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特异性非 CG DNA 甲基化标记雌性小鼠大脑中活性染色质的结构域。

Allele-specific non-CG DNA methylation marks domains of active chromatin in female mouse brain.

机构信息

Department of Cognitive Science, University of California, San Diego, CA 92037.

Department of Pathology, University of Washington, Seattle, WA 98195.

出版信息

Proc Natl Acad Sci U S A. 2017 Apr 4;114(14):E2882-E2890. doi: 10.1073/pnas.1611905114. Epub 2017 Mar 20.

Abstract

DNA methylation at gene promoters in a CG context is associated with transcriptional repression, including at genes silenced on the inactive X chromosome in females. Non-CG methylation (mCH) is a distinct feature of the neuronal epigenome that is differentially distributed between males and females on the X chromosome. However, little is known about differences in mCH on the active (Xa) and inactive (Xi) X chromosomes because stochastic X-chromosome inactivation (XCI) confounds allele-specific epigenomic profiling. We used whole-genome bisulfite sequencing in a mouse model with nonrandom XCI to examine allele-specific DNA methylation in frontal cortex. Xi was largely devoid of mCH, whereas Xa contained abundant mCH similar to the male X chromosome and the autosomes. In contrast to the repressive association of DNA methylation at CG dinucleotides (mCG), mCH accumulates on Xi in domains with transcriptional activity, including the bodies of most genes that escape XCI and at the X-inactivation center, validating this epigenetic mark as a signature of transcriptional activity. Escape genes showing CH hypermethylation were the only genes with CG-hypomethylated promoters on Xi, a well-known mark of active transcription. Finally, we found extensive allele-specific mCH and mCG at autosomal imprinted regions, some with a negative correlation between methylation in the two contexts, further supporting their distinct functions. Our findings show that neuronal mCH functions independently of mCG and is a highly dynamic epigenomic correlate of allele-specific gene regulation.

摘要

CG 环境下基因启动子的 DNA 甲基化与转录抑制有关,包括女性中失活 X 染色体上基因的沉默。非 CG 甲基化(mCH)是神经元表观基因组的一个独特特征,在 X 染色体上的男性和女性之间存在差异分布。然而,由于随机 X 染色体失活(XCI)混淆了等位基因特异性表观基因组分析,因此对于活性(Xa)和失活(Xi)X 染色体上 mCH 的差异知之甚少。我们使用非随机 XCI 的小鼠模型进行全基因组亚硫酸氢盐测序,以检查额皮质中等位基因特异性 DNA 甲基化。Xi 基本上不含 mCH,而 Xa 则含有丰富的 mCH,类似于雄性 X 染色体和常染色体。与 CG 二核苷酸(mCG)DNA 甲基化的抑制性关联相反,mCH 在转录活性区域(包括逃避 XCI 的大多数基因的体和 X 失活中心)上在 Xi 上积累,验证了这种表观遗传标记是转录活性的标志。表现出 CH 高甲基化的逃避基因是 Xi 上仅具有 CG 低甲基化启动子的唯一基因,这是活跃转录的一个众所周知的标志。最后,我们在常染色体印迹区域发现了广泛的等位基因特异性 mCH 和 mCG,其中一些在这两种情况下的甲基化之间存在负相关,进一步支持了它们的不同功能。我们的研究结果表明,神经元 mCH 独立于 mCG 发挥作用,是等位基因特异性基因调控的高度动态表观基因组相关物。

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