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Inhibitors of the Sodium Potassium ATPase that Impair Herpes Simplex Virus Replication Identified via a Chemical Screening Approach

机译:通过化学筛选方法鉴定的削弱单纯疱疹病毒复制的钠钾ATP酶抑制剂

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摘要

Small molecules can provide valuable tools to investigate virus biology. We developed a chemical screening approach to identify small molecule inhibitors of poorly understood, pre-early gene expression steps in herpes simplex virus infection, using green fluorescent protein fused to an early protein. Our assay identified ouabain, a cardiac glycoside. Ouabain reversibly decreased viral yield by 100-fold without affecting cellular metabolic activity in an overnight assay. The antiviral potencies of other cardiac glycosides correlated with their potencies against the known target of these compounds, the cellular sodium potassium ATPase. Ouabain had a reduced effect if added 8 hours post infection. It did not inhibit viral attachment or entry, but did reduce the expression of viral immediate early and early genes by at least 5 fold. Collectively, these results implicate a cellular target that was hitherto not considered important for a stage of HSV replication prior to viral gene expression.
机译:小分子可以提供有价值的工具来研究病毒生物学。我们开发了一种化学筛选方法,可以使用融合到早期蛋白质上的绿色荧光蛋白来识别单纯疱疹病毒感染中尚不了解的,早期基因表达步骤的小分子抑制剂。我们的测定方法鉴定出强心苷哇巴因。在过夜试验中,瓦巴因可逆地将病毒产量降低了100倍,而不会影响细胞的代谢活性。其他强心苷的抗病毒效力与其针对这些化合物的已知靶标(细胞钠钾ATP酶)的效力相关。如果在感染后8小时加入,则哇巴因的作用减弱。它没有抑制病毒的附着或进入,但是确实使病毒的早期和早期基因的表达降低了至少5倍。总的来说,这些结果暗示了迄今认为对病毒基因表达之前的HSV复制阶段不重要的细胞靶标。

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