首页> 外文OA文献 >Management of hepatitis B: Summary of a clinical research workshop Potential conflict of interest: Dr. Lok is a consultant and received grants from GlaxoSmithKline, Bristol-Myers Squibb, Idenix, Gilead, Roche, and Innogenetics.
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Management of hepatitis B: Summary of a clinical research workshop Potential conflict of interest: Dr. Lok is a consultant and received grants from GlaxoSmithKline, Bristol-Myers Squibb, Idenix, Gilead, Roche, and Innogenetics.

机译:乙型肝炎的管理:临床研究工作坊的总结潜在的利益冲突:Lok博士是一名顾问,并获得了葛兰素史克,百时美施贵宝,Idenix,吉列,罗氏和Innogenetics的资助。

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摘要

Chronic hepatitis B is caused by persistent infection with the hepatitis B virus (HBV), a unique DNA virus that replicates through an RNA intermediate produced from a stable covalently closed circular DNA molecule. Viral persistence appears to be due to inadequate innate and adaptive immune responses. Chronic infection has a variable course after several decades resulting in cirrhosis in up to one-third of patients and liver cancer in a proportion of those with cirrhosis. Sensitive assays for HBV DNA levels in serum have been developed that provide important insights into pathogenesis and natural history. Therapy of hepatitis B is evolving. Peginterferon induces long-term remissions in disease in one-third of patients with typical hepatitis B e antigen (HBeAg) positive chronic hepatitis B, but a lesser proportion of those without HBeAg. Several oral nucleoside analogues with activity against HBV have been shown to be effective in suppressing viral levels and improving biochemical and histological features of disease in a high proportion of patients with and without HBeAg, at least in the short term. What is uncertain is which agent or combination of agents is most effective, how long therapy should last, and which criteria should be used to start, continue, switch or stop therapy. Long-term therapy with nucleoside analogues may be the most appropriate approach to treatment, but the expense and lack of data on long-term safety and efficacy make recommendations difficult. Clearly, many basic and clinical research challenges remain in defining optimal means of management of chronic hepatitis B. (H EPATOLOGY 2007;45:1056–1075.)
机译:慢性乙型肝炎是由持续感染乙型肝炎病毒(HBV)引起的,乙型肝炎病毒是一种独特的DNA病毒,可通过稳定的共价闭合环状DNA分子产生的R​​NA中间体复制。病毒的持久性似乎是由于先天和适应性免疫反应不足引起的。几十年后,慢性感染的病程变化,导致多达三分之一的患者发生肝硬化,部分肝硬化患者则患有肝癌。已经开发出针对血清中HBV DNA水平的灵敏检测方法,可提供有关发病机理和自然史的重要见解。乙肝的治疗正在发展。聚乙二醇干扰素可在具有典型乙型肝炎e抗原(HBeAg)阳性慢性乙型肝炎的患者中三分之一导致疾病的长期缓解,但在没有HBeAg的患者中所占比例较小。至少在短期内,几种具有抗HBV活性的口服核苷类似物可有效抑制高比例的患有和不患有HBeAg的患者的病毒水平并改善疾病的生化和组织学特征。不确定的是哪种药物或药物的组合最有效,应该持续多长时间的治疗以及应该使用哪种标准开始,继续,转换或停止治疗。用核苷类似物进行长期治疗可能是最合适的治疗方法,但是由于长期安全性和有效性的数据昂贵且缺乏数据,因此难以提出建议。显然,在确定慢性乙型肝炎的最佳治疗方法方面仍存在许多基础和临床研究挑战。(H EPATOLOGY 2007; 45:1056-1075。)

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