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丙型肝炎病毒的进入与中和抗体:病毒变体带来的启示

HCV entry and neutralizing antibodies: lessons from viral variants.

作者信息

Zeisel Mirjam B, Baumert Thomas F

机构信息

Inserm, U748, Strasbourg, France.

出版信息

Future Microbiol. 2009 Jun;4(5):511-7. doi: 10.2217/fmb.09.34.

Abstract

Evaluation of: Grove J, Nielsen S, Zhong J et al.: Identification of a residue in hepatitis C virus E2 glycoprotein that determines scavenger receptor BI and CD81 receptor dependency and sensitivity to neutralizing antibodies. J. Virol. 82 (24), 12020-12029 (2008). Recent data suggest that a strong, early, broad neutralizing antibody response may contribute to the control of HCV in the acute phase of infection. However, the majority of individuals fail to clear HCV during the first months following infection and develop chronic infection despite the presence of anti-HCV antibodies. A prerequisite of the understanding behind the mechanisms of viral escape from antibody-mediated neutralization is the identification of various host-entry factors mediating the first steps of viral infection - binding and entry of HCV is believed to be a multistep process involving HCV envelope glycoproteins E1 and E2 as well as several host-cell surface molecules such as CD81, scavenger receptor class B type I, members of the claudin family and occludin. In this article, Grove et al. describe a single mutation in the HCV envelope glycoprotein E2 that alters glycoprotein structure thereby modulating viral interaction with scavenger receptor class B type I and CD81, and increasing sensitivity to neutralizing antibodies. The results of this study highlight the importance of the characterization of the interplay between HCV particles and host-cell factors for the understanding of virus neutralization by host-immune responses and pathogenesis of HCV infection.

摘要

文献评价

格罗夫(Grove J)、尼尔森(Nielsen S)、钟(Zhong J)等人:鉴定丙型肝炎病毒E2糖蛋白中的一个残基,该残基决定清道夫受体BI和CD81受体依赖性以及对中和抗体的敏感性。《病毒学杂志》82卷(24期),12020 - 12029页(2008年)。近期数据表明,强烈、早期、广泛的中和抗体反应可能有助于在感染急性期控制丙型肝炎病毒(HCV)。然而,大多数个体在感染后的头几个月未能清除HCV,尽管存在抗HCV抗体仍发展为慢性感染。理解病毒逃避抗体介导中和机制的一个前提是鉴定介导病毒感染第一步——结合和进入的各种宿主进入因子。HCV的结合和进入被认为是一个多步骤过程,涉及HCV包膜糖蛋白E1和E2以及几种宿主细胞表面分子,如CD81、I型清道夫受体B类、claudin家族成员和occludin。在本文中,格罗夫等人描述了HCV包膜糖蛋白E2中的一个单突变,该突变改变了糖蛋白结构,从而调节病毒与I型清道夫受体B类和CD81的相互作用,并增加对中和抗体的敏感性。这项研究的结果突出了表征HCV颗粒与宿主细胞因子之间相互作用对于理解宿主免疫反应介导的病毒中和以及HCV感染发病机制的重要性。

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本文引用的文献

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