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人类使用可卡因期间心率的药代动力学-药效学模型。

A pharmacokinetic-pharmacodynamic model of heart rate during cocaine administration in humans.

作者信息

Noe D A, Kumor K M

机构信息

Department of Oncology, Johns Hopkins University School of Medicine, Baltimore, Md.

出版信息

Clin Pharmacol Ther. 1991 Apr;49(4):426-32. doi: 10.1038/clpt.1991.50.

Abstract

We developed a pharmacokinetic-pharmacodynamic model of the heart rate response to cocaine consisting of the sum of the baseline heart rate, a chronotropic drug effect, and a conditioned heart rate response. The conditioned response was modeled as having a monoexponential decline. Cocaine's chronotropic effect was modeled as obeying a maximum (Emax) drug-effect relationship without tachyphylaxis. The model was tested by fitting the kinetic and heart rate data from an earlier study. The data from five subjects in that study were well fit by the model: mean Emax, 64 beats/min, and mean drug concentration producing 50% of Emax, 838 ng cocaine/ml. The data from the other three subjects in that study were fit well, employing a linear rather than an Emax drug effect relationship: mean effect coefficient, 0.035 beats/min/ng cocaine/ml. The findings emphasize the importance of conditioning in the responses to psychoactive drugs.

摘要

我们建立了一个关于可卡因对心率反应的药代动力学-药效学模型,该模型由基础心率、变时性药物效应和条件性心率反应之和组成。条件性反应被模拟为具有单指数衰减。可卡因的变时性效应被模拟为服从最大(Emax)药物效应关系且无快速耐受性。通过拟合早期研究中的动力学和心率数据对该模型进行了测试。该研究中五名受试者的数据与模型拟合良好:平均Emax为64次/分钟,产生50%Emax的平均药物浓度为838纳克可卡因/毫升。该研究中其他三名受试者的数据拟合良好,采用的是线性而非Emax药物效应关系:平均效应系数为0.035次/分钟/纳克可卡因/毫升。这些发现强调了条件作用在对精神活性药物反应中的重要性。

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