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Flares in chronic hepatitis B patients induced by the host or the virus? Relation to treatment response during Peg-interferon {alpha}-2b therapy

机译:慢性乙型肝炎患者由宿主或病毒引起的耀斑?聚乙二醇干扰素α-2b治疗期间与治疗反应的关系

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摘要

Flares are a well known phenomenon during antiviral treatment for chronic hepatitis B. Little is known about the effect of flares on response. We investigated the timing and characteristics of flares, in relation to treatment response (hepatitis B e antigen loss). A total of 266 patients, participating in a global randomised controlled study, were assigned to 52 weeks of 100 mug pegylated (Peg)-interferon alpha-2b weekly, combined with either daily lamivudine 100 mg or placebo. Sixty seven patients (25%) exhibited 75 flares, with 38 (51%) flares in the combination therapy and 37 (49%) in the monotherapy groups. Overall, 30% of patients with and 38% of patients without a flare responded to therapy (p = 0.25). In 24 patients (36%) the flare was followed by a decrease in hepatitis B virus (HBV) DNA (host induced flare). In 25 (38%) patients the flare was preceded by an increase in HBV DNA (virus induced flare). In 17 (26%) patients the flare did not meet one of these criteria (indeterminate flare). Of patients with host induced flare, 58% responded whereas only 20% of patients with virus induced flares responded (p = 0.008). Hepatitis B surface antigen loss (n = 8) was exclusively seen in patients experiencing a host induced flare. Multivariate logistic analysis showed that host induced flares was an independent predictor of response (p = 0.043). Flares are not more common in responders than in non-responders to Peg-interferon alpha-2b therapy. Virus induced flares, which occur after an increase in HBV DNA level, and most probably are indicative for increased expression of viral antigens, did not lead to treatment response. In contrast, host induced flares which were followed by a HBV DNA decrease were highly associated with treatment response
机译:在慢性乙型肝炎的抗病毒治疗期间,耀斑是众所周知的现象。耀斑对反应的影响知之甚少。我们研究了与治疗反应(乙型肝炎e抗原丢失)相关的耀斑发作的时机和特征。总共266名患者参加了一项全球随机对照研究,他们被分配为52周的每周100杯聚乙二醇化(Peg)-干扰素α-2b联合每日100 mg拉米夫定或安慰剂。 67名患者(25%)出现了75个耀斑,其中联合疗法中38个(51%)耀斑,而单一疗法组中37个(49%)。总体而言,有30%的患者和没有发作的患者中有38%的患者对治疗有反应(p = 0.25)。在24名患者(占36%)中,耀斑伴随着乙型肝炎病毒(HBV)DNA(宿主诱发的耀斑)减少。在25名(38%)的患者中,发作前是HBV DNA(病毒引起的发作)增加。在17名(26%)患者中,耀斑未满足以下标准之一(不确定耀斑)。在宿主诱发的耀斑患者中,有58%有反应,而病毒诱发的耀斑患者中只有20%有响应(p = 0.008)。乙型肝炎表面抗原的丢失(n = 8)仅在经历宿主诱发的耀斑的患者中看到。多元逻辑分析表明,宿主诱发的耀斑是反应的独立预测因子(p = 0.043)。在对Peg-干扰素α-2b治疗无反应者中,耀斑在反应者中并不普遍。 HBV DNA水平升高后发生的病毒诱发的耀斑并没有导致治疗反应,这很可能表明病毒抗原表达增加。相比之下,宿主诱发的耀斑,随后HBV DNA下降与治疗反应高度相关

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