Pharmacology Department, Pasteur University Hospital, Nice, France.
J Clin Pharmacol. 2011 Jul;51(7):1071-8. doi: 10.1177/0091270010379808. Epub 2011 Jan 5.
This study evaluated the effects of single-dose administration and steady-state concentrations of tipranavir 500 mg and ritonavir 200 mg (TPV/r) combination on the pharmacokinetics of tadalafil 10 mg (TAD) in an open-label study. Seventeen healthy male volunteers received sequential dosing of the studied product: TAD (day 1) alone in a single dose for 7 days followed by TAD (day 8) in a single dose with TPV/r (500/200 mg twice daily, days 8-18). Pharmacokinetic parameters were determined in a noncompartmental analysis. The geometric mean ratio and 90% confidence interval were used to evaluate drug interactions. The effect of a single dose of TAD on the pharmacokinetics of TPV/r resulted in a small decrease in exposure after either first-dose or steady-state TPV/r (geometric mean ratios [90% confidence interval]: area under the concentration-time curve, 0.85 [0.74-0.97]). In contrast, coadministration of TAD exposure was increased significantly (2.33 [2.02-2.69]) when administered with the first dose of TPV/r but not when TPV/r steady state was reached (1.01 [0.83-1.21]). Antiretroviral activity may not be reduced, but the dose of TAD should be reduced at the start of TPV/r therapy and then a full dose can be resumed after steady state is reached.
本研究评估了单剂量给予和稳态浓度下替诺福韦 500mg 和利托那韦 200mg(TPV/r)联合制剂对他达拉非 10mg(TAD)药代动力学的影响,这是一项开放标签研究。17 名健康男性志愿者接受了研究产品的序贯给药:单独给予 TAD(第 1 天)单剂量,连续 7 天,然后在第 8 天给予 TAD(第 8 天)单剂量,同时给予 TPV/r(500/200mg,每日 2 次,第 8-18 天)。药代动力学参数采用非房室分析方法进行评估。采用几何均数比值及其 90%置信区间评估药物相互作用。TAD 单剂量对 TPV/r 药代动力学的影响导致首次或稳态 TPV/r 后暴露量略有下降(几何均数比值[90%置信区间]:浓度-时间曲线下面积,0.85[0.74-0.97])。相反,当与 TPV/r 的首剂联合给药时,TAD 的暴露量显著增加(2.33[2.02-2.69]),但当达到 TPV/r 稳态时则没有增加(1.01[0.83-1.21])。抗逆转录病毒活性可能不会降低,但在开始 TPV/r 治疗时应减少 TAD 的剂量,然后在达到稳态后再恢复全剂量。
