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雌性生殖细胞通过调节 PRC2 相互作用蛋白启动 Polycomb 沉默。

Differentiating female germ cells initiate Polycomb silencing by regulating PRC2-interacting proteins.

机构信息

Howard Hughes Medical Institute Research Laboratories Department of Embryology, Carnegie Institution for Science, Baltimore, United States.

出版信息

Elife. 2020 Aug 10;9:e56922. doi: 10.7554/eLife.56922.

Abstract

Polycomb silencing represses gene expression and provides a molecular memory of chromatin state that is essential for animal development. We show that female germline stem cells (GSCs) provide a powerful system for studying Polycomb silencing. GSCs have a non-canonical distribution of PRC2 activity and lack silenced chromatin like embryonic progenitors. As GSC daughters differentiate into nurse cells and oocytes, nurse cells, like embryonic somatic cells, silence genes in traditional Polycomb domains and in generally inactive chromatin. Developmentally controlled expression of two Polycomb repressive complex 2 (PRC2)-interacting proteins, Pcl and Scm, initiate silencing during differentiation. In GSCs, abundant Pcl inhibits PRC2-dependent silencing globally, while in nurse cells Pcl declines and newly induced Scm concentrates PRC2 activity on traditional Polycomb domains. Our results suggest that PRC2-dependent silencing is developmentally regulated by accessory proteins that either increase the concentration of PRC2 at target sites or inhibit the rate that PRC2 samples chromatin.

摘要

多梳抑制沉默基因的表达,并为染色质状态提供分子记忆,这对动物的发育至关重要。我们表明,雌性生殖干细胞 (GSCs) 为研究多梳抑制沉默提供了一个强大的系统。GSCs 中 PRC2 活性呈非典型分布,并且缺乏像胚胎祖细胞那样的沉默染色质。随着 GSC 女儿分化为滋养细胞和卵母细胞,滋养细胞与胚胎体细胞一样,在传统多梳结构域和普遍失活的染色质中沉默基因。两个多梳抑制复合物 2 (PRC2) 相互作用蛋白 Pcl 和 Scm 的发育调控表达在分化过程中启动沉默。在 GSCs 中,丰富的 Pcl 全局抑制 PRC2 依赖性沉默,而在滋养细胞中 Pcl 下降,新诱导的 Scm 将 PRC2 活性集中在传统多梳结构域上。我们的结果表明,PRC2 依赖性沉默受辅助蛋白的发育调控,这些蛋白要么增加 PRC2 在靶位点的浓度,要么抑制 PRC2 对染色质的采样速率。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/30d7/7438113/2784821e5251/elife-56922-fig1.jpg

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