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口蹄疫病毒装配连续阶段中涉及的亚基间界面处对突变的不同功能敏感性。

Different functional sensitivity to mutation at intersubunit interfaces involved in consecutive stages of foot-and-mouth disease virus assembly.

作者信息

Rincón Verónica, Rodríguez-Huete Alicia, Mateu Mauricio G

机构信息

Centro de Biología Molecular 'Severo Ochoa' (CSIC-UAM), Universidad Autónoma de Madrid, Cantoblanco, 28049 Madrid, Spain.

出版信息

J Gen Virol. 2015 Sep;96(9):2595-2606. doi: 10.1099/vir.0.000187. Epub 2015 May 15.

DOI:10.1099/vir.0.000187
PMID:25979732
Abstract

Small spherical viruses are paradigms of supramolecular self-assembly. Identifying the specific structural determinants for virus assembly provides guidelines to develop new antiviral drugs or engineer modified viral particles for medical or technological applications. However, very few systematic studies have been carried out so far to identify those chemical groups at interfaces between virus capsid subunits that are important for viral assembly and function. Foot-and-mouth disease virus (FMDV) and other picornaviruses are assembled in a stepwise process in which different protein-protein interfaces are formed: 5 protomeric subunits oligomerize to form a pentameric intermediate, and 12 of these stable pentameric building blocks associate to form a labile capsid. In this study, a systematic mutational analysis revealed that very few amino acid side chains involved in substantial interactions between protomers within each pentamer are individually required for virus infectivity. This result contrasts sharply with the previous finding that most amino acid side chains involved in interactions between pentamers during the next assembly step are individually required for infectivity. The dramatic difference in sensitivity to single mutations between the two types of protein-protein interfaces in FMDV is discussed in terms of possible structural strategies for achieving self-assembly and genome uncoating in the face of diverse selective constraints.

摘要

小型球形病毒是超分子自组装的典范。确定病毒组装的特定结构决定因素可为开发新型抗病毒药物或设计用于医学或技术应用的修饰病毒颗粒提供指导。然而,迄今为止,很少有系统的研究来确定病毒衣壳亚基之间界面处那些对病毒组装和功能至关重要的化学基团。口蹄疫病毒(FMDV)和其他小核糖核酸病毒以逐步过程进行组装,在此过程中形成不同的蛋白质-蛋白质界面:5个原体亚基寡聚形成五聚体中间体,12个这些稳定的五聚体构建块结合形成不稳定的衣壳。在本研究中,系统的突变分析表明,每个五聚体内原体之间大量相互作用所涉及的氨基酸侧链中,只有极少数是病毒感染性单独所需的。这一结果与之前的发现形成鲜明对比,即在下一个组装步骤中五聚体之间相互作用所涉及的大多数氨基酸侧链是感染性单独所需的。针对面对各种选择限制时实现自组装和基因组脱壳的可能结构策略,讨论了FMDV中两种类型蛋白质-蛋白质界面之间对单突变敏感性的巨大差异。

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Optimized Adenoviral Vector That Enhances the Assembly of FMDV O1 Virus-Like Particles Increases Its Potential as Vaccine for Serotype O Viruses.优化的腺病毒载体可增强口蹄疫病毒O1型病毒样颗粒的组装,提高其作为O型病毒疫苗的潜力。
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