg cctcacaacg gtttgcagcc atctctctat ctgtgtcttt gtctctctct 36tggtt ttggcttact gttagcagct agccga 396 6DNA Homo sapiens 6tggtta actaaaatctcaagatctct ttatgtttgt tgagaaactt atttaacttc 6ccctc cgtttccttc actgagcagt ggagtgattg ataacctcca cctgtggttg aaggtct tgcacaagat gatatagtta aagtagctag cagtgcccac gtacggcgga ctcacaa cggtttgcmg ccatctctct atctgtgtct ttgtctctct ctcacactgg24gctta ctgttagcag ctagccgaga taagtgtgtt tatggtcttt gcatgtattg 3tgtagc atactggagg attacaagag gttggggagt gagggggcgg tgaggagtag 36ggcag ccaactcttc caagtttagc ttagaa 396 6DNA Homo sapiens 6taacct ccacctgtgg ttgctgaaggtcttgcacaa gatgatatag ttaaagtagc 6gtgcc cacgtacggc ggatgcctca caacggtttg cagccatctc tctatctgtg ttgtctc tctctcacac tggttttggc ttactgttag cagctagccg agataagtgt tatggtc tttgcatgya ttgtttctgt agcatactgg aggattacaa gaggttgggg 24ggggg cggtgaggag tagacaaagg cagccaactc ttccaagttt agcttagaag 3gagcgg taaaccctag ttgaatgttg gactgaagca ggtttgtttt tgttttgttt 36atagg gaagatctgt gcgtgtttcc aggata 396 6DNA Homo sapiens 6gaagtc agtggcatgg acagggtcaagatcacagtt agaggatgca gccttagaga 6aaggg gctcggttct ctgagcaagg agggaaagaa gagaggcaga tgcagagaag ggcacat cgtgctgctg gttgtagaaa taacctctga cttttaataa agtcatccct tatccct gggggattrg ttctatgacc tccctcggat gccaaaattc gtggatgctc 24cctga tataaaatgg catagtattt gcatttaacc tacacacatc ctccatatcc 3tttttt tttttttttt tttttttttt tttttgtgag atggagtctt gctctgtcgc 36ctgga gtacagtggc tcgatcttgg ctcact 396 6DNA Homo sapiens 6cctgat agaatgtaaa tgctatgtaaacagttgtta tactgtattg ttaaaagaca 6aagaa aaaaaatctg tacatgttca gtccagacaa atggttttct gttttttttt tttttta atatttttgg tcagtggttg gttgactcca ggaatgcaga acccgcagat gaaggtt gattatgcrt tcagaggcag ggaataccat cttgggttcc agaaagaaaa 24agcat tttctgtcat actctggtaa aaacagatct tttgaatgga caggtgtatt 3cctgtg gagctggctg ggcctggcgg ctcacgcctg taatcccagc actttgggag 36ggcag gtggatcacg aggtcaggag ttcgag 396 6DNA Homo sapiens 6ccgcag agtttgaagt cccggctgcacctctcccca gcagcaggtt gactctggaa 6cagcg ttcttaccta cagagtggga acagtactac ccattgcaca gagtgggtgc gctctgt gacggaatac atggcaagtg cccaccacat tgcctgggat gaggtgggcc cctttac gtaagagarc cctacagata cactcaaagt gggcacattc ctacagaagg 24tattt gtgtagaaaa gaaaaacatg aaaggctttt attcctatac acaataaagc 3ctttaa tgtctttttg aggaggataa tatgaaattg atgaaaagga accctgtggt 36ccctg acaatcacat gtatcccttt tttcac 396 6DNA Homo sapiens misc_feature (227)..(326) n = A,T,C or G 6gataca ctcaaagtgg gcacattcct acagaaggag tgttatttgt gtagaaaaga 6atgaa aggcttttat tcctatacac aataaagcac ccctttaatg tctttttgag gataata tgaaattgat gaaaaggaac cctgtggttg gatccctgac aatcacatgt ccttttt tcactcttra aaaaggagta aaggaataaaatagaannnn nnnnnnnnnn 24nnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn nnnnnnnnnn 3nnnnnn nnnnnnnnnn nnnnnnatgt ttcagtcact gtataataac tagccagatt 36ttgtt gttgttttgt ttttgttttt gttttt 396 6DNA Homo sapiens 6tctgaaccacagacag ttctttaccc tgaacctttg catattttgt tctcttagct 6cggcc cctctccctc cgtctgcttg gctaatttct acttgttctt cagattttat agatgtc attccctcaa ggaatccttc tgtgactcaa catggaatta agttgcctcc gaccctg aaagcaccrt gtactcaatc tcatcttggc atgactcactttgctgtgtg 24tctgc tttccttgtt tgtctattcc tttagactgt aagatcctag aaagtggggg 3gccttg ctcatgactg tgtttctaac accaaacaca gtgttcagta gagagcagct 36gtacg tttctgctaa atgacagttg atggag 396 6DNA Homo sapiens 6cttctg tgactcaacatggaattaag ttgcctcctt tgaccctgaa agcaccatgt 6atctc atcttggcat gactcacttt gctgtgtgga atgtctgctt tccttgtttg attcctt tagactgtaa gatcctagaa agtgggggcc gtgccttgct catgactgtg ctaacac caaacacart gttcagtaga gagcagctgc tgagtacgtt tctgctaaat24ttgat ggaggacatt tagggttgct tggaggtcaa gtcaaggagg catttaacat 3gtaaaa caaggaagta acaggctcct gaacatgccc acaatgaacc agatgcaaac 36ccctt ggcaggattc tttgcccata aagtgg 396 6DNA Homo sapiens 6caccat gtactcaatc tcatcttggcatgactcact ttgctgtgtg gaatgtctgc 6ttgtt tgtctattcc tttagactgt aagatcctag aaagtggggg ccgtgccttg atgactg tgtttctaac accaaacaca gtgttcagta gagagcagct gctgagtacg ctgctaa atgacagtkg atggaggaca tttagggttg cttggaggtc aagtcaagga 24ttaac attctagtaa aacaaggaag taacaggctc ctgaacatgc ccacaatgaa 3atgcaa accttttccc ttggcaggat tctttgccca taaagtggag cacgaaagca 36cagaa tgggaggagc ttccagagga ccggaa 396 6DNA Homo sapiens 6gctaaa tgacagttga tggaggacatttagggttgc ttggaggtca agtcaaggag 6taaca ttctagtaaa acaaggaagt aacaggctcc tgaacatgcc cacaatgaac atgcaaa ccttttccct tggcaggatt ctttgcccat aaagtggagc acgaaagcag ccagaat gggaggagyt tccagaggac cggaacactt gcctttgagc gggtctacac 24agtga gtcctaaccc tgatgttgct aataagtggg ggcatgggca ggggggcctc 3taggag tgatgaccac ccttaatacc acatgtctgt ctgagccaag tttctgagcg 36gaggt gaggaaggtt ggacttcacc agagag 396 6DNA Homo sapiens 6tttaac attctagtaa aacaaggaagtaacaggctc ctgaacatgc ccacaatgaa 6tgcaa accttttccc ttggcaggat tctttgccca taaagtggag cacgaaagca cccagaa tgggaggagc ttccagagga ccggaacact tgcctttgag cgggtctaca ccaagtg agtcctaamc ctgatgttgc taataagtgg gggcatgggc aggggggcct 24tagga gtgatgacca cccttaatac cacatgtctg tctgagccaa gtttctgagc 3gggagg tgaggaaggt tggacttcac cagagaggct ttgtggacac cctttatcat 36tgagt gctagtgtca aaacaaaggg agtggg 396 6DNA Homo sapiens 6ctgaac atgcccacaa tgaaccagatgcaaaccttt tcccttggca ggattctttg 6aaagt ggagcacgaa agcaggaccc agaatgggag gagcttccag aggaccggaa ttgcctt tgagcgggtc tacactgcca agtgagtcct aaccctgatg ttgctaataa ggggcat gggcagggrg gcctccttct aggagtgatg accaccctta ataccacatg 24ctgag ccaagtttct gagcgccagg gaggtgagga aggttggact tcaccagaga 3ttgtgg acacccttta tcatcttagt gagtgctagt gtcaaaacaa agggagtggg 36ggggc acattggtgg agggaggtgt gatctc 396 6DNA Homo sapiens 6ccataa agtggagcac gaaagcaggacccagaatgg gaggagcttc cagaggaccg 6cttgc ctttgagcgg gtctacactg ccaagtgagt cctaaccctg atgttgctaa gtggggg catgggcagg ggggcctcct tctaggagtg atgaccaccc ttaataccac tctgtct gagccaagyt tctgagcgcc agggaggtga ggaaggttgg acttcaccag 24ctttg tggacaccct ttatcatctt agtgagtgct agtgtcaaaa caaagggagt 3atatgg ggcacattgg tggagggagg tgtgatctct gcagcttcag aaagatctga 36tcatt tggttagaga agttgaccta tttcct 396 6DNA Homo sapiens 6aaaggg agtggggata tggggcacattggtggaggg aggtgtgatc tctgcagctt 6agatc tgaaagagtc atttggttag agaagttgac ctatttcctg tggggttaga gggttgc tactgtgaac accagccatg actcaccagt caccttcaga agccacaggc acatgct gacgacagyc ttcaactcac ccaccccttg ctcccctgcg ggtggaagtc 24gtgac accactgcat tttctaacac gggggctcct tgagcaacta gaacaagaac 3agaatg gggacattag caggtgcttt ccccctctct cattcttttc tttgaataaa 36tgttt gaaaacacct gagcggctcc taaaga 396 6DNA Homo sapiens 6tctctt ctttatgcag agtgtatttcaaggctcagc cagtggcagg catgctgggg 6ggact acggactagg ggcctgtcac agaggaaggc ctcatgctag agagctaagg gagctgg