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应激防御的第一道防线:小分子热休克蛋白及其在蛋白质稳态中的作用

A first line of stress defense: small heat shock proteins and their function in protein homeostasis.

作者信息

Haslbeck Martin, Vierling Elizabeth

机构信息

Department Chemie, Technische Universität München, Lichtenbergstrasse 4, 85 748 Garching, Germany.

Department of Biochemistry and Molecular Biology, University of Massachusetts, Life Science Laboratories, N329 240 Thatcher Road, Amherst, MA 01003-9364, USA.

出版信息

J Mol Biol. 2015 Apr 10;427(7):1537-48. doi: 10.1016/j.jmb.2015.02.002. Epub 2015 Feb 10.

Abstract

Small heat shock proteins (sHsps) are virtually ubiquitous molecular chaperones that can prevent the irreversible aggregation of denaturing proteins. sHsps complex with a variety of non-native proteins in an ATP-independent manner and, in the context of the stress response, form a first line of defense against protein aggregation in order to maintain protein homeostasis. In vertebrates, they act to maintain the clarity of the eye lens, and in humans, sHsp mutations are linked to myopathies and neuropathies. Although found in all domains of life, sHsps are quite diverse and have evolved independently in metazoans, plants and fungi. sHsp monomers range in size from approximately 12 to 42kDa and are defined by a conserved β-sandwich α-crystallin domain, flanked by variable N- and C-terminal sequences. Most sHsps form large oligomeric ensembles with a broad distribution of different, sphere- or barrel-like oligomers, with the size and structure of the oligomers dictated by features of the N- and C-termini. The activity of sHsps is regulated by mechanisms that change the equilibrium distribution in tertiary features and/or quaternary structure of the sHsp ensembles. Cooperation and/or co-assembly between different sHsps in the same cellular compartment add an underexplored level of complexity to sHsp structure and function.

摘要

小热休克蛋白(sHsps)几乎普遍存在,是一种分子伴侣,能够防止变性蛋白质发生不可逆聚集。sHsps以不依赖ATP的方式与多种非天然蛋白质形成复合物,在应激反应中,它们形成抵御蛋白质聚集的第一道防线,以维持蛋白质稳态。在脊椎动物中,它们有助于维持晶状体的透明度,在人类中,sHsp突变与肌病和神经病有关。尽管在生命的所有领域都能发现sHsps,但它们种类繁多,在后生动物、植物和真菌中独立进化。sHsp单体的大小约为12至42kDa,由一个保守的β折叠α晶状体蛋白结构域定义,两侧是可变的N端和C端序列。大多数sHsps形成大型寡聚体集合,包含广泛分布的不同球形或桶状寡聚体,寡聚体的大小和结构由N端和C端的特征决定。sHsps的活性受多种机制调节,这些机制改变了sHsp集合体三级结构和/或四级结构的平衡分布。同一细胞区室中不同sHsps之间的协同作用和/或共同组装为sHsp的结构和功能增添了一个尚未充分探索的复杂层面。

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