首页> 美国卫生研究院文献>CPT: Pharmacometrics Systems Pharmacology >Population Pharmacokinetic Model Characterizing 24-Hour Variation in the Pharmacokinetics of Oral and Intravenous Midazolam in Healthy Volunteers
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Population Pharmacokinetic Model Characterizing 24-Hour Variation in the Pharmacokinetics of Oral and Intravenous Midazolam in Healthy Volunteers

机译:表征健康志愿者口服和静脉注射咪达唑仑药代动力学24小时变化的群体药代动力学模型

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摘要

Daily rhythms in physiology may affect the pharmacokinetics of a drug. The aim of this study was to evaluate 24-hour variation in the pharmacokinetics of the CYP3A substrate midazolam. Oral (2 mg) and intravenous (1 mg) midazolam was administered at six timepoints throughout the 24-hour period in 12 healthy volunteers. Oral bioavailability (population mean value [RSE%] of 0.28 (7.1%)) showed 24-hour variation that was best parameterized as a cosine function with an amplitude of 0.04 (17.3%) and a peak at 12:14 in the afternoon. The absorption rate constant was 1.41 (4.7%) times increased after drug administration at 14:00. Clearance (0.38 L/min (4.8%)) showed a minor 24-hour variation with an amplitude of 0.03 (14.8%) L/min and a peak at 18:50. Simulations show that dosing time minimally affects the concentration time profiles after intravenous administration, while concentrations are higher during the day compared to the night after oral dosing, reflecting considerable variation in intestinal processes.
机译:生理上的日常节律可能会影响药物的药代动力学。这项研究的目的是评估CYP3A底物咪达唑仑的24小时药代动力学变化。在12个健康志愿者的整个24小时内,在六个时间点分别口服(2 mg)和静脉内(1 mg)咪达唑仑。口服生物利用度(人口平均值[RSE%]为0.28(7.1%))显示24小时变化,最好将其参数化为余弦函数,振幅为0.04(17.3%),并在下午12:14达到峰值。 14:00给药后,吸收率常数增加1.41(4.7%)倍。间隙(0.38 L / min(4.8%))显示24小时小的变化,振幅为0.03(14.8%)L / min,在18:50达到峰值。模拟表明,给药时间对静脉内给药后的浓度时间曲线影响最小,而白天的浓度要比口服给药后的夜晚高,反映了肠道过程的显着变化。

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