ccttcagttc catcccagga gcaactttga tgttcccaga gatccttcca ggggagt catggtcamc caagaaaaat gtattcagaa tgccaagaat ggtgcaaact 24caaag attcacactg cagggttgga gtccctgggc ttgctgctgg caccatggga 3gggtcc ccttcagggg taccgttggt ttcctgtgaa ttaaactggc ttcaagggat 36ctgaa caggcctata tcacactcac tgatat 396 6DNA Homo sapiens 6ctcatc taggtatttt taattgtttcagtgaggtgt aggcatgagg ggattggagg 6tctcc tccattgcag tttttcattg gctgctttgc tccctcagct ccgaaatcgc gccactc tcgaacgcat tagtacggta gtcacaggtt gattgcctgg ccccttgccc gtgggca ttttccctyt cagacagccc ctgagtactc acagtgctgc tacagtgggc 24agatc tccctctttc tccatgctcc cacgtgctct gggctccact cccttctccc 3acttct gtccagggct attccagcag tctgacctca aggaaatcct ttgctaaact 36tagag aggtttctat tttaacattt aggtct 396 6DNA Homo sapiens 6aggtat ttttaattgt ttcagtgaggtgtaggcatg aggggattgg agggggcatc 6cattg cagtttttca ttggctgctt tgctccctca gctccgaaat cgctgggcca tcgaacg cattagtacg gtagtcacag gttgattgcc tggccccttg ccctctgtgg ttttccc tttcagacwg cccctgagta ctcacagtgc tgctacagtg ggccacctag 24cctct ttctccatgc tcccacgtgc tctgggctcc actcccttct cccaagcact 3tccagg gctattccag cagtctgacc tcaaggaaat cctttgctaa actgattata 36gtttc tattttaaca tttaggtctt ccatgt 396 62NA Homo sapiens 62taggc atgaggggat tggagggggcatctcctcca ttgcagtttt tcattggctg 6ctccc tcagctccga aatcgctggg ccactctcga acgcattagt acggtagtca gttgatt gcctggcccc ttgccctctg tgggcatttt ccctttcaga cagcccctga ctcacag tgctgctaya gtgggccacc tagatctccc tctttctcca tgctcccacg 24tgggc tccactccct tctcccaagc acttctgtcc agggctattc cagcagtctg 3caagga aatcctttgc taaactgatt atagagaggt ttctatttta acatttaggt 36atgta ttaattctca gaatcaattt aagatg 396 62NA Homo sapiens 62cagac agcccctgag tactcacagtgctgctacag tgggccacct agatctccct 6tccat gctcccacgt gctctgggct ccactccctt ctcccaagca cttctgtcca ctattcc agcagtctga cctcaaggaa atcctttgct aaactgatta tagagaggtt attttaa catttaggyc ttccatgtat taattctcag aatcaattta agatgtttaa 24tgatt taagacattt taaaaccatt tggaggagag tacagaaatt atgtcacttg 3cagcct ctttgcacca tctgcagaga aagatactag agtcccgcct tggacacatc 36gcaag aggtgcaaag aaggtgtctt tgatga 396 622 396 DNA Homo sapiens 622 ttctcagaat caatttaaga tgtttaaaggtgtgatttaa gacattttaa aaccatttgg 6agtac agaaattatg tcacttgctg tcagcctctt tgcaccatct gcagagaaag ctagagt cccgccttgg acacatccac atgcaagagg tgcaaagaag gtgtctttga ggcaagg tcaaaactyc tccccagacg aaatccaaag aaagcattcc tactatgcta 24gtttg gaaagaaaaa cttctgccag gtgactgcat tctcactggt cacattgtgt 3atggac tcctcagctc aaccaatttg gagaagttat ggtgcaattt caccatatct 36gaagt taagtttcca atttgctggc aatgaa 396 623 396 DNA Homo sapiens 623 aagaaggtgt ctttgatgag gcaaggtcaaaacttctccc cagacgaaat ccaaagaaag 6ctact atgctatatc agtttggaaa gaaaaacttc tgccaggtga ctgcattctc ggtcaca ttgtgttcct atggactcct cagctcaacc aatttggaga agttatggtg tttcacc atatctggyt agaagttaag tttccaattt gctggcaatg aagaagaaat 24aggcc aggctgtgta gtttctgcca cgtgcccccg ggagtgaaca gctctgtttg 3aagcca tggtgcttag acctgggctc gctagttgcc agcctccaaa ttgcagaagt 36ttggt tggtggctat gctgtgtcac ttggga 396 624 396 DNA Homo sapiens 624 gcaacatatc tgtgtgcctg tctgggttgtaaaaagggtc aaagatcaat gcagcaggca 6atgct ggcaaaagcc agaggcagct ggtctgtttg cctgtgccag gaaaccactg atggggt tgtgtgttat tctaggagaa agtcgtccca gcagcagctt ctccaggggc caagagc actgaaaarg gttgcaagat gacccatgag gctgcaggaa gaaaagaaca 24ttaat cttgctatct gaaaagtaag acatgaagct ttcctcattt ttaatataca 3gacagt agtatgtgta tatagtttat atgcaaatat acttgttata aggttgcatg 36aattt ttggttcatg gggtgtggga tcataa 396 625 396 DNA Homo sapiens 625 cagctacatg ctggcaaaag ccagaggcagctggtctgtt tgcctgtgcc aggaaaccac 6atggg gttgtgtgtt attctaggag aaagtcgtcc cagcagcagc ttctccaggg tccaaga gcactgaaaa gggttgcaag atgacccatg aggctgcagg aagaaaagaa gcattta atcttgctrt ctgaaaagta agacatgaag ctttcctcat ttttaatata 24ggaca gtagtatgtg tatatagttt atatgcaaat atacttgtta taaggttgca 3caaaat ttttggttca tggggtgtgg gatcataaat gtttagggac catggctatc 36aaaac agcatgaagg ataaatgata ctggtg 396 626 396 DNA Homo sapiens 626 ctatctgaaa agtaagacat gaagctttcctcatttttaa tatacacatg gacagtagta 6atata gtttatatgc aaatatactt gttataaggt tgcatgctca aaatttttgg atggggt gtgggatcat aaatgtttag ggaccatggc tatcaaggaa aaacagcatg gataaat gatactggyg gattaaaaag acagatgcat gtatttttag cataaaacac 24ctgac tgatacagat agctcaagat tctggggcag ctgctgaaca gatacactag 3tgtggc tcatcggctc agacttggcc ttaattaatg ggctgtccct ccacccatct 36gaggg cagagctgag ccagggtttg agagct 396 627 396 DNA Homo sapiens 627 agtttatatg caaatatact tgttataaggttgcatgctc aaaatttttg gttcatgggg 6gatca taaatgttta gggaccatgg ctatcaagga aaaacagcat gaaggataaa tactggt ggattaaaaa gacagatgca tgtattttta gcataaaaca caactgctga atacaga tagctcaasa ttctggggca gctgctgaac agatacacta gccagtgtgg 24cggct cagacttggc cttaattaat gggctgtccc tccacccatc tcccatgagg 3agctga gccagggttt gagagctaaa aggaattgga cctggactct gttcacgtgt 36ttaat tctaattaat tcattctttt gaaaga 396 628 394 DNA Homo sapiens 628 gtatttttag cataaaacac aactgctgactgatacagat agctcaagat tctggggcag 6gaaca gatacactag ccagtgtggc tcatcggctc agacttggcc ttaattaatg tgtccct ccacccatct cccatgaggg cagagctgag ccagggtttg agagctaaaa attggac ctggactcdg ttcacgtgta tattttaatt ctaattaatt cattcttttg 24cagag tcacactctg ttgcctaggc tggagtgcag tggcacgatc ttggctcact 3cctcgg cctcccaggt tcaagttatt ctcctgcttc agcctcctga gtagctggga 36ggcac atgcccccat gcctgactaa tttt 394 629 396 DNA Homo sapiens 629 gctaaaagga attggacctg gactctgttc acgtgtatattttaattcta attaattcat 6tgaaa gacagagtca cactctgttg cctaggctgg agtgcagtgg cacgatcttg cactgca acctcggcct cccaggttca agttattctc ctgcttcagc ctcctgagta gggatta taggcacayg cccccatgcc tgactaattt ttgtattttt agtagagacg 24tcaccatgtcaggct ggtcttgaac tcctgacctc aggttatcca cccgccttgg 3tcaaag tgttggaatt acaggtgtga gccaccgtgc ctggcctgtt cacatgtata 36cagtt taatgtccta ttcccagcca atgagc 396 63NA Homo sapiens 63ttatc cacccgcctt ggcccctcaa agtgttggaattacaggtgt gagccaccgt 6gcctg ttcacatgta taaaacacag tttaatgtcc tattcccagc caatgagcat tagagca gccttggtca aagtttggtt tttggagaaa aatccttgtt agctgaccta ttcctct ttgtgagtkt aagtaagcac aggttgcaga gaggagaagg gtctctggag 24taattttctaaatgg attacaagtt catggacttt taacaggtgt tacaggggat 3agttct ttatagacag acttttgagg acgtttaagg gtattctgat tcttggtttt 36agggg aatgtattat ttaactacag acaccc 396 63NA Homo sapiens 63ccaga ataataataa tttgtcaata ggaaagacatttccactggg ggttaagaag 6cattg gaacaatgat agccaccact tattgaatgc ttactgtgag ccaggtggca caccttg tttcattctc acaacagtct agggaagtaa ttactaatgt ctccatccac ttgtaga tgagcaaayt gaggctcatt gaggctagga aatgcaccca cactcacata 24taagaggcagccatg gcattgggcc cagaccatgt gaacttcaaa gactacacga 