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Hsp90 中段磷酸化启动了一个复杂的构象程序,以募集 ATP 酶激活共伴侣 Aha1。

Hsp90 middle domain phosphorylation initiates a complex conformational program to recruit the ATPase-stimulating cochaperone Aha1.

机构信息

Urologic Oncology Branch, National Cancer Institute, Bethesda, MD, 20892, USA.

Department of Genome Sciences, University of Washington School of Medicine, Seattle, WA, 98195, USA.

出版信息

Nat Commun. 2019 Jun 12;10(1):2574. doi: 10.1038/s41467-019-10463-y.

Abstract

Complex conformational dynamics are essential for function of the dimeric molecular chaperone heat shock protein 90 (Hsp90), including transient, ATP-biased N-domain dimerization that is necessary to attain ATPase competence. The intrinsic, but weak, ATP hydrolyzing activity of human Hsp90 is markedly enhanced by the co-chaperone Aha1. However, the cellular concentration of Aha1 is substoichiometric relative to Hsp90. Here we report that initial recruitment of this cochaperone to Hsp90 is markedly enhanced by phosphorylation of a highly conserved tyrosine (Y313 in Hsp90α) in the Hsp90 middle domain. Importantly, phosphomimetic mutation of Y313 promotes formation of a transient complex in which both N- and C-domains of Aha1 bind to distinct surfaces of the middle domains of opposing Hsp90 protomers prior to ATP-directed N-domain dimerization. Thus, Y313 represents a phosphorylation-sensitive conformational switch, engaged early after client loading, that affects both local and long-range conformational dynamics to facilitate initial recruitment of Aha1 to Hsp90.

摘要

复杂的构象动力学对于二聚体分子伴侣热休克蛋白 90(Hsp90)的功能至关重要,包括瞬时的、ATP 偏向的 N 结构域二聚化,这是获得 ATP 酶能力所必需的。人 Hsp90 的内在但较弱的 ATP 水解活性显著增强由共伴侣 Aha1。然而,Aha1 的细胞浓度相对于 Hsp90 是亚化学计量的。在这里,我们报告说,该共伴侣对 Hsp90 的初始募集通过在 Hsp90 中间域中高度保守的酪氨酸(Hsp90α中的 Y313)的磷酸化显著增强。重要的是,Y313 的磷酸模拟突变促进了瞬时复合物的形成,其中 Aha1 的 N-和 C 结构域在 ATP 定向的 N 结构域二聚化之前结合到对映体 Hsp90 前体的中间域的不同表面上。因此,Y313 代表一个磷酸化敏感的构象开关,在客户加载后早期被激活,影响局部和远程构象动力学,以促进 Aha1 对 Hsp90 的初始募集。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1e89/6561935/2df30fd5cff0/41467_2019_10463_Fig1_HTML.jpg

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