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      Population pharmacokinetic analysis of tacrolimus in Mexican paediatric renal transplant patients: role of CYP3A5 genotype and formulation

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          Abstract

          Aims

          The aims of this study were (i) to develop a population pharmacokinetic (PK) model of tacrolimus in a Mexican renal transplant paediatric population ( n = 53) and (ii) to test the influence of different covariates on its PK properties to facilitate dose individualization.

          Methods

          Population PK and variability parameters were estimated from whole blood drug concentration profiles obtained at steady-state using the non-linear mixed effect modelling software NONMEM® Version 7.2.

          Results

          Tacrolimus PK profiles exhibited high inter-patient variability (IPV). A two compartment model with first order input and elimination described the tacrolimus PK profiles in the studied population. The relationship between CYP3A5 genotype and tacrolimus CL/ F was included in the final model. CL/ F in CYP3A5*1/*1 and *1/*3 carriers was approximately 2- and 1.5-fold higher than in CYP3A5*3/*3 carriers (non-expressers), respectively, and explained almost the entire IPV in CL/ F. Other covariates retained in the final model were the tacrolimus dose and formulation type. Limustin® showed markedly lower concentrations than the rest of the formulations.

          Conclusions

          Population PK modelling of tacrolimus in paediatric renal transplant recipients identified the tacrolimus formulation type as a significant covariate affecting the blood concentrations and confirmed the previously reported significant effect of CYP3A5 genotype on CL/ F. It allowed the design of a proposed dosage based on the final model that is expected to help to improve tacrolimus dosing.

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          Author and article information

          Journal
          Br J Clin Pharmacol
          Br J Clin Pharmacol
          bcp
          British Journal of Clinical Pharmacology
          John Wiley & Sons, Ltd (Chichester, UK )
          0306-5251
          1365-2125
          October 2015
          22 June 2015
          : 80
          : 4
          : 630-641
          Affiliations
          [1 ] Department of Pharmacology, CINVESTAV-IPN Mexico City, Mexico
          [2 ] Nephrology Research Laboratory, Federico Gómez Children’s Hospital of Mexico Mexico City, Mexico
          [3 ] Department of Pharmacobiology, University of Guadalajara Guadalajara, Mexico
          [4 ] Department of Pharmacology, Faculty of Medicine, National Autonomous University of Mexico Mexico City, Mexico
          [5 ] Department of Pharmacy and Pharmaceutical Technology, School of Pharmacy, University of Navarra Pamplona, Navarra, Spain
          [6 ] IdiSNA Navarra Institute for Health Research Pamplona, Spain
          Author notes
          Correspondence, Dr Gilberto Castañeda-Hernández, PhD, 2508 Instituto Politécnico Nacional avenue, Mexico City, 07360, Mexico., Tel.: +52 (55) 5747 3305, Fax: +52 (55) 57473394, E-mail: gcastane@ 123456cinvestav.mx , Prof Dr Iñaki F. Trocóniz, PhD, 1 Irunlarrea street, Navarra, Pamplona, 31080, Spain., Tel.: +34 948 425600 ext 806507, Fax: +34 948 425740, E-mail: itroconiz@ 123456unav.es
          [*]

          Submitting author: Carlos Orlando Jacobo-Cabral, PhD, 2508 Instituto Politécnico Nacional Avenue, Mexico City, Mexico, 07360, E-mail: orlandofly@ 123456hotmail.com

          Article
          PMC4594699 PMC4594699 4594699
          10.1111/bcp.12649
          4594699
          25846845
          f00de167-d419-444b-a047-1009d694854b
          © 2015 The British Pharmacological Society
          History
          : 20 November 2014
          : 27 March 2015
          Categories
          Pharmacokinetics

          renal transplant,tacrolimus,population pharmacokinetics,paediatric,formulation,CYP3A5

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