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中间结构域的相互作用将 Hsp90α 二聚体稳定在具有高亲和力结合 p23 的封闭构象中。

Interaction of the middle domains stabilizes Hsp90α dimer in a closed conformation with high affinity for p23.

机构信息

Department of Experimental Pharmacology, Mossakowski Medical Research Centre, Polish Academy of Sciences, 5 Pawinskiego St., 02-106 Warsaw, Poland.

Faculty of Chemistry, Biological and Chemical Research Centre, University of Warsaw, 1 Pasteura St., 02-093 Warsaw, Poland.

出版信息

Biol Chem. 2018 Mar 28;399(4):337-345. doi: 10.1515/hsz-2017-0172.

Abstract

The human genome encodes two highly similar cytosolic Hsp90 proteins called isoforms Hsp90α and Hsp90β. Of the 300 client proteins for Hsp90 identified so far only a handful interact specifically with one Hsp90 isoform. Here we report for the first time that Hsp90 cochaperone p23 binds preferentially to Hsp90α and that this interaction is mediated by the middle domain of Hsp90α. Based on the homology modeling, we infer that the middle domains in the Hsp90α dimer bind stronger with each other than in the Hsp90β dimer. Therefore, compared to Hsp90β, Hsp90α may adopt closed conformation more easily. Hsp90 interacts with p23 in the closed conformation. Hsp90α binds human recombinant p23 about three times stronger than Hsp90β but with significantly smaller exothermic enthalpy as determined by isothermal titration calorimetry of direct binding between the purified proteins. As p23 binds to Hsp90 in a closed conformation, stabilization of the Hsp90α dimer in the closed conformation by its middle domains explains preference of p23 to this Hsp90 isoform.

摘要

人类基因组编码两种高度相似的细胞质 Hsp90 蛋白,称为 Hsp90α 和 Hsp90β 同工型。到目前为止,已经鉴定出 300 种 Hsp90 的客户蛋白,但只有少数几种与一种 Hsp90 同工型特异性相互作用。在这里,我们首次报道 Hsp90 共伴侣 p23 优先与 Hsp90α 结合,并且这种相互作用是由 Hsp90α 的中间结构域介导的。基于同源建模,我们推断 Hsp90α 二聚体的中间结构域相互结合的强度比 Hsp90β 二聚体更强。因此,与 Hsp90β 相比,Hsp90α 可能更容易采用封闭构象。Hsp90 与 p23 在封闭构象中相互作用。Hsp90α 与人重组 p23 的结合强度比 Hsp90β 强约 3 倍,但根据纯化蛋白之间直接结合的等温滴定量热法测定,其放热焓显著较小。由于 p23 以封闭构象与 Hsp90 结合,因此其中间结构域稳定 Hsp90α 二聚体处于封闭构象,从而解释了 p23 对这种 Hsp90 同工型的偏好。

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