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首页> 外文期刊>Brazilian Journal of Medical and Biological Research >Recurrent hepatitis C treatment with direct acting antivirals – a real life study at a Brazilian liver transplant center
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Recurrent hepatitis C treatment with direct acting antivirals – a real life study at a Brazilian liver transplant center

机译:直接代理抗病毒药的复发性丙型肝炎治疗 - 巴西肝移植中心的真实生活研究

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Recurrent hepatitis C (HCV) after liver transplantation (LT) is an important cause of morbidity and mortality. Antiviral treatment is recommended to avoid unfavorable outcomes. Direct-acting antivirals (DAA) have transformed HCV treatment, with higher efficacy and fewer side-effects than interferon-based therapies traditionally used. To evaluate DAA treatment outcomes at a Brazilian transplant unit, data of patients who finished HCV treatment at the Liver Transplant Unit of the University of Campinas were analyzed. Treatment consisted of sofosbuvir, daclatasvir, and ribavirin, for 12 or 24 weeks, according to the national guidelines. Fifty-five patients completed antiviral treatment and 54 had HCV-viral load results available. The majority of patients were male (78%), 58 years old on average, 65% had hepatocellular carcinoma (HCC) before LT, and 67% were interferon treatment-experienced. Most patients had HCV genotype 1 (65%), 35% had genotype 3, and started treatment on an average of 38 months after LT (range: 2–228). Fifty-eight percent were treated for 12 weeks and 42% for 24 weeks, using a mean dose of ribavirin of 10.1 mg/kg (4.2–16.1). There were no treatment interruptions due to serious side effects. The sustained virological response rate was 98%. Only one patient relapsed, a genotype 3 cirrhotic treated for 12 weeks. The average follow-up after starting antivirals was 20 months. There were no recurrences of HCC, but there was one rejection episode and one cirrhosis decompensation episode, both 12 weeks after treatment. DAA treatment is safe and effective in the post-LT setting and was not associated to HCC recurrence in the cohort studied.
机译:肝移植(LT)后复发性丙型肝炎(HCV)是发病率和死亡率的重要原因。建议抗病毒治疗以避免不利的结果。直效抗病毒(DAA)转化了HCV治疗,效率越高,副作用较少,而不是传统上使用的基于干扰素的疗法。为了评估巴西移植单位的DAA治疗结果,分析了在坎皮纳大学肝移植单位完成HCV治疗的患者的数据。根据国家指南,治疗由Sofosbuvir,Daclatasvir和利巴韦林组成12或24周。五十五名患者完成抗病毒治疗,54例有HCV病毒载荷可用。大多数患者是男性(78%),平均为58岁,65%在LT之前患有肝细胞癌(HCC),67%是干扰素治疗。大多数患者具有HCV基因型1(65%),35%有基因型3,并在LT(范围:2-228)后平均使用38个月进行治疗。使用10.1mg / kg(4.2-16.1)的平均用力霉素(4.2-16.1),将五十八百百分之24周待治疗12周和42%。由于严重的副作用,没有治疗中断。持续的病毒学反应率为98%。只有一个患者复发,一个基因型3肝硬化治疗12周。起始抗病毒药物后的平均随访时间为20个月。没有HCC的复发,但在治疗后12周,还有一次抑制发作和一个肝硬化失代偿情节。 DAA治疗在邮政后的情况下是安全的,有效的,并且与研究中的群组中的HCC复发无关。

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