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Hepatitis C virus NS3-4A protease inhibitors: countering viral subversion in vitro and showing promise in the clinic.

机译:丙型肝炎病毒NS3-4A蛋白酶抑制剂:在体外对抗病毒颠覆并在临床上显示出希望。

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摘要

Hepatitis C virus (HCV) NS3.4A protease inhibitors have potential for treating chronic HCV disease. Robust antiviral effects have been reported for the three HCV NS3.4A inhibitors (BILN-2061 (ciluprevir), telaprevir (VX-950; Vertex Pharmaceuticals Inc./Janssen Pharnmaceutica NV/Mitsubishi Pharma Corp.) and SCH-503034; Schering-Plough Research Institute) that have been studied in clinical trials to date in HCV-infected patients, and new inhibitor molecules continue to appear on the horizon. Herein, toe relate the remarkable progress of these drug candidates to recent evidence that suggests HCV might depend on NS3.4A protease to subvert multiple innate cellular defense mechanisms.
机译:丙型肝炎病毒(HCV)NS3.4A蛋白酶抑制剂具有治疗慢性HCV疾病的潜力。三种HCV NS3.4A抑制剂(BILN-2061(ciluprevir),telaprevir(VX-950; Vertex Pharmaceuticals Inc./Janssen Pharnmaceutica NV / Mitsubishi Pharma Corp.)和SCH-503034;先灵Sch雅(Schering-Plough)的抗病毒作用已有报道迄今为止,已经在HCV感染患者的临床试验中进行了研究,并且新的抑制剂分子继续出现。在本文中,脚趾与这些候选药物的显着进展与最近的证据相关,这些证据表明HCV可能依赖于NS3.4A蛋白酶来破坏多种先天的细胞防御机制。

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