3ccactg ggcagctgtc atggctaaag ccacttgaat tcagcccagc agcaaccccc 36aggag gggcacataa gcttgcagct ttgggt 396 632 396 DNA Homo sapiens 632 ataataataa tttgtcaata ggaaagacat ttccactgggggttaagaag gaagacattg 6atgat agccaccact tattgaatgc ttactgtgag ccaggtggca cttcaccttg cattctc acaacagtct agggaagtaa ttactaatgt ctccatccac ctcttgtaga gcaaact gaggctcayt gaggctagga aatgcaccca cactcacata gcccataaga 24ccatggcattgggcc cagaccatgt gaacttcaaa gactacacga gcagccactg 3gctgtc atggctaaag ccacttgaat tcagcccagc agcaaccccc tctccaggag 36cataa gcttgcagct ttgggtagaa gctgca 396 633 396 DNA Homo sapiens 633 gcacttgaag tcctggatgg cgagagggac tggcttgagccagagccagg aacaaggctc 6atatt ctggaaatcc acaggaggaa cccattttct tacagctggg agaatttcat actccag gctgaccatg ttttattagg aacgaaggtg acttgaacta atagtcagga gttgaat acggacccra tgtcaaatca ctaggcagtt cacatttcta atgagcaaat 24agacaattaagaatt tttttccttt tgcataaccc agacaaaatc gctacttaaa 3aaccaa agacccgaaa catgagaaag agaaggaagc aggggaaatc tttggtacta 36ttttt aaacaataag agcaccagat atttta 396 634 396 DNA Homo sapiens 634 atgagcaaat cccttagaca attaagaatt tttttccttttgcataaccc agacaaaatc 6ttaaa aacaaaccaa agacccgaaa catgagaaag agaaggaagc aggggaaatc ggtacta ataagttttt aaacaataag agcaccagat attttacccc atcagacaca tgttatt cgaataacsa aaaaaggaat tttttctcta agtttcttga actggaaaat 24atattttctcagtcc tgaggctgca attttgtgcc tctagtaaca tataagaata 3tgatgc cagtgcccag tagctgctgc aattgttact tggggacctg tttattcact 36cttca ccccagtgat aaatttgtag gggcct
396 635 396 DNA Homo sapiens 635 ccgtgtccat tagatcagtg gaaattctgg gattcagagc actttgcaag gtcagcaggg 6ctctt tctgtcctgt tcctggtttt tggttgtgcc tggattccag ggtaggtttc tctgtta ccttcataga cttctccaga aaaggatctt ttgaccatca gaggaccacg attccat tggtgaggyg cagataacct gatctctctg ggttctctgc agggcacaga 24ggctg gccattccca agttctcagt ggtaccactg aggcatgaga ccctaatggt 3atgagc agtttgaaaa ttgcatcttt gtttttacct atataatcac atgaaacccg 36ctcaa acgtcagcag gcatcagcat cacatg 396636 396 DNA Homo sapiens 636 tcagtggtac cactgaggca tgagacccta atggtttgca tgagcagttt gaaaattgca 6gtttt tacctatata atcacatgaa acccgtggtt ctcaaacgtc agcaggcatc atcacat ggagggcttg ttaaaacaga tttctgggcc ccaacacaga gttttaaatt aaggcctgaggtgggyg tgaacatttg catttctaac atgttctcga tgctgctgcc 24tggtc ccgagagcat gcctggagaa ctgccacctt cgaccatgga ctgtgagaat 3atggac ctcagaatta taatcagtct ctcagtttta cagataagga aactaaatcc 36gattg ttttgccaat ggtgaacagc tggtta 396 637 396 DNAHomo sapiens 637 atggtttgca tgagcagttt gaaaattgca tctttgtttt tacctatata atcacatgaa 6tggtt ctcaaacgtc agcaggcatc agcatcacat ggagggcttg ttaaaacaga ctgggcc ccaacacaga gttttaaatt ctgaaggcct gaggtgggtg tgaacatttg ttctaac atgttctcratgctgctgcc gcctctggtc ccgagagcat gcctggagaa 24acctt cgaccatgga ctgtgagaat tcacatggac ctcagaatta taatcagtct 3gtttta cagataagga aactaaatcc agagagattg ttttgccaat ggtgaacagc 36aaagt caggatggag actttaatcc tagtca 396 638 396 DNA Homosapiens 638 gagcagtttg aaaattgcat ctttgttttt acctatataa tcacatgaaa cccgtggttc 6cgtca gcaggcatca gcatcacatg gagggcttgt taaaacagat ttctgggccc cacagag ttttaaattc tgaaggcctg aggtgggtgt gaacatttgc atttctaaca tctcgat gctgctgcyg cctctggtcccgagagcatg cctggagaac tgccaccttc 24tggac tgtgagaatt cacatggacc tcagaattat aatcagtctc tcagttttac 3aaggaa actaaatcca gagagattgt tttgccaatg gtgaacagct ggttaaagtc 36ggaga ctttaatcct agtcaagtga cctttc 396 639 396 DNA Homo sapiens 639agtttgaaaa ttgcatcttt gtttttacct atataatcac atgaaacccg tggttctcaa 6agcag gcatcagcat cacatggagg gcttgttaaa acagatttct gggccccaac gagtttt aaattctgaa ggcctgaggt gggtgtgaac atttgcattt ctaacatgtt gatgctg ctgccgcckc tggtcccgag agcatgcctggagaactgcc accttcgacc 24ctgtg agaattcaca tggacctcag aattataatc agtctctcag ttttacagat 3aaacta aatccagaga gattgttttg ccaatggtga acagctggtt aaagtcagga 36acttt aatcctagtc aagtgacctt tcctct 396 64NA Homo sapiens 64ttgtttttacctata taatcacatg aaacccgtgg ttctcaaacg tcagcaggca 6atcac atggagggct tgttaaaaca gatttctggg ccccaacaca gagttttaaa tgaaggc ctgaggtggg tgtgaacatt tgcatttcta acatgttctc gatgctgctg cctctgg tcccgagakc atgcctggag aactgccacc ttcgaccatggactgtgaga 24catgg acctcagaat tataatcagt ctctcagttt tacagataag gaaactaaat 3agagat tgttttgcca atggtgaaca gctggttaaa gtcaggatgg agactttaat 36tcaag tgacctttcc tctgtattta tttccc 396 64NA Homo sapiens 64tgaca tcctgaaccatagtaaaagg gtgttttttg tttttttgag acagagtctt 6gttgc ctgggctgga gtgcagtggt gtgatcttgg ctcgctgcaa cctccgcctc ggttcaa gtgattctcc tgcctcagcc tcctgagtag ctgggattac aggtgcttgc cacacct ggctatttkt tgtgttttta gtagagacag ggtttcacca tgttggccag24tcttg aactcctgac cttgtgatct gcctgcctca gcctcccaaa ttgctgggat 3aggcgt gttgttttaa gccactcagt ttgtggccac ttgttacagc agcaagagga 36ataca gttatcatgt gaactcacag gaatat 396 642 396 DNA Homo sapiens 642 gatctgcctg cctcagcctc ccaaattgctgggattacaa ggcgtgttgt tttaagccac 6ttgtg gccacttgtt acagcagcaa gaggaaactc atacagttat catgtgaact aggaata tggtgagtta aaaagagagg aagggtgcaa aacatccacg gtagagtgag tctccag ggagtgagra ctgtgcccag catacagtga tcaccctctt agtaagctaa 24tgagc accagctttt ttgagttgac tttgttgtct ttaacatttg aagatcaccc 3ttgctc agcctggctt gcagacctgg gctgatttgt ggatctgata gaaaagtttc 36ttggg ctcttctccc cgaccacccc catgcc 396 643 396 DNA Homo sapiens 643 tgcctcagcc tcccaaattg ctgggattacaaggcgtgtt gttttaagcc actcagtttg 6acttg ttacagcagc aagaggaaac tcatacagtt atcatgtgaa ctcacaggaa ggtgagt taaaaagaga ggaagggtgc aaaacatcca cggtagagtg agaactctcc gagtgag gactgtgcmc agcatacagt gatcaccctc ttagtaagct aagtttctga 24agctt ttttgagttg actttgttgt ctttaacatt tgaagatcac ccttctttgc 3cctggc ttgcagacct gggctgattt gtggatctga tagaaaagtt tccttagttg 36ttctc cccgaccacc cccatgccag tgtggc 396 644 396 DNA Homo sapiens 644 gctactttgc agccaaggta actcagacttccctttgttc attctccttc tataaagtgc 6aagga ggttcaaagg gcaggctttt tgttgaaagg actttgcctg acctctggct atctgtg aagccctgga gaggtgagag ccctcgggag gccgtgtttc aggcatgctc acccgtg cagagcgcrt gtgataatgc attgctaatg cttgctccct ggtggctggc 24gctgc tgtgctgaca agggtggttt aaggctaaat gtgactcaga atccttaagc 3ttagtt cagatacaag ggcattataa atgagagtgc ctgagggatc tattttggga 36gtcac ttggctcttc tgctaataag cttcca 396 645 396 DNA Homo sapiens 645 acagttatca gcagcccaca ggcttgacttgagcaagttg gaaagacaaa tcaacttcca 6gattt aacattgagt ggaaatcagt catacttttg gtcccctttc ggggccacgc gcactgt gcctggtggc agatcggcat gaactggcca gcttctgtgg ccctggaggg aggcaga aaggccacrc tcagtcccat gatgaactgt ttaagactta ttgttgtctc 24tctgt aaagtagata gagtggattt tatgtccctt attacctttc aggatacttt 3caggga gataaagtaa cttgggtaca gctactcagc tggtgaagaa cacaggcaga 36tgcct gggtcttttg acttaaaatt ctggat 396 646 396 DNA Homo sapiens 646 