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组蛋白变体 H2A.B-H2B 二聚体在核小体中可自发与典型的 H2A-H2B 进行交换。

Histone variant H2A.B-H2B dimers are spontaneously exchanged with canonical H2A-H2B in the nucleosome.

机构信息

Laboratory of Chromatin Structure and Function, Institute for Quantitative Biosciences, The University of Tokyo, Bunkyo-ku, Tokyo, Japan.

Department of Biological Sciences, Graduate School of Science, The University of Tokyo, Bunkyo-ku, Tokyo, Japan.

出版信息

Commun Biol. 2021 Feb 12;4(1):191. doi: 10.1038/s42003-021-01707-z.

Abstract

H2A.B is an evolutionarily distant histone H2A variant that accumulates on DNA repair sites, DNA replication sites, and actively transcribing regions in genomes. In cells, H2A.B exchanges rapidly in chromatin, but the mechanism has remained enigmatic. In the present study, we found that the H2A.B-H2B dimer incorporated within the nucleosome exchanges with the canonical H2A-H2B dimer without assistance from additional factors, such as histone chaperones and nucleosome remodelers. High-speed atomic force microscopy revealed that the H2A.B nucleosome, but not the canonical H2A nucleosome, transiently forms an intermediate "open conformation", in which two H2A.B-H2B dimers may be detached from the H3-H4 tetramer and bind to the DNA regions near the entry/exit sites. Mutational analyses revealed that the H2A.B C-terminal region is responsible for the adoption of the open conformation and the H2A.B-H2B exchange in the nucleosome. These findings provide mechanistic insights into the histone exchange of the H2A.B nucleosome.

摘要

H2A.B 是一种进化上较远的组蛋白 H2A 变体,它在基因组中的 DNA 修复位点、DNA 复制位点和活跃转录区域积累。在细胞中,H2A.B 在染色质中快速交换,但机制仍然神秘。在本研究中,我们发现核小体中的 H2A.B-H2B 二聚体在没有组蛋白伴侣和核小体重塑因子等额外因子的帮助下,与经典的 H2A-H2B 二聚体交换。高速原子力显微镜显示,H2A.B 核小体而不是经典的 H2A 核小体,暂时形成一种中间的“开放构象”,其中两个 H2A.B-H2B 二聚体可能从 H3-H4 四聚体上脱离,并与进入/退出位点附近的 DNA 区域结合。突变分析表明,H2A.B 末端区域负责核小体中开放构象的形成和 H2A.B-H2B 的交换。这些发现为 H2A.B 核小体的组蛋白交换提供了机制上的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ca1f/7881002/0d8f329505e2/42003_2021_1707_Fig1_HTML.jpg

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