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核小体DNA的不对称解旋会促使组蛋白核心发生不对称开放和解离。

Asymmetric unwrapping of nucleosomal DNA propagates asymmetric opening and dissociation of the histone core.

作者信息

Chen Yujie, Tokuda Joshua M, Topping Traci, Meisburger Steve P, Pabit Suzette A, Gloss Lisa M, Pollack Lois

机构信息

School of Applied and Engineering Physics, Cornell University, Ithaca, NY 14853.

School of Molecular Biosciences, Washington State University, Pullman, WA 99164.

出版信息

Proc Natl Acad Sci U S A. 2017 Jan 10;114(2):334-339. doi: 10.1073/pnas.1611118114. Epub 2016 Dec 27.

Abstract

The nucleosome core particle (NCP) is the basic structural unit for genome packaging in eukaryotic cells and consists of DNA wound around a core of eight histone proteins. DNA access is modulated through dynamic processes of NCP disassembly. Partly disassembled structures, such as the hexasome (containing six histones) and the tetrasome (four histones), are important for transcription regulation in vivo. However, the pathways for their formation have been difficult to characterize. We combine time-resolved (TR) small-angle X-ray scattering and TR-FRET to correlate changes in the DNA conformations with composition of the histone core during salt-induced disassembly of canonical NCPs. We find that H2A-H2B histone dimers are released sequentially, with the first dimer being released after the DNA has formed an asymmetrically unwrapped, teardrop-shape DNA structure. This finding suggests that the octasome-to-hexasome transition is guided by the asymmetric unwrapping of the DNA. The link between DNA structure and histone composition suggests a potential mechanism for the action of proteins that alter nucleosome configurations such as histone chaperones and chromatin remodeling complexes.

摘要

核小体核心颗粒(NCP)是真核细胞中基因组包装的基本结构单元,由缠绕在八个组蛋白核心周围的DNA组成。DNA的可及性通过NCP解聚的动态过程进行调节。部分解聚的结构,如六体(包含六个组蛋白)和四体(四个组蛋白),对体内转录调控很重要。然而,它们的形成途径一直难以表征。我们结合时间分辨(TR)小角X射线散射和TR-FRET,以关联在盐诱导的经典NCP解聚过程中DNA构象变化与组蛋白核心组成的变化。我们发现H2A-H2B组蛋白二聚体是顺序释放的,第一个二聚体在DNA形成不对称解旋的泪滴状DNA结构后释放。这一发现表明八体到六体的转变是由DNA的不对称解旋引导的。DNA结构与组蛋白组成之间的联系提示了改变核小体构型的蛋白质(如组蛋白伴侣和染色质重塑复合物)发挥作用的潜在机制。

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