ctgtgcctgg tggcagatcg gcatgaactggccagcttct gtggccctgg agggcacagg 6aggcc acactcagtc ccatgatgaa ctgtttaaga cttattgttg tctccccgct taaagta gatagagtgg attttatgtc ccttattacc tttcaggata ctttgactca agataaa gtaacttgsg tacagctact cagctggtga agaacacagg cagaatgagt 24ggtct tttgacttaa aattctggat ttttcacaaa gatcctctta ctttattcat 3ataata aatatatatt gaagagctac tctgtgccaa gccctgtgcc tagatataca 36aaata aagagtagct tctagaggtc acctgg 396 647 396 DNA Homo sapiens 647 aagttcagtg atagagagca gaggtgaggcggcagcagaa accacttaag ggacaccacg 6ctcct tctgtgctga gaaggctgtc agtaagctca ccatttattt cctattttct ctgagtt aaataggaaa catgtctcgc attacttgaa aaatcaagtc aaactatgct actagga gttatggtyc tttttatgtc ttagatgatg cttgatctag atgaatgcgg 24ctgta gctagataaa tacaatggga gtttgaaggt gtttcgtagc cctggaaata 3tttcct gtcaaaacaa gctttgtcat tgccagcaga caaaagcatc agtaaccttg 36taatc gtcatttctt aggaataaag tagact 396 648 396 DNA Homo sapiens 648 gtatttcctg tcaaaacaag ctttgtcattgccagcagac aaaagcatca gtaaccttgg 6aatcg tcatttctta ggaataaagt agactgtaga atttttttta gcagaaagga ccaaaga taattctagt gcaaatccct cactttatag agcagaagct caagtcccag aacaagt ggcttgaayg aacatcagaa ttttaggggc tggatttgta ccctcctggt 24cagcc cacttccctg caggaggcac tcaccttcct tgcacagggg tatgagtgtg 3ttttcc acccataatc tctgttagct catgttcaat tgggttccca ttgaaagaaa 36accag taagttggag cagaatcatt cagatg 396 649 396 DNA Homo sapiens 649 agctttgtca ttgccagcag acaaaagcatcagtaacctt ggttgataat cgtcatttct 6ataaa gtagactgta gaattttttt tagcagaaag gaaacccaaa gataattcta caaatcc ctcactttat agagcagaag ctcaagtccc agaggaacaa gtggcttgaa acatcag aattttagkg gctggatttg taccctcctg gtgccagcag cccacttccc 24gaggc actcaccttc cttgcacagg ggtatgagtg tggccatttt ccacccataa 3tgttag ctcatgttca attgggttcc cattgaaaga aaaatggacc agtaagttgg 36aatca ttcagatggt ataacataag gaaaaa 396 65NA Homo sapiens 65aaatt gcttttatat ctgtagctctagataacact agttccagct tagttaactc 6tccaa gccttcagga cttcatagag ttattggggt gctgctcttg gcagtttccc aagctag aatgcagagg gaatctcctt cccaaaaagc tagaatgcag agggaatctc cccaaaa ggctagaayg cagagggaat ctccttccca aaaagctaga atgcagaggg 24ccttc ccaaaaggct agaacgcaga gggaatctcc ttcccaaaag gctagaacgc 3ggaatc tccttcccaa aaggctagaa tgcagaggga atgtccttct cttctaaatg 36tgtta gttcaagaaa ggttaaacat tgtgct 396 65NA Homo sapiens 65gtttg ctggactgat gtacttgtttgtgaggcaaa agtactttgt cggttaccta 6gagaa cgcagaggta ggtaactggg actactaaag aactgtggag cgattcctga ttgagca ggaagagtga caattcaaaa cagtatttga ctagattcac ggctccgtag ccccttg ggtgggagsg ggaaggctga ctaggacctc tgattcttct ttccctgagc 24aggct ctgaaaatac agctgggggg acttgcccag ttttcttatt aagcaattcc 3catggt gctggctttc aaagggtgct tcagtgctgt ttgctgcacg tgccttgcag 36caccc tgcactcccg ccctgcagag tctggc 396 652 396 DNA Homo sapiens 652 gaggcaaaag tactttgtcg gttacctaggagagagaacg cagaggtagg taactgggac 6aagaa ctgtggagcg attcctgatt tttgagcagg aagagtgaca attcaaaaca tttgact agattcacgg ctccgtagca tccccttggg tgggaggggg aaggctgact acctctg attcttctyt ccctgagctt tgaaggctct gaaaatacag ctggggggac 24cagtt ttcttattaa gcaattcctc cgcatggtgc tggctttcaa agggtgcttc 3ctgttt gctgcacgtg ccttgcagcc ccacaccctg cactcccgcc ctgcagagtc 36ctgga atgacatttt aggtctgggt tcccag 396 653 396 DNA Homo sapiens 653 tatctttcag ggaccagaag aaagaatgttgggaaaataa gatgcagtaa gatgcagaca 6gcagg gtgcagcggc tcacgcctat aatcccagca ctttgggagg ctgaggtggg atcacct gaggtcagga gtttgagacc agcctggcca acatggtgaa accccgtctc taaaaaa tatacaaarc attagccagg catggtggtg ggcgcctgta atcccagcta 24taggc tgaggctgga gaatcgcttg aacccaggag gcagaggttg cagtgagccg 3tgcgcc actgcactcc agcctgggca acaaaagcaa aactccatct caaaaaaaaa 36aaaaa aaaaaaaaga tgcagacacg agactg 396 654 396 DNA Homo sapiens 654 tgggcgcctg taatcccagc tactccataggctgaggctg gagaatcgct tgaacccagg 6gaggt tgcagtgagc cgagattgcg ccactgcact ccagcctggg caacaaaagc actccat ctcaaaaaaa aaaaaaaaaa aaaaaaaaaa gatgcagaca cgagactgtg ctgacta gcatcaccwt tgcattgttt atagatgttg ccagacagaa agccccaaag 24cagta ccttcctgac atctggacta ggaaatctag attttagtaa aatacatgct 3cttaca gaagaaatgt cggcgttaga gtatgccgtc agttccttag agattgcaat 36atgca ctagtatggt ttcaggtgcc aggaac 396 655 396 DNA Homo sapiens 655 actccatctc aaaaaaaaaa aaaaaaaaaaaaaaaaagat gcagacacga gactgtgaaa 6tagca tcaccattgc attgtttata gatgttgcca gacagaaagc cccaaagcag agtacct tcctgacatc tggactagga aatctagatt ttagtaaaat acatgctaat tacagaa gaaatgtcrg cgttagagta tgccgtcagt tccttagaga ttgcaattcc 24cacta gtatggtttc aggtgccagg aacacgttct gtgaggctgc tgccccaggt 3acccca gccttccaca ccattttcct tccttgtgtt cacagccgct ctgtctttta 36gcacc cctctctagt ggctaatggg ctctat 396 656 396 DNA Homo sapiens 656 aaaaaaaaaa aaaaaaaaaa aagatgcagacacgagactg tgaaactgac tagcatcacc 6attgt ttatagatgt tgccagacag aaagccccaa agcagcacag taccttcctg tctggac taggaaatct agattttagt aaaatacatg ctaatactta cagaagaaat ggcgtta gagtatgcyg tcagttcctt agagattgca attcctaatg cactagtatg 24aggtg ccaggaacac gttctgtgag gctgctgccc caggtgctga ccccagcctt 3accatt ttccttcctt gtgttcacag ccgctctgtc ttttacaata gcacccctct 36ggcta atgggctcta tgattagata gcatcc 396 657 396 DNA Homo sapiens 657 tttcaggtgc caggaacacg ttctgtgaggctgctgcccc aggtgctgac cccagccttc 6cattt tccttccttg tgttcacagc cgctctgtct tttacaatag cacccctctc tggctaa tgggctctat gattagatag catccttcag tagtgataaa ggcagtgaca tagggag gtcagcggkt gaaagcgcta tatctggaaa acctgagagc ctgtgaagct 24acttg acggggttag accgtgagcc gggctgcagc tggaaaaaga atgactgttc 3agcaga tccttccctg tgccatctct ttcttcattc ctctctagtg gcattcttat 36ctcta aaaccacaat tccattatct ctccta 396 658 396 DNA Homo sapiens 658 gagggtcttc tcttttgcct ggctccctatgcagccctat cttaccccct gcaaagtccc 6tgtgg ctcagtcact gctcctctct tcatctgtca ccacttgctt gagatcctac tgcttta attccgagac catctgcaga acatgacaaa atttgtccac ctacccacat cttttaa ctttaaagrc tttactaact gattcctatt agggaatgaa cagaggtggc 24taaac aataggagat tgatttacaa gaaatcttta aaatagtaga tttcttcgga 3attgaa atataaatgg cctgccttct tgtgtccctc cctggtctcc ctctttaggt 36gaaga agatcctgcc agccccataa cccgcc 396 659 396 DNA Homo sapiens 659 ttaaaatagt agatttcttc ggacctcattgaaatataaa tggcctgcct tcttgtgtcc 6tggtc tccctcttta ggtgataaga agaagatcct gccagcccca taacccgcca gcgcggg ttctagaccc ccttctcctc ccctctggcc gtggtaggca ttactgatga atggtgc tctttcttmc agagaccaaa cctggcctcg gaatccttct taacacagat 24ttaac acaaccactc tgagcagctg tcataagtag aagtaataga tactagaaga 3tctaag cctaatctag accaaaatac ggcctgatat agatgcaagc cagaggggct 36gttaa atgcaaggag attttcaacc ctgccg 396 66NA Homo sapiens 66ctccc tctttaggtg ataagaagaagatcctgcca gccccataac ccgccatctg 6gttct agaccccctt ctcctcccct ctggccgtgg taggcattac tgatgaatca tgctctt