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WFDC8(短期平衡)在欧洲人和 SPINT4(不完全选择清除)在非洲人中的进化历史不同。

Differing evolutionary histories of WFDC8 (short-term balancing) in Europeans and SPINT4 (incomplete selective sweep) in Africans.

机构信息

Institute of Molecular Pathology and Immunology of the University of Porto, Porto, Portugal.

出版信息

Mol Biol Evol. 2011 Oct;28(10):2811-22. doi: 10.1093/molbev/msr106. Epub 2011 May 2.

Abstract

The whey acidic protein four-disulfide core (WFDC) gene cluster on human chromosome 20q13, harbors 15 small serine protease inhibitor genes with roles in innate immunity, reproduction, and regulation of endogenous proteases kallikreins. The WFDC cluster has emerged as a prime example of rapid diversification and adaptive evolution in primates. This study sought a better understanding of the evolutionary history of WFDC genes in humans and focused on exploring the adaptive selection signatures found in populations of European (Utah residents with ancestry from northern and western Europe [CEU]) and African (Yoruba from Ibadan, in Nigeria [YRI]) ancestry in a genome-wide scan for putative targets of recent adaptive selection. Our approach included resequencing coding and noncoding regions of WFDC6, EPPIN, and WFDC8 in 20 CEU and of SPINT4 in 20 YRI individuals. We generated 302 kb and 60 kb of high-quality sequence data from CEU and of YRI populations, respectively, enabling the identification of 72 single nucleotide polymorphisms. Using classic neutrality tests, empirical and haplotype-based analysis, we pinpointed WFDC8 and SPINT4 as the likely targets of short-term balancing selection in the CEU population, and recent positive selection (incomplete selective sweep) in the YRI population. Putative candidate variants targeted by selection include 44A (rs7273669A) for WFDC8, which may downregulate gene expression by abolishing the binding site of two transcription factors; and a haplotype configuration [Ser73+98A] (rs6017667A-rs6032474A) for SPINT4, which may simultaneously affect protein function and gene regulation. We propose that the evolution of WFDC8 and SPINT4 has been shaped by complex selective scenarios due to the interdependence of variant fitness and ecological variables.

摘要

人类染色体 20q13 上的乳清酸性蛋白四硫键核心 (WFDC) 基因簇,包含 15 个小丝氨酸蛋白酶抑制剂基因,在先天免疫、生殖和内源性蛋白酶激肽释放酶的调节中发挥作用。WFDC 簇已成为灵长类动物快速多样化和适应性进化的主要范例。本研究旨在更好地了解人类 WFDC 基因的进化历史,并专注于探索欧洲(犹他州居民,祖先来自北欧和西欧 [CEU])和非洲(尼日利亚伊巴丹的约鲁巴人 [YRI])人群中 WFDC 基因的适应性选择特征,进行全基因组扫描以寻找最近适应性选择的潜在目标。我们的方法包括对 20 个 CEU 和 20 个 YRI 个体中的 WFDC6、EPPIN 和 WFDC8 的编码和非编码区域以及 SPINT4 进行重新测序。我们从 CEU 和 YRI 人群中分别生成了 302 kb 和 60 kb 的高质量序列数据,从而能够鉴定出 72 个单核苷酸多态性。使用经典中性测试、经验和基于单倍型的分析,我们确定 WFDC8 和 SPINT4 是 CEU 人群中短期平衡选择的可能目标,而 YRI 人群中存在近期正选择(不完全选择清除)。选择的候选变体包括 WFDC8 的 44A(rs7273669A),它可能通过破坏两个转录因子的结合位点来下调基因表达;以及 SPINT4 的单倍型配置 [Ser73+98A](rs6017667A-rs6032474A),它可能同时影响蛋白质功能和基因调控。我们提出,WFDC8 和 SPINT4 的进化受到复杂选择情景的影响,这是由于变体适应性和生态变量的相互依存关系所致。

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