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在尿流和pH值未得到控制的情况下多形性氟卡尼的处置情况

Polymorphic flecainide disposition under conditions of uncontrolled urine flow and pH.

作者信息

Gross A S, Mikus G, Fischer C, Eichelbaum M

机构信息

Dr. Margarete Fischer-Bosch-Institute of Clinical Pharmacology, Stuttgart, FRG.

出版信息

Eur J Clin Pharmacol. 1991;40(2):155-62. doi: 10.1007/BF00280070.

Abstract

The pharmacokinetics of R- and S-flecainide have been determined in five poor (PM) and five extensive (EM) metabolisers of sparteine/debrisoquine under conditions of uncontrolled urine flow and pH. The half-lives of R- and S-flecainide in PMs (R 19.3 h; S 16.1 h) were approximately twice those observed in EMs (R 8.8 h; S 9.1 h). The apparent oral clearances of R- and S-flecainide were lower in PMs (R 313 ml.min-1; S 379 ml.min-1) than in EMs (R 783 ml.min-1; S 828 ml.min-1). The renal clearance, however, was comparable for both enantiomers in both EMs and PMs, and therefore the phenotypic differences in flecainide disposition observed must be due to differences in metabolic clearance. The nonrenal clearance of both enantiomers was significantly lower in poor (R 123 ml.min-1; S 201 ml.min-1) relative to extensive metabolisers (R 533 ml.min-1; S 586 ml.min-1). The partial clearance to the two major metabolites meta-O-dealkylated flecainide (MODF) and the meta-O-dealkylated lactam of flecainide (MODLF) was significantly lower in poor (62 ml.min-1) than extensive (267 ml.min-1) metabolisers. The impairment in flecainide metabolism in poor metabolisers of sparteine/debrisoquine has therefore been confirmed. Under conditions reflecting the clinical situation the difference in disposition between EMs and PMs would be considerable. However, it may be predicted that at standard doses concentrations greater than 1000 ng.ml-1 would not be attained in the PMs studied.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在尿流和pH值未受控制的条件下,已对5名司巴丁/异喹胍代谢缓慢者(PM)和5名代谢正常者(EM)测定了R-和S-氟卡尼的药代动力学。PM中R-和S-氟卡尼的半衰期(R为19.3小时;S为16.1小时)约为EM中观察到的半衰期(R为8.8小时;S为9.1小时)的两倍。PM中R-和S-氟卡尼的表观口服清除率(R为313 ml·min⁻¹;S为379 ml·min⁻¹)低于EM(R为783 ml·min⁻¹;S为828 ml·min⁻¹)。然而,两种对映体在EM和PM中的肾清除率相当,因此观察到的氟卡尼处置的表型差异必定是由于代谢清除的差异。相对于代谢正常者(R为533 ml·min⁻¹;S为586 ml·min⁻¹),代谢缓慢者中两种对映体的非肾清除率显著较低(R为123 ml·min⁻¹;S为201 ml·min⁻¹)。代谢缓慢者中氟卡尼代谢的损害因此得到证实。在反映临床情况的条件下,EM和PM之间的处置差异会相当大。然而,可以预测,在所研究的PM中,标准剂量下不会达到大于1000 ng·ml⁻¹的浓度。(摘要截短为250字)

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