tcttccagag accaaacctg gcctcggaat ccttcttaac acagatactg aacacaa ccactctgrg cagctgtcat aagtagaagt aatagatact agaagaaatg 24gccta atctagacca aaatacggcc tgatatagat gcaagccaga ggggctttat 3aaatgc aaggagattt tcaaccctgc cgtctagaag ctacttgctg agatcttctt 36gggcc catctcctcc ccaggcctct cttctg 396 66NA Homo sapiens 66acccg ccatctgcgc gggttctagacccccttctc ctcccctctg gccgtggtag 6actga tgaatcatgg tgctctttct tccagagacc aaacctggcc tcggaatcct taacaca gatactgctt aacacaacca ctctgagcag ctgtcataag tagaagtaat tactaga agaaatgtmt aagcctaatc tagaccaaaa tacggcctga tatagatgca 24gaggg gctttatggt taaatgcaag gagattttca accctgccgt ctagaagcta 3ctgaga tcttcttcag ttgggcccat ctcctcccca ggcctctctt ctgttcctgg 36gtcac acttggactc tgcagacacc taatgc 396 662 396 DNA Homo sapiens 662 tggtaggcat tactgatgaa tcatggtgctctttcttcca gagaccaaac ctggcctcgg 6ttctt aacacagata ctgcttaaca caaccactct gagcagctgt cataagtaga aatagat actagaagaa atgtctaagc ctaatctaga ccaaaatacg gcctgatata gcaagcc agaggggckt tatggttaaa tgcaaggaga ttttcaaccc tgccgtctag 24acttg ctgagatctt cttcagttgg gcccatctcc tccccaggcc tctcttctgt 3gggcta tgtcacactt ggactctgca gacacctaat gctcttggga cctgctttag 36gacct caccaaccga ggaggaattg ctagat 396 663 396 DNA Homo sapiens 663 cagagaccaa acctggcctc ggaatccttcttaacacaga tactgcttaa cacaaccact 6cagct gtcataagta gaagtaatag atactagaag aaatgtctaa gcctaatcta caaaata cggcctgata tagatgcaag ccagaggggc tttatggtta aatgcaagga tttcaac cctgccgtyt agaagctact tgctgagatc ttcttcagtt gggcccatct 24ccagg cctctcttct gttcctgggc tatgtcacac ttggactctg cagacaccta 3tcttgg gacctgcttt agttcttgac ctcaccaacc gaggaggaat tgctagatga 36ttccc ccggaatttc tctcttgaac cccaga 396 664 396 DNA Homo sapiens 664 gggctttatg gttaaatgca aggagattttcaaccctgcc gtctagaagc tacttgctga 6tcttc agttgggccc atctcctccc caggcctctc ttctgttcct gggctatgtc cttggac tctgcagaca cctaatgctc ttgggacctg ctttagttct tgacctcacc cgaggag gaattgctmg atgagatcct tcccccggaa tttctctctt gaaccccaga 24cgttg cccctttcca gaagttgctc cagccctgtc cgcttaggaa gttcagtgtc 3ttgatc cagtgggtag ggaagacatt ccataatgaa tgccccagtc tgagcttctt 36aggct tcaggctgcc ctgcgaggat tttgca 396 665 396 DNA Homo sapiens 665 gtagctgaga ctacaggtgt gcactaccacacccagctaa ttttttgtat ttttagtaga 6ggttt agctatgttg gccaggctgg tctcgaactg ctgaactcaa gcaatctgcc cccggcc tcccaaagta ctgggagtat aggcataagc cacccatgat gcccagcctg cttggtt tcttccccrt tcatttaagc tattacctgg gcctgaactc aatggcacct 24caact ggcaactgac tcttggtctt ttattaccta ccttccctag caggcactgg 3ctccct cttcctatcc catggagtcc tgtcctctgt tggggctcct actgatcctc 36aatat gaagttctca gctcaatggt gggtgg 396 666 396 DNA Homo sapiens 666 cccggcctcc caaagtactg ggagtataggcataagccac ccatgatgcc cagcctgaat 6tttct tccccattca tttaagctat tacctgggcc tgaactcaat ggcacctggc aactggc aactgactct tggtctttta ttacctacct tccctagcag gcactgggtt ccctctt cctatcccrt ggagtcctgt cctctgttgg ggctcctact gatcctcttg 24atgaa gttctcagct caatggtggg tgggcaatga ctgccaactc ttgaggccaa 3ctcagg ttaccccact cctcctcctc ctgagttgct cactcactcc tcattcactc 36tgatt cagtagatat ttgctacctg ctctgt 396 667 396 DNA Homo sapiens 667 ccggcctccc aaagtactgg gagtataggcataagccacc catgatgccc agcctgaatc 6ttctt ccccattcat ttaagctatt acctgggcct gaactcaatg gcacctggca actggca actgactctt ggtcttttat tacctacctt ccctagcagg cactgggttg cctcttc ctatcccayg gagtcctgtc ctctgttggg gctcctactg atcctcttgg 24tgaag ttctcagctc aatggtgggt gggcaatgac tgccaactct tgaggccaat 3tcaggt taccccactc ctcctcctcc tgagttgctc actcactcct cattcactca 36gattc agtagatatt tgctacctgc tctgtg 396 668 396 DNA Homo sapiens 668 ggcataagcc acccatgatg cccagcctgaatcttggttt cttccccatt catttaagct 6ctggg cctgaactca atggcacctg gcaccaactg gcaactgact cttggtcttt tacctac cttccctagc aggcactggg ttgctccctc ttcctatccc
atggagtcct ctctgtt ggggctccya ctgatcctct tggcaatatg aagttctcag ctcaatggtg 24gcaat gactgccaac tcttgaggcc aatgaactca ggttacccca ctcctcctcc 3gagttg ctcactcact cctcattcac tcaacattga ttcagtagat atttgctacc 36tgtgccaggtaccag gtcagttgct gaagga 396 669 396 DNA Homo sapiens 669 cctggcacca actggcaact gactcttggt cttttattac ctaccttccc tagcaggcac 6tgctc cctcttccta tcccatggag tcctgtcctc tgttggggct cctactgatc ttggcaa tatgaagttc tcagctcaat ggtgggtgggcaatgactgc caactcttga caatgaa ctcaggttwc cccactcctc ctcctcctga gttgctcact cactcctcat 24caaca ttgattcagt agatatttgc tacctgctct gtgccaggta ccaggtcagt 3gaagga gtaacagtga acatgacgga gtctttgtcc ccaaggagac ccaaggtgtc 36gagccaggggcacat tgcaagacca aatata 396 67NA Homo sapiens 67aactg actcttggtc ttttattacc taccttccct agcaggcact gggttgctcc 6cctat cccatggagt cctgtcctct gttggggctc ctactgatcc tcttggcaat aagttct cagctcaatg gtgggtgggc aatgactgccaactcttgag gccaatgaac ggttacc ccactcctyc tcctcctgag ttgctcactc actcctcatt cactcaacat 24cagta gatatttgct acctgctctg tgccaggtac caggtcagtt gctgaaggag 3agtgaa catgacggag tctttgtccc caaggagacc caaggtgtct cctagagcca 36acattgcaagaccaa atatattcaa cttacc 396 67NA Homo sapiens 67gagtc ctgtcctctg ttggggctcc tactgatcct cttggcaata tgaagttctc 6aatgg tgggtgggca atgactgcca actcttgagg ccaatgaact caggttaccc tcctcct cctcctgagt tgctcactca ctcctcattcactcaacatt gattcagtag tttgcta cctgctctrt gccaggtacc aggtcagttg ctgaaggagt aacagtgaac 24ggagt ctttgtcccc aaggagaccc aaggtgtctc ctagagccag gggcacattg 3accaaa tatattcaac ttaccaaaat aatcatagac ctagttctca aaaagcaaga 36gattcctcgttgtca tttctcctcc tcagca 396 672 396 DNA Homo sapiens 672 ttagagtctg tgggcccctc caagtgtgga gtatggtgtt acttcaccag agtttgagga 6attct tcttttggaa ggccggggag catagatgga tatcaaggct gctgtttcta gcgaaac ccaccaaaca acagtattag aatcatctgtggtgcttatt aaagatacag cctgggc cccatcccmg acttatgaat cagaatctct gccagaggaa gcctgagaat 24ttctc agatgattct gcattctcag ataacacatt ctttaggtga ttcttacaca 3ggagtt tgggaatcgc tgaaggctgt tcacttctct tttctgagaa atgattcatt 36cagaaatatttgcag aggtccttat ttattg 396 673 396 DNA Homo sapiens 673 tggcctcatt cgtgtgataa atctgagcca ccacgatatt tgacttttca caatttaatt 6gaacc ctctattctc tggctaaaaa atatccctta cttggacttc tttattttat caattcc cttaccagca ctagcagggg actctgtactcatctgctgg cgctgccata aagcact gcagcctgkg gggctcaaac cacagaattt attctctcac agtcctagag 24aagtc caagatcaaa gtgtgggcag ggtcggtttc tcctgcagcc tctctccttg 3atagag tgccaccttc tacctgtgtc ttcacatcat cacctcactg agcatgtctg 36aaatctccccttctt ataagacccc agtcat 396 674 396 DNA Homo sapiens 674 tctccttggc ttatagagtg ccaccttcta cctgtgtctt cacatcatca cctcactgag 6ctgtg tccaaatctc cccttcttat aagaccccag tcatactgga tgaggatcca atatgag ttcattttac cttaattatc tctttaaacaccctgtctcc aaatacagtc ttctgag gaactgagrg taaagattca acatatgaat tttggaaggg acctaattca 24caaca ccctcttttg ggatgtttat