Developmental pharmacogenetics of CYP2C19 in neonates and young infants: omeprazole as a probe drug.

Aims: Although substantial progress has been made in understanding of ontogeny of drug metabolism, there is still a gap of knowledge in developmental pharmacogenetics in neonates. We hypothesized that both age and pharmacogenetics might explain the developmental pattern of CYP2C19. We conducted a population pharmacokinetic–pharmacogenetic study to quantify the developmental pharmacogenetics of CYP2C19 in neonates and young infants using omeprazole as a probe drug. Methods: Pharmacokinetic samples were collected from 51 Caucasian neonates and young infants, who were receiving omeprazole treatment. Population pharmacokinetic–pharmacogenetic analysis of omeprazole and its metabolites was performed using NONMEM. Results: Data fitted a one‐compartment parent and metabolite model with first‐order absorption and elimination. CYP2C19 and CYP3A4 are predominantly involved in the metabolism of omeprazole despite their relatively low activities compared to adults. The clearance of omeprazole converted to 5‐hydroxy‐omeprazole (CL_OMZ‐M1) increases with postnatal age. In CYP2C19 poor and intermediate metabolizers, model‐predicted CL_OMZ‐M1 are 12.5% (5–95% percentile: 3–14.9%) and 44.9% (5–95% percentile: 29.9–72.6%) of the value in extensive/ultrarapid metabolizer, respectively. Model‐predicted absorption rate constant of omeprazole is 6.93 (5–95% percentile: 3.01–14.61) times higher in ABCB1 homozygous mutant patients, 1.86 (5–95% percentile: 0.86–3.47) times higher in ABCB1 heterozygous patients than that in ABCB1 homozygous wild‐type patients. Conclusions: Developmental pharmacogenetics of CYP2C19 was quantitatively described in neonates and young infants using omeprazole as a probe drug. Our findings emphasize the importance of semiphysiological developmental pharmacokinetic modelling approach when evaluating developmental pharmacogenetics of drugs with multiple routes of biotransformation. [ABSTRACT FROM AUTHOR]