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A novel small-molecule inhibitor of influenza A virus acts by suppressing PA endonuclease activity of the viral polymerase

机译:一种新型的甲型流感病毒小分子抑制剂通过抑制病毒聚合酶的PA核酸内切酶活性发挥作用

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摘要

The RNA-dependent RNA polymerase of influenza A virus comprises conserved and independently-folded subdomains with defined functionalities. The N-terminal domain of the PA subunit (PAN) harbors the endonuclease function so that it can serve as a desired target for drug discovery. To identify a class of anti-influenza inhibitors that impedes PAN endonuclease activity, a screening approach that integrated the fluorescence resonance energy transfer based endonuclease inhibitory assay with the DNA gel-based endonuclease inhibitory assay was conducted, followed by the evaluation of antiviral efficacies and potential cytotoxicity of the primary hits in vitro and in vivo. A small-molecule compound ANA-0 was identified as a potent inhibitor against the replication of multiple subtypes of influenza A virus, including H1N1, H3N2, H5N1, H7N7, H7N9 and H9N2, in cell cultures. Combinational treatment of zanamivir and ANA-0 exerted synergistic anti-influenza effect in vitro. Intranasal administration of ANA-0 protected mice from lethal challenge and reduced lung viral loads in H1N1 virus infected BALB/c mice. In summary, ANA-0 shows potential to be developed to novel anti-influenza agents.
机译:甲型流感病毒的RNA依赖性RNA聚合酶包含具有确定功能的保守且独立折叠的亚结构域。 PA亚基(PAN)的N末端结构域具有核酸内切酶功能,因此可以用作药物发现的理想靶标。为了鉴定一类阻碍PAN核酸内切酶活性的抗流感抑制剂,进行了将基于荧光共振能量转移的核酸内切酶抑制分析与基于DNA凝胶的核酸内切酶抑制分析相结合的筛选方法,然后评估了抗病毒效果和潜力体外和体内原发命中的细胞毒性。小分子化合物ANA-0被确定为有效的抑制剂,可在细胞培养物中阻止多种亚型的流感病毒复制,包括H1N1,H3N2,H5N1,H7N7,H7N9和H9N2。扎那米韦和ANA-0的联合治疗在体外发挥协同抗流感作用。鼻内注射ANA-0可保护小鼠免受致命的攻击,并减少感染H1N1病毒的BALB / c小鼠的肺病毒载量。总而言之,ANA-0显示出有可能被开发为新型抗流感药物。

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