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位置相关的 DNA 甲基化与哺乳动物编码外显子进化率的相关性。

Position-dependent correlations between DNA methylation and the evolutionary rates of mammalian coding exons.

机构信息

Physical and Computational Genomics Division, Genomics Research Center, Academia Sinica, Taipei 115, Taiwan.

出版信息

Proc Natl Acad Sci U S A. 2012 Sep 25;109(39):15841-6. doi: 10.1073/pnas.1208214109. Epub 2012 Sep 10.

Abstract

DNA cytosine methylation is a central epigenetic marker that is usually mutagenic and may increase the level of sequence divergence. However, methylated genes have been reported to evolve more slowly than unmethylated genes. Hence, there is a controversy on whether DNA methylation is correlated with increased or decreased protein evolutionary rates. We hypothesize that this controversy has resulted from the differential correlations between DNA methylation and the evolutionary rates of coding exons in different genic positions. To test this hypothesis, we compare human-mouse and human-macaque exonic evolutionary rates against experimentally determined single-base resolution DNA methylation data derived from multiple human cell types. We show that DNA methylation is significantly related to within-gene variations in evolutionary rates. First, DNA methylation level is more strongly correlated with C-to-T mutations at CpG dinucleotides in the first coding exons than in the internal and last exons, although it is positively correlated with the synonymous substitution rate in all exon positions. Second, for the first exons, DNA methylation level is negatively correlated with exonic expression level, but positively correlated with both nonsynonymous substitution rate and the sample specificity of DNA methylation level. For the internal and last exons, however, we observe the opposite correlations. Our results imply that DNA methylation level is differentially correlated with the biological (and evolutionary) features of coding exons in different genic positions. The first exons appear more prone to the mutagenic effects, whereas the other exons are more influenced by the regulatory effects of DNA methylation.

摘要

DNA 胞嘧啶甲基化是一种重要的表观遗传标记,通常具有诱变作用,可能会增加序列分歧程度。然而,已报道甲基化基因的进化速度比非甲基化基因慢。因此,关于 DNA 甲基化是否与蛋白质进化率的增加或减少有关存在争议。我们假设这种争议源于 DNA 甲基化与不同基因位置编码外显子进化率之间的相关性差异。为了验证这一假设,我们比较了人类-鼠和人类-恒河猴的外显子进化率与从多种人类细胞类型中获得的实验确定的单碱基分辨率 DNA 甲基化数据。结果表明,DNA 甲基化与基因内进化率的变化显著相关。首先,DNA 甲基化水平与第一个编码外显子中 CpG 二核苷酸的 C 到 T 突变相关性更强,而与所有外显子位置的同义替换率呈正相关。其次,对于第一个外显子,DNA 甲基化水平与外显子表达水平呈负相关,但与非同义替换率和 DNA 甲基化水平的样本特异性呈正相关。然而,对于内部和最后外显子,我们观察到相反的相关性。我们的结果表明,DNA 甲基化水平与不同基因位置编码外显子的生物学(和进化)特征呈差异相关。第一个外显子似乎更容易受到诱变作用的影响,而其他外显子则更容易受到 DNA 甲基化的调控作用的影响。

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Assessing determinants of exonic evolutionary rates in mammals.评估哺乳动物外显子进化率的决定因素。
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