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单纯疱疹 I 型病毒糖蛋白 B 的两个融合环的生物物理特性和膜相互作用。

Biophysical characterization and membrane interaction of the two fusion loops of glycoprotein B from herpes simplex type I virus.

机构信息

Division of Biostructures, Department of Biological Sciences, University of Naples Federico II, Napoli, Italy.

出版信息

PLoS One. 2012;7(2):e32186. doi: 10.1371/journal.pone.0032186. Epub 2012 Feb 23.

DOI:10.1371/journal.pone.0032186
PMID:22384173
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3285657/
Abstract

The molecular mechanism of entry of herpesviruses requires a multicomponent fusion system. Cell invasion by Herpes simplex virus (HSV) requires four virally encoded glycoproteins: namely gD, gB and gH/gL. The role of gB has remained elusive until recently when the crystal structure of HSV-1 gB became available and the fusion potential of gB was clearly demonstrated. Although much information on gB structure/function relationship has been gathered in recent years, the elucidation of the nature of the fine interactions between gB fusion loops and the membrane bilayer may help to understand the precise molecular mechanism behind herpesvirus-host cell membrane fusion. Here, we report the first biophysical study on the two fusion peptides of gB, with a particular focus on the effects determined by both peptides on lipid bilayers of various compositions. The two fusion loops constitute a structural subdomain wherein key hydrophobic amino acids form a ridge that is supported on both sides by charged residues. When used together the two fusion loops have the ability to significantly destabilize the target membrane bilayer, notwithstanding their low bilayer penetration when used separately. These data support the model of gB fusion loops insertion into cholesterol enriched membranes.

摘要

疱疹病毒进入的分子机制需要一个多组分融合系统。单纯疱疹病毒 (HSV) 的细胞入侵需要四种病毒编码的糖蛋白:gD、gB 和 gH/gL。直到最近,当获得 1 型单纯疱疹病毒 (HSV-1) gB 的晶体结构并清楚地证明了 gB 的融合潜力时,gB 的作用才变得难以捉摸。尽管近年来收集了大量关于 gB 结构/功能关系的信息,但阐明 gB 融合环与膜双层之间精细相互作用的性质可能有助于了解疱疹病毒-宿主细胞膜融合背后的确切分子机制。在这里,我们报告了 gB 的两个融合肽的第一个生物物理研究,特别关注这两个肽对各种组成的脂质双层的确定影响。这两个融合环构成了一个结构亚域,其中关键的疏水性氨基酸形成一个脊,由带电荷的残基支撑在两侧。当一起使用时,这两个融合环能够显著破坏靶双层膜的稳定性,尽管它们单独使用时穿透双层膜的能力较低。这些数据支持 gB 融合环插入富含胆固醇的膜的模型。

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