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药物滥用可能性评估中的药代动力学考量

Pharmacokinetic considerations in abuse liability evaluation.

作者信息

Farré M, Camí J

机构信息

Institut Municipal d'Investigació Mèdica, Barcelona, Spain.

出版信息

Br J Addict. 1991 Dec;86(12):1601-6. doi: 10.1111/j.1360-0443.1991.tb01754.x.

Abstract

The behavioral effects of a drug are related to three factors: its intrinsic pharmacological activity, its physicochemical properties, and its pharmacokinetic parameters. In many cases differences in absorption, distribution, metabolism, and elimination may explain the different abuse liability profiles of drugs from within the same pharmacological class. Rapid absorption rate and high lipid solubility are the most important factors contributing to early drug concentrations in the brain. Differences in drug metabolism may be related to dose-dependent kinetics, first-pass metabolism, and variations in genetic traits (e.g. poor or extensive metabolizers). Metabolic pathways may produce active metabolites with similar or greater pharmacological activity than the parent substance. Drugs with a rapid elimination rate have been associated with greater self-administration and with early emergence of withdrawal symptoms. More pharmacokinetic studies are needed in human drug abuse liability evaluations. Knowledge of the plasma concentrations of drugs and their pharmacokinetic parameters can be essential to interpret differences among similar drugs in human abuse liability assessments.

摘要

药物的行为效应与三个因素有关

其内在药理活性、理化性质及其药代动力学参数。在许多情况下,吸收、分布、代谢和消除的差异可以解释同一药理类别中药物不同的滥用倾向特征。快速吸收速率和高脂溶性是导致大脑中药物早期浓度的最重要因素。药物代谢的差异可能与剂量依赖性动力学、首过代谢以及遗传特征的变化(例如代谢缓慢或广泛的代谢者)有关。代谢途径可能产生具有与母体物质相似或更大药理活性的活性代谢物。消除速率快的药物与更高的自我给药率以及戒断症状的早期出现有关。在人类药物滥用倾向评估中需要更多的药代动力学研究。了解药物的血浆浓度及其药代动力学参数对于解释人类滥用倾向评估中相似药物之间的差异至关重要。

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