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Large-Scale Screening and Identification of Novel Ebola Virus and Marburg Virus Entry Inhibitors

机译:新型埃博拉病毒和马尔堡病毒进入抑制剂的大规模筛选和鉴定

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Filoviruses are highly infectious, and no FDA-approved drug therapy for filovirus infection is available. Most work to find a treatment has involved only a few strains of Ebola virus and testing of relatively small drug libraries or compounds that have shown efficacy against other virus types. Here we report the findings of a high-throughput screening of 319,855 small molecules from the Molecular Libraries Small Molecule Repository library for their activities against Marburg virus and Ebola virus. Nine of the most potent, novel compounds that blocked infection by both viruses were analyzed in detail for their mechanisms of action. The compounds inhibited known key steps in the Ebola virus infection mechanism by blocking either cell surface attachment, macropinocytosis-mediated uptake, or endosomal trafficking. To date, very few specific inhibitors of macropinocytosis have been reported. The 2 novel macropinocytosis inhibitors are more potent inhibitors of Ebola virus infection and less toxic than ethylisopropylamiloride, one commonly accepted macropinocytosis inhibitor. Each compound blocked infection of primary human macrophages, indicating their potential to be developed as new antifiloviral therapies.
机译:丝状病毒具有高度传染性,目前尚无FDA批准的丝状病毒感染药物治疗方法。寻找治疗方法的大多数工作仅涉及几株埃博拉病毒,并测试了相对较小的药物文库或化合物,这些化合物或化合物已显示出对其他病毒类型的功效。在这里,我们报告了从分子库小分子储存库中对319,855个小分子进行高通量筛选的结果,这些小分子具有针对马堡病毒和埃博拉病毒的活性。详细分析了阻止两种病毒感染的最有效的九种新型化合物的作用机理。这些化合物通过阻断细胞表面附着,巨胞饮介导的摄取或内体运输来抑制埃博拉病毒感染机制中的已知关键步骤。迄今为止,已经报道了很少有特异的巨胞饮抑制剂。两种新型的巨胞饮抑制剂是一种有效的埃博拉病毒感染抑制剂,并且比乙基异丙基阿米洛利(一种普遍接受的巨胞饮抑制剂)毒性更小。每种化合物均阻止了人类原发性巨噬细胞的感染,表明它们有可能被开发为新的抗丝状病毒疗法。

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