醋硝香豆素与细胞色素P450 2C9基因型相关的药代动力学

Acenocoumarol pharmacokinetics in relation to cytochrome P450 2C9 genotype.

作者信息

Thijssen Henk H W, Ritzen Bas

机构信息

Department of Pharmacology, Cardiovascular Research Institute Maastricht, University of Maastricht, The Netherlands.

出版信息

Clin Pharmacol Ther. 2003 Jul;74(1):61-8. doi: 10.1016/S0009-9236(03)00088-2.

DOI:10.1016/S0009-9236(03)00088-2

PMID:12844136

Abstract

BACKGROUND AND OBJECTIVES

Cytochrome P450 (CYP) 2C9 is one of the major CYP enzymes involved in the biotransformation of drugs, among others, the oral anticoagulant acenocoumarol. The enzyme has several polymorphisms, with the CYP2C92 and CYP2C93 variants most commonly present in white patients. Patients with the CYP2C93 variant are known to require a lower maintenance dose of racemic acenocoumarol. We investigated the impact of the polymorphisms CYP2C92 and CYP2C9*3 on the pharmacokinetics of R- and S-acenocoumarol.

METHODS AND RESULTS

In the first study 26 healthy volunteers with the genotype *1/*1 (n = 9), *1/*2 (n = 7), *1/*3 (n = 6), *2/*3 (n = 3), and *2/*2 (n = 1) were given 8 mg of racemic acenocoumarol as a single oral dose. Plasma R- and S-acenocoumarol concentrations were assayed at 4, 7, and 24 hours. Mean plasma S-acenocoumarol concentrations at 7 hours were higher in subjects with a variant allele; the differences were significant (P =.01) for the *1/*3 and *2/*3 genotypes. In the second study, the oral pharmacokinetics of acenocoumarol was investigated in 6 subjects (*1/*1 [n = 3] and *1/3 [n = 3]). The mean oral clearance of S-acenocoumarol was 45% lower in the CYP2C91/*3 genotypes (10.9 +/- 3.0 L/h versus 19.8 +/- 3.1 L/h, P =.02). Plasma half-life was prolonged from 1.0 +/- 0.2 hours to 2.0 +/- 0.7 hours (P =.09). R-acenocoumarol pharmacokinetics did not differ between the genotypes. There was no difference in mean international normalized ratio at 24 hours, which was 1.2 in both groups. In vitro enzyme kinetics showed reduced (85%) intrinsic activity of the *3 enzyme to catalyze the hydroxylations of S-acenocoumarol. The lower activity resulted from higher Michaelis-Menten constant (2-fold) and lower maximum rate of metabolism by an enzyme-mediated reaction (by 70%). The activity of the *2 enzyme was 50% of the wild-type one.

CONCLUSION

The results show S-acenocoumarol pharmacokinetics to be dependent on CYP2C9 polymorphism. In particular, the presence of the CYP2C9*3 allele impairs oral clearance of the coumarin.

摘要

背景与目的

细胞色素P450（CYP）2C9是参与药物生物转化的主要CYP酶之一，尤其是口服抗凝剂醋硝香豆素。该酶存在多种多态性，其中CYP2C92和CYP2C93变体在白人患者中最为常见。已知携带CYP2C93变体的患者需要较低剂量的消旋醋硝香豆素维持治疗。我们研究了CYP2C92和CYP2C9*3多态性对R-和S-醋硝香豆素药代动力学的影响。

方法与结果

在第一项研究中，26名基因型为*1/*1（n = 9）、*1/*2（n = 7）、*1/*3（n = 6）、*2/3（n = 3）和2/*2（n = 1）的健康志愿者单次口服8 mg消旋醋硝香豆素。在4、7和24小时测定血浆R-和S-醋硝香豆素浓度。携带变异等位基因的受试者在7小时时的平均血浆S-醋硝香豆素浓度较高；*1/3和2/*3基因型的差异具有统计学意义（P = 0.01）。在第二项研究中，对6名受试者（*1/1 [n = 3]和1/3 [n = 3]）的醋硝香豆素口服药代动力学进行了研究。CYP2C91/*3基因型的S-醋硝香豆素平均口服清除率降低了45%（10.9±3.0 L/h对19.8±3.1 L/h，P = 0.02）。血浆半衰期从1.0±0.2小时延长至2.0±0.7小时（P = 0.09）。不同基因型之间R-醋硝香豆素的药代动力学没有差异。两组在24小时时的平均国际标准化比值没有差异，均为1.2。体外酶动力学显示，*3酶催化S-醋硝香豆素羟化的内在活性降低（85%）。活性降低是由于米氏常数较高（2倍）以及酶介导反应的最大代谢速率较低（降低70%）。*2酶的活性为野生型的50%。