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Combinatorial Conflicting Homozygosity (CCH) analysis enables the rapid identification of shared genomic regions in the presence of multiple phenocopies

机译:组合冲突纯合性(CCH)分析可在存在多个表型的情况下快速鉴定共享的基因组区域

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摘要

BackgroundThe ability to identify regions of the genome inherited with a dominant trait in one or more families has become increasingly valuable with the wide availability of high throughput sequencing technology. While a number of methods exist for mapping of homozygous variants segregating with recessive traits in consanguineous families, dominant conditions are conventionally analysed by linkage analysis, which requires computationally demanding haplotype reconstruction from marker genotypes and, even using advanced parallel approximation implementations, can take substantial time, particularly for large pedigrees. In addition, linkage analysis lacks sensitivity in the presence of phenocopies (individuals sharing the trait but not the genetic variant responsible). Combinatorial Conflicting Homozygosity (CCH) analysis uses high density biallelic single nucleotide polymorphism (SNP) marker genotypes to identify genetic loci within which consecutive markers are not homozygous for different alleles. This allows inference of identical by descent (IBD) inheritance of a haplotype among a set or subsets of related or unrelated individuals.
机译:背景技术随着高通量测序技术的广泛应用,鉴定一个或多个家族中具有显性性状遗传的基因组区域的能力变得越来越有价值。虽然有许多方法可以绘制近亲家庭中隐性性状分离的纯合变异体的图谱,但通常通过连锁分析来分析优势条件,这需要从标记基因型上计算出需要单倍型的重建,即使使用高级的并行近似实现,也可能要花费大量时间,特别是对于大型血统书。此外,连锁分析缺乏对表型(个体共享特征但不负责任的遗传变异)的敏感性。组合冲突纯合性(CCH)分析使用高密度双等位基因单核苷酸多态性(SNP)标记基因型来鉴定遗传位点,其中连续的标记对于不同等位基因不是纯合的。这允许在相关或不相关个体的集合或子集中的单倍型通过继承(IBD)继承进行推断。

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