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Genome-Wide Identification of Regulatory Sequences Undergoing Accelerated Evolution in the Human Genome

机译:人类基因组中加速进化的调控序列的全基因组鉴定

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摘要

Accelerated evolution of regulatory sequence can alter the expression pattern of target genes, and cause phenotypic changes. In this study, we used DNase I hypersensitive sites (DHSs) to annotate putative regulatory sequences in the human genome, and conducted a genome-wide analysis of the effects of accelerated evolution on regulatory sequences. Working under the assumption that local ancient repeat elements of DHSs are under neutral evolution, we discovered that ∼0.44% of DHSs are under accelerated evolution (ace-DHSs). We found that ace-DHSs tend to be more active than background DHSs, and are strongly associated with epigenetic marks of active transcription. The target genes of ace-DHSs are significantly enriched in neuron-related functions, and their expression levels are positively selected in the human brain. Thus, these lines of evidences strongly suggest that accelerated evolution on regulatory sequences plays important role in the evolution of human-specific phenotypes.
机译:调控序列的加速进化可以改变靶基因的表达模式,并引起表型变化。在这项研究中,我们使用DNase I超敏位点(DHS)注释人类基因组中假定的调控序列,并对加速进化对调控序列的影响进行了全基因组分析。在假设DHS的本地古代重复元素处于中性进化的假设下,我们发现约0.44%的DHS处于加速进化(ace-DHS)。我们发现ace-DHS比背景DHS更具活性,并且与主动转录的表观遗传标记密切相关。 ace-DHS的靶基因在神经元相关功能中显着丰富,并且它们在人脑中的表达水平得到了积极的选择。因此,这些证据强烈表明,调控序列的加速进化在人类特异性表型的进化中起着重要作用。

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