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How to optimize HCV therapy in genotype 2 patients

机译:基因2型患者如何优化HCV治疗

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摘要

Hepatitis C Virus (HCV) Genotype 2 accounts for 10% of the patients with chronic HCV worldwide. The current standard of care (SOC) in these patients is 24 weeks of Pegylated Interferon (PEG-IFN) plus Ribavirin (RBV), with sustained virological response rates (SVR) of 80-90%. However, there are subgroups of patients with HCV-2, such as those with advanced fibrosis/cirrhosis, in whom SVR rates are still suboptimal, and highly responsive groups in whom SVR rates reach 95%. Treatment optimization is necessary to maximize efficacy in the former group and reduce treatment-related side effects in the latter. Unfortunately, any attempt to modify the duration or dosing of the SOC according to baseline factors has been disappointing and should not be continued at present. On the other hand on-treatment HCV RNA kinetics are fundamental for individualized treatment regimens because achieving negative HCV RNA at week 4 (rapid virological response, RVR) is the key factor when the duration of PEG-IFN/RBV is tailored in HCV-2 patients. Several studies have shown that treatment can be shortened to 16 weeks in HCV-2 patients with a RVR, without increasing the risk of post-treatment relapse, thus increasing tolerance to treatment while reducing healthcare costs. On the other hand, patients who do not achieve a RVR correspond to a population of difficult-to-cure HCV-2 patients who need alternative treatment strategies which are not yet available.
机译:丙型肝炎病毒(HCV)基因型2占全球慢性HCV患者的10%。这些患者的当前护理标准(SOC)为24周的聚乙二醇干扰素(PEG-IFN)加利巴韦林(RBV),持续病毒学应答率(SVR)为80-90%。但是,有HCV-2患者亚组,例如晚期纤维化/肝硬化患者,其SVR率仍不理想,而高反应性人群中SVR率达到95%。为了使前者的疗效最大化并减少后者的治疗相关副作用,必须进行治疗优化。不幸的是,根据基线因素改变SOC的持续时间或剂量的任何尝试都令人失望,目前不应继续。另一方面,治疗中HCV RNA动力学是个体化治疗方案的基础,因为在HCV-2中调整PEG-IFN / RBV持续时间的关键因素是在第4周达到阴性HCV RNA(快速病毒学应答,RVR)耐心。几项研究表明,具有RVR的HCV-2患者可以将治疗缩短至16周,而不会增加治疗后复发的风险,从而在降低医疗成本的同时提高了对治疗的耐受性。另一方面,未达到RVR的患者对应于难以治愈的HCV-2患者群体,这些患者需要尚未可用的替代治疗策略。

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