Physiologically based pharmacokinetic model for 6-mercpatopurine: exploring the role of genetic polymorphism in TPMT enzyme activity

Kayode Ogungbenro; Leon Aarons; CRESim & Epi-CRESim Project Groups

doi:10.1111/bcp.12588

Physiologically based pharmacokinetic model for 6-mercpatopurine: exploring the role of genetic polymorphism in TPMT enzyme activity

Br J Clin Pharmacol. 2015 Jul;80(1):86-100. doi: 10.1111/bcp.12588. Epub 2015 Jun 1.

Authors

Kayode Ogungbenro¹, Leon Aarons¹; CRESim & Epi-CRESim Project Groups

Collaborators

CRESim & Epi-CRESim Project Groups:
Leon Aarons, Agathe Bajard, Clément Ballot, Yves Bertrand, Frank Bretz, Daan Caudri, Charlotte Castellan, Sylvie Chabaud, Catherine Cornu, Frank Dufour, Nathalie Eymard, Roland Fisch, Renzo Guerrini, Vincent Jullien, Behrouz Kassaï, Patrice Nony, Kayode Ogungbenro, David Pérol, Gérard Pons, Harm Tiddens, Anna Rosati, Corinne Alberti, Catherine Chiron, Catherine Cornu, Polina Kurbatova, Rima Nabbout

Affiliation

¹ Centre for Applied Pharmacokinetics Research, Manchester Pharmacy School, The University of Manchester, Oxford Road, Manchester, M13 9PT, United Kingdom.

Abstract

Aims: To extend the physiologically based pharmacokinetic (PBPK) model developed for 6-mercaptopurine to account for intracellular metabolism and to explore the role of genetic polymorphism in the TPMT enzyme on the pharmacokinetics of 6-mercaptopurine.

Methods: The developed PBPK model was extended for 6-mercaptopurine to account for intracellular metabolism and genetic polymorphism in TPMT activity. System and drug specific parameters were obtained from the literature or estimated using plasma or intracellular red blood cell concentrations of 6-mercaptopurine and its metabolites. Age-dependent changes in parameters were implemented for scaling, and variability was also introduced for simulation. The model was validated using published data.

Results: The model was extended successfully. Parameter estimation and model predictions were satisfactory. Prediction of intracellular red blood cell concentrations of 6-thioguanine nucleotide for different TPMT phenotypes (in a clinical study that compared conventional and individualized dosing) showed results that were consistent with observed values and reported incidence of haematopoietic toxicity. Following conventional dosing, the predicted mean concentrations for homozygous and heterozygous variants, respectively, were about 10 times and two times the levels for wild-type. However, following individualized dosing, the mean concentration was around the same level for the three phenotypes despite different doses.

Conclusions: The developed PBPK model has been extended for 6-mercaptopurine and can be used to predict plasma 6-mercaptopurine and tissue concentration of 6-mercaptopurine, 6-thioguanine nucleotide and 6-methylmercaptopurine ribonucleotide in adults and children. Predictions of reported data from clinical studies showed satisfactory results. The model may help to improve 6-mercaptopurine dosing, achieve better clinical outcome and reduce toxicity.

Keywords: 6-mercaptopurine; PBPK model; TPMT; acute lymphoblastic leukaemia; modelling; pharmacokinetics.

Publication types

Research Support, Non-U.S. Gov't
Validation Study

MeSH terms

Adult
Age Factors
Child
Computer Simulation*
Humans
Mercaptopurine / blood
Mercaptopurine / pharmacokinetics*
Methyltransferases / genetics*
Models, Biological*
Nucleic Acid Synthesis Inhibitors / blood
Nucleic Acid Synthesis Inhibitors / pharmacokinetics
Phenotype
Polymorphism, Genetic*
Tissue Distribution
Young Adult

Substances

Nucleic Acid Synthesis Inhibitors
Mercaptopurine
Methyltransferases
thiopurine methyltransferase

Grants and funding

MC_G1100157/MRC_/Medical Research Council/United Kingdom