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Alu元件突变谱:分子钟与DNA甲基化的影响

Alu element mutation spectra: molecular clocks and the effect of DNA methylation.

作者信息

Xing Jinchuan, Hedges Dale J, Han Kyudong, Wang Hui, Cordaux Richard, Batzer Mark A

机构信息

Department of Biological Sciences, Biological Computation and Visualization Center, Center for Bio-Modular Microsystems, Louisiana State University, 202 Life Sciences Building, Baton Rouge, LA 70803, USA.

出版信息

J Mol Biol. 2004 Nov 26;344(3):675-82. doi: 10.1016/j.jmb.2004.09.058.

DOI:10.1016/j.jmb.2004.09.058
PMID:15533437
Abstract

In primate genomes more than 40% of CpG islands are found within repetitive elements. With more than one million copies in the human genome, the Alu family of retrotransposons represents the most successful short interspersed element (SINE) in primates and CpG dinucleotides make up about 20% of Alu sequences. It is generally thought that CpG dinucleotides mutate approximately ten times faster than other dinucleotides due to cytosine methylation and the subsequent deamination and conversion of C-->T. However, the disparity of Alu subfamily age estimations based upon CpG or non-CpG substitution density indicates a more complex relationship between CpG and non-CpG substitutions within the Alu elements. Here we report an analysis of the mutation patterns for 5296 Alu elements comprising 20 subfamilies. Our results indicate a relatively constant CpG versus non-CpG substitution ratio of approximately 6 for the young (AluY) and intermediate (AluS) Alu subfamilies. However, a more complex non-linear relationship between CpG and non-CpG substitutions was observed when old (AluJ) subfamilies were included in the analysis. These patterns may be the result of the slowdown of the neutral mutation rate during primate evolution and/or an increase in the CpG mutation rate as the consequence of increased DNA methylation in response to a burst of retrotransposition activity approximately 35 million years ago.

摘要

在灵长类动物基因组中,超过40%的CpG岛存在于重复元件内。逆转录转座子的Alu家族在人类基因组中有超过一百万个拷贝,是灵长类动物中最成功的短散在元件(SINE),并且CpG二核苷酸约占Alu序列的20%。一般认为,由于胞嘧啶甲基化以及随后的脱氨作用和C→T的转换,CpG二核苷酸的突变速度比其他二核苷酸快约十倍。然而,基于CpG或非CpG取代密度对Alu亚家族年龄的估计存在差异,这表明Alu元件内CpG和非CpG取代之间的关系更为复杂。在此,我们报告了对包含20个亚家族的5296个Alu元件的突变模式分析。我们的结果表明,对于年轻的(AluY)和中间的(AluS)Alu亚家族,CpG与非CpG取代率相对恒定,约为6。然而,当将古老的(AluJ)亚家族纳入分析时,观察到CpG和非CpG取代之间存在更复杂的非线性关系。这些模式可能是灵长类动物进化过程中中性突变率减缓的结果,和/或大约3500万年前逆转录转座活性爆发导致DNA甲基化增加,从而使CpG突变率上升的结果。

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