Kempf D J, Marsh K C, Kumar G, Rodrigues A D, Denissen J F, McDonald E, Kukulka M J, Hsu A, Granneman G R, Baroldi P A, Sun E, Pizzuti D, Plattner J J, Norbeck D W, Leonard J M
Department of Infectious Diseases Research, Abbott Laboratories, Illinois 60064, USA.
Antimicrob Agents Chemother. 1997 Mar;41(3):654-60. doi: 10.1128/AAC.41.3.654.
Coadministration with the human immunodeficiency virus (HIV) protease inhibitor ritonavir was investigated as a method for enhancing the levels of other peptidomimetic HIV protease inhibitors in plasma. In rat and human liver microsomes, ritonavir potently inhibited the cytochrome P450 (CYP)-mediated metabolism of saquinavir, indinavir, nelfinavir, and VX-478. The structural features of ritonavir responsible for CYP binding and inhibition were examined. Coadministration of other protease inhibitors with ritonavir in rats and dogs produced elevated and sustained plasma drug levels 8 to 12 h after a single dose. Drug exposure in rats was elevated by 8- to 46-fold. A > 50-fold enhancement of the concentrations of saquinavir in plasma was observed in humans following a single codose of ritonavir (600 mg) and saquinavir (200 mg). These results indicate that ritonavir can favorably alter the pharmacokinetic profiles of other protease inhibitors. Combination regimens of ritonavir and other protease inhibitors may thus play a role in the treatment of HIV infection. Because of potentially substantial drug level increases, however, such combinations require further investigation to establish safe regimens for clinical use.
研究了与人类免疫缺陷病毒(HIV)蛋白酶抑制剂利托那韦合用,作为提高血浆中其他拟肽类HIV蛋白酶抑制剂水平的一种方法。在大鼠和人肝微粒体中,利托那韦强烈抑制细胞色素P450(CYP)介导的沙奎那韦、茚地那韦、奈非那韦和VX - 478的代谢。研究了利托那韦中负责与CYP结合和抑制的结构特征。在大鼠和狗中,其他蛋白酶抑制剂与利托那韦合用后,单次给药8至12小时后血浆药物水平升高且持续。大鼠体内的药物暴露量提高了8至46倍。在人类中,单次联合服用利托那韦(600毫克)和沙奎那韦(200毫克)后,观察到血浆中沙奎那韦浓度提高了50倍以上。这些结果表明,利托那韦可以有利地改变其他蛋白酶抑制剂的药代动力学特征。因此,利托那韦与其他蛋白酶抑制剂的联合用药方案可能在HIV感染治疗中发挥作用。然而,由于药物水平可能大幅升高,此类联合用药需要进一步研究以确定安全的临床使用方案。
