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Assessment of activity levels for CYP2D6*1, CYP2D6*2, and CYP2D6*41 genes by population pharmacokinetics of dextromethorphan

机译:通过右美沙芬的群体药代动力学评估CYP2D6 * 1,CYP2D6 * 2和CYP2D6 * 41基因的活性水平

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摘要

The pharmacokinetics of dextromethorphan (DM) is markedly influenced by cytochrome P450 2D6 (CYP2D6) enzyme polymorphisms. The aim of this study was to quantify the effects of the CYP2D6*1, *2, and *41 variants on DM metabolism in vivo and to identify other sources of pharmacokinetic variability. Concentrations of DM and dextrorphan (DO) in plasma and urine were evaluated in 36 healthy Caucasian men. These volunteers participated in three clinical studies and received a single oral dose of 30 mg DM-HBr. Data were modeled simultaneously using the population pharmacokinetics NONMEM software. A five-compartment model adequately described the data. The activity levels of the alleles assessed differed significantly. The clearance attributable to an individual CYP2D6*1 copy was 2.5-fold higher as compared with CYP2D6*2 (5,010 vs. 2,020 l/h), whereas the metabolic activity of CYP2D6*41 was very low (85 l/h). Urinary pH was confirmed as a significant covariate for DM renal clearance. These results refine genotype-based predictions of pharmacokinetics for DM and presumably for other CYP2D6 substrates as well.
机译:右美沙芬(DM)的药代动力学受细胞色素P450 2D6(CYP2D6)酶多态性的显着影响。这项研究的目的是量化CYP2D6 * 1,* 2和* 41变体对体内DM代谢的影响,并确定药代动力学变异性的其他来源。在36名健康的白人男性中评估了血浆和尿液中DM和右旋芬(DO)的浓度。这些志愿者参加了三项临床研究,并接受了30 mg DM-HBr的单次口服剂量。使用群体药代动力学NONMEM软件同时对数据进行建模。五室模型充分描述了数据。评估的等位基因的活性水平显着不同。归因于单个CYP2D6 * 1拷贝的清除率比CYP2D6 * 2高2.5倍(5,010对2,020 l / h),而CYP2D6 * 41的代谢活性非常低(85 l / h)。尿液pH被证实是DM肾清除率的重要协变量。这些结果完善了基于基因型的DM药代动力学的预测,也可能是其他CYP2D6底物的预测。

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