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Novel RU486 (mifepristone) analogues with increased activity against Venezuelan Equine Encephalitis Virus but reduced progesterone receptor antagonistic activity

机译:新型RU486(米非司酮)类似物具有增强的抗委内瑞拉马脑炎病毒活性但孕酮受体拮抗活性降低

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摘要

There are currently no therapeutics to treat infection with the alphavirus Venezuelan equine encephalitis virus (VEEV), which causes flu-like symptoms leading to neurological symptoms in up to 14% of cases. Large outbreaks of VEEV can result in 10,000 s of human cases and mass equine death. We previously showed that mifepristone (RU486) has anti-VEEV activity (EC50 = 20 μM) and only limited cytotoxicity (CC50 > 100 μM), but a limitation in its use is its abortifacient activity resulting from its ability to antagonize the progesterone receptor (PR). Here we generate a suite of new mifepristone analogues with enhanced antiviral properties, succeeding in achieving >11-fold improvement in anti-VEEV activity with no detectable increase in toxicity. Importantly, we were able to derive a lead compound with an EC50 of 7.2 µM and no detectable PR antagonism activity. Finally, based on our SAR analysis we propose avenues for the further development of these analogues as safe and effective anti-VEEV agents.
机译:目前尚无可治疗甲型病毒委内瑞拉马脑炎病毒(VEEV)的疗法,该病毒可导致多达14%的病例出现类似流感的症状,并导致神经系统症状。 VEEV的大爆发可能导致10,000例人类病例和大规模马死亡。先前我们已经证明米非司酮(RU486)具有抗VEEV活性(EC50 = 20μM),并且细胞毒性有限(CC50> 100μM),但由于其拮抗孕激素受体的能力而导致其流产活性受到限制( PR)。在这里,我们产生了一套具有增强的抗病毒特性的新的米非司酮类似物,成功实现了抗VEEV活性提高> 11倍的改善,而没有可检测到的毒性增加。重要的是,我们能够获得EC50为7.2μm且无可检测的PR拮抗活性的先导化合物。最后,基于我们的SAR分析,我们提出了进一步开发这些类似物作为安全有效的抗VEEV药物的途径。

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