FKBP38与热休克蛋白90的MEEVD四肽重复序列结合基序形成复合物的结构。

The structure of FKBP38 in complex with the MEEVD tetratricopeptide binding-motif of Hsp90.

作者信息

Blundell Katie L I M, Pal Mohinder, Roe S Mark, Pearl Laurence H, Prodromou Chrisostomos

机构信息

Genome Damage and Stability Centre, School of Life Sciences, University of Sussex, Falmer, Brighton BN1 9RQ, England.

出版信息

PLoS One. 2017 Mar 9;12(3):e0173543. doi: 10.1371/journal.pone.0173543. eCollection 2017.

DOI:10.1371/journal.pone.0173543

PMID:28278223

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5344419/

Abstract

Tetratricopeptide (TPR) domains are known protein interaction domains. We show that the TPR domain of FKBP8 selectively binds Hsp90, and interactions upstream of the conserved MEEVD motif are critical for tight binding. In contrast FKBP8 failed to bind intact Hsp70. The PPIase domain was not essential for the interaction with Hsp90 and binding was completely encompassed by the TPR domain alone. The conformation adopted by Hsp90 peptides, containing the conserved MEEVD motif, in the crystal structure were similar to that seen for the TPR domains of CHIP, AIP and Tah1. The carboxylate clamp interactions with bound Hsp90 peptide were a critical component of the interaction and mutation of Lys 307, involved in the carboxylate clamp, completely disrupted the interaction with Hsp90. FKBP8 binding to Hsp90 did not substantially influence its ATPase activity.

摘要

四肽重复序列（TPR）结构域是已知的蛋白质相互作用结构域。我们发现FKBP8的TPR结构域选择性地结合Hsp90，并且保守的MEEVD基序上游的相互作用对于紧密结合至关重要。相比之下，FKBP8无法结合完整的Hsp70。肽脯氨酰顺反异构酶（PPIase）结构域对于与Hsp90的相互作用并非必需，且结合完全由单独的TPR结构域完成。在晶体结构中，包含保守MEEVD基序的Hsp90肽所采用的构象与CHIP、AIP和Tah1的TPR结构域所观察到的构象相似。与结合的Hsp90肽的羧酸盐钳相互作用是相互作用的关键组成部分，参与羧酸盐钳的赖氨酸307的突变完全破坏了与Hsp90的相互作用。FKBP8与Hsp90的结合并未显著影响其ATP酶活性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0dcd/5344419/9c87024a3488/pone.0173543.g001.jpg

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FKBP38与热休克蛋白90的MEEVD四肽重复序列结合基序形成复合物的结构。

The structure of FKBP38 in complex with the MEEVD tetratricopeptide binding-motif of Hsp90.

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