无干扰素治疗丙型肝炎病毒基因型 1 的 2b 期临床试验。
Phase 2b trial of interferon-free therapy for hepatitis C virus genotype 1.
机构信息
From the Digestive Disease Institute, Virginia Mason Medical Center, Seattle (K.V.K.); Texas Liver Institute, University of Texas Health Science Center, San Antonio (E.L., F.P.); AbbVie, North Chicago (D.E.C., W.X., T.P.-M., G.L., L.L., A.K., T.P., B.B.); University of Florida College of Medicine, Gainesville (D.R.N.); J.W. Goethe University, Frankfurt, Germany (S.Z.); University of Colorado Denver, Aurora (G.T.E.); Indiana University, Indianapolis (P.K.); Queen Mary, University of London, Barts Health, London (G.R.F.); and Johns Hopkins University, Baltimore (M.S.S.).
出版信息
N Engl J Med. 2014 Jan 16;370(3):222-32. doi: 10.1056/NEJMoa1306227.
BACKGROUND
An interferon-free combination of the protease inhibitor ABT-450 with ritonavir (ABT-450/r), the nonnucleoside polymerase inhibitor ABT-333, and ribavirin showed efficacy against the hepatitis C virus (HCV) in a pilot study involving patients with HCV genotype 1 infection. The addition of another potent agent, the NS5A inhibitor ABT-267, may improve efficacy, especially in difficult-to-treat patients. This study was designed to evaluate multiple regimens of direct-acting antiviral agents and ribavirin in patients with HCV genotype 1 infection who had not received therapy previously or who had no response to prior therapy with pegylated interferon and ribavirin.
METHODS
In this phase 2b, open-label study with 14 treatment subgroups, 571 patients without cirrhosis who had not received treatment previously or who had not had a response to prior therapy were randomly assigned to a regimen of ABT-450/r, combined with ABT-267 or ABT-333 or both, for 8, 12, or 24 weeks and received at least one dose of therapy. All the subgroups but 1 also received ribavirin (dose determined according to body weight). The primary end point was sustained virologic response at 24 weeks after the end of treatment. The primary efficacy analysis compared rates between previously untreated patients who received three direct-acting antiviral agents and ribavirin for 8 weeks and those who received the same therapy for 12 weeks.
RESULTS
Among previously untreated patients who received three direct-acting antiviral agents (with the ABT-450/r dose administered as 150 mg of ABT-450 and 100 mg of ritonavir) plus ribavirin, the rate of sustained virologic response at 24 weeks after treatment was 88% among those who received the therapy for 8 weeks and 95% among those who received the therapy for 12 weeks (difference, -7 percentage points; 95% confidence interval, -19 to 5; P=0.24). The rates of sustained virologic response across all treatment subgroups ranged from 83 to 100%. The most frequent adverse events were fatigue, headache, nausea, and insomnia. Eight patients (1%) discontinued treatment owing to adverse events.
CONCLUSIONS
In this phase 2b study, all-oral regimens of antiviral agents and ribavirin were effective both in patients with HCV genotype 1 infection who had not received therapy previously and in those who had not had a response to prior therapy. (Funded by AbbVie; ClinicalTrials.gov number, NCT01464827.).
背景
蛋白酶抑制剂 ABT-450 与利托那韦(ABT-450/r)、非核苷聚合酶抑制剂 ABT-333 和利巴韦林组成的无干扰素联合方案在一项涉及 HCV 基因型 1 感染患者的初步研究中显示出对 HCV 的疗效。添加另一种强效药物 NS5A 抑制剂 ABT-267 可能会提高疗效,尤其是在难治性患者中。本研究旨在评估无先前治疗或对聚乙二醇干扰素和利巴韦林先前治疗无反应的 HCV 基因型 1 感染患者的多种直接作用抗病毒药物和利巴韦林治疗方案。
方法
在这项涉及 14 个治疗亚组的 2b 期、开放性标签研究中,571 名无肝硬化且未接受治疗或对先前的聚乙二醇干扰素和利巴韦林治疗无反应的患者被随机分配至接受 ABT-450/r 联合 ABT-267 或 ABT-333 或两者联合治疗 8、12 或 24 周,并接受至少一剂治疗。除 1 个亚组外,所有亚组均接受利巴韦林(根据体重确定剂量)。主要终点是治疗结束后 24 周时的持续病毒学应答。主要疗效分析比较了接受三种直接作用抗病毒药物和利巴韦林治疗 8 周与接受相同治疗 12 周的无先前治疗患者之间的比率。
结果
在接受三种直接作用抗病毒药物(ABT-450/r 剂量为 150 mg ABT-450 和 100 mg 利托那韦)加利巴韦林治疗的无先前治疗患者中,治疗 8 周和 12 周时的持续病毒学应答率分别为 88%和 95%(差异为-7 个百分点;95%置信区间为-19 至 5;P=0.24)。所有治疗亚组的持续病毒学应答率均在 83%至 100%之间。最常见的不良反应是疲劳、头痛、恶心和失眠。8 名患者(1%)因不良事件停止治疗。
结论
在这项 2b 期研究中,无先前治疗或对先前治疗无反应的 HCV 基因型 1 感染患者的抗病毒药物和利巴韦林联合口服方案均有效。(由 AbbVie 资助;ClinicalTrials.gov 编号,NCT01464827)。
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