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蛋白酶抑制剂 GS-9256 和非核苷聚合酶抑制剂替诺福韦酯单独使用,或与利巴韦林、聚乙二醇干扰素联合利巴韦林治疗丙型肝炎。

The protease inhibitor, GS-9256, and non-nucleoside polymerase inhibitor tegobuvir alone, with ribavirin, or pegylated interferon plus ribavirin in hepatitis C.

机构信息

University Hospital, JW Goethe University, Frankfurt, Germany.

出版信息

Hepatology. 2012 Mar;55(3):749-58. doi: 10.1002/hep.24744.

DOI:10.1002/hep.24744
PMID:22006408
Abstract

UNLABELLED

Tegobuvir (GS-9190), a non-nucleoside nonstructural protein (NS)5B polymerase inhibitor, and GS-9256, an NS3 serine protease inhibitor, individually have activity against hepatitis C virus (HCV) genotype 1. The antiviral activity of tegobuvir and GS-9256 as oral combination therapy, or together with ribavirin (RBV) or pegylated interferon (Peg-IFN) alpha-2a and RBV, was assessed in a phase II, randomized, open-label trial. Treatment-naïve patients with genotype 1 HCV were assigned 28 days of tegobuvir 40 mg twice-daily (BID) and GS-9256 75 mg BID (n = 16), tegobuvir and GS-9256 plus RBV 1,000-1,200 mg daily (n = 15), or tegobuvir and GS-9256 plus Peg-IFN alpha-2a (180 μg once-weekly)/RBV (n = 15). The primary efficacy endpoint was rapid virologic response (RVR), with HCV RNA <25 IU/mL at day 28. After 28 days, all patients received Peg-IFN/RBV. All patients with viral rebound or nonresponse, defined as >0.5-log(10) increase in HCV RNA from nadir or <2-log decrease at day 5, initiated Peg-IFN/RBV immediately. Median maximal reductions in HCV RNA were -4.1 log(10) IU/mL for tegobuvir/GS-9256, -5.1 log(10) IU/mL for tegobuvir/GS-9256/RBV, and -5.7 log(10) IU/mL for tegobuvir/9256/Peg-IFN/RBV. RVR was observed in 7% (1 of 15) of patients receiving tegobuvir/GS-9256, 38% (5 of 13) receiving tegobuvir/GS-9256/RBV, and 100% (14 of 14) receiving tegobuvir/9256/PEG-IFN/RBV. The addition of Peg-IFN/RBV at day 28 or earlier resulted in HCV RNA <25 IU/mL at week 24 in 67% (10 of 15), 100% (13 of 13), and 94% (13 of 14) of patients in the three treatment groups. Transient elevations in serum bilirubin occurred in all treatment groups.

CONCLUSION

In genotype 1 HCV, adding RBV or RBV with Peg-IFN provides additive antiviral activity to combination therapy with tegobuvir and GS-9256.

摘要

目的

评估替诺福韦(GS-9190)和GS-9256(一种 NS3 丝氨酸蛋白酶抑制剂)在 HCV 基因型 1 患者中作为口服联合治疗的抗病毒活性,以及联合利巴韦林(RBV)或聚乙二醇干扰素(Peg-IFN)α-2a 和 RBV 的抗病毒活性。

方法

未经治疗的 HCV 基因型 1 患者被分配接受替诺福韦 40 mg 每日两次(BID)和 GS-9256 75 mg BID(n = 16),替诺福韦和 GS-9256 加 RBV 1000-1200 mg 每日(n = 15),或替诺福韦和 GS-9256 加 Peg-IFNα-2a(180μg 每周一次)/RBV(n = 15)。主要疗效终点为快速病毒学应答(RVR),定义为第 28 天 HCV RNA<25 IU/mL。28 天后,所有患者均接受 Peg-IFN/RBV 治疗。所有病毒反弹或无应答的患者(定义为 HCV RNA 从最低点增加>0.5-log(10)或第 5 天降低<2-log)立即开始接受 Peg-IFN/RBV 治疗。替诺福韦/GS-9256、替诺福韦/GS-9256/RBV 和替诺福韦/GS-9256/Peg-IFN/RBV 的 HCV RNA 最大降低中位数分别为-4.1 log(10)IU/mL、-5.1 log(10)IU/mL 和-5.7 log(10)IU/mL。接受替诺福韦/GS-9256 的患者中有 7%(15 例中的 1 例),接受替诺福韦/GS-9256/RBV 的患者中有 38%(13 例中的 5 例),接受替诺福韦/GS-9256/Peg-IFN/RBV 的患者中有 100%(14 例中的 14 例)达到 RVR。在第 28 天或更早时加用 Peg-IFN/RBV 治疗,三组患者在第 24 周时 HCV RNA<25 IU/mL 的比例分别为 67%(10/15)、100%(13/13)和 94%(13/14)。所有治疗组患者的血清胆红素均短暂升高。

结论

在 HCV 基因型 1 患者中,联合利巴韦林或利巴韦林联合聚乙二醇干扰素可增强替诺福韦和 GS-9256 联合治疗的抗病毒活性。

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