Combining Therapeutic Drug Monitoring and Pharmacokinetic Modelling Deconvolutes Physiological and Environmental Sources of Variability in Clozapine Exposure

Kenneth H. Wills; Stephen J. Behan; Michael J. Nance; Jessica L. Dawson; Thomas M. Polasek; Ashley M. Hopkins; Madelé van Dyk; Andrew Rowland

doi:10.3390/pharmaceutics14010047

Pharmaceutics (Dec 2021)

Combining Therapeutic Drug Monitoring and Pharmacokinetic Modelling Deconvolutes Physiological and Environmental Sources of Variability in Clozapine Exposure

Kenneth H. Wills,
Stephen J. Behan,
Michael J. Nance,
Jessica L. Dawson,
Thomas M. Polasek,
Ashley M. Hopkins,
Madelé van Dyk,
Andrew Rowland

Affiliations

Kenneth H. Wills: College of Medicine and Public Health, Flinders University, Adelaide, SA 5042, Australia
Stephen J. Behan: College of Medicine and Public Health, Flinders University, Adelaide, SA 5042, Australia
Michael J. Nance: Flinders Medical Centre, Adelaide, SA 5042, Australia
Jessica L. Dawson: SA Pharmacy, Southern Adelaide Local Health Network, Adelaide, SA 5042, Australia
Thomas M. Polasek: Centre for Medicine Use and Safety, Monash University, Melbourne, VIC 3000, Australia
Ashley M. Hopkins: College of Medicine and Public Health, Flinders University, Adelaide, SA 5042, Australia
Madelé van Dyk: College of Medicine and Public Health, Flinders University, Adelaide, SA 5042, Australia
Andrew Rowland: College of Medicine and Public Health, Flinders University, Adelaide, SA 5042, Australia

DOI: https://doi.org/10.3390/pharmaceutics14010047
Journal volume & issue: Vol. 14, no. 1
p. 47

Abstract

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Background: Clozapine is a key antipsychotic drug for treatment-resistant schizophrenia but exhibits highly variable pharmacokinetics and a propensity for serious adverse effects. Currently, these challenges are addressed using therapeutic drug monitoring (TDM). This study primarily sought to (i) verify the importance of covariates identified in a prior clozapine population pharmacokinetic (popPK) model in the absence of environmental covariates using physiologically based pharmacokinetic (PBPK) modelling, and then to (ii) evaluate the performance of the popPK model as an adjunct or alternative to TDM-guided dosing in an active TDM population. Methods: A popPK model incorporating age, metabolic activity, sex, smoking status and weight was applied to predict clozapine trough concentrations (Cmin) in a PBPK-simulated population and an active TDM population comprising 142 patients dosed to steady state at Flinders Medical Centre in Adelaide, South Australia. Post hoc analyses were performed to deconvolute the impact of physiological and environmental covariates in the TDM population. Results: Analysis of PBPK simulations confirmed age, cytochrome P450 1A2 activity, sex and weight as physiological covariates associated with variability in clozapine Cmin (R2 = 0.7698; p = 0.0002). Prediction of clozapine Cmin using a popPK model based on these covariates accounted for min in the TDM population. Conclusions: Variability in clozapine exposure was primarily driven by environmental covariates in an active TDM population. Pharmacokinetic modelling can be used as an adjunct to TDM to deconvolute sources of variability in clozapine exposure.

Published in Pharmaceutics

ISSN: 1999-4923 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Medicine: Pharmacy and materia medica
Website: http://www.mdpi.com/journal/pharmaceutics/

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