García Sánchez M J, Manzanares C, Santos-Buelga D, Blázquez A, Manzanares J, Urruzuno P, Medina E
Pharmacy Department, University of Salamanca, Spain.
Clin Pharmacokinet. 2001 Jan;40(1):63-71. doi: 10.2165/00003088-200140010-00005.
To analyse the influence of covariates on the apparent clearance (CL) of tacrolimus in paediatric liver transplant recipients being converted from cyclosporin to tacrolimus.
Retrospective modelling study.
18 children, 13 girls and 5 boys, aged 4 months to 16 years (median 9.1 years) who required conversion to tacrolimus because of acute or chronic rejection or cyclosporin toxicity.
287 whole-blood tacrolimus concentrations from therapeutic drug monitoring were used to build a nonlinear mixed-effects population model (NONMEM program) for the apparent clearance of tacrolimus. Variables considered were age, total bodyweight (TBW), body surface area (BSA), time after initiation of treatment (T), gender, haematocrit (Hct), albumin (Alb), aspartate aminotransferase (AST), alanine aminotransferase (ALT), gamma-glutamyl transpeptidase (gammaGT), alkaline phosphatase (ALP), bilirubin (BIL), creatinine clearance (CL(CR)) and dosage of concomitant corticosteroids (EST).
TBW, T, BIL and ALT were the covariates that displayed a significant influence on CL according to the final regression model: CL (L/h) = 10.4(TBW/70)3/4 x e(-0.00032 T) x e(-0.057 BIL) x (1 - 0.079 ALT). With this model, the estimates of the coefficients of variation were 24.3% and 29.5% for interpatient variability in CL and residual variability, respectively.
The proposed model for tacrolimus CL can be applied for a priori dosage calculations, although the results should be used with caution because of the unexplained variability in the CL. We therefore recommended close monitoring of tacrolimus whole blood concentrations, especially within the first months of treatment. The best use of the model would be its application in dosage adjustment based on therapeutic drug monitoring and the Bayesian approach.
分析协变量对从环孢素转换为他克莫司的小儿肝移植受者他克莫司表观清除率(CL)的影响。
回顾性建模研究。
18名儿童,13名女孩和5名男孩,年龄4个月至16岁(中位数9.1岁),因急性或慢性排斥反应或环孢素毒性而需要转换为他克莫司。
使用来自治疗药物监测的287个全血他克莫司浓度建立他克莫司表观清除率的非线性混合效应群体模型(NONMEM程序)。考虑的变量包括年龄、总体重(TBW)、体表面积(BSA)、治疗开始后的时间(T)、性别、血细胞比容(Hct)、白蛋白(Alb)、天冬氨酸转氨酶(AST)、丙氨酸转氨酶(ALT)、γ-谷氨酰转肽酶(γGT)、碱性磷酸酶(ALP)、胆红素(BIL)、肌酐清除率(CL(CR))和同时使用的皮质类固醇剂量(EST)。
根据最终回归模型,TBW、T、BIL和ALT是对CL有显著影响的协变量:CL(L/h)= 10.4(TBW/70)3/4×e(-0.00032T)×e(-0.057BIL)×(1 - 0.079ALT)。使用该模型,CL的患者间变异性和残差变异性的变异系数估计值分别为24.3%和29.5%。
所提出的他克莫司CL模型可用于先验剂量计算,尽管由于CL中存在无法解释的变异性,结果应谨慎使用。因此,我们建议密切监测他克莫司全血浓度,尤其是在治疗的头几个月内。该模型的最佳用途是基于治疗药物监测和贝叶斯方法将其应用于剂量调整。
