健康志愿者中奈非那韦与低剂量利托那韦每日一次联合用药的药代动力学、食物摄入要求及耐受性
Pharmacokinetics, food intake requirements and tolerability of once-daily combinations of nelfinavir and low-dose ritonavir in healthy volunteers.
作者信息
Aarnoutse R E, Droste J A H, van Oosterhout J J G, Koopmans P P, Popescu M, Reiss P, Hekster Y A, Burger D M
机构信息
Department of Clinical Pharmacy, University Medical Centre Nijmegen, Nijmegen, The Netherlands.
出版信息
Br J Clin Pharmacol. 2003 Feb;55(2):115-25. doi: 10.1046/j.1365-2125.2003.01756.x.
AIMS
This study was performed to evaluate the steady-state pharmacokinetics, food intake requirements and short-term tolerability of once-daily combinations of nelfinavir and low-dose ritonavir.
METHODS
Twenty-seven healthy volunteers were randomized over three groups to receive a once-daily regimen of nelfinavir/ritonavir 2,000/200 mg (group 1), 2,000/400 mg (group 2) or 2,500/200 mg (group 3) with food for 14 days. Pharmacokinetic parameters for nelfinavir and its active metabolite M8 were assessed on study days 15 and 16, after administration of the regimens with a full (610 kcal) or light (271 kcal) breakfast, respectively.
RESULTS
Pharmacokinetic data were evaluable for eight volunteers in group 1, eight in group 2 and four in group 3. Administration of nelfinavir/ritonavir with a full breakfast resulted in geometric mean (GM) nelfinavir AUC(24h) values of 76.8, 51.3, and 61.9 h*mg/l in group 1, 2 and 3, respectively. GM 24-h Cmin concentrations of nelfinavir were 0.76 mg l(-1), 0.43 mg l(-1) and 0.47 mg l(-1), respectively. Co-administration of ritonavir increased M8 concentrations more than nelfinavir concentrations, resulting in GM AUC(24h) and Cmin values for nelfinavir plus M8 that were higher than or comparable to reference values for the approved regimen of nelfinavir (1,250 mg BID without ritonavir). In the 2,000/200 mg group, seven out of eight subjects had a Cmin value of nelfinavir plus M8 above a threshold of 1.0 mg l-1. Administration of the combinations with a light breakfast resulted in significant decreases in the AUC(24h) and Cmin of nelfinavir and nelfinavir plus M8, compared with intake with a full breakfast. For the Cmin of nelfinavir plus M8, the GM ratio (light/full breakfast) was 0.76 (90% confidence interval 0.67-0.86, participants from all groups combined). Short-term tolerability was satisfactory, apart from a higher than expected incidence of mild rash (12%).
CONCLUSIONS
Administration of nelfinavir in a once-daily regimen appears feasible. A nelfinavir/ritonavir 2,000/200 mg combination appears appropriate for further evaluation. Once-daily nelfinavir/ritonavir should be taken with a meal containing at least 600 kcal.
目的
本研究旨在评估奈非那韦与低剂量利托那韦每日一次联合用药的稳态药代动力学、食物摄入要求及短期耐受性。
方法
27名健康志愿者被随机分为三组,接受为期14天的每日一次奈非那韦/利托那韦方案,分别为2000/200毫克(第1组)、2000/400毫克(第2组)或2500/200毫克(第3组),与食物同服。在第15天和第16天,分别在服用含全量(610千卡)或少量(271千卡)早餐的方案后,评估奈非那韦及其活性代谢物M8的药代动力学参数。
结果
第1组8名志愿者、第2组8名志愿者和第3组4名志愿者的药代动力学数据可评估。与全量早餐同服奈非那韦/利托那韦后,第1组、第2组和第3组奈非那韦的几何平均(GM)AUC(24h)值分别为76.8、51.3和61.9小时·毫克/升。奈非那韦的GM 24小时Cmin浓度分别为0.76毫克/升、0.43毫克/升和0.47毫克/升。利托那韦与奈非那韦合用时使M8浓度升高的幅度大于奈非那韦浓度,导致奈非那韦加M8的GM AUC(24h)和Cmin值高于或与奈非那韦批准方案(每日两次1250毫克,不含利托那韦)的参考值相当。在2000/200毫克组中,8名受试者中有7名奈非那韦加M8的Cmin值高于1.0毫克/升的阈值。与全量早餐相比,与少量早餐同服这些联合用药导致奈非那韦及奈非那韦加M8的AUC(24h)和Cmin显著降低。对于奈非那韦加M8的Cmin,GM比值(少量早餐/全量早餐)为0.76(90%置信区间0.67 - 0.86,所有组的参与者合并计算)。除轻度皮疹发生率高于预期(12%)外,短期耐受性良好。
结论
每日一次服用奈非那韦似乎可行。奈非那韦/利托那韦2000/200毫克的联合用药似乎适合进一步评估。每日一次的奈非那韦/利托那韦应与至少含600千卡热量的餐食同服。
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