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使用模拟残基构象之间的互信息比较 DnaK 和 BiP 中的别构信号传导。

Comparison of allosteric signaling in DnaK and BiP using mutual information between simulated residue conformations.

机构信息

TUM Center for Functional Protein Assemblies and TUM School of Life Sciences, Technische Universität München, Freising, Bavaria, Germany.

出版信息

Proteins. 2023 Feb;91(2):237-255. doi: 10.1002/prot.26425. Epub 2022 Oct 12.

DOI:10.1002/prot.26425
PMID:36111439
Abstract

The heat shock protein 70 kDa (Hsp70) chaperone system serves as a critical component of protein quality control across a wide range of prokaryotic and eukaryotic organisms. Divergent evolution and specialization to particular organelles have produced numerous Hsp70 variants which share similarities in structure and general function, but differ substantially in regulatory aspects, including conformational dynamics and activity modulation by cochaperones. The human Hsp70 variant BiP (also known as GRP78 or HSPA5) is of therapeutic interest in the context of cancer, neurodegenerative diseases, and viral infection, including for treatment of the pandemic virus SARS-CoV-2. Due to the complex conformational rearrangements and high sequential variance within the Hsp70 protein family, it is in many cases poorly understood which amino acid mutations are responsible for biochemical differences between protein variants. In this study, we predicted residues associated with conformational regulation of human BiP and Escherichia coli DnaK. Based on protein structure networks obtained from molecular dynamics simulations, we analyzed the shared information between interaction timelines to highlight residue positions with strong conformational coupling to their environment. Our predictions, which focus on the binding processes of the chaperone's substrate and cochaperones, indicate residues filling potential signaling roles specific to either DnaK or BiP. By combining predictions of individual residues into conformationally coupled chains connecting ligand binding sites, we predict a BiP specific secondary signaling pathway associated with substrate binding. Our study sheds light on mechanistic differences in signaling and regulation between Hsp70 variants, which provide insights relevant to therapeutic applications of these proteins.

摘要

热休克蛋白 70kDa(Hsp70)伴侣系统作为一个关键的蛋白质质量控制系统组件,广泛存在于原核生物和真核生物中。在不同的细胞器中,Hsp70 发生了分歧进化和特化,产生了许多具有相似结构和一般功能的 Hsp70 变体,但在调节方面存在很大差异,包括构象动力学和共伴侣的活性调节。人类 Hsp70 变体 BiP(也称为 GRP78 或 HSPA5)在癌症、神经退行性疾病和病毒感染的治疗中具有重要意义,包括治疗 SARS-CoV-2 大流行病毒。由于 Hsp70 蛋白家族内的复杂构象重排和高序列变异性,在许多情况下,人们并不清楚哪些氨基酸突变导致了蛋白变体之间的生化差异。在这项研究中,我们预测了与人类 BiP 和大肠杆菌 DnaK 构象调节相关的残基。基于从分子动力学模拟中获得的蛋白质结构网络,我们分析了相互作用时间线之间的共享信息,以突出与环境具有强构象耦合的残基位置。我们的预测集中在伴侣的底物和共伴侣的结合过程上,表明残基具有特定于 DnaK 或 BiP 的潜在信号作用。通过将单个残基的预测组合成连接配体结合位点的构象偶联链,我们预测了与底物结合相关的 BiP 特异性二级信号通路。我们的研究揭示了 Hsp70 变体在信号和调节方面的机制差异,为这些蛋白质的治疗应用提供了相关见解。

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