慢性乙型肝炎的管理。

Timothy J Wilt, Tatyana Shamliyan, Aasma Shaukat, Brent C Taylor, Roderick MacDonald, Jian-Min Yuan, James R Johnson, James Tacklind, Indulis Rutks, Robert L Kane
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引用次数: 0

摘要

目的:综合慢性乙型肝炎(CHB)的自然史以及抗病毒药物对临床、病毒学、组织学和生化结果的影响和危害的证据。数据来源:MEDLINE、电子数据库和系统综述的人工搜索。检查方法:我们纳入了原始观察性研究,以评估成人慢性乙型肝炎的自然病史和随机对照试验(RCTs),如果它们报告了死亡率、肝细胞癌(HCC)发病率、肝硬化或衰竭、HBeAg或HBsAg、病毒载量(HBV DNA)、丙氨酸氨基转移酶(ALT)水平、组织学坏死炎症和纤维化评分,以及干扰素α -2b、聚乙二醇化干扰素α - 2a、拉米夫定、阿德福韦,恩替卡韦,替诺韦或替比夫定。我们排除了孕妇、移植患者和接受癌症化疗的个体。我们计算了治疗结束和治疗后的相对风险或绝对风险差异。结果:观察性研究(41篇出版物)表明,男性、丙型肝炎、丁型肝炎或HIV合并感染、HBV DNA升高和肝硬化与HCC和死亡风险增加相关。在16项非设计用于测试长期临床结果的随机对照试验中,药物没有减少死亡、肝衰竭或HCC。来自60项随机对照试验的93份出版物的证据表明,药物在治疗结束时对病毒载量或复制、肝酶和组织学有影响,并在治疗结束后持续3至6个月。没有一种治疗方法能改善所有结果,关于比较效果的证据有限。两项随机对照试验显示,与安慰剂相比,干扰素α -2b增加了CHB溶液。干扰素α -2b或拉米夫定改善治疗后HBV DNA和HBeAg清除率、血清转化和ALT正常化。阿德福韦改善治疗后ALT正常化和HBV DNA清除。聚乙二醇化干扰素α 2-a与拉米夫定相比,改善了治疗后HBV DNA和HBeAg的清除率和血清转化,ALT正常化和肝脏组织学。拉米夫定联合干扰素α -2b与拉米夫定相比,改善了治疗期HBV DNA清除率和HBeAg血清转化,并减少了HBV DNA突变。与拉米夫定相比,聚乙二醇化干扰素α 2-a联合拉米夫定改善了治疗后HBV DNA和HBeAg的清除率、血清转化和ALT正常化,但与拉米夫定相比,聚乙二醇化干扰素α 2-a单药治疗没有改善。不良事件是常见的,但通常是轻微的,并没有导致治疗中断的增加。较长的肝炎病程、男性、基线病毒载量和基因型、HBeAg和组织学状态可能会改变治疗对中期结果的影响。阿德福韦和聚乙二醇干扰素α 2-a联合拉米夫定改善了HBeAg阴性患者的治疗后病毒清除率。没有足够的证据来确定生化、病毒或组织学测量是否是治疗对死亡率、肝功能衰竭或癌症效果的有效替代。结论:成年慢性乙型肝炎患者发生死亡、肝脏失代偿和HCC的风险增加。单一或联合药物治疗改善了选定的病毒学、生化和组织学标志物,但对所有检查结果没有一致的影响。患者和疾病特征可能改变治疗诱导的中间结果。证据不足以评估治疗对临床结果的影响,预测个体化患者的反应,或确定中间措施是否是可靠的替代品。未来的研究应评估药物对临床结果和患者亚群的长期影响。
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Management of chronic hepatitis B.

Objectives: Synthesize evidence of the natural history of chronic hepatitis B (CHB) and effects and harms of antiviral drugs on clinical, virological, histological, and biochemical outcomes.

Data sources: MEDLINE, electronic databases, and manual searches of systematic reviews.

Review methods: We included original observational studies to assess natural history and randomized controlled trials (RCTs) of adults with CHB published in English to assess treatment effects and harms if they reported mortality, incidence of hepato-cellular carcinoma (HCC), cirrhosis or failure, HBeAg or HBsAg, viral load (HBV DNA), alanine aminotransferase (ALT) levels, histological necroinflammatory and fibrosis scores, and adverse events after interferon alfa-2b, pegylated interferon alfa 2-a, lamivudine, adefovir, entecavir, tenovir or telbivudine. We excluded pregnant women, transplant patients, and individuals undergoing cancer chemotherapy. We calculated relative risk or absolute risk differences at end of treatment and post-treatment.

Results: Observational studies (41 publications) suggested that male gender, coinfection with hepatitis C, D, or HIV, increased HBV DNA, and cirrhosis were associated with increased risk of HCC and death. Drugs did not reduce death, liver failure, or HCC in 16 RCTs not designed to test long-term clinical outcomes. Evidence from 93 publications of 60 RCTs suggested drug effects on viral load or replication, liver enzymes, and histology at end of treatment and lasting from 3 to 6 months off treatment. No one treatment improved all outcomes and there was limited evidence on comparative effects. Two RCTs suggested interferon alfa-2b increased CHB solution versus placebo. Interferon alfa-2b or lamivudine improved off treatment HBV DNA and HBeAg clearance and seroconversion and ALT normalization. Adefovir improved off treatment ALT normalization and HBV DNA clearance. Pegylated interferon alfa 2-a versus lamivudine improved off-treatment HBV DNA and HBeAg clearance and seroconversion, ALT normalization and liver histology. Lamivudine combined with interferon alfa-2b versus lamivudine improved off treatment HBV DNA clearance and HBeAg seroconversion and reduced HBV DNA mutations. Pegylated interferon alfa 2-a plus lamivudine improved off treatment HBV DNA and HBeAg clearance and seroconversion and ALT normalization compared to lamivudine but not pegylated interferon alfa 2-a monotherapy. Adverse events were common but generally mild and did not result in increased treatment discontinuation. Longer hepatitis duration, male gender, baseline viral load and genotype, HBeAg, and histological status may modify treatment effect on intermediate outcomes. Adefovir and pegylated interferon alfa 2-a with lamivudine improved off treatment viral clearance in HBeAg negative patients. There was insufficient evidence to determine if biochemical, viral, or histological measures are valid surrogates of treatment effect on mortality, liver failure, or cancer.

Conclusion: Adults with CHB have an increased risk of death, hepatic decompensation, and HCC. Mono or combined drug therapy improves selected virological, biochemical, and histological markers with no consistent effects on all examined outcomes. Patient and disease characteristics may modify treatment-induced intermediate outcomes. Evidence was insufficient to assess treatment effect on clinical outcomes, predict individualized patient response, or determine if intermediate measures are reliable surrogates. Future research should assess long-term drug effects on clinical outcomes and among patient subpopulations.

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