首页> 美国卫生研究院文献>Journal of Korean Medical Science >Distinct Linkage Disequilibrium (LD) Runs of Single Nucleotide Polymorphisms and Microsatellite Markers; Implications for Use of Mixed Marker Haplotypes in LD-based Mapping
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Distinct Linkage Disequilibrium (LD) Runs of Single Nucleotide Polymorphisms and Microsatellite Markers; Implications for Use of Mixed Marker Haplotypes in LD-based Mapping

机译:单核苷酸多态性和微卫星标记的独特连锁不平衡(LD)运行;在基于LD的映射中使用混合标记单倍型的含义

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摘要

It has been suggested that the haplotypic relationship between microsatellite markers and single nucleotide polymorphisms (SNPs) is of considerable importance, as microsatellite markers can potentially be incorporated into haplotypes containing SNPs to increase marker density across a region of interest. However, SNPs and microsatellite markers have different mutation rates and durations, and it is conceivable that the linkage disequilibrium (LD) patterns between the genetic markers may considerably differ. We assessed the LD patterns using 1,661 SNPs and 65 microsatellite markers along chromosome 22 and investigated whether common patterns of LD between the two genetic markers are deduced from the results. The results demonstrated that the patterns of LD among microsatellite markers varied considerably and the LD runs of SNPs and microsatellite markers showed distinct patterns. Microsatellite markers have a much higher mutation rate and the evolution of microsatellite markers is a more complex process which has distinct mutation properties from those of SNPs. We consider that these might contribute to the different LD patterns between the two genetic markers. Therefore, it would seem inadvisable to make assumptions about persistence of LD across even a relatively small genetic distance among microsatellite markers and to construct mixed marker haplotypes/LD maps employing microsatellite markers.
机译:已经提出,微卫星标记和单核苷酸多态性(SNP)之间的单倍型关系是相当重要的,因为微卫星标记可以潜在地掺入含有SNP的单倍型中以增加整个感兴趣区域的标记密度。但是,SNP和微卫星标记具有不同的突变率和持续时间,并且可以想象,遗传标记之间的连锁不平衡(LD)模式可能存在很大差异。我们评估了沿22号染色体使用的1,661个SNP和65个微卫星标记的LD模式,并研究了是否从结果中推论出两个遗传标记之间的LD常见模式。结果表明,微卫星标记之间的LD模式变化很大,SNPs和微卫星标记的LD运行显示出独特的模式。微卫星标记具有更高的突变率,微卫星标记的进化是一个更复杂的过程,具有与SNP不同的突变特性。我们认为这些可能导致两个遗传标记之间的LD模式不同。因此,不建议在微卫星标记之间甚至相对较小的遗传距离上对LD的持久性进行假设,并使用微卫星标记构建混合标记单倍型/ LD图。

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