tttccccctt aaggagctag ttaggatgtc 3ctcatg aacatgactg tgaacaggaa aacagggaga gaatgaagct ggccaaggaa 36ctggtgtcagctagc agtgcttttc tgatgt 396 675 396 DNA Homo sapiens 675 cattttacct taattatctc tttaaacacc ctgtctccaa atacagtccc attctgagga 6gagta aagattcaac atatgaattt tggaagggac ctaattcagc ccacaacacc ttttggg atgtttattt tcccccttaa ggagctagttaggatgtctt atctcatgaa gactgtg aacaggaara cagggagaga atgaagctgg ccaaggaaca gggctggtgt 24agcag tgcttttctg atgtgagtgg gtcccacagg gagcttgtta aaatgcagat 3attcat taggttccag agggacctga gatttcccat ttctgacaag tttccagtgt 36ctgatgctgctggtc cacggaccat actttg 396 676 396 DNA Homo sapiens 676 gggagagaat gaagctggcc aaggaacagg gctggtgtca gctagcagtg cttttctgat 6tgggt cccacaggga gcttgttaaa atgcagattc tgattcatta ggttccagag cctgaga tttcccattt ctgacaagtt tccagtgtgggggctgatgc tgctggtcca accatac tttgagtakc aaggagcttg atacataatg gctgagtgac tttcagactc 24gtaga aaaattatga gttggctggg cgtggtggct cacgcctgta atcccagcac 3ggaggc cgaggtgggc agatcacctg aggtcaggag ttcgagacca gcctggccaa 36tgaaacaccatctct accaaaaata caaaaa 396 677 396 DNA Homo sapiens 677 acttaagccc agaagactga ggttgcagtg agccgagatt gcaccactgc actccagctt 6acaga gtgagactct atctcaaaaa caaagaaaca aacaacaaca ataacaacaa ccaagtc tctccctcca ctcaaaaatg caagggcctgtctcccattg ctgggtgccc tctcatg aatgtagaya tgaattattc cagtcagcct caggagaata gaatgagccc 24tgccg aagcaccttt cagattccac cggttttatc ggctcattta aacttcactt 3cacagt cctgcattac acacgtgtct gtcgttatgg gcagctgcag agagggtctt 36tcctaatgctcagtg aggatgccca atggtc 396 678 396 DNA Homo sapiens 678 ctcaaaaaca aagaaacaaa caacaacaat aacaacaaaa accaagtctc tccctccact 6atgca agggcctgtc tcccattgct gggtgcccag gtctcatgaa tgtagatatg tattcca gtcagcctca ggagaataga atgagccctcagatgccgaa gcacctttca tccaccg gttttatcrg ctcatttaaa cttcacttct aacacagtcc tgcattacac 24tctgt cgttatgggc agctgcagag agggtcttaa tggtcctaat gctcagtgag 3cccaat ggtcaacaga acctgccatc ttcaggccat caaggagctc tggagttaag 36catgagagcacagag gggcgggtac agcaga 396 679 396 DNA Homo sapiens 679 tgtagatatg aattattcca gtcagcctca ggagaataga atgagccctc agatgccgaa 6tttca gattccaccg gttttatcgg ctcatttaaa cttcacttct aacacagtcc attacac acgtgtctgt cgttatgggc agctgcagagagggtcttaa tggtcctaat cagtgag gatgcccart ggtcaacaga acctgccatc ttcaggccat caaggagctc 24ttaag gaaatcatga gagcacagag gggcgggtac agcagagccc tcgtggtaat 3tttgag gtctaggctc tcttcacttg ggtttgaaat aagttcaatg actagtaata 36gacacttctaccctt caaatgaagt aaatgg 396 68NA Homo sapiens 68ctttc agattccacc ggttttatcg gctcatttaa acttcacttc taacacagtc 6ttaca cacgtgtctg tcgttatggg cagctgcaga gagggtctta atggtcctaa tcagtga ggatgcccaa tggtcaacag aacctgccatcttcaggcca tcaaggagct gagttaa ggaaatcawg agagcacaga ggggcgggta cagcagagcc ctcgtggtaa 24tttga ggtctaggct ctcttcactt gggtttgaaa taagttcaat gactagtaat 3gagaca cttctaccct tcaaatgaag taaatgggaa aatggagcat tgttgagtcc 36gctataatttaaacc ccatatatct aaaagg 396 68NA Homo sapiens 68gtgtc tgtcgttatg ggcagctgca gagagggtct taatggtcct aatgctcagt 6tgccc aatggtcaac agaacctgcc atcttcaggc catcaaggag ctctggagtt gaaatca tgagagcaca gaggggcggg tacagcagagccctcgtggt aatgggtttt gtctagg ctctcttcrc ttgggtttga aataagttca atgactagta atagctgaga 24ctacc cttcaaatga agtaaatggg aaaatggagc attgttgagt ccagggagct 3tttaaa ccccatatat ctaaaagggg taacattttt gtgtgtgtga aattggtgtc 36cactgcatctacagt tttctttttc cttctc 396 682 396 DNA Homo sapiens 682 acatatttgg gaaacgcatc atactcttcc tgttcctcat gtccgttgct ggcatattca 6tacct catcttcttt ttcggaagtg actttgaaaa ctacataaag acgatctcca ccatctc ccctctactt ctcattccct aactctctgctgaatatggg gttggtgttc tctaatc aatacctaya agtcatcata attcagctct tgagagcatt ctgctcttct 24tggct gtaaatctat tggccatctg ggcttcacag cttgagttaa ccttgctttt 3gaacaa aatgatgtca tgtcagctcc gccccttgaa catgaccgtg gccccaaatt 36ttcccatgcattttg tttgtttctt cactta 396 683 396 DNA Homo sapiens 683 tggtgttctc atctaatcaa tacctacaag tcatcataat tcagctcttg agagcattct 6tcttt agatggctgt aaatctattg gccatctggg cttcacagct tgagttaacc cttttcc gggaacaaaa tgatgtcatg tcagctccgccccttgaaca tgaccgtggc aaatttg ctattcccrt gcattttgtt tgtttcttca cttatcctgt tctctgaaga 24tgtga ccaggtttgt gttttcttaa aataaaatgc agagacatgt tttaagctga 3tgaggg gttttgttaa tggcttttgg gggatttatc tctataccca caaacgacta 36ttttcctcaaactaa atgataatat taaaaa 396 684 396 DNA Homo sapiens 684 ttatctctat acccacaaac gactagtttg ttttcctcaa actaaatgat aatattaaaa 6catcc tggccaggtg tggtggctca tacctgtaat cccagcactt tgggaggccg caggtgg atcacttgag gtcaggaatt aagaccagcctggccaatat ggtgaaagcc ctgtact aaaaatacra aaattagcca ggtatgctgg tggatgctta taatcccagc 24gggag gttgaggcag gagaattgct tgaacccggg aggtagaggt tgcagtgagc 3atcatg ccactgcact ccagcttggg caacagagtg agactccatc tcaaattaaa 36tacacatctggcttc tggaaaaatt acttga 396 685 396 DNA Homo sapiens 685 gatcatgcca ctgcactcca gcttgggcaa cagagtgaga ctccatctca aattaaaaaa 6acatc tggcttctgg aaaaattact tgaagatctt ttatgacatc catccctctt acagcca tgtgaattag gttggtatct tcatatactagcatcgtgcc cagcacttcc ttataca gtttaaaakg ttctgtaatt ccctgtggga acctaagata atgcgaggac 24tacgt gcccccaaat attggcaaac caatgaataa atgaatgaat gagtttatga 3ctaact ggctgtattt aatgaagtat gtgtgttgag ccatttccca cagtgtggac 36tgtcccacaatatgg gcctcttccc aaaggc 396 686 396 DNA Homo sapiens 686 aattaaaaaa aatacacatc tggcttctgg aaaaattact tgaagatctt ttatgacatc 6ctctt cacacagcca tgtgaattag gttggtatct tcatatacta gcatcgtgcc cacttcc atgttataca gtttaaaatg ttctgtaattccctgtggga acctaagata cgaggac cgtcatacrt gcccccaaat attggcaaac caatgaataa atgaatgaat 24tatga atcgctaact ggctgtattt aatgaagtat gtgtgttgag ccatttccca 3gtggac agatttgtcc cacaatatgg gcctcttccc aaaggcccta ccacctaatg 36acactggggatttga tttcaacatg tgaatt 396 687 396 DNA Homo sapiens 687 agttcatagt gacagtgatc cagccactgt catgacaggt gccacttggc agaaacagca 6tggaa gatggcgggg tgtagtcaag attccaggat ccccaacaga gaagccagct atagggg agccattcat caggattgaa ctctcaatcgagctggacag taataggtgg tgtgtta ttccccagrt gagtatcatg acagtcacaa tcctaggaag gatgtgaagc 24ccagc tctcctccag ttgcctgctt gggcagcaga gatgatggaa tgtggagtct 3tggtct gaggcctgaa tccatgtgcc tcatgtatga tgctcaggca agaggatctc 36tcaagggagagggcc tgaatgagcc ttgctt 396 688 396 DNA Homo sapiens 688 cttggcagaa acagcacagc ttggaagatg gcggggtgta gtcaagattc caggatcccc 6agaag ccagctctta taggggagcc attcatcagg attgaactct caatcgagct cagtaat aggtgggtct gtgttattcc ccagatgagtatcatgacag tcacaatcct aaggatg tgaagcctyc cccagctctc ctccagttgc ctgcttgggc agcagagatg 24atgtg gagtctggcg tggtctgagg cctgaatcca tgtgcctcat gtatgatgct 3caagag gatctctcaa ttcaagggag agggcctgaa tgagccttgc tttccaggcc 36gatggtccaggctga agcccctcct ggcttg 396 