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从多态性和分化模式推断作用于人类候选顺式调控区域的进化过程。

Evolutionary processes acting on candidate cis-regulatory regions in humans inferred from patterns of polymorphism and divergence.

作者信息

Torgerson Dara G, Boyko Adam R, Hernandez Ryan D, Indap Amit, Hu Xiaolan, White Thomas J, Sninsky John J, Cargill Michele, Adams Mark D, Bustamante Carlos D, Clark Andrew G

机构信息

Department of Molecular Biology and Genetics, Cornell University, Ithaca, New York, USA.

出版信息

PLoS Genet. 2009 Aug;5(8):e1000592. doi: 10.1371/journal.pgen.1000592. Epub 2009 Aug 7.

Abstract

Analysis of polymorphism and divergence in the non-coding portion of the human genome yields crucial information about factors driving the evolution of gene regulation. Candidate cis-regulatory regions spanning more than 15,000 genes in 15 African Americans and 20 European Americans were re-sequenced and aligned to the chimpanzee genome in order to identify potentially functional polymorphism and to characterize and quantify departures from neutral evolution. Distortions of the site frequency spectra suggest a general pattern of selective constraint on conserved non-coding sites in the flanking regions of genes (CNCs). Moreover, there is an excess of fixed differences that cannot be explained by a Gamma model of deleterious fitness effects, suggesting the presence of positive selection on CNCs. Extensions of the McDonald-Kreitman test identified candidate cis-regulatory regions with high probabilities of positive and negative selection near many known human genes, the biological characteristics of which exhibit genome-wide trends that differ from patterns observed in protein-coding regions. Notably, there is a higher probability of positive selection in candidate cis-regulatory regions near genes expressed in the fetal brain, suggesting that a larger portion of adaptive regulatory changes has occurred in genes expressed during brain development. Overall we find that natural selection has played an important role in the evolution of candidate cis-regulatory regions throughout hominid evolution.

摘要

对人类基因组非编码部分的多态性和分化进行分析,可得出有关驱动基因调控进化因素的关键信息。对15名非裔美国人和20名欧裔美国人中跨越15000多个基因的候选顺式调控区域进行重测序,并与黑猩猩基因组比对,以识别潜在的功能性多态性,并表征和量化与中性进化的偏差。位点频率谱的畸变表明了对基因侧翼区域保守非编码位点(CNCs)的选择性限制的一般模式。此外,存在大量固定差异,无法用有害适应性效应的伽马模型来解释,这表明在CNCs上存在正选择。麦克唐纳-克赖特曼检验的扩展确定了许多已知人类基因附近具有高正选择和负选择概率的候选顺式调控区域,其生物学特征呈现出全基因组范围的趋势,与在蛋白质编码区域观察到的模式不同。值得注意的是,在胎儿大脑中表达的基因附近的候选顺式调控区域中,正选择的概率更高,这表明在大脑发育过程中表达的基因中发生了更大比例的适应性调控变化。总体而言,我们发现自然选择在整个人科动物进化过程中候选顺式调控区域的进化中发挥了重要作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/631d/2714078/4bd2183ff646/pgen.1000592.g001.jpg

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