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通过整合药代动力学-药效学模型描述多巴胺激动剂CQP201-403催乳素抑制作用的时间过程。

Description of the time course of the prolactin suppressant effect of the dopamine agonist CQP201-403 by an integrated pharmacokinetic-pharmacodynamic model.

作者信息

Grevel J, Brownell J, Steimer J L, Gaillard R C, Rosenthaler J

出版信息

Br J Clin Pharmacol. 1986 Jul;22(1):1-13. doi: 10.1111/j.1365-2125.1986.tb02872.x.

Abstract

Six male volunteers (mean age 24 years) received a single oral dose of 0.025 mg CQP201-403 and placebo in a randomised double-blind crossover design. Fifteen plasma samples were collected over 48 h and were assayed by radioimmunoassay for drug substance and prolactin (PRL). Three of the samples were drawn during sleep on the first study day. The pharmacological effect (E%) of CQP201-403 was expressed as reduction in plasma PRL levels. The pharmacokinetic (PK)-pharmacodynamic (PD) model consisted of two kinetic compartments and an effect compartment linked to the central compartment. A sigmoid Emax model (Hill equation) described the relationship between the drug concentration in the effect compartment and E%. Curve-fitting of PK and PD data provided individual parameter estimates which served to generate computer-simulated PK and PD profiles after single and multiple doses in order to: investigate the in vivo concentration-effect relationship; evaluate the consequence of dosage reduction on the steady-state PD profile; and study the robustness of the response to changes in drug potency and bioavailability.

摘要

六名男性志愿者(平均年龄24岁)在随机双盲交叉设计中接受了单次口服0.025毫克CQP201 - 403和安慰剂。在48小时内采集了15份血浆样本,并通过放射免疫分析法测定药物和催乳素(PRL)。其中三份样本是在第一个研究日睡眠期间采集的。CQP201 - 403的药理效应(E%)以血浆PRL水平的降低来表示。药代动力学(PK)-药效学(PD)模型由两个动力学室和一个与中央室相连的效应室组成。一个S形Emax模型(希尔方程)描述了效应室中的药物浓度与E%之间的关系。PK和PD数据的曲线拟合提供了个体参数估计值,这些估计值用于生成单剂量和多剂量后的计算机模拟PK和PD曲线,以便:研究体内浓度-效应关系;评估剂量降低对稳态PD曲线的影响;以及研究对药物效力和生物利用度变化的反应的稳健性。

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