Evaluation of the Potential Impact of Age- and Gender-Specific Pharmacokinetic Differences on Tissue Dosimetry

doi:10.1093/toxsci/kfh109

ToxSci Advance Access originally published online on March 31, 2004

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Toxicological Sciences 79, 381-393 (2004)
Toxicological Sciences vol. 79 no. 2 © Society of Toxicology; all rights reserved.

Evaluation of the Potential Impact of Age- and Gender-Specific Pharmacokinetic Differences on Tissue Dosimetry

Harvey J. Clewell^*^,1, P. Robinan Gentry^*, Tammie R. Covington^*, Ramesh Sarangapani^,2 and Justin G. Teeguarden^*

^* ENVIRON Health Sciences Institute, Ruston, Louisiana 71270; and K. S. Crump Group, Inc., ICF Consulting, Research Triangle Park,North Carolina 27709

Received June 23, 2003; accepted February 12, 2004

The physiological and biochemical processes that determine thetissue concentration time courses (pharmacokinetics) of xenobioticsvary, in some cases significantly, with age and gender. Whileit is known that age- and gender-specific differences have thepotential to affect tissue concentrations and, hence, individualrisk, the relative importance of the contributing processesand the quantitative impact of these differences for variouslife stages are not well characterized. The objective of thisstudy was to identify age- and gender-specific differences inphysiological and biochemical processes that affect tissue dosimetryand integrate them into a predictive physiologically based pharmacokinetic(PBPK) life-stage model. The life-stage model was exercisedfor several environmental chemicals with a variety of physicochemical,biochemical, and mode-of-action properties. In general, predictionsof average pharmacokinetic dose metrics for a chemical acrosslife stages were within a factor of two, although larger transientvariations were predicted, particularly during the neonatalperiod. The most important age-dependent pharmacokinetic factorappears to be the potential for decreased clearance of a toxicchemical in the perinatal period due to the immaturity of manymetabolic enzyme systems, although this same factor may alsoreduce the production of a reactive metabolite. Given the potentialfor age-dependent pharmacodynamic factors during early life,there may be chemicals and health outcomes for which decreasedclearance over a relatively brief period could have a substantialimpact on risk.

Key Words: pharmacokinetics; PBPK; children; age; gender; dosimetry.

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