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蛋白编码和调控变化对鼠形亚目啮齿动物适应性分子进化的贡献。

Contributions of protein-coding and regulatory change to adaptive molecular evolution in murid rodents.

机构信息

Institute of Evolutionary Biology, University of Edinburgh, Edinburgh, United Kingdom.

出版信息

PLoS Genet. 2013;9(12):e1003995. doi: 10.1371/journal.pgen.1003995. Epub 2013 Dec 5.

Abstract

The contribution of regulatory versus protein change to adaptive evolution has long been controversial. In principle, the rate and strength of adaptation within functional genetic elements can be quantified on the basis of an excess of nucleotide substitutions between species compared to the neutral expectation or from effects of recent substitutions on nucleotide diversity at linked sites. Here, we infer the nature of selective forces acting in proteins, their UTRs and conserved noncoding elements (CNEs) using genome-wide patterns of diversity in wild house mice and divergence to related species. By applying an extension of the McDonald-Kreitman test, we infer that adaptive substitutions are widespread in protein-coding genes, UTRs and CNEs, and we estimate that there are at least four times as many adaptive substitutions in CNEs and UTRs as in proteins. We observe pronounced reductions in mean diversity around nonsynonymous sites (whether or not they have experienced a recent substitution). This can be explained by selection on multiple, linked CNEs and exons. We also observe substantial dips in mean diversity (after controlling for divergence) around protein-coding exons and CNEs, which can also be explained by the combined effects of many linked exons and CNEs. A model of background selection (BGS) can adequately explain the reduction in mean diversity observed around CNEs. However, BGS fails to explain the wide reductions in mean diversity surrounding exons (encompassing ~100 Kb, on average), implying that there is a substantial role for adaptation within exons or closely linked sites. The wide dips in diversity around exons, which are hard to explain by BGS, suggest that the fitness effects of adaptive amino acid substitutions could be substantially larger than substitutions in CNEs. We conclude that although there appear to be many more adaptive noncoding changes, substitutions in proteins may dominate phenotypic evolution.

摘要

调控变化与蛋白质变化对适应性进化的贡献一直存在争议。原则上,可以根据物种之间核苷酸替换的过剩来定量评估功能遗传元件内的适应速度和强度,这种过剩超过了中性预期,或者可以根据近期替换对连锁位点核苷酸多样性的影响来定量评估。在这里,我们使用野生家鼠的全基因组多样性模式及其与相关物种的分化,推断作用于蛋白质、其 UTR 和保守非编码元件 (CNE) 的选择压力的性质。通过应用 McDonald-Kreitman 检验的扩展,我们推断适应性替换在蛋白质编码基因、UTR 和 CNE 中广泛存在,并且我们估计 CNE 和 UTR 中的适应性替换至少是蛋白质中的四倍。我们观察到非同义位点(无论它们是否经历了近期替换)周围的平均多样性明显降低。这可以通过对多个连锁 CNE 和外显子的选择来解释。我们还观察到蛋白质编码外显子和 CNE 周围的平均多样性(在控制了分化之后)有显著下降,这也可以通过许多连锁外显子和 CNE 的共同作用来解释。背景选择 (BGS) 的模型可以充分解释 CNE 周围观察到的平均多样性减少。然而,BGS 无法解释外显子周围广泛的平均多样性降低(平均约 100 Kb),这意味着外显子或紧密连锁的位点内存在大量的适应性。外显子周围多样性的广泛下降,很难用 BGS 来解释,这表明适应性氨基酸替换的适应度效应可能比 CNE 中的替换大得多。我们得出的结论是,尽管似乎有更多的适应性非编码变化,但蛋白质中的替换可能主导表型进化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0d95/3854965/82452b8165ae/pgen.1003995.g001.jpg

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