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口蹄疫病毒衣壳的热稳定性由致死性和生存能力恢复性补偿氨基酸取代调节。

Thermostability of the Foot-and-Mouth Disease Virus Capsid Is Modulated by Lethal and Viability-Restoring Compensatory Amino Acid Substitutions.

机构信息

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

National Veterinary Institute, Technical University of Denmark, Kalvehave, Denmark.

出版信息

J Virol. 2019 May 1;93(10). doi: 10.1128/JVI.02293-18. Print 2019 May 15.

Abstract

Infection by viruses depends on a balance between capsid stability and dynamics. This study investigated biologically and biotechnologically relevant aspects of the relationship in foot-and-mouth disease virus (FMDV) between capsid structure and thermostability and between thermostability and infectivity. In the FMDV capsid, a substantial number of amino acid side chains at the interfaces between pentameric subunits are charged at neutral pH. Here a mutational analysis revealed that the essential role for virus infection of most of the 8 tested charged groups is not related to substantial changes in capsid protein expression or processing or in capsid assembly or stability against a thermally induced dissociation into pentamers. However, the positively charged side chains of R2018 and H3141, located at the interpentamer interfaces close to the capsid 2-fold symmetry axes, were found to be critical both for virus infectivity and for keeping the capsid in a state of weak thermostability. A charge-restoring substitution (N2019H) that was repeatedly fixed during amplification of viral genomes carrying deleterious mutations reverted both the lethal and capsid-stabilizing effects of the substitution H3141A, leading to a double mutant virus with close to normal infectivity and thermolability. H3141A and other thermostabilizing substitutions had no detectable effect on capsid resistance to acid-induced dissociation into pentamers. The results suggest that FMDV infectivity requires limited local stability around the 2-fold axes at the interpentamer interfaces of the capsid. The implications for the mechanism of genome uncoating in FMDV and the development of thermostabilized vaccines against foot-and-mouth disease are discussed. This study provides novel insights into the little-known structural determinants of the balance between thermal stability and instability in the capsid of foot-and-mouth disease virus and into the relationship between capsid stability and virus infectivity. The results provide new guidelines for the development of thermostabilized empty capsid-based recombinant vaccines against foot-and-mouth disease, one of the economically most important animal diseases worldwide.

摘要

病毒感染取决于衣壳稳定性和动力学之间的平衡。本研究调查了口蹄疫病毒(FMDV)衣壳结构与热稳定性之间以及热稳定性与感染性之间的生物学和生物技术相关方面的关系。在 FMDV 衣壳中,五聚体亚基之间界面处的大量氨基酸侧链在中性 pH 值下带电荷。在这里,突变分析表明,在 8 个测试的带电基团中,大多数对于病毒感染至关重要的作用与衣壳蛋白表达或加工、衣壳组装或对热诱导解聚为五聚体的稳定性没有实质性变化有关。然而,位于接近衣壳 2 倍对称轴的五聚体间界面处的正带电侧链 R2018 和 H3141 对于病毒感染性和保持衣壳处于弱热稳定性状态都是至关重要的。在携带有害突变的病毒基因组扩增过程中反复固定的电荷恢复取代(N2019H),恢复了 H3141A 取代的致死和衣壳稳定作用,导致具有接近正常感染性和热敏性的双突变病毒。H3141A 和其他热稳定取代对衣壳抵抗酸诱导解聚为五聚体没有可检测的影响。结果表明,FMDV 感染性需要衣壳在五聚体间界面的 2 倍轴周围有一定的局部稳定性。讨论了这些结果对口蹄疫病毒基因组脱壳机制和针对口蹄疫的热稳定疫苗开发的意义。本研究为口蹄疫病毒衣壳中热稳定性和不稳定性之间平衡的未知结构决定因素以及衣壳稳定性与病毒感染性之间的关系提供了新的见解。结果为针对口蹄疫的热稳定空衣壳基于重组疫苗的开发提供了新的指导方针,口蹄疫是全球最重要的动物疾病之一。

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