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选择作用下的基因型推断的危害:以乳糖酶基因区域为例的案例研究。

The hazards of genotype imputation in chromosomal regions under selection: A case study using the Lactase gene region.

机构信息

University College London Research Department of Genetics Evolution and Environment, London, UK.

出版信息

Ann Hum Genet. 2022 Jan;86(1):24-33. doi: 10.1111/ahg.12444. Epub 2021 Sep 15.

Abstract

Although imputation of missing SNP results has been widely used in genetic studies, claims about the quality and usefulness of imputation have outnumbered the few studies that have questioned its limitations. But it is becoming clear that these limitations are real-for example, disease association signals can be missed in regions of LD breakdown. Here, as a case study, using the chromosomal region of the well-known lactase gene, LCT, we address the issue of imputation in the context of variants that have become frequent in a limited number of modern population groups only recently, due to selection. We study SNPs in a 500 bp region covering the enhancer of LCT, and compare imputed genotypes with directly genotyped data. We examine the haplotype pairs of all individuals with discrepant and missing genotypes. We highlight the nonrandom nature of the allelic errors and show that most incorrect imputations and missing data result from long haplotypes that are evolutionarily closely related to those carrying the derived alleles, while some relate to rare and recombinant haplotypes. We conclude that bias of incorrectly imputed and missing genotypes can decrease the accuracy of imputed results substantially.

摘要

虽然缺失 SNP 结果的推断已在遗传研究中广泛使用,但对其质量和有用性的断言却超过了为数不多的质疑其局限性的研究。但现在越来越清楚的是,这些局限性是真实存在的,例如,在 LD 断裂的区域,疾病关联信号可能会丢失。在这里,我们将乳糖酶基因(LCT)的染色体区域作为一个案例研究,针对由于选择而在最近仅在少数现代人群中变得频繁的变体,探讨推断中的问题。我们研究了覆盖 LCT 增强子的 500bp 区域内的 SNP,并将推断的基因型与直接基因分型数据进行比较。我们检查了所有具有不一致和缺失基因型的个体的单倍型对。我们强调了等位基因错误的非随机性,并表明大多数错误的推断和缺失数据是由与携带衍生等位基因的序列进化上密切相关的长单倍型引起的,而有些则与罕见的重组单倍型有关。我们得出结论,不正确推断和缺失基因型的偏差会大大降低推断结果的准确性。

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