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Long-term outcome of hepatitis B virus-related Chronic Hepatitis under protracted nucleos(t)ide analogues

机译:长期的核苷酸类似物对乙型肝炎病毒相关的慢性肝炎的长期疗效

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Long-term outcome of patients with chronic hepatitis B virus (HBV) infection under continuous nucleos(t)ide analogues (NUCs) has been poorly elucidated. We enrolled 121 anti-HBe-positive patients into a prospective surveillance programme while on (>36 months) NUCs therapy. HBV-DNA clearance, add-on therapy and safety were evaluated. Development of cirrhosis, events of liver decompensation and hepatocellular carcinoma (HCC) during the follow-up were the main endpoints, as the complication-free survival. At baseline, 74 patients (61%) had chronic hepatitis, the remainders a cirrhotic liver. HBV-DNA levels >38 000 IU/mL were discovered in 103 patients. At enrolment, 79 patients were na?ve to NUCs treatment. Lamivudine monotherapy (n = 70) or a different NUC (n = 51) was administered. At month 6 of therapy, HBV-DNA clearance was documented in 88 patients (73%). Treatment schedule was modified in 52 patients due to breakthrough or suboptimal response. During a mean follow-up of 6 ± 3 years, viral clearance was achieved in the majority of patients. Ten of 74 patients (13.5%) with chronic hepatitis progressed to cirrhosis, 1 patient developed a HCC. In the 47 patients with cirrhosis at presentation, HCC occurred in 14 (30%) and liver decompensation in 5 (11%). The 5 and 10-year event-free survivals were, respectively, 89.3% (95% CI, 81.7 -96.9) and 75.6% (95% CI, 61.5 -89.7) for patients with chronic hepatitis, and 70.2% (95% CI, 56.3 -84.1) and 40.4% (95% CI, 16.9 -63.9) for those with cirrhosis. Protracted, effective treatment with oral NUCs affects the natural history of chronic HBV infection by reducing the incidence of cirrhosis and risk of complications, but does not guarantee against the development of HCC in cirrhosis at presentation.
机译:在连续核苷酸类似物(NUCs)下长期感染慢性乙型肝炎病毒(HBV)的患者的远期结果尚不清楚。我们在(> 36个月)NUCs治疗期间招募了121位抗HBe阳性的患者纳入前瞻性监测计划。评估了HBV-DNA清除率,附加疗法和安全性。肝硬化的发生,随访期间的肝失代偿和肝细胞癌(HCC)事件是无并发症生存的主要终点。基线时,有74例(61%)患有慢性肝炎,其余为肝硬化肝。在103名患者中发现HBV-DNA水平> 38 000 IU / mL。入组时,79名患者未接受过NUCs治疗。给予拉米夫定单药治疗(n = 70)或其他NUC(n = 51)。在治疗的第6个月,有88位患者(73%)记录了HBV-DNA清除率。由于突破或反应欠佳,对52例患者的治疗方案进行了修改。在平均随访6±3年中,大多数患者均实现了病毒清除。 74例慢性肝炎患者中有10例(13.5%)发展为肝硬化,其中1例发生了HCC。在47例肝硬化患者中,肝癌发生率14例(占30%),肝脏代偿失调5例(占11%)。慢性肝炎患者的5年和10年无事件生存率分别为89.3%(95%CI,81.7 -96.9)和75.6%(95%CI,61.5 -89.7),以及70.2%(95%CI) ,56.3 -84.1)和40.4%(95%CI,16.9 -63.9)。长期,有效的口服NUC治疗可通过降低肝硬化的发生率和并发症的风险来影响慢性HBV感染的自然病程,但不能保证肝硬化时肝癌的发展。

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