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正常受试者和冠状动脉痉挛患者的维拉帕米动力学

Verapamil kinetics in normal subjects and patients with coronary artery spasm.

作者信息

Freedman S B, Richmond D R, Ashley J J, Kelly D T

出版信息

Clin Pharmacol Ther. 1981 Nov;30(5):644-52. doi: 10.1038/clpt.1981.216.

Abstract

Verapamil kinetics after intravenous and single and long-term oral dosing were studied in 12 patients with coronary artery spasm and four normal subjects. The decline in plasma concentration after intravenous doses was described by triexponential decay equation, with a terminal half-life (t1/2) of 5 hr. After a single oral dose the bioavailability was only 24%, probably because of the first-pass metabolism. During long-term oral doses of 80 mg every 6 hr, mean peak and trough concentrations were 255 +/- 90 and 105 +/- 38 ng/ml, and mean time at which peak concentration occurred was 1.2 +/- 0.5 hr. Norverapamil, the major active metabolite of verapamil, cumulated during oral dosing and may account for a small proportion of the overall pharmacologic effect. Mean elimination t1/2 during long-term oral dosing was longer than after a single dose (9.6 and 5.7 hr, P less than 0.05). Also, during long-term dosing the area under the curve was more than double that of a single dose, and the apparent oral clearance fell from 4.2 to 1.8 l/min (P less than 0.01). These changes may partly be explained by reduction in presystemic metabolism during long-term therapy. Kinetic predictions based on single doses will not give reliable estimates for long-term oral dosage. Less frequent dose schedule may be possible for prolonged therapy.

摘要

对12例冠状动脉痉挛患者和4名正常受试者进行了静脉注射、单次及长期口服维拉帕米后的动力学研究。静脉注射剂量后血浆浓度的下降可用三指数衰减方程描述,终末半衰期(t1/2)为5小时。单次口服给药后生物利用度仅为24%,可能是由于首过代谢。在每6小时口服80mg的长期给药期间,平均峰浓度和谷浓度分别为255±90和105±38ng/ml,达到峰浓度的平均时间为1.2±0.5小时。维拉帕米的主要活性代谢产物去甲维拉帕米在口服给药期间会蓄积,可能占总体药理作用的一小部分。长期口服给药期间的平均消除t1/2比单次给药后更长(分别为9.6和5.7小时,P<0.05)。此外,在长期给药期间,曲线下面积比单次给药时增加了一倍多,表观口服清除率从4.2降至1.8l/min(P<0.01)。这些变化可能部分归因于长期治疗期间首过代谢的减少。基于单次剂量的动力学预测无法为长期口服剂量提供可靠的估计。长期治疗可能可以采用给药频率较低的方案。

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