McPhee Fiona, Hernandez Dennis, Zhou Nannan, Yu Fei, Ueland Joseph, Monikowski Aaron, Chayama Kazuaki, Toyota Joji, Izumi Namiki, Yokosuka Osamu, Kawada Norifumi, Osaki Yukio, Hughes Eric A, Watanabe Hideaki, Ishikawa Hiroki, Kumada Hiromitsu
Bristol-Myers Squibb, Wallingford, CT, USA.
Antivir Ther. 2014;19(5):479-90. doi: 10.3851/IMP2729. Epub 2014 Jan 22.
Daclatasvir (DCV; BMS-790052) is a picomolar inhibitor of HCV non-structural protein 5A (NS5A) and has demonstrated efficacy in patients chronically infected with HCV.
In the double-blind, randomized studies AI444021 and AI444022, 71 Japanese patients chronically infected with HCV genotype 1 (predominantly genotype 1b) received DCV (10 mg or 60 mg) plus peginterferon alfa-2b or alfa-2a and ribavirin. Virological failure occurred in 14% (5/36) of treatment-naive patients and 54% (19/35) of prior alfa/ribavirin non-responders. Resistance testing was performed on baseline samples and samples with HCV RNA≥1,000 IU/ml at week 1 through post-treatment week 24.
Baseline NS5A resistance-associated polymorphisms had less impact on virological response rates than IL28B genotype. All patients with virological failure had NS5A DCV-resistant variants at the time of failure. The predominant NS5A variants were L31V/M/I plus Y93H; this combination was detected in 100% (5/5) of treatment-naive patients and 74% (14/19) of non-responders with failure. Emergent resistance variants in prior non-responders (four viral breakthroughs, one relapse) were more varied with novel combinations such as L31F-ΔP32 and L28M-R30Q-A92K detected. Significant loss in DCV antiviral activity was generally only seen with ≥ two resistance-associated NS5A substitutions. All DCV-resistant variants were still detected at end of study.
Virological failure in HCV genotype 1b treatment-naive Japanese patients receiving DCV plus alfa-2a/ribavirin or alfa-2b/ribavirin was associated with enrichment of NS5A resistance variants L31V/M-Y93H. In prior non-responders, emergent variants associated with failure also included NS5A-A92K or NS5A-ΔP32. As with L31-Y93 variants, these variants persisted.
达卡他韦(DCV;BMS-790052)是一种针对丙型肝炎病毒非结构蛋白5A(NS5A)的皮摩尔级抑制剂,已在慢性丙型肝炎病毒感染患者中显示出疗效。
在双盲、随机研究AI444021和AI444022中,71例慢性感染丙型肝炎病毒基因1型(主要为基因1b型)的日本患者接受了DCV(10毫克或60毫克)联合聚乙二醇干扰素α-2b或α-2a及利巴韦林治疗。初治患者中14%(5/36)发生病毒学失败,既往α/利巴韦林治疗无应答者中54%(19/35)发生病毒学失败。对基线样本以及治疗第1周直至治疗后第24周HCV RNA≥1000 IU/ml的样本进行耐药性检测。
与IL28B基因型相比,基线NS5A耐药相关多态性对病毒学应答率的影响较小。所有发生病毒学失败的患者在失败时均有NS5A DCV耐药变异。主要的NS5A变异为L31V/M/I加Y93H;在100%(5/5)的初治患者和74%(14/19)治疗失败的无应答者中检测到这种组合。既往无应答者中出现的耐药变异(4例病毒突破,1例复发)更多样化,检测到新的组合如L31F-ΔP32和L28M-R30Q-A92K。通常仅在出现≥两个与耐药相关的NS5A替换时才观察到达卡他韦抗病毒活性显著丧失。在研究结束时仍能检测到所有达卡他韦耐药变异。
接受DCV联合α-2a/利巴韦林或α-2b/利巴韦林治疗的基因1b型初治日本丙型肝炎患者发生病毒学失败与NS5A耐药变异L31V/M-Y93H的富集有关。在既往无应答者中,与治疗失败相关的新出现变异还包括NS5A-A92K或NS-AΔP32。与L31-Y93变异一样,这些变异持续存在。
