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Evaluation of effects of polymorphism for metabolic enzymes on pharmacokinetics of carvedilol by population pharmacokinetic analysis.

机译:群体药代动力学分析评价群体药代动力学分析对卡维地洛醇药代动力学的代谢酶作用评价。

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In our previous study it was observed that the frequencies of UGT1A1*6, UGT2B7*3 and CYP2D6*10 in patients who have a low level ability of glucuronidation were significantly higher than those in patients with a high level of ability of glucuronidation. The same tendency was found in the frequency of CYP2D6*5, though there was no significant difference. The purpose of this study was to evaluate the effects of the polymorphism on pharmacokinetics of carvedilol by population pharmacokinetic analysis. Population pharmacokinetic analysis was performed using 373 plasma concentrations from 41 patients with chronic heart failure or angina pectoris. A one compartment pharmacokinetic model with first-order absorption (for oral dosing) was used to describe the concentration-versus-time data for carvedilol. We examined the effects of various clinical and genetic covariables in the regression models for clearance and volume of distribution. The results suggested that the factors of interindividual variation for carvedilol clearance were creatinine clearance and polymorphisms of UGT2B7 and CYP2D6 in the Japanese population with heart disease. It was estimated that UGT2B7*3 decreased the clearance of carvedilol by 37%, but UGT2B7*2 did not show any effect. Clearance in the patients who have intermediate activity of CYP2D6 was decreased by 39%.
机译:在我们以前的研究中,观察到,血糖尿糖含量低的患者的UGT1A1 * 6,UGT2B7 * 3和CYP2D6 * 10的频率显着高于血糖尿血糖能力高患者的患者。在CYP2D6 * 5的频率中发现了相同的趋势,尽管没有显着差异。本研究的目的是通过人群药代动力学分析评估多态性对卡维地洛的药代动力学的影响。使用来自41例慢性心力衰竭或心绞痛患者的373例血浆浓度进行人口药代动力学分析。使用一流的吸收(用于口服给药)的一个隔室药代动力学模型来描述卡维地洛的浓度 - 与时间数据。我们研究了各种临床和遗传协变量在回归模型中的效果,以进行清除和分布量。结果表明,Carvedilol间隙的细胞间变异因素是日本人群心脏病的UGT2B7和CYP2D6的肌酐清除和多态性。据估计,UGT2B7 * 3减少了卡维地洛的间隙37%,但UGT2B7 * 2没有显示出任何影响。 CYP2D6中间活性的患者的许可减少了39%。

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