CYP2C9基因多态性对健康志愿者中(-)-3S,5R-氟伐他汀和(+)-3R,5S-氟伐他汀药代动力学及降胆固醇活性的影响。

Influence of CYP2C9 polymorphisms on the pharmacokinetics and cholesterol-lowering activity of (-)-3S,5R-fluvastatin and (+)-3R,5S-fluvastatin in healthy volunteers.

作者信息

Kirchheiner Julia, Kudlicz Dirk, Meisel Christian, Bauer Steffen, Meineke Ingolf, Roots Ivar, Brockmöller Jürgen

机构信息

Institute of Clinical Pharmacology, Charité, Humboldt University of Berlin, Berlin, Germany.

出版信息

Clin Pharmacol Ther. 2003 Aug;74(2):186-94. doi: 10.1016/S0009-9236(03)00121-8.

DOI:10.1016/S0009-9236(03)00121-8

PMID:12891229

Abstract

INTRODUCTION

In vitro data indicate that biotransformation of the synthetic 3-hydroxy-3-methylglutaryl-coenzyme A reductase inhibitor fluvastatin is catalyzed by the cytochrome P450 (CYP) enzyme 2C9. The consequences of CYP2C9 genetic polymorphisms on fluvastatin pharmacokinetics and on its efficacy have not been investigated in humans thus far.

METHODS

Twenty-four healthy heterozygous or homozygous carriers of the CYP2C9 variants Arg144Cys (*2) and Ile359Leu (*3) and 2 individuals with the deficient CYP2D6 genotype *4/*4 took 40 mg racemic fluvastatin daily for 14 days. All subjects had also been genotyped for CYP2C8, CYP2C19, and CYP2D6 polymorphisms. Pharmacokinetics was analyzed after the first fluvastatin administration. Serum lipid concentrations were measured before fluvastatin intake and on day 15. Plasma concentrations of (+)-3R,5S-fluvastatin and of (-)-3S,5R-fluvastatin were quantified by enantiospecific HPLC.

RESULTS

Pharmacokinetics of both enantiomers showed statistically significant differences according to the number of CYP2C93 alleles (P <.0001, F test). Mean (and SD) values for area under the curve of the active (+)-3R,5S-fluvastatin in carriers of the genotype CYP2C91/*1, *1/*3, and *3/3 were 173 (85) micro g. L(-1). h, 231 (85) micro g. L(-1). h, and 533 (120) micro g. L(-1). h, respectively. The corresponding values for area under the curve of (-)-3S,5R-fluvastatin were 227 (133) micro g. L(-1). h, 360 (103) micro g. L(-1). h, and 1126 (311) micro g. L(-1). h for CYP2C91/*1, *1/3, and 3/3, respectively. The CYP2C92 variant did not have any significant influence on fluvastatin kinetics, nor did the CYP2C83 allele, which was tightly linked with CYP2C92. Total serum cholesterol and low-density lipoprotein cholesterol concentrations decreased significantly during the 14-day treatment period (P <.001), but no correlation with the CYP2C9 genotype was found.

CONCLUSIONS

The pharmacokinetics of both enantiomers of fluvastatin depended on the CYP2C9 genotype, with a 3-fold group mean difference in the active enantiomer and even greater differences in the inactive enantiomer, but differences in plasma concentrations were not reflected in cholesterol lowering after 14 days of fluvastatin intake in healthy volunteers.

摘要

引言

体外数据表明，合成的3-羟基-3-甲基戊二酰辅酶A还原酶抑制剂氟伐他汀的生物转化由细胞色素P450（CYP）酶2C9催化。迄今为止，尚未在人体中研究CYP2C9基因多态性对氟伐他汀药代动力学及其疗效的影响。

方法

24名CYP2C9变体Arg144Cys（*2）和Ile359Leu（3）的健康杂合子或纯合子携带者以及2名CYP2D6基因型4/*4缺陷的个体，每天服用40mg消旋氟伐他汀，持续14天。所有受试者也已针对CYP2C8、CYP2C19和CYP2D6多态性进行基因分型。在首次服用氟伐他汀后分析药代动力学。在服用氟伐他汀前和第15天测量血清脂质浓度。通过对映体特异性HPLC定量（+）-3R，5S-氟伐他汀和（-）-3S，5R-氟伐他汀的血浆浓度。

结果

根据CYP2C93等位基因数量，两种对映体的药代动力学显示出统计学上的显著差异（P<.0001，F检验）。基因型CYP2C91/*1、*1/3和3/3携带者中活性（+）-3R，5S-氟伐他汀曲线下面积的平均值（和标准差）分别为173（85）μg·L（-1）·h、231（85）μg·L（-1）·h和533（120）μg·L（-1）·h。（-）-3S，5R-氟伐他汀曲线下面积的相应值，对于CYP2C91/1、1/3和3/3分别为227（133）μg·L（-1）·h、360（103）μg·L（-1）·h和1126（311）μg·L（-1）·h。CYP2C92变体对氟伐他汀动力学没有任何显著影响，与CYP2C92紧密连锁的CYP2C83等位基因也没有。在14天治疗期间，总血清胆固醇和低密度脂蛋白胆固醇浓度显著降低（P<.001），但未发现与CYP2C9基因型相关。