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Treatment of HBeAg positive chronic hepatitis B: Interferon or nucleoside analogues

机译:HBeAg阳性慢性乙型肝炎的治疗:干扰素或核苷类似物

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摘要

Interferon alpha has restricted efficacy in as much as only a proportion of patients show a response. However, in appropriately selected HBeAg-positive and HBeAg-negative patients, sustained suppression of viral replication can be achieved, and HBeAg or even HBsAg seroconversion can be attained. Thus, finite course of interferon alpha can be successful, and offer an advantage to patient. Interferon (IFN) remains a benchmark therapy for chronic hepatitis B. The main advantages of IFN-α over nucleoside analogues are the absence of resistance and the possibility of immune-mediated clearance of hepatitis B. Unfortunately, side effects preclude the use of interferon alpha in substantial proportions of patients, and prolonged maintenance therapy to suppress hepatitis B virus (HBV) is not feasible. Nucleoside analogues are given by mouth, once per day, and the safety, potency and efficacy have improved and facilitated treatment. However, maintenance of long-term suppression is required for the majority of patients. In general, treatment of chronic hepatitis B should target patients with active disease and viral replication, preferably before the signs and symptoms of cirrhosis or significant injury has occurred. Current EASL guidelines suggest that treatment be based on the evaluation of three criteria: Serum aminotransferase levels, serum HBV DNA levels and histological grade and stage. Many questions remain unanswered on the optimal treatment of patients with chronic hepatitis B with a nucleoside vs interferon alpha. Both forms of treatment have benefits and the choice should be selected and tailored. Stopping or futility rules can be implemented in patients who fail interferon. Recent data suggest the safety and efficacy of nucleoside analogues in the third trimester of pregnancy to reduce the risk of transmission from mothers to their children.
机译:干扰素α的疗效有限,只有一部分患者表现出反应。但是,在适当选择的HBeAg阳性和HBeAg阴性患者中,可以实现病毒复制的持续抑制,并且可以获得HBeAg甚至HBsAg血清转化。因此,干扰素α的有限病程可能是成功的,并为患者带来了好处。干扰素(IFN)仍然是慢性乙型肝炎的基准疗法。与核苷类似物相比,IFN-α的主要优势是无耐药性和可能通过免疫介导的乙型肝炎清除。不幸的是,副作用排除了干扰素α的使用在相当大比例的患者中,延长维持治疗以抑制乙型肝炎病毒(HBV)并不可行。每天口服一次核苷类似物,其安全性,效力和功效得到改善并促进了治疗。但是,大多数患者需要长期抑制。通常,慢性乙型肝炎的治疗应针对活动性疾病和病毒复制的患者,最好是在肝硬化的迹象和症状或严重伤害发生之前。当前的EASL指南建议治疗应基于以下三个标准的评估:血清转氨酶水平,血清HBV DNA水平以及组织学等级和阶段。关于用核苷和干扰素α对慢性乙型肝炎患者进行最佳治疗的许多问题仍然没有答案。两种形式的治疗都有益处,应选择和调整选择。干扰素治疗失败的患者可以实施停止或无效的规则。最近的数据表明,核苷类似物在妊娠晚期的安全性和有效性可降低从母亲传播给孩子的风险。

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