Cocohoba Jennifer, Dong Betty J
Department of Clinical Pharmacy, School of Pharmacy, University of California San Francisco, San Francisco, California 94143, USA.
Clin Ther. 2008 Oct;30(10):1747-65. doi: 10.1016/j.clinthera.2008.10.012.
The availability of new classes of antiretroviral drugs has made it possible for HIV-infected individuals who are highly treatment experienced to achieve the goals of immunologic recovery and virologic suppression. Raltegravir is the first integrase inhibitor to be approved by the US Food and Drug Administration for use in antiretroviral treatment- experienced adult patients with viral resistance.
This article reviews the pharmacology, pharmacokinetics, pharmacodynamics, efficacy, tolerability, resistance profile, drug interactions, and dosing and administration of raltegravir.
Searches of MEDLINE and International Pharmaceutical Abstracts from 1964 to July 2008 were conducted using the terms integrase, raltegravir, and MK-0518. Relevant information was extracted from the identified clinical trials and review articles. Abstracts from the Conference on Retroviruses and Opportunistic Infections (1998-2008); Interscience Conference on Antimicrobial Agents and Chemotherapy (1999-2007); International AIDS Society Conference on HIV Pathogenesis, Treatment and Prevention (2001-2007); and European AIDS Conference (2001-2007) were also searched.
Raltegravir blocks HIV replication by inhibiting essential strand-transfer activities of integrase. Raltegravir is rapidly absorbed, with a median T(max) of approximately 4 hours in the fasting state. No dose adjustment is recommended in patients with moderate renal or hepatic insufficiency, and raltegravir may be taken without regard to meals. In Phase II studies in treatment-naive patients, raltegravir had efficacy similar to that of standard initial therapies. In 2 interrelated Phase III clinical studies in treatment-experienced patients with drug-resistant disease, the addition of raltegravir to an optimized background regimen significantly lowered HIV RNA compared with optimized background treatment alone (62.1% vs 32.9%, respectively; P < 0.001). Raltegravir was generally well tolerated. The most common adverse effects reported in Phase II/III trials in treatment-experienced patients were diarrhea (16.6%), nausea (9.9%), and headache (9.7%). Cytochrome P450-related drug interactions are not expected, as raltegravir is not a CYP substrate, inducer, or inhibitor. However, to prevent failure of raltegravir, the drug should not be coadministered with rifampin.
Raltegravir is a potent and generally well tolerated antiretroviral agent that may play an important role in the treatment of patients harboring resistance to other antiretrovirals.
新型抗逆转录病毒药物的出现,使那些有丰富治疗经验的HIV感染者有可能实现免疫恢复和病毒抑制的目标。拉替拉韦是美国食品药品监督管理局批准用于抗逆转录病毒治疗的、有病毒耐药性的成年患者的首个整合酶抑制剂。
本文综述拉替拉韦的药理学、药代动力学、药效学、疗效、耐受性、耐药情况、药物相互作用以及剂量和用法。
使用整合酶、拉替拉韦和MK-0518等检索词,检索1964年至2008年7月的MEDLINE和国际药学文摘数据库。从已确定的临床试验和综述文章中提取相关信息。还检索了逆转录病毒与机会性感染会议(1998 - 2008年)、抗菌药物和化疗跨学科会议(1999 - 2007年)、国际艾滋病协会关于HIV发病机制、治疗和预防会议(2001 - 2007年)以及欧洲艾滋病会议(2001 - 2007年)的摘要。
拉替拉韦通过抑制整合酶的关键链转移活性来阻断HIV复制。拉替拉韦吸收迅速,禁食状态下中位达峰时间约为4小时。中度肾功能或肝功能不全患者无需调整剂量,拉替拉韦服用时无需考虑进餐情况。在初治患者的II期研究中,拉替拉韦的疗效与标准初始疗法相似。在两项针对有耐药性疾病的有治疗经验患者的相关III期临床研究中,与单独的优化背景治疗相比(分别为62.1%对32.9%;P < 0.001),在优化背景方案中加用拉替拉韦可显著降低HIV RNA水平。拉替拉韦总体耐受性良好。在有治疗经验患者的II/III期试验中报告的最常见不良反应为腹泻(16.6%)、恶心(9.9%)和头痛(9.7%)。由于拉替拉韦不是细胞色素P450的底物、诱导剂或抑制剂,预计不存在与细胞色素P450相关的药物相互作用。然而,为防止拉替拉韦治疗失败,该药不应与利福平同时服用。
拉替拉韦是一种强效且总体耐受性良好的抗逆转录病毒药物,可能在治疗对其他抗逆转录病毒药物耐药的患者中发挥重要作用。
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