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Use of a Dense Single Nucleotide Polymorphism Map for In Silico Mapping in the Mouse

机译:密集的单核苷酸多态性图在鼠标中的计算机电子地图的使用。

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Rapid expansion of available data, both phenotypic and genotypic, for multiple strains of mice has enabled the development of new methods to interrogate the mouse genome for functional genetic perturbations. In silico mapping provides an expedient way to associate the natural diversity of phenotypic traits with ancestrally inherited polymorphisms for the purpose of dissecting genetic traits. In mouse, the current single nucleotide polymorphism (SNP) data have lacked the density across the genome and coverage of enough strains to properly achieve this goal. To remedy this, 470,407 allele calls were produced for 10,990 evenly spaced SNP loci across 48 inbred mouse strains. Use of the SNP set with statistical models that considered unique patterns within blocks of three SNPs as an inferred haplotype could successfully map known single gene traits and a cloned quantitative trait gene. Application of this method to high-density lipoprotein and gallstone phenotypes reproduced previously characterized quantitative trait loci (QTL). The inferred haplotype data also facilitates the refinement of QTL regions such that candidate genes can be more easily identified and characterized as shown for adenylate cyclase 7.
机译:表型和基因型的可用数据的快速扩展,可用于多种小鼠品系,从而可以开发出新的方法来研究小鼠基因组的功能性遗传扰动。电子计算机制图提供了一种方便的方法,可以将表型性状的自然多样性与祖先遗传的多态性联系起来,以剖析遗传性状。在小鼠中,当前的单核苷酸多态性(SNP)数据缺乏整个基因组的密度和足够的菌株覆盖范围,无法正确实现此目标。为了解决这个问题,在48个近交小鼠品系中,为10,990个均匀间隔的SNP位点产生了470,407个等位基因调用。将SNP集与统计模型一起使用,该统计模型将三个SNP块内的独特模式视为推断的单倍型,可以成功定位已知的单基因性状和克隆的定量性状基因。该方法在高密度脂蛋白和胆结石表型上的应用,该表型是先前表征的数量性状基因座(QTL)的特征。推断的单倍型数据还促进了QTL区域的细化,从而可以更容易地鉴定和表征候选基因,如腺苷酸环化酶7所示。

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