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使用单分子光学镊子研究热休克蛋白 90 分子伴侣的构象循环。

Using Single-Molecule Optical Tweezers to Study the Conformational Cycle of the Hsp90 Molecular Chaperone.

机构信息

Groningen Biomolecular Sciences and Biotechnology Institute (GBB), University of Groningen, Groningen, The Netherlands.

Department of Physics, Technical University of Munich, Garching-bei-München, Germany.

出版信息

Methods Mol Biol. 2022;2478:401-425. doi: 10.1007/978-1-0716-2229-2_15.

Abstract

The heat shock protein 90 (Hsp90) family of chaperones are well-known, highly important components of the cellular systems which regulate protein homeostasis. Essential in eukaryotes, Hsp90s is also found in prokaryotes, including archaea. Hsp90 is a dimeric protein, with each monomer consisting of three separate structural domains, and undergoes large conformational changes as part of its functional cycle. This cycle is driven by interactions with nucleotides, cochaperone proteins, client proteins and allosteric effects enacted by these and by posttranslational modifications. All of these influence the rate and degree of the opening and closing of the dimer as well as the relative domain orientations and its overall rigidity. Optical tweezers, which can access many of these functionally important conformational changes, therefore provide a unique tool for the study of this large and complex molecular chaperone. Here, we provide protocols for the design and implementation of different Hsp90 constructs and optical tweezers experiments for addressing the many open questions about the function of this important molecular chaperone.

摘要

热休克蛋白 90(Hsp90)家族伴侣是调节蛋白质稳态的细胞系统中众所周知的、高度重要的组成部分。在真核生物中是必需的,Hsp90 也存在于原核生物中,包括古细菌。Hsp90 是一种二聚体蛋白,每个单体由三个独立的结构域组成,并在其功能循环中经历大的构象变化。该循环由与核苷酸、共伴侣蛋白、客户蛋白的相互作用以及由这些和翻译后修饰引起的变构效应驱动。所有这些都影响二聚体的打开和关闭的速率和程度,以及相对的结构域取向及其整体刚性。光学镊子可以获得许多这些功能上重要的构象变化,因此为研究这种大型复杂的分子伴侣提供了独特的工具。在这里,我们提供了设计和实施不同 Hsp90 结构构建体和光学镊子实验的方案,以解决关于这种重要分子伴侣功能的许多悬而未决的问题。

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