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ATP 依赖的核小体重塑

ATP-dependent nucleosome remodeling.

作者信息

Becker Peter B, Hörz Wolfram

机构信息

Adolf-Butenandt-Institut, Molekularbiologie, 80336 Munich, Germany.

出版信息

Annu Rev Biochem. 2002;71:247-73. doi: 10.1146/annurev.biochem.71.110601.135400. Epub 2001 Nov 9.

Abstract

It has been a long-standing challenge to decipher the principles that enable cells to both organize their genomes into compact chromatin and ensure that the genetic information remains accessible to regulatory factors and enzymes within the confines of the nucleus. The discovery of nucleosome remodeling activities that utilize the energy of ATP to render nucleosomal DNA accessible has been a great leap forward. In vitro, these enzymes weaken the tight wrapping of DNA around the histone octamers, thereby facilitating the sliding of histone octamers to neighboring DNA segments, their displacement to unlinked DNA, and the accumulation of patches of accessible DNA on the surface of nucleosomes. It is presumed that the collective action of these enzymes endows chromatin with dynamic properties that govern all nuclear functions dealing with chromatin as a substrate. The diverse set of ATPases that qualify as the molecular motors of the nucleosome remodeling process have a common history and are part of a superfamily. The physiological context of their remodeling action builds on the association with a wide range of other proteins to form distinct complexes for nucleosome remodeling. This review summarizes the recent progress in our understanding of the mechanisms underlying the nucleosome remodeling reaction, the targeting of remodeling machines to selected sites in chromatin, and their integration into complex regulatory schemes.

摘要

长期以来,破译使细胞既能将其基因组组织成紧密染色质,又能确保遗传信息在细胞核范围内对调节因子和酶保持可及性的原理一直是一项挑战。利用ATP能量使核小体DNA可及的核小体重塑活性的发现是一个巨大的飞跃。在体外,这些酶削弱了DNA围绕组蛋白八聚体的紧密缠绕,从而促进组蛋白八聚体向相邻DNA片段的滑动、它们向未连接DNA的位移以及核小体表面可及DNA片段的积累。据推测,这些酶的集体作用赋予染色质动态特性,这些特性支配着所有以染色质为底物的核功能。符合核小体重塑过程分子马达资格的各种ATP酶有着共同的历史,并且是一个超家族的一部分。它们重塑作用的生理背景建立在与多种其他蛋白质的关联之上,以形成用于核小体重塑的不同复合物。本综述总结了我们在理解核小体重塑反应背后的机制、重塑机器靶向染色质中选定位点以及它们整合到复杂调节方案方面的最新进展。

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