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一种石蒜碱衍生物抗肠道病毒和丙型肝炎病毒的保守抑制机制

A Conserved Inhibitory Mechanism of a Lycorine Derivative against Enterovirus and Hepatitis C Virus.

作者信息

Guo Yu, Wang Yaxin, Cao Lin, Wang Peng, Qing Jie, Zheng Qizhen, Shang Luqing, Yin Zheng, Sun Yuna

机构信息

College of Pharmacy and State Key Laboratory of Medicinal Chemical Biology, Nankai University, Tianjin, China.

College of Pharmacy and State Key Laboratory of Medicinal Chemical Biology, Nankai University, Tianjin, China Collaborative Innovation Center for Biotherapy, Tsinghua University, Beijing, China.

出版信息

Antimicrob Agents Chemother. 2015 Nov 23;60(2):913-24. doi: 10.1128/AAC.02274-15. Print 2016 Feb.

Abstract

Enterovirus 71 (EV71) (Picornaviridae family) and hepatitis C virus (HCV) (Flaviviridae family) are the causative agents of human hand, foot, and mouth disease (HFMD) and hepatitis C, resulting in a severe pandemic involving millions of infections in the Asia-Pacific region and worldwide. The great impact of EV71 and HCV on public health highlights the need to further our understanding of the biology of these two viruses and develop effective therapeutic antivirals. Here, we evaluated a total of 32 lycorine derivatives and demonstrated that 1-acetyllycorine suppressed the proliferation of multiple strains of EV71 in various cells. The results of the drug resistance analysis revealed that 1-acetyllycorine targeted a phenylalanine (F76) in EV71 2A protease (2A(pro)) to stabilize the conformation of a unique zinc finger. Most interestingly, the zinc binding site in EV71 2A(pro) is the exclusive homolog of HCV NS3 among all viruses. Further analysis revealed that 1-acetyllycorine also inhibits HCV with high efficacy, and the mutation on R118 in HCV NS3, which corresponds to F76 in EV71 2A(pro), confers the resistance of HCV to 1-acetyllycorine. These results revealed a conserved mechanism of 1-acetyllycorine against EV71 and HCV through targeting viral proteases. We also documented the significant synergistic anti-EV71 and anti-HCV effects of 1-acetyllycorine with reported inhibitors, supporting potential combination therapy for the treatment of EV71 and HCV infections.

摘要

肠道病毒71型(EV71)(属于小核糖核酸病毒科)和丙型肝炎病毒(HCV)(属于黄病毒科)分别是人类手足口病(HFMD)和丙型肝炎的病原体,在亚太地区乃至全球范围内引发了涉及数百万感染病例的严重疫情。EV71和HCV对公共卫生的巨大影响凸显了进一步了解这两种病毒生物学特性并开发有效抗病毒治疗药物的必要性。在此,我们共评估了32种石蒜碱衍生物,结果表明1-乙酰石蒜碱可抑制多种EV71毒株在多种细胞中的增殖。耐药性分析结果显示,1-乙酰石蒜碱靶向EV71 2A蛋白酶(2A(pro))中的苯丙氨酸(F76)以稳定独特锌指结构的构象。最有趣的是,EV71 2A(pro)中的锌结合位点是所有病毒中HCV NS3的唯一同源物。进一步分析表明,1-乙酰石蒜碱也能高效抑制HCV,并且HCV NS3中与EV71 2A(pro)中的F76相对应的R118位点发生突变会使HCV对1-乙酰石蒜碱产生耐药性。这些结果揭示了1-乙酰石蒜碱通过靶向病毒蛋白酶对EV71和HCV产生作用的保守机制。我们还记录了1-乙酰石蒜碱与已报道的抑制剂联合使用时对EV71和HCV具有显著的协同抗病毒作用,这为治疗EV71和HCV感染的潜在联合疗法提供了支持。

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