R/S-维拉帕米在慢性心房颤动患者中的处置及药理作用:单剂量与多剂量比较研究
Disposition and pharmacologic effects of R/S-verapamil in patients with chronic atrial fibrillation: an investigation comparing single and multiple dosing.
作者信息
Busse D, Fromm M F, Mörike K, Drescher S, Kühlkamp V, Eichelbaum M
机构信息
Dr Margarete Fischer-Bosch-Institute of Clinical Pharmacology, and the Division of Clinical Pharmacology and the Department of Internal Medicine III, Eberhard Karl's University, Germany.
出版信息
Clin Pharmacol Ther. 2001 May;69(5):324-32. doi: 10.1067/mcp.2001.115125.
BACKGROUND
Racemic (R /S)- verapamil is widely used in the management of chronic atrial fibrillation. The negative dromotropic effect is mainly mediated by the S -enantiomer, which is preferentially metabolized. Previous studies report an accumulation of R /S- verapamil during long-term oral treatment of patients with chronic atrial fibrillation. However, the specific disposition of S -verapamil and the pharmacologic effects were not assessed. Therefore uncertainties about the need for dose adjustments remain.
METHODS
Using stable isotope technology and a stereospecific assay, we compared the pharmacokinetics and pharmacodynamics of intravenous (10 mg of d(7)-R /S -verapamil) and oral (240 mg of slow release (SR) d(0)-R /S -verapamil) R -verapamil and S -verapamil after the first dose (day 1) and after 3 weeks (day 21) of continuous oral therapy in 8 patients with long-term atrial fibrillation. On both study days, serum samples were obtained for the analysis of d(7)- and d(0)-R -verapamil and S -verapamil. Heart rate (HR) was monitored with electrocardiography (with each blood sample) and Holter electrocardiography (before the study, on day 1, and on day 21).
RESULTS
Compared with day 1, clearance of oral R -verapamil and S -verapamil was significantly reduced on day 21 (1007 +/- 380 versus 651 +/- 253 mL/min [-35%] and 5481 +/- 2731 versus 2855 +/- 1097 mL/min [-48%], respectively; P <.05), whereas only a moderate decrease was observed for intravenous R -verapamil and S -verapamil (-23% and -14%, respectively, not significant). Mean HR (89 +/- 11 bpm before verapamil) was effectively reduced, with the same effects on day 1 (68 +/- 8 bpm) and day 21 (68 +/- 8 bpm). Compared with day 1, the HR reduction per ng/mL of S -verapamil (calculated by the area under the curve [from 0-24 hours] ratio of HR reduction and S -verapamil concentration) was significantly lower on day 21 (0.7 +/- 0.4 versus 1.2 +/- 0.7 [bpm]. ng/mL, for day 21 versus day 1; P <.01).
CONCLUSIONS
In patients with chronic atrial fibrillation, clearance of oral, but not intravenous, S -verapamil and R -verapamil is significantly reduced with multiple doses compared with a single dose, thereby indicating predominant impairment of prehepatic rather than hepatic metabolism as the underlying mechanism. However, this kinetic change is clinically compensated by a decrease in the responsiveness to S -verapamil observed with regular dosing. The data suggest that despite accumulation of the drug individual verapamil doses can be maintained during long-term oral rate control therapy.
背景
消旋(R/S)-维拉帕米广泛用于慢性房颤的治疗。负性变传导作用主要由优先代谢的S-对映体介导。既往研究报道,慢性房颤患者长期口服治疗期间R/S-维拉帕米会蓄积。然而,未评估S-维拉帕米的具体处置情况及药理作用。因此,关于是否需要调整剂量仍存在不确定性。
方法
我们采用稳定同位素技术和立体特异性分析方法,比较了8例长期房颤患者静脉注射(10mg d(7)-R/S-维拉帕米)和口服(240mg缓释(SR)d(0)-R/S-维拉帕米)R-维拉帕米和S-维拉帕米首剂(第1天)及连续口服治疗3周(第21天)后的药代动力学和药效学。在两个研究日,均采集血清样本分析d(7)-和d(0)-R-维拉帕米及S-维拉帕米。通过心电图(每次采集血样时)和动态心电图(研究前、第1天和第21天)监测心率(HR)。
结果
与第1天相比,第21天时口服R-维拉帕米和S-维拉帕米的清除率显著降低(分别为1007±380与651±253 mL/min[-35%],以及5481±2731与2855±1097 mL/min[-48%];P<.05),而静脉注射R-维拉帕米和S-维拉帕米仅出现中度降低(分别为-23%和-14%,无统计学意义)。平均HR(维拉帕米治疗前为89±11次/分)有效降低,第1天(68±8次/分)和第21天(68±8次/分)效果相同。与第1天相比,第21天时每ng/mL S-维拉帕米导致的HR降低幅度(通过HR降低幅度与S-维拉帕米浓度的曲线下面积[0至24小时]比值计算)显著降低(第21天与第1天相比,分别为0.7±0.4与1.2±0.7[次/分·(ng/mL)(-¹)];P<.01)。
结论
在慢性房颤患者中,与单剂量相比,多次口服S-维拉帕米和R-维拉帕米后清除率显著降低,但静脉注射后未出现这种情况,这表明潜在机制是肝前代谢而非肝代谢受到主要损害。然而,这种动力学变化在临床上通过长期给药时对S-维拉帕米反应性的降低得到了代偿。数据表明,尽管药物会蓄积,但在长期口服心率控制治疗期间可维持维拉帕米的个体剂量。
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