689 396 DNA Homo sapiens 689 ctggcgtggt ctgaggcctg aatccatgtg cctcatgtat gatgctcagg caagaggatc 6attca agggagaggg cctgaatgag ccttgctttc caggcctgtc tgatggtcca tgaagcc cctcctggct tgcactgcca gacctcatccagcaggagct ccttggcatt tgcttca ggatagttsc ttctgctctg agtgctctct aaagagcagt gctctaccat 24ctggg cttttctttt cttcttgctg atagggaagg catgggacat tgcaggatgg 3ggcccc caggccttct catgcctggg cttggtttgg aaggtggtca ggtgatcaat 36tgattggcctggcat tgaggagttt tcctgg 396 69NA Homo sapiens 69tctaa agagcagtgc tctaccatcc aagctgggct tttcttttct tcttgctgat 6aggca tgggacattg caggatggaa gtggccccca ggccttctca tgcctgggct tttggaa ggtggtcagg tgatcaataa tcctgattggcctggcattg aggagttttc ggatgtg gtcctttcrg ttttttaaaa attattttta ttgatacaca tatttgtagg 24gtggg gtgcatgtga tactttatta tgtgtgtgga ttgtgtaatg atgaagtcag 3tttagg gtcttcatca ccttgattat catttctatg tgttgagaac atttcaagtt 36ttccagctattttga aatagacagt ccattt 396 69NA Homo sapiens 69tttat tatgtgtgtg gattgtgtaa tgatgaagtc agggcattta gggtcttcat 6tgatt atcatttcta tgtgttgaga acatttcaag ttctcagttc cagctatttt atagaca gtccattttg ttagctacag tcacccaacccggctgtcag acattggaac ctcctat tgaactgtrt atttgtaccc attcaccaaa ctctctttgg gctttcagtt 24actgg gatgatcctg ggaaaactaa agtaaatcag acacccgacg tgtgagctag 3taatat gcccagtgga ccctggggac atcttagctt tcagaggtca tgctgtccaa 36ctgtggggcttccag aaggtgggga gaggaa 396 692 396 DNA Homo sapiens 692 tatgtgtgtg gattgtgtaa tgatgaagtc agggcattta gggtcttcat caccttgatt 6ttcta tgtgttgaga acatttcaag ttctcagttc cagctatttt gaaatagaca cattttg ttagctacag tcacccaacc cggctgtcagacattggaac ttactcctat actgtgt atttgtacyc attcaccaaa ctctctttgg gctttcagtt ttacaactgg 24tcctg ggaaaactaa agtaaatcag acacccgacg tgtgagctag gttataatat 3agtgga ccctggggac atcttagctt tcagaggtca tgctgtccaa gctgactgtg 36tccagaaggtgggga gaggaaatga tgcaat 396 693 396 DNA Homo sapiens 693 tgggaaaact aaagtaaatc agacacccga cgtgtgagct aggttataat atgcccagtg 6tgggg acatcttagc tttcagaggt catgctgtcc aagctgactg tggggcttcc aggtggg gagaggaaat gatgcaatgg cccatcagaggcactacttg gggcctgggg gagtgca tgtctaagsc attaagggga ggggagagca gccttcataa ttatgaagag 24tcagg tgcacagctt ctgatgaggg acagcttcta attgaagaca gcattgtgta 3tcaaac tccctgtctt cagagtgcct gctgtatccc accatcagtt ctgtgacttc 36aagcctcaattttgc atgtgttaca ttggga 396 694 396 DNA Homo sapiens 694 cctgcatagc aaattcttgc aaatgtaggg actcaaaaca atataaattt attatctgac 6ttctg ggtcagaggt cttactaggc tgtaatcaga gggcaaccaa agctgtgatc gctgaag ctcaggattc tcttccaagc tcactggttgttggcagaat tcagttcttt gttggaa gactaaagyc tacagtcttc agtctctaga agccttttct ctggcacagg 24ctaca acatggccat ttatgtcttt aaggccaata ggagaacatg attagcatat 3tttaag tgaactttag accctttttt aaaggcctat ctgattaggc caggcccaag 36tttaagtcaactgat tagagatctt aattac 396 695 396 DNA Homo sapiens 695 ctgaagctca ggattctctt ccaagctcac tggttgttgg cagaattcag ttctttccag 6agact aaagcctaca gtcttcagtc tctagaagcc ttttctctgg cacaggtttc acaacat ggccatttat gtctttaagg ccaataggagaacatgatta gcatattttt aagtgaa ctttagacyc ttttttaaag gcctatctga ttaggccagg cccaagtgag 24agtca actgattaga gatcttaatt acatctgcaa agtcccttca tgtttaccgt 3cataac ttagtgaaag gagtgaaatt gcaaccaggt tctgcctgca ctccacggaa 36ttctgcagaagtgtg ggtcacgggg gggtta 396 696 396 DNA Homo sapiens 696 agaacatgat tagcatattt tttttaagtg aactttagac ccttttttaa aggcctatct 6ggcca ggcccaagtg agctttaagt caactgatta gagatcttaa ttacatctgc gtccctt catgtttacc gtataacata acttagtgaaaggagtgaaa ttgcaaccag ctgcctg cactccacrg aaggggattc tgcagaagtg tgggtcacgg gggggttatt 24attct gcctacgtca ctgagtcaaa agaagctgaa tggttgtgat gctgaggttt 3gcagca gcagtgtgtg tgtgtgagtg aattcatacg tatgaccacc tgggaagaaa 36ctgtggtttcctcca cctcctggca gacaga 396 697 396 DNA Homo sapiens 697 gggattacag acacacactg ccacgcctgg ctaatttttg tatttttagt agagacgagg 6ccatg ttggccaggc tggtcttgaa ctcctgacct caagtgatcc gcccacctca tcccaaa gtgctgggat tacagacgtg agccaccattaaccattttt ctatctcctg gaaaggg cacagtgara gaacagatga agctgagaca tacaagtgaa ctcctccctc 24cattt agactaaaat aggattattc atactgagat tctccctggt tgcaaagaga 3ctgtgc aactgggttt ttacaattat ccctacccta tgctttcctc atctgtcttc 36agtcagctcaggctg ctataacaaa acacca 396 698 396 DNA Homo sapiens 698 ggcagattcg gtgtctaatg aggtcctgct ttccagttta tagacagtgc cttatcgcta 6ttaca cagtggaagg agaggacgag aagctccttg ggcttttttt tgtttctttc ctctctc tctctctttt tttttttttt aataaggtcactatcttagt ccattttgtg ctaaaag gaacatctra ggttgagtaa tttattttat tttaaaaagt ggccaggcat 24cttat cctgtaaccc taatccttta ggaggccaaa acagcaggat tgtttgaggc 3agttca agaccagcct aggcaagata gtgagacccc atctacccca tctctactaa 36taaaaaattagctgt gtgttgtaaa gtgtgc 396 699 396 DNA Homo sapiens 699 aatttatttt attttaaaaa gtggccaggc atggaggctt atcctgtaac cctaatcctt 6ggcca aaacagcagg attgtttgag gccaggagtt caagaccagc ctaggcaaga tgagacc ccatctaccc catctctact aaaattttaaaaaattagct gtgtgttgta tgtgctt gtagtcccrg ccacttgaga ggctgaggtg ggtggagttc aaggctgcag 24tatga ttgagccact gcactccaac ccgggtaacg gggcaagacc ttgtctctat 3aaaaaa aaaatcttta tgtggctcac tattctgggt ggctggaaag ttcaagattg 36ctgcatctggtgaca gcctcatgtc gcttcc 396 7DNA Homo sapiens 7cctaat cctttaggag gccaaaacag caggattgtt tgaggccagg agttcaagac 6taggc aagatagtga gaccccatct accccatctc tactaaaatt ttaaaaaatt tgtgtgt tgtaaagtgt gcttgtagtc ccggccacttgagaggctga ggtgggtgga caaggct gcagtgagwt atgattgagc cactgcactc caacccgggt aacggggcaa 24tgtct ctatttaaaa aaaaaaaatc tttatgtggc tcactattct gggtggctgg 3ttcaag attgggcatc tgcatctggt gacagcctca tgtcgcttcc agtcatgggg 36cgaaggagagctggc acgtgcagat atcacg 396 7DNA Homo sapiens 7tttagg aggccaaaac agcaggattg tttgaggcca ggagttcaag accagcctag 6atagt gagaccccat ctaccccatc tctactaaaa ttttaaaaaa ttagctgtgt gtaaagt gtgcttgtag tcccggccac ttgagaggctgaggtgggtg gagttcaagg cagtgag ttatgattra gccactgcac tccaacccgg gtaacggggc aagaccttgt 24tttaa aaaaaaaaaa tctttatgtg gctcactatt ctgggtggct ggaaagttca 3tgggca tctgcatctg gtgacagcct catgtcgctt ccagtcatgg gggaagacga 36agctggcacgtgcag
