Rate and Predictors of Treatment Failure to All-Oral HCV Regimens outside Clinical Trials

医学 利巴韦林 内科学 莱迪帕斯维尔 共感染 丙型肝炎 索福斯布维尔 临床试验 丙型肝炎病毒 西梅普雷维尔 胃肠病学 免疫学 人类免疫缺陷病毒(HIV) 病毒
作者
Ana Arias,Antonio Aguilera,Vincent Soriano,Laura Benítez‐Gutiérrez,Gema M. Lledó,Daniel Navarro,Ana Treviño,E Van den Eynde Otero,José M. Peña,Valentín Cuervas‐Mons,Carmen de Mendoza
出处
期刊:Antiviral Therapy [SAGE Publishing]
卷期号:22 (4): 307-312 被引量:59
标识
DOI:10.3851/imp3061
摘要

Background Cure rates above 90% have been reported in most Phase III clinical trials using distinct all-oral direct-acting antivirals (DAAs) in chronic hepatitis C patients. Preliminary results in real-world patients have confirmed this, although efficacy tends to be lower. Methods All consecutive chronic hepatitis C patients treated with all-oral DAA regimens at three hepatitis clinics in Spain were retrospectively examined. Host and viral factors were tested as predictors of treatment failure. Results A total of 363 chronic hepatitis C patients had completed a course of all-oral DAA therapy outside clinical trials up to the end of 2015. All but 14 (4%) patients achieved sustained virological response. There were 10 failures that occurred after 12 weeks of sofosbuvir-ledipasvir, despite 5 of them being on ribavirin. All failures but one were relapses. The only patient with viral breakthrough selected NS5B L159F and NS5A Y93H. In multivariate analyses, only advanced liver fibrosis (Metavir F3–F4) and HIV coinfection were significantly associated with treatment failure. A trend towards lower response was seen for HCV genotype 4. Conclusions Treatment failures outside clinical trials are roughly seen in 4% of chronic hepatitis C patients who complete a course of all-oral DAA therapy, resembling what is seen in registration trials. In our series, outcomes were not significantly influenced by ribavirin addition, IL28B polymorphisms, HCV genotype, high baseline HCV RNA or prior interferon failure. However, advanced liver fibrosis and HIV coinfection were significantly associated with treatment failure. Our findings support that there is still room for individualization of current DAA therapy.

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