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在初治的儿科肾移植患者中,霉酚酸酯给药后的霉酚酸群体药代动力学和药物遗传学。

Population pharmacokinetics and pharmacogenetics of mycophenolic acid following administration of mycophenolate mofetil in de novo pediatric renal-transplant patients.

机构信息

Department of Pediatric Pharmacology and Pharmacogenetics, Hôpital Robert Debré, Paris, France.

出版信息

J Clin Pharmacol. 2010 Nov;50(11):1280-91. doi: 10.1177/0091270009357429. Epub 2010 Feb 10.

DOI:10.1177/0091270009357429
PMID:20147615
Abstract

The objective was to develop a population pharmacokinetic-pharmacogenetic model of mycophenolic acid following administration of mycophenolate mofetil (MMF) in de novo pediatric renal-transplant patients and identify factors that explain variability. The pharmacokinetic samples were collected from 89 de novo pediatric renal-transplant patients treated with MMF and studied during the first 60 postoperative days. All patients were genotyped for UGT1A8-A9, UGT2B7, and ABCC2. Population pharmacokinetic analysis was performed with the NONMEM and was validated using bootstrap visual predictive check. The pharmacokinetic data were best described by a 2-compartment model with Erlang distribution to describe the absorption phase. The covariate analysis identified body weight as an individual factor influencing central volume of distribution and concomitant immunosuppressive medication and identified body weight and UGT2B7 802C>T genotype as individual factors influencing apparent oral clearance (CL/F) of MMF. CL/F in cyclosporine-MMF-treated patients was 33% higher than in tacrolimus-MMF-treated patients. The CL/F was significantly lower in patients with UGT2B7 802 C/C genotype compared with patients with UGT2B7 802 C/T and 802T/T genotypes, and this effect was independent of concomitant immunosuppressive medication or body weight. The population pharmacokinetic-pharmacogenetic model of mycophenolic acid was validated. Body weight, concomitant medication, and UGT2B7 genotype contribute significantly to the interindividual variability of MMF disposition in pediatric renal-transplant patients.

摘要

目的在于建立霉酚酸在新诊断的儿科肾移植患者中应用霉酚酸酯(MMF)后的群体药代动力学-药效学模型,并确定解释变异的因素。对 89 例新诊断的接受 MMF 治疗的儿科肾移植患者进行了药代动力学采样,并在术后第 60 天内进行了研究。所有患者均进行 UGT1A8-A9、UGT2B7 和 ABCC2 基因分型。采用 NONMEM 进行群体药代动力学分析,并采用 Bootstrap 视觉预测检查进行验证。药代动力学数据最好用 2 室模型和 Erlang 分布来描述吸收阶段。协变量分析确定体重是影响中央分布容积的个体因素,同时免疫抑制药物确定体重和 UGT2B7 802C>T 基因型是影响 MMF 表观口服清除率(CL/F)的个体因素。环孢素-MMF 治疗患者的 CL/F 比他克莫司-MMF 治疗患者高 33%。与 UGT2B7 802C/T 和 802T/T 基因型患者相比,UGT2B7 802C/C 基因型患者的 CL/F 显著降低,且该效应与同时使用免疫抑制剂或体重无关。霉酚酸的群体药代动力学-药效学模型得到了验证。体重、同时使用的药物和 UGT2B7 基因型对儿科肾移植患者 MMF 处置的个体间变异性有显著影响。

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