atatcacgtg ttgagg 396 7DNA Homo sapiens 7aaaatt agctgtgtgt tgtaaagtgt gcttgtagtc ccggccactt gagaggctga 6gtgga gttcaaggct gcagtgagtt atgattgagc cactgcactc caacccgggt ggggcaa gaccttgtct ctatttaaaa aaaaaaaatc tttatgtggctcactattct tggctgg aaagttcarg attgggcatc tgcatctggt gacagcctca tgtcgcttcc 24tgggg gaagacgaag gagagctggc acgtgcagat atcacgtgtt gagggcagaa 3gagaga gaggggagag atgccaggct ctttttaaca accagcactg gggaaactaa 36tgaga gctcactgactcctgaggga ggacat 396 7DNA Homo sapiens 7gggaag acgaaggaga gctggcacgt gcagatatca cgtgttgagg gcagaagcga 6agagg ggagagatgc caggctcttt ttaacaacca gcactgggga aactaataga agagctc actgactcct gagggaggac attaatctat tgatgagcgacctgcctcca cccaaac acctccaayg ataccccacc tccaacactg ccacactagg gattaacttt 24tgaga tttagagggg ggaaacttac aaactatcgc aggcactaat accactcatg 3ctccac cttcatgacc taatcacttc ctaaaggcct tacctcttaa tctcatcaca 36gattc gatttcaacttgaattttgg ggggac 396 7DNA Homo sapiens 7ctgcca cctgaaatta gatcatttat ttaccccttt atttgttcag tttgccttgt 6agaat ataagcttcc aaagggcagg agctttgcct atattgttag gccgggcata tgagcac tcaaaaaaat atttgatgag tgtatgaaag aacagactgggttatgtaat gcctact tacctatayg accgtgtggt ggggtttatg gtgggtgtgg tggtgatggc 24ggcta taagcaaatt tgggacaggg agtctaagaa atgttcttaa attttagtaa 3agcatc ctctacagaa cctgtcttaa aacatgaaag ttccttagtg ctacccccag 36tgatt tggtaggtcaaggatagggc ctggaa 396 7DNA Homo sapiens 7acctga aattagatca tttatttacc cctttatttg ttcagtttgc cttgtccgtt 6ataag cttccaaagg gcaggagctt tgcctatatt gttaggccgg gcatacaatg actcaaa aaaatatttg atgagtgtat gaaagaacag actgggttatgtaattgtgc cttacct atatgaccrt gtggtggggt ttatggtggg tgtggtggtg atggctatag 24taagc aaatttggga cagggagtct aagaaatgtt cttaaatttt agtaagcaaa 3cctcta cagaacctgt cttaaaacat gaaagttcct tagtgctacc cccagaggta 36tggta ggtcaaggatagggcctgga aattca 396 7DNA Homo sapiens 7tcttaa aacatgaaag ttccttagtg ctacccccag aggtatgatt tggtaggtca 6agggc ctggaaattc acattcttgt taagatgttc ttcatccggg gtttgttgac cttttca gaagattttt gctctgtagc tgtactaccc aatgcagtagttcgtagtca tggctcc tgagccctyg aagtgtagct cctctgaact gagacgtgct gtaaatgtaa 24acacc ggagtttgaa gagttaatac aaagaaaaag gaatgcaaaa catctcatta 3tgcttt acactgatta catattgaaa tggtaatctt gtagatatag tgcgttaaat 36atact gttaggcttaatttcacgtc tttata 396 7DNA Homo sapiens 7ccaatc aacaagaggg caaaagaaca aacatttgat gtgtaattac ttaatttagt 6tgcat ttgggtcctc aatgtcagca ctatggcaac cagaacatgg ccacaataac ctggaaa tgtctattct tacctggacc cagcaggcca tgccccactgattatataat cctctct ccttgttayg gtctgaatgc ttgcatccct caaaaattca tgtgttgaaa 24acccc caaggtgatg atattaggag gtcggccttt tgagaggtaa ttaggtcatg 3cagcat cctcatgaat gggattagtg tccttataaa ataggcccaa gggagctcat 36ttgtc caccatgtgagaacacagcg agaggg 396 7DNA Homo sapiens 7gttacg gtctgaatgc ttgcatccct caaaaattca tgtgttgaaa tcctaacccc 6tgatg atattaggag gtcggccttt tgagaggtaa ttaggtcatg aagacagcat catgaat gggattagtg tccttataaa ataggcccaa gggagctcattcactttgtc catgtga gaacacagyg agagggcacc atttatgcac caggaaatgg gccttttcca 24tctgt cggtgcctgg atcttggact tcacagcctc tagaactgtg agaaattaat 3ttttta taagccacca aatctatggt tttttttata gaaaccgtaa tggactaaaa 36cctaa ttatatttaaacttatcagt gcactg 396 7DNA Homo sapiens 7ccccca aggtgatgat attaggaggt cggccttttg agaggtaatt aggtcatgaa 6catcc tcatgaatgg gattagtgtc cttataaaat aggcccaagg gagctcattc ttgtcca ccatgtgaga acacagcgag agggcaccat ttatgcaccaggaaatgggc ttccaga caatctgtyg gtgcctggat cttggacttc acagcctcta gaactgtgag 24aattt gttttttata agccaccaaa tctatggttt tttttataga aaccgtaatg 3aaaaca ctccctaatt atatttaaac ttatcagtgc actgggcagt gacatattaa 36tgctg gccaacgtaattgacaccat aaggct 396 7DNA Homo sapiens 7ctcatt ttaacctttt gtttcaaagc ctctcttttc atgacttccc cgccttcatt 6catat ggtggggtta ttattaagac attaaatgag agtggacagg taggcaaagg tgggttg caggggagtt gagggttgcc tgtgtacttt tctagactgttccacttcac agtgaaa tattcccart tgatactatc atgaaacaaa gcaaatgaaa tgctgagcac 24ttcgt cttgatgaaa tgctgaaaga aaagaaagga aaaataaagt agccattatt 3cccttc ctcccacccc catgtttact actcttattt ctcttttgta ttgttgtgtt 36cacag catcagaaaaactcccagtt ttgaga 396 7DNA Homo sapiens 7gtaggc aaaggaggtg ggttgcaggg gagttgaggg ttgcctgtgt acttttctag 6tccac ttcacatcag tgaaatattc ccaattgata ctatcatgaa acaaagcaaa aatgctg agcacggagc ttcgtcttga tgaaatgctg aaagaaaagaaaggaaaaat gtagcca ttatttttrc ccttcctccc acccccatgt ttactactct tatttctctt 24ttgtt gtgttggaag cacagcatca gaaaaactcc cagttttgag agataactca 3ttagtt cacttaaacc tgagaaagga gaagaggatg ccaccgtgag gtccaggacg 36aggaa aaaaacagacaaaaaaatcc atatga 396 7DNA Homo sapiens 7taggca aaggaggtgg gttgcagggg agttgagggt tgcctgtgta cttttctaga 6ccact tcacatcagt gaaatattcc caattgatac tatcatgaaa caaagcaaat atgctga gcacggagct tcgtcttgat gaaatgctga aagaaaagaaaggaaaaata tagccat tatttttgmc cttcctccca cccccatgtt tactactctt atttctcttt 24tgttg tgttggaagc acagcatcag aaaaactccc agttttgaga gataactcag 3tagttc acttaaacct gagaaaggag aagaggatgc caccgtgagg tccaggacgt 36ggaaa aaaacagacaaaaaaatcca tatgaa 396 7DNA Homo sapiens 7tcttga tgaaatgctg aaagaaaaga aaggaaaaat aaagtagcca ttatttttgc 6ctccc acccccatgt ttactactct tatttctctt ttgtattgtt gtgttggaag agcatca gaaaaactcc cagttttgag agataactca gtgtttagttcacttaaacc gaaagga gaagaggayg ccaccgtgag gtccaggacg taaagaggaa aaaaacagac 24aatcc atatgaaatg aaaatgtgaa agaggcgctt tcgagcagat gagtgttgta 3acagtg ttgagagctg tttgtgtcca gagctgcttg ctgcacctgg cgggataaac 36tctaa cagaggatccttgtttcaag gaggct 396 7DNA Homo sapiens 7aaagaa aggaaaaata aagtagccat tatttttgcc cttcctccca cccccatgtt 6ctctt atttctcttt tgtattgttg tgttggaagc acagcatcag aaaaactccc tttgaga gataactcag tgtttagttc acttaaacct gagaaaggagaagaggatgc cgtgagg tccaggacrt aaagaggaaa aaaacagaca aaaaaatcca tatgaaatga 24tgaaa gaggcgcttt cgagcagatg agtgttgtag attacagtgt tgagagctgt 3gtccag agctgcttgc tgcacctggc gggataaaca ctggtctaac agaggatcct 36caagg aggctgccttttatttgggg ggacaa 396 7DNA Homo sapiens 7tttttg cccttcctcc cacccccatg tttactactc ttatttctct tttgtattgt 6tggaa gcacagcatc agaaaaactc ccagttttga gagataactc agtgtttagt cttaaac ctgagaaagg agaagaggat gccaccgtga ggtccaggacgtaaagagga aaacaga caaaaaaayc catatgaaat gaaaatgtga aagaggcgct ttcgagcaga 24gttgt agattacagt gttgagagct gtttgtgtcc agagctgctt gctgcacctg 3gataaa cactggtcta acagaggatc cttgtttcaa ggaggctgcc ttttatttgg 36caaaa ttgttcttgaaagctgctca gtggtt 396 7DNA Homo sapiens 7tattgt tgtgttggaa gcacagcatc agaaaaactc ccagttttga gagataactc 6ttagt tcacttaaac ctgagaaagg agaagaggat gccaccgtga ggtccaggac aagagga aaaaaacaga caaaaaaatc catatgaaat gaaaatgtgaaagaggcgct gagcaga tgagtgttrt agattacagt gttgagagct gtttgtgtcc agagctgctt 24acctg gcgggataaa cactggtcta acagaggatc cttgtttcaa ggaggctgcc 3atttgg ggggacaaaa ttgttcttga aagctgctca gtggttcaag ctacagcatg 36ctagc agaatggactccagggcctc cgagga 396 7DNA Homo sapiens 7gagaga taactcagtg tttagttcac ttaaacctga gaaaggagaa gaggatgcca 6aggtc caggacgtaa agaggaaaaa aacagacaaa aaaatccata tgaaatgaaa tgaaaga ggcgctttcg agcagatgag tgttgtagat tacagtgttgagagctgttt tccagag ctgcttgcyg cacctggcgg gataaacact ggtctaacag aggatccttg 24aggag gctgcctttt atttgggggg acaaaattgt tcttgaaagc tgctcagtgg 3agctac agcatggtgg actagcagaa tggactccag ggcctccgag gagacagtga 36gccag aaatagtcaaggatagaaag gaagga 396
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