A Whole-Body Physiologically Based Pharmacokinetic Model for Colistin and Colistin Methanesulfonate in Rat

Salim Bouchene; Sandrine Marchand; William Couet; Lena E Friberg; Patrice Gobin; Isabelle Lamarche; Nicolas Grégoire; Sven Björkman; Mats O Karlsson

doi:10.1111/bcpt.13026

A Whole-Body Physiologically Based Pharmacokinetic Model for Colistin and Colistin Methanesulfonate in Rat

Basic Clin Pharmacol Toxicol. 2018 Oct;123(4):407-422. doi: 10.1111/bcpt.13026. Epub 2018 Jun 8.

Authors

Salim Bouchene¹, Sandrine Marchand^{2

3}, William Couet^{2

3}, Lena E Friberg¹, Patrice Gobin², Isabelle Lamarche², Nicolas Grégoire^{2

3}, Sven Björkman¹, Mats O Karlsson¹

Affiliations

¹ Department of Pharmaceutical Biosciences, Uppsala University, Uppsala, Sweden.
² INSERM U-1070, Pôle Biologie Santé, Poitiers, France.
³ Laboratoire de Toxicologie et Pharmacocinétique, CHU de Poitiers, Poitiers, France.

PMID: 29665289
DOI: 10.1111/bcpt.13026

Abstract

Colistin is a polymyxin antibiotic used to treat patients infected with multidrug-resistant Gram-negative bacteria (MDR-GNB). The objective of this work was to develop a whole-body physiologically based pharmacokinetic (WB-PBPK) model to predict tissue distribution of colistin in rat. The distribution of a drug in a tissue is commonly characterized by its tissue-to-plasma partition coefficient, K_p . Colistin and its prodrug, colistin methanesulfonate (CMS) K_p priors, were measured experimentally from rat tissue homogenates or predicted in silico. The PK parameters of both compounds were estimated fitting in vivo their plasma concentration-time profiles from six rats receiving an i.v. bolus of CMS. The variability in the data was quantified by applying a nonlinear mixed effect (NLME) modelling approach. A WB-PBPK model was developed assuming a well-stirred and perfusion-limited distribution in tissue compartments. Prior information on tissue distribution of colistin and CMS was investigated following three scenarios: K_p was estimated using in silico K_p priors (I) or K_p was estimated using experimental K_p priors (II) or K_p was fixed to the experimental values (III). The WB-PBPK model best described colistin and CMS plasma concentration-time profiles in scenario II. Colistin-predicted concentrations in kidneys in scenario II were higher than in other tissues, which was consistent with its large experimental K_p prior. This might be explained by a high affinity of colistin for renal parenchyma and active reabsorption into the proximal tubular cells. In contrast, renal accumulation of colistin was not predicted in scenario I. Colistin and CMS clearance estimates were in agreement with published values. The developed model suggests using experimental priors over in silico K_p priors for kidneys to provide a better prediction of colistin renal distribution. Such models might serve in drug development for interspecies scaling and investigate the impact of disease state on colistin disposition.

Publication types

Comparative Study

MeSH terms

Activation, Metabolic
Animals
Anti-Bacterial Agents / administration & dosage
Anti-Bacterial Agents / pharmacokinetics*
Colistin / administration & dosage
Colistin / analogs & derivatives*
Colistin / pharmacokinetics
Computer Simulation
Injections, Intravenous
Male
Models, Biological*
Prodrugs / administration & dosage
Prodrugs / pharmacokinetics*
Rats, Sprague-Dawley
Tissue Distribution

Substances

Anti-Bacterial Agents
Prodrugs
colistinmethanesulfonic acid
Colistin

Abstract

Publication types

MeSH terms

Substances

Grants and funding