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GrpE,一种DnaK的核苷酸交换因子。

GrpE, a nucleotide exchange factor for DnaK.

作者信息

Harrison Celia

机构信息

Boston Biomedical Research Institute, 64 Grove Street, Watertown, MA 02472, USA.

出版信息

Cell Stress Chaperones. 2003 Fall;8(3):218-24. doi: 10.1379/1466-1268(2003)008<0218:ganeff>2.0.co;2.

Abstract

The cochaperone GrpE functions as a nucleotide exchange factor to promote dissociation of adenosine 5'-diphosphate (ADP) from the nucleotide-binding cleft of DnaK. GrpE and the DnaJ cochaperone act in concert to control the flux of unfolded polypeptides into and out of the substrate-binding domain of DnaK by regulating the nucleotide-bound state of DnaK. DnaJ stimulates nucleotide hydrolysis, and GrpE promotes the exchange of ADP for adenosine triphosphate (ATP) and also augments peptide release from the DnaK substrate-binding domain in an ATP-independent manner. The eukaryotic cytosol does not contain GrpE per se because GrpE-like function is provided by the BAG1 protein, which acts as a nucleotide exchange factor for cytosolic Hsp70s. GrpE, which plays a prominent role in mitochondria, chloroplasts, and bacterial cytoplasms, is a fascinating molecule with an unusual quaternary structure. The long alpha-helices of GrpE have been hypothesized to act as a thermosensor and to be involved in the decrease in GrpE-dependent nucleotide exchange that is observed in vitro at temperatures relevant to heat shock. This review describes the molecular biology of GrpE and focuses on the structural and kinetic aspects of nucleotide exchange, peptide release, and the thermosensor hypothesis.

摘要

辅助伴侣蛋白GrpE作为核苷酸交换因子,促进二磷酸腺苷(ADP)从DnaK的核苷酸结合裂隙中解离。GrpE和辅助伴侣蛋白DnaJ协同作用,通过调节DnaK的核苷酸结合状态,控制未折叠多肽进出DnaK底物结合结构域的通量。DnaJ刺激核苷酸水解,而GrpE促进ADP与三磷酸腺苷(ATP)的交换,并且还以不依赖ATP的方式增强从DnaK底物结合结构域释放的肽。真核细胞质本身不含GrpE,因为BAG1蛋白提供了类似GrpE的功能,该蛋白作为胞质Hsp70的核苷酸交换因子。GrpE在线粒体、叶绿体和细菌细胞质中发挥重要作用,是一种具有不寻常四级结构的迷人分子。GrpE的长α螺旋被认为可作为热传感器,并参与在与热休克相关的温度下体外观察到的GrpE依赖性核苷酸交换的减少。本综述描述了GrpE的分子生物学,并重点关注核苷酸交换、肽释放和热传感器假说的结构和动力学方面。

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