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利用高通量位点饱和诱变和生物物理方法阐明影响埃博拉病毒基质蛋白二聚化的残基水平决定因素。

Elucidating Residue-Level Determinants Affecting Dimerization of Ebola Virus Matrix Protein Using High-Throughput Site Saturation Mutagenesis and Biophysical Approaches.

作者信息

Narkhede Yogesh B, Bhardwaj Atul, Motsa Balindile B, Saxena Roopashi, Sharma Tej, Chapagain Prem P, Stahelin Robert V, Wiest Olaf

机构信息

Department of Chemistry and Biochemistry, University of Notre Dame, Notre Dame, Indiana 46556, United States.

Department of Medicinal Chemistry & Molecular Pharmacology, Purdue Institute of Inflammation, Immunology, and Infectious Disease, Purdue University, West Lafayette, Indiana 47907, United States.

出版信息

J Phys Chem B. 2023 Jul 27;127(29):6449-6461. doi: 10.1021/acs.jpcb.3c01759. Epub 2023 Jul 17.

DOI:10.1021/acs.jpcb.3c01759
PMID:37458567
Abstract

The Ebola virus (EBOV) is a filamentous virus that acquires its lipid envelope from the plasma membrane of the host cell it infects. EBOV assembly and budding from the host cell plasma membrane are mediated by a peripheral protein, known as the matrix protein VP40. VP40 is a 326 amino acid protein with two domains that are loosely linked. The VP40 N-terminal domain (NTD) contains a hydrophobic α-helix, which mediates VP40 dimerization. The VP40 C-terminal domain has a cationic patch, which mediates interactions with anionic lipids and a hydrophobic region that mediates VP40 dimer-dimer interactions. The VP40 dimer is necessary for trafficking to the plasma membrane inner leaflet and interactions with anionic lipids to mediate the VP40 assembly and oligomerization. Despite significant structural information available on the VP40 dimer structure, little is known on how the VP40 dimer is stabilized and how residues outside the NTD hydrophobic portion of the α-helical dimer interface contribute to dimer stability. To better understand how VP40 dimer stability is maintained, we performed computational studies using per-residue energy decomposition and site saturation mutagenesis. These studies revealed a number of novel keystone residues for VP40 dimer stability just adjacent to the α-helical dimer interface as well as distant residues in the VP40 CTD that can stabilize the VP40 dimer form. Experimental studies with representative VP40 mutants in vitro and in cells were performed to test computational predictions that reveal residues that alter VP40 dimer stability. Taken together, these studies provide important biophysical insights into VP40 dimerization and may be useful in strategies to weaken or alter the VP40 dimer structure as a means of inhibiting the EBOV assembly.

摘要

埃博拉病毒(EBOV)是一种丝状病毒,其脂质包膜来自被它感染的宿主细胞的质膜。EBOV从宿主细胞质膜的组装和出芽由一种外周蛋白介导,该蛋白被称为基质蛋白VP40。VP40是一种由326个氨基酸组成的蛋白质,有两个松散连接的结构域。VP40的N端结构域(NTD)包含一个疏水α螺旋,它介导VP40二聚化。VP40的C端结构域有一个阳离子斑块,它介导与阴离子脂质的相互作用以及一个介导VP40二聚体 - 二聚体相互作用的疏水区域。VP40二聚体对于转运到质膜内小叶以及与阴离子脂质相互作用以介导VP40的组装和寡聚化是必需的。尽管关于VP40二聚体结构有大量的结构信息,但对于VP40二聚体如何稳定以及α螺旋二聚体界面的NTD疏水部分之外的残基如何对二聚体稳定性有贡献却知之甚少。为了更好地理解VP40二聚体稳定性是如何维持的,我们使用逐个残基能量分解和位点饱和诱变进行了计算研究。这些研究揭示了一些紧邻α螺旋二聚体界面的对于VP40二聚体稳定性至关重要的新关键残基,以及VP40 CTD中可以稳定VP40二聚体形式的远距离残基。对体外和细胞中的代表性VP40突变体进行了实验研究,以测试揭示改变VP40二聚体稳定性的残基的计算预测。综上所述,这些研究为VP40二聚化提供了重要的生物物理见解,并且可能在作为抑制EBOV组装手段的削弱或改变VP40二聚体结构的策略中有用。

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引用本文的文献

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Variants of the Ebola virus matrix protein VP40 have differential effects on oligomerization and plasma membrane interactions.埃博拉病毒基质蛋白VP40的变体对寡聚化和质膜相互作用有不同影响。
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2
Design of a stapled peptide that binds to the Ebola virus matrix protein dimer interface.一种与埃博拉病毒基质蛋白二聚体界面结合的订书肽的设计。
RSC Chem Biol. 2025 Apr 25. doi: 10.1039/d5cb00048c.
3
A fatty acid-ordered plasma membrane environment is critical for Ebola virus matrix protein assembly and budding.
脂肪酸有序的质膜环境对于埃博拉病毒基质蛋白组装和出芽至关重要。
J Lipid Res. 2024 Nov;65(11):100663. doi: 10.1016/j.jlr.2024.100663. Epub 2024 Oct 5.
4
Computational and experimental identification of keystone interactions in Ebola virus matrix protein VP40 dimer formation.计算和实验鉴定埃博拉病毒基质蛋白 VP40 二聚体形成中的关键相互作用。
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Minor changes in electrostatics robustly increase VP40 membrane binding, assembly, and budding of Ebola virus matrix protein derived virus-like particles.静电的微小变化有力地增强了埃博拉病毒基质蛋白衍生的病毒样颗粒的VP40膜结合、组装和出芽。
bioRxiv. 2024 Jan 31:2024.01.30.578092. doi: 10.1101/2024.01.30.578092.