*School of Pharmacy, University of Queensland, Brisbane, Australia; †Department of Pharmacology, Aarhus University, Aarhus, Denmark; and ‡Department of Nephrology, University of Queensland at the Princess Alexandra Hospital, Brisbane, Australia.
Ther Drug Monit. 2014 Feb;36(1):62-70. doi: 10.1097/FTD.0b013e31829f1ab8.
The aims of this study were to develop a population pharmacokinetic model of tacrolimus in adult kidney transplant recipients, to use this model to compare cytochrome P450 3A5 (CYP3A5) genotype-based initial dosing of tacrolimus with standard per-kilogram-based dosing, and to predict the best starting dose of tacrolimus based on patient genotype to achieve a trough concentration between 6 and 10 µg/L by day 5 posttransplantation.
Population analysis was performed using the software program NONMEM. Tacrolimus dosing regimens were compared by predicting tacrolimus trough concentrations in a simulated data set by running NONMEM with population parameters fixed at the final model estimates. Data from 173 patients with 1554 tacrolimus concentration-time measurements were modeled.
Tacrolimus disposition was well described by a 2-compartment model with first-order elimination and first-order absorption after a lag time. Patient CYP3A5 genotype (rs776746), weight, hematocrit, and postoperative day were identified as significant covariates effecting tacrolimus apparent oral clearance (CL/F), with higher CL/F in CYP3A51 allele carriers, heavier patients, patients with low hematocrit, and in the immediate posttransplantation period. Typical population estimates for tacrolimus CL/F in CYP3A51 allele carriers and noncarriers were 40.8 and 25.5 L/h, respectively.
In patients carrying the CYP3A51 allele, a per-kilogram dose of 0.075 mg/kg twice daily seemed too much low with approximately 65% of simulated subjects predicted to achieve a trough below 6 µg/L at day 5 posttransplantation. To reduce the risk of under immunosuppression in the immediate posttransplantation period, carriers of a CYP3A51 allele are likely to benefit from a tacrolimus starting dose of either 10 mg or 0.115 mg/kg twice daily.
本研究旨在建立成人肾移植受者他克莫司的群体药代动力学模型,利用该模型比较基于细胞色素 P450 3A5(CYP3A5)基因型的他克莫司初始给药剂量与标准按体重给药剂量,并预测基于患者基因型的他克莫司最佳起始剂量,以在移植后第 5 天达到 6 至 10μg/L 的谷浓度。
使用 NONMEM 软件程序进行群体分析。通过使用 NONMEM 运行模拟数据集,将群体参数固定在最终模型估计值,以预测模拟数据集中他克莫司的谷浓度,从而比较他克莫司的给药方案。对 173 例患者的 1554 次他克莫司浓度-时间测量值进行了建模。
他克莫司的处置可以通过一个两室模型很好地描述,该模型具有滞后时间后的一级消除和一级吸收。患者 CYP3A5 基因型(rs776746)、体重、红细胞压积和术后天数被确定为影响他克莫司表观口服清除率(CL/F)的显著协变量,CYP3A51 等位基因携带者、体重较重的患者、红细胞压积较低的患者和移植后即刻的 CL/F 较高。CYP3A51 等位基因携带者和非携带者的他克莫司 CL/F 的典型群体估计值分别为 40.8 和 25.5 L/h。
在携带 CYP3A51 等位基因的患者中,每日两次 0.075mg/kg 的剂量似乎过低,大约 65%的模拟患者在移植后第 5 天预计谷浓度低于 6μg/L。为了降低移植后即刻免疫抑制不足的风险,CYP3A51 等位基因携带者可能受益于他克莫司起始剂量为 10mg 或每日两次 0.115mg/kg。
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