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首页> 外文期刊>European journal of drug metabolism and pharmacokinetics >Effect of CYP2C9 Polymorphisms on the Pharmacokinetics of Indomethacin During Pregnancy
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Effect of CYP2C9 Polymorphisms on the Pharmacokinetics of Indomethacin During Pregnancy

机译:CYP2C9多态性对妊娠期吲哚美辛的药代动力学的影响

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Background and ObjectiveCytochrome P450 (CYP)2C9 catalyzes the biotransformation of indomethacin to its inactive metabolite O-desmethylindomethacin (DMI). The aim of this work was to determine the effect of CYP2C9 polymorphisms on indomethacin metabolism in pregnant women.MethodsPlasma concentrations of indomethacin and DMI at steady state were analyzed with a validated LC-MS/MS method. DNA was isolated from subject blood and buccal smear samples. Subjects were grouped by genotype for comparisons of pharmacokinetic parameters.ResultsFor subjects with the *1/*2 genotype, the meansteady-state apparent oral clearance (CL/F-ss)of indomethacin was 13.57.7 L/h (n=4) and the mean metabolic ratio (AUC(DMI)/AUC(indomethacin)) was 0.291 +/- 0.133. For subjects with the *1/*1 genotype, these values were 12.4 +/- 2.7 L/h and 0.221 +/- 0.078, respectively (n=14). Of note, we identified one subject who was a carrier of both the *3 and *4 alleles, resulting in an amino acid change (I359P) which has not been reported previously. This subject had a metabolic ratio of 0.390 and a CL/F-ss of indomethacin (24.3 L/h) that was nearly double the wild-type clearance.ConclusionAlthough our results are limited by sample size and are not statistically significant, these data suggest that certain genetic polymorphisms of CYP2C9 may lead to an increased metabolic ratio and an increase in the clearance of indomethacin. More data are needed to assess the impact of CYP2C9 genotype on the effectiveness of indomethacin as a tocolytic agent.
机译:背景和客观致毒性P450(CYP)2C9催化Indomethacin的生物转化,以其无活性代谢物O-去甲基吲哚汀(DMI)。这项工作的目的是确定CYP2C9多态性对孕妇中的吲哚美嗪代谢的影响。用验证的LC-MS / MS法分析稳态稳态的吲哚美辛素和DMI的水平。从受试者血液和颊涂片样品中分离DNA。受试者被基因型分组以进行药代动力学参数的比较。具有* 1 / * 2基因型的受试者,Indomethacin的均值状态表观口腔间隙(Cl / F-SS)为13.57.7 L / h(n = 4)而平均代谢比(AUC(DMI)/ AUC(吲哚美辛))为0.291 +/- 0.133。对于具有* 1 / * 1基因型的受试者,这些值分别为12.4 +/- 2.7L / h和0.221 +/- 0.078(n = 14)。值得注意的是,我们确定了一个作为* 3和* 4等位基因载体的一个受试者,导致尚未报道的氨基酸变化(I359P)。该受试者的代谢比为0.390和Indomethacin(24.3L / h)的Cl / F-s,几乎是野生型清除的两倍。虽然我们的结果受到样本大小的限制并且没有统计学意义,但这些数据表明CYP2C9的某些遗传多态性可能导致代谢比增加,并且吲哚美辛的间隙增加。需要更多数据来评估CYP2C9基因型对吲哚美辛作为托殖剂的有效性的影响。

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