| Predicting Plasma Concentrations of Bisphenol A in Children Younger Than 2 Years of Age after Typical Feeding Schedules, using a Physiologically Based Toxicokinetic Model Andrea N. Edginton1 and Len Ritter2 1School of Pharmacy, University of Waterloo, Waterloo, Ontario, Canada; 2Department of Environmental Biology, University of Guelph, Guelph, Ontario, Canada Abstract
Background: Concerns have recently been raised regarding the safety of potential human exposure to bisphenol A (BPA) , an industrial chemical found in some polycarbonate plastics and epoxy resins. Of particular interest is the exposure of young children to BPA via food stored in BPA-containing packaging. Objectives: In this study we assessed the age dependence of the toxicokinetics of BPA and its glucuronidated metabolite, BPA-Glu, using a coupled BPA–BPA-Glu physiologically based toxicokinetic (PBTK) model. Methods: Using information gathered from toxicokinetic studies in adults, we built a PBTK model. We then scaled the model to children < 2 years of age based on the age dependence of physiologic parameters relevant for absorption, distribution, metabolism, and excretion. Results: We estimated the average steady-state BPA plasma concentration in newborns to be 11 times greater than that in adults when given the same weight-normalized dose. Because of the rapid development of the glucuronidation process, this ratio dropped to 2 by 3 months of age. Simulation of typical feeding exposures, as estimated by regulatory authorities, showed a 5-fold greater steady-state BPA plasma concentration in 3- and 6-month-olds compared with adults, reflecting both a reduced capacity for BPA metabolism and a greater weight-normalized BPA exposure. Because of uncertainty in defining the hepatic BPA intrinsic clearance in adults, these values represent preliminary estimates. Conclusions: Simulations of the differential BPA dosimetry between adults and young children point to the need for more sensitive analytical methods for BPA to define, with greater certainty, the adult hepatic BPA intrinsic clearance, as well as a need for external exposure data in young children. Key words: bisphenol A, ontogeny, http://dx.doi.org/ [Online+14+November+2008]" rel="tag">physiologically based toxicokinetics. Environ Health Perspect 117:645–652 (2009) . [Online 14 November 2008]
Address correspondence to A.N. Edginton, School of Pharmacy, University of Waterloo, 200 University Ave. W, Waterloo, ON, Canada N2L 3G1. Telephone: (519) 888-4567 ext. 21315. Fax: (519) 888-7910. E-mail: aedginto@uwaterloo.ca Supplemental Material is available online at http://www.ehponline.org/members/2008/0800073/suppl.pdf We thank M. Sevestre for assistance with the sensitivity analysis. The authors declare they have no competing financial interests. Received 6 August 2008 ; accepted 14 November 2008.
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