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蛋白质在动态核小体景观上的固有无序。

Protein intrinsic disorder on a dynamic nucleosomal landscape.

机构信息

Department of Biochemistry, Science Institute, University of Iceland, Reykjavík, Iceland.

School of Chemical Science, University of Auckland, Auckland, New Zealand.

出版信息

Prog Mol Biol Transl Sci. 2021;183:295-354. doi: 10.1016/bs.pmbts.2021.06.006. Epub 2021 Jul 28.

Abstract

The complex nucleoprotein landscape of the eukaryotic cell nucleus is rich in dynamic proteins that lack a stable three-dimensional structure. Many of these intrinsically disordered proteins operate directly on the first fundamental level of genome compaction: the nucleosome. Here we give an overview of how disordered interactions with and within nucleosomes shape the dynamics, architecture, and epigenetic regulation of the genetic material, controlling cellular transcription patterns. We highlight experimental and computational challenges in the study of protein disorder and illustrate how integrative approaches are increasingly unveiling the fine details of nuclear interaction networks. We finally dissect sequence properties encoded in disordered regions and assess common features of disordered nucleosome-binding proteins. As drivers of many critical biological processes, disordered proteins are integral to a comprehensive molecular view of the dynamic nuclear milieu.

摘要

真核细胞核的复杂核蛋白景观富含缺乏稳定三维结构的动态蛋白。这些无规卷曲蛋白中的许多直接作用于基因组紧缩的第一个基本水平:核小体。在这里,我们概述了无规卷曲与核小体相互作用如何影响遗传物质的动力学、结构和表观遗传调控,控制细胞转录模式。我们强调了在研究蛋白质无序性方面的实验和计算挑战,并说明了综合方法如何越来越多地揭示核相互作用网络的细节。最后,我们剖析无序区编码的序列特性,并评估无序核小体结合蛋白的常见特征。作为许多关键生物过程的驱动因素,无序蛋白是动态核环境综合分子观点的组成部分。

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