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首页> 外文期刊>Antiviral therapy >Adefovir dipivoxil resistance patterns in patients with lamivudine-resistant chronic hepatitis B.
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Adefovir dipivoxil resistance patterns in patients with lamivudine-resistant chronic hepatitis B.

机译:拉米夫定耐药的慢性乙型肝炎患者对阿德福韦酯的耐药模式。

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BACKGROUND: Lamivudine (3TC)-resistant chronic hepatitis B patients demonstrated a higher rate of adefovir dipivoxil (ADV) resistance compared with nucleoside-naive patients. This study describes ADV mutation patterns in 3TC-resistant patients treated with ADV+3TC or ADV monotherapy, investigating whether mutations selected during 3TC therapy predispose to ADV resistance. Risk factors for ADV resistance were also evaluated. METHODS: A total of 60 3TC-experienced patients were treated with (or switched to) ADV monotherapy (30 patients) or ADV+3TC combination therapy (30 patients), and followed for at least 12 months. In all patients the hepatitis B virus reverse transcriptase (RT) region was amplified and directly sequenced before initiating ADV. The RT sequence was reevaluated for virological breakthrough patients and phenotypic analysis was performed for several patients. RESULTS: In total, 14 (23%) patients showed virological breakthrough (10/30 on ADV monotherapy and 4/30 on ADV+3TC). ADV resistance mutations (rtA181V/T and rtN236T) were detected alone or in combination for 11/14 patients, whereas novel substitutions were present in 3 patients. Before ADV treatment, apart from 3TC resistance signature mutations, additional changes were found, including the rtA181T mutation, which was already present in 2/14 ADV-resistant patients. CONCLUSIONS: Although most patients showed virological breakthrough because of the well known rtA181V/T and rtN236T substitutions, more complex patterns were also found. ADV monotherapy, dose reduction and suboptimal virological response after 48 weeks of therapy were significantly associated with ADV resistance.
机译:背景:与未使用过核苷的患者相比,对拉米夫定(3TC)耐药的慢性乙型肝炎患者表现出较高的阿德福韦酯(ADV)耐药率。这项研究描述了在接受ADV + 3TC或ADV单药治疗的3TC耐药患者中的ADV突变模式,研究了在3TC治疗期间选择的突变是否易引起ADV耐药。还评估了抗ADV的危险因素。方法:共有60名3TC经验患者接受(或改用)ADV单一疗法(30例)或ADV + 3TC联合疗法(30例),并随访至少12个月。在所有患者中,乙型肝炎病毒逆转录酶(RT)区域均已扩增,并在开始ADV之前直接测序。重新评估了病毒学突破患者的RT序列,并对几例患者进行了表型分析。结果:总共有14例(23%)患者表现出病毒学突破(ADV单药治疗为10/30,ADV + 3TC治疗为4/30)。 11/14例患者单独或联合检测到ADV耐药性突变(rtA181V / T和rtN236T),而3例患者出现新的替代。在进行ADV治疗之前,除了3TC耐药性标记突变外,还发现了其他变化,包括rtA181T突变,该突变已存在于2/14抗ADV的患者中。结论:尽管大多数患者由于已知的rtA181V / T和rtN236T替代而表现出病毒学突破,但也发现了更复杂的模式。治疗48周后,ADV单一疗法,剂量降低和病毒学反应欠佳与ADV耐药性显着相关。

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