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小鼠生殖细胞发育过程中动态染色质景观和 DNA 甲基化的机制。

The dynamic chromatin landscape and mechanisms of DNA methylation during mouse germ cell development.

机构信息

Department of Stem Cell Biology and Medicine, Graduate School of Medical Sciences, Kyushu University.

出版信息

Genes Genet Syst. 2022 Jun 4;97(1):3-14. doi: 10.1266/ggs.21-00069. Epub 2022 Apr 16.

Abstract

Epigenetic marks including DNA methylation (DNAme) play a critical role in the transcriptional regulation of genes and retrotransposons. Defects in DNAme are detected in infertility, imprinting disorders and congenital diseases in humans, highlighting the broad importance of this epigenetic mark in both development and disease. While DNAme in terminally differentiated cells is stably propagated following cell division by the maintenance DNAme machinery, widespread erasure and subsequent de novo establishment of this epigenetic mark occur early in embryonic development as well as in germ cell development. Combined with deep sequencing, low-input methods that have been developed in the past several years have enabled high-resolution and genome-wide mapping of both DNAme and histone post-translational modifications (PTMs) in rare cell populations including developing germ cells. Epigenome studies using these novel methods reveal an unprecedented view of the dynamic chromatin landscape during germ cell development. Furthermore, integrative analysis of chromatin marks in normal germ cells and in those deficient in chromatin-modifying enzymes uncovers a critical interplay between histone PTMs and de novo DNAme in the germline. This review discusses work on mechanisms of the erasure and subsequent de novo DNAme in mouse germ cells as well as the outstanding questions relating to the regulation of the dynamic chromatin landscape in germ cells.

摘要

表观遗传标记物,包括 DNA 甲基化(DNAme),在基因和逆转座子的转录调控中发挥着关键作用。在人类的不育症、印迹障碍和先天性疾病中,都检测到了 DNAme 的缺陷,这突出表明了这种表观遗传标记在发育和疾病中的广泛重要性。虽然在终末分化细胞中,通过维持 DNAme 机制,DNAme 在细胞分裂后能够稳定地传递,但在胚胎发育早期以及生殖细胞发育过程中,这种表观遗传标记会广泛擦除,并随后重新建立。结合深度测序,过去几年中开发的低输入方法已经能够在包括发育中的生殖细胞在内的稀有细胞群体中,对 DNAme 和组蛋白翻译后修饰(PTMs)进行高分辨率和全基因组作图。使用这些新方法进行的表观基因组研究揭示了生殖细胞发育过程中动态染色质景观的前所未有的观点。此外,在正常生殖细胞和缺乏染色质修饰酶的生殖细胞中对染色质标记物进行综合分析,揭示了组蛋白 PTMs 和新生 DNAme 在生殖系中的关键相互作用。这篇综述讨论了在小鼠生殖细胞中擦除和随后重新建立新生 DNAme 的机制,以及与生殖细胞中动态染色质景观调控相关的悬而未决的问题。

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