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药物过量的药代动力学。

Pharmacokinetics of drug overdose.

作者信息

Rosenberg J, Benowitz N L, Pond S

出版信息

Clin Pharmacokinet. 1981 May-Jun;6(3):161-92. doi: 10.2165/00003088-198106030-00001.

DOI:10.2165/00003088-198106030-00001
PMID:7016383
Abstract

Pharmacokinetics of drugs taken in overdose may differ from those observed following therapeutic doses. Differences are due both to dose-dependent changes and to effects of drugs or pathophysiological consequences of the overdose on kinetics. Dose-dependent changes in rate and extent of absorption, bioavailability (saturation of first-pass metabolism), distribution (saturation of protein binding sites) and metabolism are discussed. Gastrointestinal motility is affected both by specific drug actions, such as delayed gastric emptying by anticholinergic drugs, and by general nervous system depression caused by many drugs. Drug-induced circulatory insufficiency may retard tissue distribution and reduce clearance. Disturbances in blood and urine pH may alter distribution and clearance of weak acids and bases. Drug-induced renal or hepatic failure can significantly decrease clearance. Hypothermia is a common complication of drug overdose and might retard distribution and also reduce clearance. The data concerning pharmacokinetics during overdose are usually incomplete and difficult to interpret. Doses and times of ingestion are uncertain, duration of blood and urine sampling is often inadequate to distinguish absorption from distribution and elimination phases, active metabolites are not measured, protein binding is not determined and clinical features of patients not adequately described. We have, however, reviewed available data for salicylate, paracetamol (acetaminophen), barbiturates, ethchlorvynol, glutethimide, chloral hydrate, tricyclic antidepressants, lithium, phenytoin, ethanol, theophylline, digoxin, amphetamine and phencyclidine.

摘要

药物过量服用时的药代动力学可能与治疗剂量下观察到的情况有所不同。差异既源于剂量依赖性变化,也源于药物或过量服用的病理生理后果对药代动力学的影响。本文讨论了吸收速率和程度、生物利用度(首过代谢饱和)、分布(蛋白质结合位点饱和)及代谢方面的剂量依赖性变化。胃肠道蠕动既受特定药物作用的影响,如抗胆碱能药物导致胃排空延迟,也受许多药物引起的一般神经系统抑制的影响。药物引起的循环功能不全可能会延缓组织分布并降低清除率。血液和尿液pH值的改变可能会改变弱酸和弱碱的分布及清除率。药物引起的肾衰竭或肝衰竭可显著降低清除率。体温过低是药物过量的常见并发症,可能会延缓分布并降低清除率。关于药物过量时药代动力学的数据通常不完整且难以解释。摄入剂量和时间不确定,血液和尿液采样时间往往不足以区分吸收、分布和消除阶段,未测定活性代谢物,未确定蛋白质结合情况,且未充分描述患者的临床特征。然而,我们已查阅了有关水杨酸盐、对乙酰氨基酚、巴比妥类药物、乙氯维诺、格鲁米特、水合氯醛、三环类抗抑郁药、锂、苯妥英、乙醇、茶碱、地高辛、苯丙胺和苯环利定的现有数据。

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