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连接组蛋白缺失的染色质中核小体核心结构的改变。

Alterations in nucleosome core structure in linker histone-depleted chromatin.

作者信息

Usachenko S I, Gavin I M, Bavykin S G

机构信息

W. A. Engelhardt Institute of Molecular Biology, Academy of Sciences of Russia, Vavilova, 32, 117984 Moscow B-334, Russia.

出版信息

J Biol Chem. 1996 Feb 16;271(7):3831-6. doi: 10.1074/jbc.271.7.3831.

Abstract

We have previously shown that the sequential arrangement of histone-DNA contacts is essentially the same in the nucleosomal core of sea urchin sperm nuclei, where chromatin is highly condensed and repressed, and in nuclei from lily bud sepals or yeast, where chromatin is highly active in transcription and replication and is significantly or completely depleted of histone H1. However, the difference in the strength of some histone-DNA contacts has not been understood or discussed. In this work, we demonstrate that some of these differences are due to a conformational change in the nucleosomal core. We show that the nucleosomal core in linker histone-depleted chromatin is in a different conformational state compared with the nucleosomal core in folded chromatin or in isolated core nucleosomes. This conformational state is characterized by altered strengths in the histone H4 and H2A/H2B contacts with the regions of sharply bent nucleosomal DNA around sites +/-1 and +/-4 and site +/-5, respectively. We demonstrate that this conformation, which we call the "stretched nucleosome," is a general feature of unfolded linker histone-depleted chromatin and may occur during chromatin activation. Our results suggest that this nucleosome structural alteration does not depend on chromatin sources and histone variants studied in this work. In addition, we show that this alteration is reversible and is caused by the stretching of linker DNA during chromatin unfolding.

摘要

我们之前已经表明,在海胆精子细胞核的核小体核心中,组蛋白与DNA的接触顺序基本相同,在那里染色质高度浓缩且受到抑制;而在百合花蕾萼片或酵母的细胞核中,染色质在转录和复制中高度活跃,并且组蛋白H1显著或完全缺失,组蛋白与DNA的接触顺序也基本相同。然而,一些组蛋白与DNA接触强度的差异尚未得到理解或讨论。在这项工作中,我们证明其中一些差异是由于核小体核心的构象变化所致。我们表明,与折叠染色质或分离的核心核小体中的核小体核心相比,缺乏连接组蛋白的染色质中的核小体核心处于不同的构象状态。这种构象状态的特征是,组蛋白H4与核小体DNA在±1和±4位点附近急剧弯曲区域的接触强度改变,以及组蛋白H2A/H2B与核小体DNA在±5位点的接触强度改变。我们证明这种构象,我们称之为“拉伸核小体”,是缺乏连接组蛋白的未折叠染色质的一个普遍特征,并且可能在染色质激活过程中出现。我们的结果表明,这种核小体结构改变不依赖于本研究中所研究的染色质来源和组蛋白变体。此外,我们表明这种改变是可逆的,并且是由染色质解折叠过程中连接DNA的拉伸所引起的。

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