A unique chaperoning mechanism in class A JDPs recognizes and stabilizes mutant p53.

IF 14.5 1区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY Molecular Cell Pub Date : 2024-04-18 Epub Date: 2024-03-19 DOI:10.1016/j.molcel.2024.02.018
Guy Zoltsman, Thi Lieu Dang, Miriam Kuchersky, Ofrah Faust, Micael S Silva, Tal Ilani, Anne S Wentink, Bernd Bukau, Rina Rosenzweig
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Abstract

J-domain proteins (JDPs) constitute a large family of molecular chaperones that bind a broad spectrum of substrates, targeting them to Hsp70, thus determining the specificity of and activating the entire chaperone functional cycle. The malfunction of JDPs is therefore inextricably linked to myriad human disorders. Here, we uncover a unique mechanism by which chaperones recognize misfolded clients, present in human class A JDPs. Through a newly identified β-hairpin site, these chaperones detect changes in protein dynamics at the initial stages of misfolding, prior to exposure of hydrophobic regions or large structural rearrangements. The JDPs then sequester misfolding-prone proteins into large oligomeric assemblies, protecting them from aggregation. Through this mechanism, class A JDPs bind destabilized p53 mutants, preventing clearance of these oncoproteins by Hsp70-mediated degradation, thus promoting cancer progression. Removal of the β-hairpin abrogates this protective activity while minimally affecting other chaperoning functions. This suggests the class A JDP β-hairpin as a highly specific target for cancer therapeutics.

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A 类 JDPs 中的一种独特伴侣机制可识别并稳定突变 p53。
J-结构域蛋白(JDPs)构成了一个庞大的分子伴侣家族,它们能与多种底物结合,并将其定向到 Hsp70 上,从而决定了整个伴侣功能周期的特异性并激活整个功能周期。因此,JDPs 的功能失常与人类的各种疾病密不可分。在这里,我们发现了伴侣识别人类 A 类 JDPs 中存在的错误折叠客户的独特机制。通过一个新发现的β-发夹位点,这些伴侣在错误折叠的初始阶段,即疏水区域暴露或大的结构重排之前,就能检测到蛋白质动态的变化。然后,JDPs 将易发生错误折叠的蛋白质封闭在大型低聚物集合体中,保护它们不发生聚集。通过这种机制,A 类 JDPs 与不稳定的 p53 突变体结合,阻止 Hsp70 介导的降解清除这些肿瘤蛋白,从而促进癌症进展。去掉β-发夹后,这种保护性活性就会消失,而对其他伴侣功能的影响却很小。这表明 A 类 JDP β-发夹是癌症疗法的高度特异性靶点。
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来源期刊
Molecular Cell
Molecular Cell 生物-生化与分子生物学
CiteScore
26.00
自引率
3.80%
发文量
389
审稿时长
1 months
期刊介绍: Molecular Cell is a companion to Cell, the leading journal of biology and the highest-impact journal in the world. Launched in December 1997 and published monthly. Molecular Cell is dedicated to publishing cutting-edge research in molecular biology, focusing on fundamental cellular processes. The journal encompasses a wide range of topics, including DNA replication, recombination, and repair; Chromatin biology and genome organization; Transcription; RNA processing and decay; Non-coding RNA function; Translation; Protein folding, modification, and quality control; Signal transduction pathways; Cell cycle and checkpoints; Cell death; Autophagy; Metabolism.
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