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Rapid virological response tailors the duration of treatment in hepatitis C virus genotype 3 patients treated with pegylated interferon alfa-2a and ribavirin in Pakistan

机译:快速的病毒学应答可以根据巴基斯坦的聚乙二醇化干扰素α-2a和利巴韦林对丙型肝炎病毒基因型3患者的治疗时间进行调整

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Background: Rapid virological response (RVR) is now thought to be the strongest predictor of sustained virological response (SVR) in hepatitis C virus (HCV) patients undergoing antiviral therapy. It can be used as a guide to individualize treatment duration. The aim of this study was to assess the role of RVR in tailoring the duration of treatment. Methods: Patients with HCV genotype 3 infections were enrolled and treated with pegylated interferon alfa-2a (PEG IFN alfa-2a) 180@mg/week and ribavirin. HCV RNA was analyzed at weeks 4, 12, 16, and 24. Treatment duration was individualized on the basis of RVR. Patients who achieved RVR and who were aged @?40 years with a body mass index (BMI) @?27kg/m^2 received 16 weeks of treatment (group A). Patients who achieved RVR and were aged >40 years with a BMI >27kg/m^2, aged >40 years with a BMI @?27kg/m^2, and aged @?40 years with a BMI >27kg/m^2 received 24 weeks of treatment (group B). Patients who did not achieve RVR but who achieved an early virological response (EVR; HCV PCR-negative or >=2 log drop in HCV RNA at week 12) were treated with 24 weeks of therapy (group C). Results: SVR was observed in 86% in group A, 82.2% in group B, and 46.8% in group C. A difference was observed in SVR for patients with and without RVR and receiving the standard duration of treatment (82.2% vs. 46.8%, p<0 .001). The results show that the rate of SVR is not inferior in those with RVR treated with 16 weeks of therapy compared to 24 weeks (86% vs. 82.2%, p=0.004). Conclusions: RVR is useful to individualize the duration of treatment and to predict the treatment outcome. A short treatment of 16 weeks is as effective as 24 weeks in HCV genotype 3 patients who achieve RVR, who have a low BMI, and are younger in age.
机译:背景:快速病毒学应答(RVR)现在被认为是接受抗病毒治疗的丙型肝炎病毒(HCV)患者持续病毒应答(SVR)的最强预测因子。它可以用作个体化治疗时间的指南。这项研究的目的是评估RVR在调整治疗时间方面的作用。方法:招募丙型干扰素α-2a(PEG IFN alfa-2a)180mg /周和利巴韦林治疗HCV基因型3感染的患者。在第4、12、16和24周对HCV RNA进行了分析。根据RVR个体化治疗时间。达到RVR且年龄≥40岁且体重指数(BMI)≥27kg/ m ^ 2的患者接受了16周的治疗(A组)。达到RVR且年龄大于40岁且BMI> 27kg / m ^ 2的患者,年龄大于40岁且BMI @?27kg / m ^ 2的患者以及年龄大于40岁且BMI> 27kg / m ^ 2的患者接受了24周的治疗(B组)。未达到RVR但达到早期病毒学应答(EVR; HCV PCR阴性或HCV RNA在第12周下降≥2log)的患者接受了24周的治疗(C组)。结果:A组中观察到SVR的比例为86%,B组中为82.2%,C组中为46.8%。无论是否接受RVR且接受标准治疗时间的患者,SVR均存在差异(82.2%对46.8%) %,p <0.001)。结果表明,接受RVR治疗16周的患者的SVR率不逊于24周(86%vs. 82.2%,p = 0.004)。结论:RVR有助于个体化治疗时间并预测治疗结果。对于达到RVR,BMI低且年龄较小的HCV基因型3型患者,短短的16周治疗与24周一样有效。

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