The multipartite system that mediates entry of herpes simplex virus into the cell

外域 疱疹病毒糖蛋白B 单纯疱疹病毒 糖蛋白 脂质双层融合 病毒进入 融合蛋白 七肽重复区 受体 生物 细胞生物学 病毒学 化学 病毒 重组DNA 分子生物学 生物化学 肽序列 病毒复制 基因
作者
Gabriella Campadelli‐Fiume,Michele Amasio,Elisa Avitabile,Arianna Cerretani,Cristina Forghieri,Tatiana Gianni,Laura Menotti
出处
期刊:Reviews in Medical Virology [Wiley]
卷期号:17 (5): 313-326 被引量:145
标识
DOI:10.1002/rmv.546
摘要

Abstract The multipartite entry‐fusion system of herpes simplex virus is made of a quartet of glycoproteins—gD, gB, gH·gL—and three alternative gD receptors, herpesvirus entry mediator (HVEM), nectin1 and modified sites on heparan sulphate. This multipartite system recapitulates the basic steps of virus—cell fusion, i.e. receptor recognition, triggering of fusion and fusion execution. Specifically, in addition to serving as the receptor‐binding glycoprotein, gD triggers fusion through a specialised domain, named pro‐fusion domain (PFD), located C‐terminally in the ectodomain. In the unliganded gD the C‐terminal region folds around the N‐terminal region, such that gD adopts a closed autoinhibited conformation. In HVEM‐ and nectin1‐bound gD the C‐terminal region is displaced (opened conformation). gD is the tool for modification of HSV tropism, through insertion of ligands to heterologous tumour‐specific receptors. It is discussed whether gD responds to the interaction with the natural and the heterologous receptors by adopting similar conformations, and whether the closed‐to‐open switch in conformation is a generalised mechanism of activation. A peculiar recombinant highlighted that the central Ig‐folded core of gD may not encode executable functions for entry and that the 219–314 aa segment may be sufficient to trigger fusion. With respect to fusion execution, gB appears to be a prospective fusogen based on its coiled‐coil trimeric structure, similar to that of another fusion glycoprotein. On the other hand, gH exhibits molecular elements typical of class 1 fusion glycoproteins, in particular heptad repeats and strong tendency to interact with lipids. Whether fusion execution is carried out by gB or gH·gL, or both glycoproteins in complex or sequentially remains to be determined. Copyright © 2007 John Wiley & Sons, Ltd.
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