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热休克蛋白70(Hsp70)辅助伴侣蛋白Bag2进行核苷酸交换和与客户蛋白结合的结构基础。

Structural basis of nucleotide exchange and client binding by the Hsp70 cochaperone Bag2.

作者信息

Xu Zhen, Page Richard C, Gomes Michelle M, Kohli Ekta, Nix Jay C, Herr Andrew B, Patterson Cam, Misra Saurav

机构信息

Department of Molecular Cardiology, Lerner Research Institute, NB50, 9500 Euclid Avenue, The Cleveland Clinic, Cleveland, Ohio 44195, USA.

出版信息

Nat Struct Mol Biol. 2008 Dec;15(12):1309-17. doi: 10.1038/nsmb.1518. Epub 2008 Nov 23.

Abstract

Cochaperones are essential for Hsp70- and Hsc70-mediated folding of proteins and include nucleotide-exchange factors (NEFs) that assist protein folding by accelerating ADP-ATP exchange on Hsp70. The cochaperone Bag2 binds misfolded Hsp70 clients and also acts as an NEF, but the molecular basis for its function is unclear. We show that, rather than being a member of the Bag domain family, Bag2 contains a new type of Hsp70 NEF domain, which we call the 'brand new bag' (BNB) domain. Free and Hsc70-bound crystal structures of Bag2-BNB show its dimeric structure, in which a flanking linker helix and loop bind to Hsc70 to promote nucleotide exchange. NMR analysis demonstrates that the client binding sites and Hsc70-interaction sites of the Bag2-BNB overlap, and that Hsc70 can displace clients from Bag2-BNB, indicating a distinct mechanism for the regulation of Hsp70-mediated protein folding by Bag2.

摘要

共伴侣蛋白对于Hsp70和Hsc70介导的蛋白质折叠至关重要,包括核苷酸交换因子(NEFs),它们通过加速Hsp70上的ADP-ATP交换来协助蛋白质折叠。共伴侣蛋白Bag2结合错误折叠的Hsp70底物蛋白,并且也作为一种NEF发挥作用,但其功能的分子基础尚不清楚。我们发现,Bag2并非Bag结构域家族的成员,而是包含一种新型的Hsp70 NEF结构域,我们将其称为“全新的Bag”(BNB)结构域。Bag2-BNB的游离和与Hsc70结合的晶体结构显示出其二聚体结构,其中侧翼连接螺旋和环与Hsc70结合以促进核苷酸交换。核磁共振分析表明,Bag2-BNB的底物蛋白结合位点和Hsc70相互作用位点重叠,并且Hsc70可以将底物蛋白从Bag2-BNB上置换下来,这表明Bag2对Hsp70介导的蛋白质折叠具有独特的调控机制。

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