Infectious Diseases Unit, Ospedale Papa Giovanni XXIII, Piazza OMS 1 (BG), 24127, Italy.
Expert Rev Anti Infect Ther. 2014 Jan;12(1):13-29. doi: 10.1586/14787210.2014.863708. Epub 2013 Nov 28.
Rilpivirine (RPV) is a next-generation non-nucleoside reverse transcriptase inhibitor (NNRTI) of the diarylpyrimidine family. RPV can be given once daily, is well absorbed and should be administered with food. It is eliminated mainly by hepatic metabolism. Two phase III noninferiority trials (ECHO and THRIVE), compared RPV 25mg with efavirenz (EFV) 600 mg, both given once daily, and combined with 2NRTI backbone. At week 48, response rate for pooled data were 84 versus 82% (difference: 2%; 95% CI: -2.0 to 6.0%). EFV arms performed better than RPV arms when at higher baseline HIV RNA, so RPV was approved for treatment-naïve patients with HIV RNA below 100,000 copies/ml. Approximately 90% of viruses phenotypically resistant to RPV showed cross-resistance to ETR. Conversely, phenotypic analysis showed that in EFV arm, none were resistant to the second-generation NNRTIs. CD4 count increases were similar between groups, but RPV showed a lower rate of discontinuation due to adverse events and lower rates of central nervous system effects, rash and lipid abnormalities. Potency, tolerability and co-formulation in a single tablet (Eviplera(®), Complera(®)) make this drug a new and attractive option for the treatment of HIV.
利匹韦林(RPV)是二芳基嘧啶类家族的下一代非核苷类逆转录酶抑制剂(NNRTI)。RPV 可每日给药 1 次,吸收良好,应与食物同服。它主要通过肝脏代谢消除。两项 III 期非劣效性试验(ECHO 和 THRIVE)比较了每日 1 次给予 RPV 25mg 与依非韦伦(EFV)600mg 的疗效,两者均与 2 种 NRTI 骨干药物联合使用。在第 48 周时,汇总数据的应答率分别为 84%和 82%(差异:2%;95%CI:-2.0 至 6.0%)。在基线 HIV RNA 较高时,EFV 组的疗效优于 RPV 组,因此批准 RPV 用于 HIV RNA 低于 100,000 拷贝/ml 的初治患者。约 90%表型对 RPV 耐药的病毒对 ETR 显示交叉耐药。相反,表型分析显示 EFV 组无一例对第二代 NNRTIs 耐药。两组的 CD4 计数增加相似,但因不良反应而停药率 RPV 较低,中枢神经系统作用、皮疹和血脂异常的发生率也较低。单一片剂(Eviplera(®)、Complera(®))中的效能、耐受性和复方制剂使该药物成为治疗 HIV 的一种新的有吸引力的选择。
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