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首页> 外文期刊>Gut and Liver >Long-Term Outcomes and Dynamics of Mutants Associated with Lamivudine-Adefovir Rescue Therapy in Patients with Lamivudine-Resistant Chronic Hepatitis B
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Long-Term Outcomes and Dynamics of Mutants Associated with Lamivudine-Adefovir Rescue Therapy in Patients with Lamivudine-Resistant Chronic Hepatitis B

机译:耐拉米夫定的慢性乙型肝炎患者拉米夫定-阿德福韦酯治疗相关突变体的长期结果和动力学

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Background/AimsTo investigate the association between the baseline profiles and dynamics of hepatitis B virus (HBV) DNA polymerase gene mutations and the long-term virological response of lamivudine (LAM)-adefovir (ADV) combination therapy in patients with LAM-resistant chronic hepatitis B.MethodsSeventy-five patients who received LAM-ADV combination therapy for more than 12 months were analyzed. Restriction fragment mass polymorphism assays were used to detect and monitor the dynamics of LAM- and ADV-resistant mutations.ResultsThe median duration of LAM-ADV combination therapy was 26 months (range, 12 to 58 months). The baseline mutation profiles, rtM204I (p=0.992), rtM204I/V (p=0.177), and rtL180M (p=0.051), were not correlated with the cumulative virological response, and the baseline HBV DNA level (p=0.032) was the only independent predictive factor for cumulative virological response. Tests for LAM- and ADV-resistant mutations were performed in 12 suboptimal responders in weeks 48 and 96. The population of rtM204 mutants persisted or increased in 8 of 12 patients, and rtA181T mutants newly emerged as a minor population in four patients until 96 weeks. Nevertheless, the viral loads progressively decreased during rescue therapy, and these dynamics did not correlate with virological response.ConclusionsThe baseline profile and dynamics of LAM-resistant mutations during LAM-ADV combination therapy are not associated with a virological response.
机译:背景/目的探讨在LAM耐药的慢性肝炎患者中,乙型肝炎病毒(HBV)DNA聚合酶基因突变的基线特征和动态与拉米夫定(LAM)-阿德福韦(ADV)联合治疗的长期病毒学应答之间的关系B.方法分析了接受LAM-ADV联合治疗超过12个月的55例患者。应用限制性片段质量多态性检测和监测LAM和ADV耐药突变的动态。结果LAM-ADV联合治疗的中位时间为26个月(范围12至58个月)。基线突变谱rtM204I(p = 0.992),rtM204I / V(p = 0.177)和rtL180M(p = 0.051)与累积病毒学应答无关,基线HBV DNA水平(p = 0.032)为累积病毒学应答的唯一独立预测因素。在第48周和第96周,对12位次优反应者进行了LAM和ADV耐药突变的测试。rtM204突变体的群体在12位患者中的8位持续或增加,直到96周,新出现的rtA181T突变是少数患者中的4位。然而,在抢救治疗期间病毒载量逐渐下降,并且这些动力学与病毒学应答无关。结论在LAM-ADV联合治疗期间,LAM耐药突变的基线特征和动力学与病毒学应答无关。

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