Danoprevir, a small-molecule NS3/4A protease inhibitor for the potential oral treatment of HCV infection.

Melanie Deutsch, George V Papatheodoridis
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Abstract

Danoprevir (ITMN-191; RG-7227), under development by InterMune Inc and Roche Holding AG, is a promising, potent NS3/4A protease inhibitor for the oral treatment of HCV infection. Preclinical data demonstrated that danoprevir binds with high affinity and dissociates slowly from the HCV NS3 protease, allowing high liver drug exposure with only modest plasma drug exposure. A phase Ib, 'IFN-free' clinical trial demonstrated that danoprevir, combined with the HCV polymerase inhibitor RG-7128 (Pharmasset Inc/Roche Holding AG), was effective in reducing HCV-RNA levels in a large proportion of treatment-naïve patients with HCV infection and in approximately half of previously non-responsive patients with HCV-1 infection, without resistance or safety concerns. In a phase IIb trial in treatment-naïve patients with HCV-1 infection, danoprevir plus pegylated IFNalpha2a and ribavirin resulted in undetectable levels of HCV-RNA in the majority of patients, without any evidence of viral resistance; however, the high-dose danoprevir arm was prematurely terminated because of grade 4 ALT elevations. Phase I trials have also demonstrated that ritonavir boosting improved the pharmacokinetic profile of danoprevir; therefore, at the time of publication, a phase IIb trial to evaluate ritonavir-boosted, low-dose danoprevir in combination with RG-7128 was planned.

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Danoprevir是一种小分子NS3/4A蛋白酶抑制剂,可用于口服治疗HCV感染。
Danoprevir (itmn - 191;RG-7227)由InterMune Inc .和罗氏控股公司(Roche Holding AG)联合开发,是一种有前景的有效NS3/4A蛋白酶抑制剂,可用于口服治疗HCV感染。临床前数据表明,danoprevir与HCV NS3蛋白酶具有高亲和力结合并缓慢解离,允许高肝脏药物暴露,仅适度的血浆药物暴露。一项Ib期“无ifn”临床试验表明,danoprevir联合HCV聚合酶抑制剂RG-7128 (Pharmasset Inc . /Roche Holding AG)可有效降低大部分treatment-naïve HCV感染患者和大约一半先前无反应的HCV-1感染患者的HCV- rna水平,无耐药或安全性问题。在treatment-naïve HCV-1感染患者的IIb期试验中,danoprevir加聚乙二醇化IFNalpha2a和利巴韦林导致大多数患者的HCV-RNA水平检测不到,没有任何病毒耐药性的证据;然而,由于4级ALT升高,高剂量danoprevir组过早终止。I期试验也表明,利托那韦增强改善了达诺韦的药代动力学特征;因此,在本文发表时,一项评估利托那韦增强、低剂量danoprevir与RG-7128联合的IIb期试验正在计划中。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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