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人类主要组织相容性复合体中心区域的传递比失真研究。

An investigation of transmission ratio distortion in the central region of the human MHC.

作者信息

Hanchard N, Rockett K, Udalova I, Wilson J, Keating B, Koch O, Nijnik A, Diakite M, Herbert M, Kwiatkowski D

机构信息

Wellcome Trust Centre for Human Genetics, Oxford, UK.

出版信息

Genes Immun. 2006 Jan;7(1):51-8. doi: 10.1038/sj.gene.6364277.

Abstract

Transmission ratio distortion (TRD) describes a significant departure from expected Mendelian inheritance ratios that is fundamental to both the biology of reproduction and statistical genetics. The relatively high fetal wastage in humans, with consequent selection of alleles in utero, makes it likely that TRD is prevalent in the human genome. The central region of the human major histocompatibility complex (MHC) is a strong TRD candidate, as it houses a number of immune and regulatory genes that may be important in pregnancy outcome. We used a nonhaplotype-based method to select 13 tagging SNPs from three central MHC candidate regions, and analysed their transmission in 380 newborns and their parents (1138 individuals). A TRD of 54:46 was noted in favour of the common allele of a promoter SNP in the CLIC1 gene (P = 0.025), with a similar distortion using haplotypes across the same gene region (P = 0.016). We also found evidence that markers in the CLIC1 gene region may have been subject to recent selection (P < 0.001). The study illustrates the potential benefits of screening for TRD and highlights the difficulties encountered therein.

摘要

传递比率失真(TRD)描述了与预期孟德尔遗传比率的显著偏差,这对于生殖生物学和统计遗传学而言都是至关重要的。人类中相对较高的胎儿损耗率,以及随之而来的子宫内等位基因选择,使得TRD很可能在人类基因组中普遍存在。人类主要组织相容性复合体(MHC)的中心区域是TRD的一个有力候选区域,因为它包含许多可能对妊娠结局很重要的免疫和调节基因。我们使用一种基于非单倍型的方法从三个MHC中心候选区域中选择了13个标签单核苷酸多态性(tagging SNPs),并分析了它们在380名新生儿及其父母(共1138人)中的传递情况。在CLIC1基因的一个启动子SNP的常见等位基因上观察到54:46的TRD(P = 0.025),在同一基因区域使用单倍型时也有类似的失真情况(P = 0.016)。我们还发现有证据表明CLIC1基因区域的标记可能经历了近期的选择(P < 0.001)。该研究说明了筛查TRD的潜在益处,并突出了其中遇到的困难。

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