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哺乳动物基因复制后,DNA 甲基化会重新平衡基因剂量。

DNA methylation rebalances gene dosage after mammalian gene duplications.

机构信息

Division of Biostatistics & Bioinformatics, Institute of Population Health Sciences, National Health Research Institutes, Taiwan, Republic of China.

出版信息

Mol Biol Evol. 2012 Jan;29(1):133-44. doi: 10.1093/molbev/msr174. Epub 2011 Aug 6.

Abstract

Although gene duplication plays a major role in organismal evolution, it may also lead to gene dosage imbalance, thereby having an immediate adverse effect on an organism's fitness. Investigating the evolution of the expression patterns of genes that duplicated after the divergence of rodents and primates, we confirm that adaptive evolution has been involved in dosage rebalance after gene duplication. To understand mechanisms underlying this process, we examined 1) microRNA (miRNA)-mediated gene regulation, 2) cis-regulatory sequence modifications, and 3) DNA methylation. Neither miRNA-mediated regulation nor cis-regulatory changes was found to be associated with expression reduction of duplicate genes. By contrast, duplicate genes, especially lowly expressed copies, were heavily methylated in the upstream region. However, for duplicate genes encoding proteins that are members of macromolecular complexes, heavy methylation in the genic region was not consistently observed. This result held after controlling potential confounding factors, such as enrichment in functional categories. Our results suggest that during mammalian evolution, DNA methylation plays a dominant role in dosage rebalance after gene duplication by inhibiting transcription initiation of duplicate genes.

摘要

虽然基因复制在生物进化中起着主要作用,但它也可能导致基因剂量失衡,从而对生物体的适应性产生直接的负面影响。本研究调查了在啮齿动物和灵长类动物分化后复制的基因的表达模式的进化,我们证实适应性进化已经参与了基因复制后的剂量平衡。为了了解这个过程的机制,我们研究了 1)miRNA(microRNA)介导的基因调控,2)顺式调控序列的改变,和 3)DNA 甲基化。miRNA 介导的调控或顺式调控变化都与重复基因的表达减少无关。相比之下,重复基因,特别是低表达的拷贝,在上游区域被高度甲基化。然而,对于编码大分子复合物成员的重复基因,在基因区域中并没有观察到强烈的甲基化。在控制潜在的混杂因素(如功能类别中的富集)后,这一结果仍然成立。我们的研究结果表明,在哺乳动物进化过程中,DNA 甲基化通过抑制重复基因的转录起始,在基因复制后的剂量平衡中发挥主导作用。

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