Sources of interindividual variability in IVIVE of clearance: an investigation into the prediction of benzodiazepine clearance using a mechanistic population-based pharmacokinetic model

Helen E Cubitt; Karen R Yeo; Eleanor M Howgate; Amin Rostami-Hodjegan; Zoe E Barter

doi:10.3109/00498254.2011.560294

Sources of interindividual variability in IVIVE of clearance: an investigation into the prediction of benzodiazepine clearance using a mechanistic population-based pharmacokinetic model

Xenobiotica. 2011 Aug;41(8):623-38. doi: 10.3109/00498254.2011.560294. Epub 2011 Mar 24.

Authors

Helen E Cubitt¹, Karen R Yeo, Eleanor M Howgate, Amin Rostami-Hodjegan, Zoe E Barter

Affiliation

¹ Simcyp Limited, Blades Enterprise Centre, Sheffield, UK. h.cubitt@simcyp.com

PMID: 21434772
DOI: 10.3109/00498254.2011.560294

Abstract

Prediction of metabolic clearance in extreme individuals rather than the 'average human' is becoming an attractive tool within the pharmaceutical industry. The current study involved prediction of variability in metabolic clearance for alprazolam, triazolam and midazolam with emphasis on the following factors: first, evaluation of clearance prediction accuracy using intrinsic clearance (CL(int)) data from in vitro metabolic data and back-calculation from in vivo clearance data. Second, the sensitivity of predicted in vivo variability to changes in variability for physiological parameters (e.g. liver weight, haematocrit, CYP3A abundance). Finally, reported estimates of variability in hepatic CYP3A4 abundance (coefficient of variation (CV) 95%) were refined by separating experimental from interindividual variability using a repeat measurement protocol in 52 human liver samples. Using in vitro metabolic data, predicted clearances were within 2-fold of observed for triazolam and midazolam. Clearance of alprazolam was overpredicted by 2.0- to 3.7-fold. Use of in vivo CL(int) values improved prediction of intravenous clearance to within 2-fold of observed for all drugs. Initially, the variability in clearance was overestimated for all drugs (by 1.8- to 3.6-fold). Use of a reduced hepatic CYP3A4 CV of 41%, representative of interindividual variability alone improved predictions of variability in clearance for all drugs to within 2-fold of observed.

MeSH terms

Alprazolam / pharmacokinetics
Benzodiazepines / pharmacokinetics*
Cytochrome P-450 CYP3A / genetics
Cytochrome P-450 CYP3A / metabolism
Humans
Kinetics
Liver / metabolism
Metabolic Clearance Rate
Midazolam / pharmacokinetics
Triazolam / pharmacokinetics

Substances

Benzodiazepines
Triazolam
Cytochrome P-450 CYP3A
CYP3A4 protein, human
Midazolam
Alprazolam