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药物剂量的反应优化:妥卡尼的抗心律失常研究

Response optimization of drug dosage: antiarrhythmic studies with tocainide.

作者信息

Meffin P J, Winkle R A, Blaschke T F, Fitzgerald J, Harrison D C, Harapat S R, Bell P A

出版信息

Clin Pharmacol Ther. 1977 Jul;22(1):42-57. doi: 10.1002/cpt197722142.

Abstract

The benefits of using antiarrhythmic response to optimize dosage regimens of antiarrhythmic drugs in individual patients have been examined. Graded antiarrhythmic response and simultaneously measured plasma drug concentrations have been obtained in 15 patients receiving multiple oral doses of a new antiarrhythmic, tocainide. Plasma drug concentration-antiarrhythmic response data from each of 11 subjects responding to the drug have been fitted by a generalized concentration effect function which is valid over the entire range of response. With the use of experimentally determined pharmacokinetic parameters to define the dose-plasma concentration relationship and plasma drug concentration-response parameters estimated for individual patients, simulations were carried out to show the effect of various dosage regimens on antiarrhythmic response in individual patients. Such simulations provide a means of assessing antiarrhythmic effect in the range of clinical interest (80% to 100% of maximum effect), where the antiarrhythmic effect is a nonlinear function of dose, plasma drug concentration, or their logarithms. The simulations also demonstrate that for identical daily doses and dosing intervals patients show marked variability in antiarrhythmic response.

摘要

已对通过抗心律失常反应来优化个体患者抗心律失常药物给药方案的益处进行了研究。在15名接受新型抗心律失常药物妥卡尼多剂量口服给药的患者中,获得了分级抗心律失常反应以及同时测量的血浆药物浓度。对11名对该药物有反应的受试者中的每一位的血浆药物浓度-抗心律失常反应数据,都采用了一个在整个反应范围内有效的广义浓度效应函数进行拟合。利用实验确定的药代动力学参数来定义剂量-血浆浓度关系,并为个体患者估算血浆药物浓度-反应参数,进行了模拟以显示各种给药方案对个体患者抗心律失常反应的影响。此类模拟提供了一种在临床相关范围内(最大效应的80%至100%)评估抗心律失常效果的方法,在此范围内抗心律失常效果是剂量、血浆药物浓度或其对数的非线性函数。模拟还表明,对于相同的每日剂量和给药间隔,患者的抗心律失常反应存在显著差异。

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