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定义基因组甲基化模式精细和粗糙结构的染色质和序列特征。

Chromatin and sequence features that define the fine and gross structure of genomic methylation patterns.

机构信息

Center for Pharmacogenomics, Department of Medicine, Washington University School of Medicine, St. Louis, Missouri 63110, USA.

出版信息

Genome Res. 2010 Jul;20(7):972-80. doi: 10.1101/gr.101535.109. Epub 2010 May 20.

Abstract

Abnormalities of genomic methylation patterns are lethal or cause disease, but the cues that normally designate CpG dinucleotides for methylation are poorly understood. We have developed a new method of methylation profiling that has single-CpG resolution and can address the methylation status of repeated sequences. We have used this method to determine the methylation status of >275 million CpG sites in human and mouse DNA from breast and brain tissues. Methylation density at most sequences was found to increase linearly with CpG density and to fall sharply at very high CpG densities, but transposons remained densely methylated even at higher CpG densities. The presence of histone H2A.Z and histone H3 di- or trimethylated at lysine 4 correlated strongly with unmethylated DNA and occurred primarily at promoter regions. We conclude that methylation is the default state of most CpG dinucleotides in the mammalian genome and that a combination of local dinucleotide frequencies, the interaction of repeated sequences, and the presence or absence of histone variants or modifications shields a population of CpG sites (most of which are in and around promoters) from DNA methyltransferases that lack intrinsic sequence specificity.

摘要

基因组甲基化模式的异常是致命的或导致疾病的,但正常指定 CpG 二核苷酸进行甲基化的线索知之甚少。我们开发了一种新的甲基化分析方法,具有单 CpG 分辨率,可以解决重复序列的甲基化状态问题。我们使用这种方法来确定来自乳腺和脑组织的人类和小鼠 DNA 中超过 2750 万个 CpG 位点的甲基化状态。大多数序列的甲基化密度被发现与 CpG 密度呈线性增加,并在非常高的 CpG 密度下急剧下降,但转座子即使在更高的 CpG 密度下仍保持高度甲基化。组蛋白 H2A.Z 和组蛋白 H3 赖氨酸 4 二甲基化或三甲基化的存在与未甲基化的 DNA 强烈相关,主要发生在启动子区域。我们得出结论,甲基化是哺乳动物基因组中大多数 CpG 二核苷酸的默认状态,局部二核苷酸频率的组合、重复序列的相互作用以及组蛋白变体或修饰的存在或缺失,使一群 CpG 位点(其中大多数位于启动子及其周围)免受缺乏固有序列特异性的 DNA 甲基转移酶的影响。

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