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一种漏斗状构象景观控制黄病毒融合肽与脂膜的相互作用。

A Funneled Conformational Landscape Governs Flavivirus Fusion Peptide Interaction with Lipid Membranes.

机构信息

Bioinformatics Institute (A*STAR) , 30 Biopolis Street, #07-01 Matrix , Singapore 138671.

School of Biological Sciences , Nanyang Technological University , 60 Nanyang Drive , Singapore 63755.

出版信息

J Chem Theory Comput. 2018 Jul 10;14(7):3920-3932. doi: 10.1021/acs.jctc.8b00438. Epub 2018 Jun 20.

DOI:10.1021/acs.jctc.8b00438
PMID:29874075
Abstract

During host cell infection by flaviviruses such as dengue and Zika, acidic pH within the endosome triggers a conformational change in the envelope protein on the outer surface of the virion. This results in exposure of the ∼15 residue fusion peptide (FP) region, freeing it to induce fusion between the viral and endosomal membranes. A better understanding of the conformational dynamics of the FP in the presence of membranes, and the basis for its selectivity for anionic lipid species present within the endosome, would facilitate its therapeutic targeting with antiviral drugs and antibodies. In this work, multiscale modeling, simulations, and free energy calculations (including a total of ∼75 μs of atomic-resolution sampling), combined with imaging total internal reflection fluorescence correlation spectroscopy experiments, were employed to investigate the mechanisms of interaction of FP variants with lipid bilayers. Wild-type FPs (in the presence or absence of a fluorescein isothiocyanate tag) were shown to possess a funneled conformational landscape governing their exit from solvent and penetration into the lipid phase and to exhibit an electrostatically favored >2-fold affinity for membranes containing anionic species over purely zwitterionic ones. Conversely, the landscape was abolished in a nonfunctional point mutant, leading to a 2-fold drop in host membrane affinity. Collectively, our data reveal how the highly conserved flavivirus FP has evolved to funnel its conformational space toward a maximally fusogenic state anchored within the endosomal membrane. Therapeutically targeting the accessible ensemble of FP conformations may represent a new, rational strategy for blocking viral infection.

摘要

在黄病毒(如登革热和寨卡病毒)感染宿主细胞时,内体中的酸性 pH 值会触发病毒粒子外表面包膜蛋白的构象变化。这导致约 15 个残基的融合肽(FP)区域暴露,从而自由诱导病毒和内体膜之间的融合。更好地了解 FP 在膜存在下的构象动力学及其对存在于内体中的阴离子脂质种类的选择性的基础,将有助于用抗病毒药物和抗体对其进行治疗靶向。在这项工作中,采用多尺度建模、模拟和自由能计算(总共包括约 75 μs 的原子分辨率采样),结合荧光全内反射相关光谱学实验,研究了 FP 变体与脂质双层相互作用的机制。野生型 FP(存在或不存在异硫氰酸荧光素标记)被证明具有控制其从溶剂中逸出并渗透到脂质相的漏斗状构象景观,并表现出对含有阴离子物质的膜的静电优先性,亲和力是纯两性离子的 2 倍以上。相反,在无功能点突变体中,该景观被废除,导致对宿主膜的亲和力降低 2 倍。总之,我们的数据揭示了高度保守的黄病毒 FP 是如何进化为将其构象空间引导到内体膜内的最大融合状态。针对可及的 FP 构象集合进行治疗靶向可能代表一种阻断病毒感染的新的、合理的策略。

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A Funneled Conformational Landscape Governs Flavivirus Fusion Peptide Interaction with Lipid Membranes.一种漏斗状构象景观控制黄病毒融合肽与脂膜的相互作用。
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