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非核苷类逆转录酶抑制剂在抗逆转录病毒治疗中的新作用。

The emerging roles of non-nucleoside reverse transcriptase inhibitors in antiretroviral therapy.

作者信息

Moyle G

机构信息

HIV Research, Chelsea and Westminster Hospital, London, England.

出版信息

Drugs. 2001;61(1):19-26. doi: 10.2165/00003495-200161010-00003.

Abstract

The availability of potent non-nucleoside reverse transcriptase inhibitor (NNRTI)-based regimens for antiretroviral therapy and concerns regarding protease inhibitor (PI)-related metabolic disturbances have led to significant shifts in treatment practices in HIV infection. NNRTI-based regimens may have several advantages over PI-based therapy for initial or prolonged therapy, including more convenient administration regimens, lower tablet volume, fewer drug interactions, and central nervous system penetration. No data from prospective clinical trials currently exist comparing the 3 approved agents (efavirenz, nevirapine or delavirdine). Both efavirenz and nevirapine have been compared to triple therapy with the PI indinavir over 48 weeks as initial therapy, with similar responses being observed with nevirapine regimens and superiority observed with efavirenz. A smaller 24-week study has suggested nevirapine may be superior to the PI nelfinavir. Limited comparative data in patients with high viral loads treated with nevirapine- or delavirdine-based regimens currently exist. However, cohort data and selected patient data from clinical trials suggest comparable activity to PI-based regimens in these patients. The superiority of efavirenz over indinavir-based regimens has been observed in comparative data in a subset of patients with high viral loads. In treatment-experienced patients, available uncontrolled data suggest these agents contribute to regimen efficacy in NNRTI-naïve, treatment-experienced patients. Efavirenz has demonstrated superiority over nelfinavir in nucleoside-experienced patients, although combining these 2 agents may represent the best approach in these circumstances. The tolerability of NNRTIs appears generally good with few individuals discontinuing in clinical studies as a result of adverse drug events. The majority of adverse events with NNRTIs occur within the first month, and are predictable and manageable without therapy interruption.

摘要

基于高效非核苷类逆转录酶抑制剂(NNRTI)的抗逆转录病毒治疗方案的出现,以及对蛋白酶抑制剂(PI)相关代谢紊乱的担忧,导致了HIV感染治疗实践的重大转变。基于NNRTI的治疗方案在初始或长期治疗方面可能比基于PI的治疗具有多个优势,包括给药方案更方便、片剂体积更小、药物相互作用更少以及对中枢神经系统的渗透性更强。目前尚无前瞻性临床试验数据比较三种已获批药物(依非韦伦、奈韦拉平或地拉韦定)。依非韦伦和奈韦拉平都曾与PI茚地那韦三联疗法进行过48周的初始治疗比较,奈韦拉平治疗方案的反应相似,而依非韦伦则显示出优势。一项规模较小的24周研究表明,奈韦拉平可能优于PI奈非那韦。目前关于接受基于奈韦拉平或地拉韦定治疗方案的高病毒载量患者的比较数据有限。然而,队列数据和临床试验中的部分患者数据表明,这些患者中基于NNRTI的治疗方案与基于PI的治疗方案活性相当。在部分高病毒载量患者的比较数据中,已观察到依非韦伦优于基于茚地那韦的治疗方案。在有治疗经验的患者中,现有非对照数据表明,这些药物对未接受过NNRTI治疗、有治疗经验的患者的治疗方案疗效有贡献。在核苷类药物治疗经验丰富的患者中,依非韦伦已显示出优于奈非那韦的效果,尽管在这种情况下联合使用这两种药物可能是最佳方法。NNRTI的耐受性总体上似乎良好,在临床研究中因药物不良事件而停药的个体较少。NNRTI的大多数不良事件发生在第一个月内,且可预测且无需中断治疗即可处理。

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