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Hsp70 分子伴侣的核苷酸交换因子。

The nucleotide exchange factors of Hsp70 molecular chaperones.

机构信息

Department of Cellular Biochemistry, Max-Planck-Institute of Biochemistry Martinsried, Germany.

出版信息

Front Mol Biosci. 2015 Apr 7;2:10. doi: 10.3389/fmolb.2015.00010. eCollection 2015.

Abstract

Molecular chaperones of the Hsp70 family form an important hub in the cellular protein folding networks in bacteria and eukaryotes, connecting translation with the downstream machineries of protein folding and degradation. The Hsp70 folding cycle is driven by two types of cochaperones: J-domain proteins stimulate ATP hydrolysis by Hsp70, while nucleotide exchange factors (NEFs) promote replacement of Hsp70-bound ADP with ATP. Bacteria and organelles of bacterial origin have only one known NEF type for Hsp70, GrpE. In contrast, a large diversity of Hsp70 NEFs has been discovered in the eukaryotic cell. These NEFs belong to the Hsp110/Grp170, HspBP1/Sil1, and BAG domain protein families. In this short review we compare the structures and molecular mechanisms of nucleotide exchange factors for Hsp70 and discuss how these cochaperones contribute to protein folding and quality control in the cell.

摘要

Hsp70 家族的分子伴侣在细菌和真核生物的细胞蛋白折叠网络中形成一个重要的中心,将翻译与蛋白折叠和降解的下游机制连接起来。Hsp70 折叠循环由两种类型的共伴侣驱动:J 结构域蛋白刺激 Hsp70 的 ATP 水解,而核苷酸交换因子(NEF)促进 Hsp70 结合的 ADP 被 ATP 取代。细菌和细菌起源的细胞器只有一种已知的 Hsp70 的 NEF,即 GrpE。相比之下,在真核细胞中发现了大量的 Hsp70 NEF。这些 NEF 属于 Hsp110/Grp170、HspBP1/Sil1 和 BAG 结构域蛋白家族。在这篇简短的综述中,我们比较了 Hsp70 的核苷酸交换因子的结构和分子机制,并讨论了这些共伴侣如何促进细胞中的蛋白折叠和质量控制。

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