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干扰素α治疗慢性乙型肝炎感染:延长治疗可提高疗效。欧洲病毒性肝炎联合行动(EUROHEP)。

Interferon alfa for chronic hepatitis B infection: increased efficacy of prolonged treatment. The European Concerted Action on Viral Hepatitis (EUROHEP).

作者信息

Janssen H L, Gerken G, Carreño V, Marcellin P, Naoumov N V, Craxi A, Ring-Larsen H, Kitis G, van Hattum J, de Vries R A, Michielsen P P, ten Kate F J, Hop W C, Heijtink R A, Honkoop P, Schalm S W

机构信息

Department of Hepatogastroenterology, Erasmus University Hospital, Rotterdam, The Netherlands.

出版信息

Hepatology. 1999 Jul;30(1):238-43. doi: 10.1002/hep.510300113.

Abstract

Interferon alfa (IFN-alpha) is the primary treatment for chronic hepatitis B. The standard duration of IFN-alpha therapy is considered 16 weeks; however, the optimal treatment length is still poorly defined. We evaluated the efficacy and acceptability of prolonged IFN-alpha treatment in patients with chronic hepatitis B. To investigate whether treatment prolongation could enhance the rate of hepatitis B e antigen (HBeAg) seroconversion, we conducted a prospective, controlled, multicenter trial in which all patients were treated with a standard regimen of 10 million units IFN-alpha 3 times per week over 16 weeks. Patients who were still HBeAg-positive after 16 weeks of therapy were randomized to prolongation of the identical regimen up to 32 weeks (prolonged therapy) or discontinuation of treatment (standard therapy). Among the 162 patients who entered the study, 27 (17%) were HBeAg-negative after the first 16 weeks of treatment, and 118 were randomized to standard or prolonged therapy. After randomization, a response (HBeAg seroconversion and sustained hepatitis B virus [HBV]-DNA negativity) was observed in 7 of the 57 (12%) patients assigned to standard therapy versus 17 of the 61 (28%) patients assigned to prolonged therapy (P =.04). A low level of viral replication after 16 weeks of treatment, as indicated by serum HBV-DNA values under 10 pg/mL, was found to be the only independent predictor of response (52% vs. 0%; P <.001) during prolonged therapy. The prolonged IFN-alpha schedule was well tolerated in the large majority of patients. In chronic hepatitis B, prolongation of IFN-alpha therapy up to 32 weeks is superior to a standard course of 16 weeks. Those patients who exhibit a low level of viral replication at the end of the standard regimen benefit most from prolonged treatment.

摘要

干扰素α(IFN-α)是慢性乙型肝炎的主要治疗方法。IFN-α治疗的标准疗程被认为是16周;然而,最佳治疗时长仍未明确界定。我们评估了延长IFN-α治疗对慢性乙型肝炎患者的疗效和可接受性。为研究延长治疗是否能提高乙肝e抗原(HBeAg)血清学转换率,我们开展了一项前瞻性、对照、多中心试验,所有患者均接受标准方案治疗,即每周3次、每次1000万单位IFN-α,疗程为16周。治疗16周后仍为HBeAg阳性的患者被随机分为两组,一组将相同方案延长至32周(延长治疗组),另一组停止治疗(标准治疗组)。在162例进入研究的患者中,27例(17%)在最初16周治疗后HBeAg呈阴性,118例被随机分配至标准治疗组或延长治疗组。随机分组后,标准治疗组57例患者中有7例(12%)出现应答(HBeAg血清学转换和乙肝病毒[HBV]DNA持续阴性),而延长治疗组61例患者中有17例(28%)出现应答(P = 0.04)。治疗16周后血清HBV-DNA值低于10 pg/mL表明病毒复制水平较低,这是延长治疗期间唯一的独立应答预测因素(52%对0%;P < 0.001)。绝大多数患者对延长IFN-α疗程耐受性良好。在慢性乙型肝炎中,将IFN-α治疗延长至32周优于16周的标准疗程。在标准疗程结束时病毒复制水平较低的患者从延长治疗中获益最大。

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