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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:通过抑制病毒聚合酶的PA内切核酸酶活性,通过抑制病毒聚合酶的PA内切核酸酶活性作用的小型小分子抑制剂

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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 (PA(N)) 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 PA(N) 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:流感的RNA依赖性RNA聚合酶病毒包括具有定义函数的保守和独立折叠的子域。 PA亚基的N-末端结构域(PA(n))留地核酸酶函数,使其可以作为药物发现的所需靶标。为了鉴定阻抗PA(n)内切核酸酶活性的一类抗流感抑制剂,对荧光共振能量转移的内切核酸酶抑制试验进行了一种筛选方法,进行了DNA凝胶基内核酸酶抑制抑制测定,然后进行抗病毒的评价体外和体内初级击中的疗效和潜在细胞毒性。将小分子化合物Ana-0鉴定为符合细胞培养物中的多种流感病毒的多种亚型病毒亚型的有效抑制剂,包括H1N1,H3N2,H5N1,H7N7,H7N9和H9N2。 Zanamivir和ANA-0的组合治疗在体外施加协同抗流感作用。 H1N1病毒感染BALB / C小鼠的致死攻击和降低肺病病毒载体的鼻内施用ANA-0保护小鼠。总之,ANA-0显示出于新型抗流感剂的潜力。

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