阿芬太尼对大鼠脑电图影响的药代动力学-药效学建模：快速功能适应性评估

Pharmacokinetic-pharmacodynamic modelling of the EEG effect of alfentanil in rats: assessment of rapid functional adaptation.

作者信息

Cox E H, Kuipers J A, Danhof M

机构信息

Leiden/Amsterdam Center for Drug Research, Division of Pharmacology, Leiden University, Sylvius Laboratory, The Netherlands.

出版信息

Br J Pharmacol. 1998 Aug;124(7):1534-40. doi: 10.1038/sj.bjp.0701972.

DOI:10.1038/sj.bjp.0701972

PMID:9723968

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1565531/

Abstract

The purpose of the present investigation was to quantify rapid functional adaptation in the concentration-pharmacological effect relationship of alfentanil in rats using quantitative EEG parameters as a pharmacodynamic endpoint. Three groups of 6-7 rats received in a randomized fashion two consecutive infusions of 2.00, 3.14, or 4.24 mg/kg(-1) of alfentanil in 20, 40 or 60 min, respectively. The EEG was continuously recorded and frequent arterial blood samples were collected for determination of the alfentanil concentration by gas chromatography. 2. The pharmacokinetics of alfentanil were most adequately described by a bi-exponential function. The values (mean+/-s.e., n=20) of clearance, volume of distribution at steady-state and terminal half-life were 45+/-3 ml x min(-1) x kg(-1), 0.91+/-0.09 l/kg(-1) and 23+/-1 min, respectively, and independent of the administered dose. 3. Increase in power in the 0.5-4.5 Hz (delta) frequency band of the EEG was used as the measure of the pharmacological response. By pharmacokinetic-pharmacodynamic modeling the individual concentration-EEG effect relationships of alfentanil were derived which were successfully quantified by the sigmoidal Emax pharmacodynamic model. When the results of the first of the two consecutive infusions were compared, no systematic differences in the pharmacodynamic parameters were observed for the different infusion rates. The averaged values of the pharmacodynamic parameters of alfentanil were (mean+/-s.e., n=20): E0=56+/-3 microV, Emax=93+/-8 microV, EC50=235+/-27 ng x ml(-1) and Hill factor=1.6+/-0.1, respectively. For the second of the two consecutive infusions a significantly higher value of the EC50 of 404+/-56 ng x ml(-1) was observed (P < 0.05), while the values of the other pharmacodynamic parameters were unchanged. Simulations according to a mechanism-based model indicated that the observed change in concentration effect relationship can be explained by a 40% loss of functional mu-opioid receptors. 4. The results of the present study show that upon the administration of a single intravenous dose, acute functional adaptation does not interfere with the assessment of the concentration-EEG effect relationship of alfentanil. Upon repeated administration however functional adaptation may be a complicating factor.

摘要

本研究的目的是，以定量脑电图参数作为药效学终点，对大鼠中阿芬太尼浓度-药理效应关系中的快速功能适应性进行量化。三组6至7只大鼠以随机方式分别在20、40或60分钟内接受两次连续输注，剂量分别为2.00、3.14或4.24mg/kg⁻¹的阿芬太尼。持续记录脑电图，并频繁采集动脉血样，通过气相色谱法测定阿芬太尼浓度。2. 阿芬太尼的药代动力学最适合用双指数函数描述。清除率、稳态分布容积和终末半衰期的值（均值±标准误，n = 20）分别为45±3ml·min⁻¹·kg⁻¹、0.91±0.09l/kg⁻¹和23±1分钟，且与给药剂量无关。3. 脑电图0.5 - 4.5Hz（δ）频段功率的增加用作药理反应的度量。通过药代动力学-药效学建模得出阿芬太尼的个体浓度-脑电图效应关系，并用S形Emax药效学模型成功进行了量化。比较两次连续输注中第一次的结果时，未观察到不同输注速率下药效学参数的系统差异。阿芬太尼药效学参数的平均值（均值±标准误，n = 20）分别为：E0 = 56±3μV、Emax = 93±8μV、EC50 = 235±27ng·ml⁻¹和希尔系数 = 1.6±0.1。在两次连续输注的第二次中，观察到EC50值显著升高，为404±56ng·ml⁻¹（P < 0.05），而其他药效学参数的值未变。根据基于机制的模型进行的模拟表明，观察到的浓度效应关系变化可由功能性μ-阿片受体损失40%来解释。4. 本研究结果表明，单次静脉给药时，急性功能适应性不会干扰阿芬太尼浓度-脑电图效应关系的评估。然而，重复给药时，功能适应性可能是一个复杂因素。