The Relative Bioavailability and Metabolism of Bisphenol A in Rats Is Dependent upon the Route of Administration

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Toxicological Sciences 54, 3-18 (2000)
Copyright © 2000 by the Society of Toxicology

The Relative Bioavailability and Metabolism of Bisphenol A in Rats Is Dependent upon the Route of Administration

Lynn H. Pottenger^*, Jeanne Y. Domoradzki, Dan A. Markham, Steven C. Hansen, Stuart Z. Cagen and John M. Waechter, Jr.^,1

^* Toxicology and Environmental Research and Consulting, Dow Europe, Horgen, Switzerland; Toxicology and Environmental Research and Consulting, The Dow Chemical Company, Midland, Michigan 48674; and Health, Safety and Environment, Shell Chemical Company, Houston, Texas 77210

Bisphenol A (BPA) is used to produce polymers for food contactapplications, thus there is potential for oral exposure of humansto trace amounts via the diet. BPA was weakly estrogenic inscreening assays measuring uterine weight/response, althoughmuch higher oral doses of BPA were required to elicit a uterotropicresponse as compared to other routes of administration. Theobjective of this study was to determine if a route dependencyexists in the pharmacokinetics and metabolism of ¹⁴C-labeledBPA following single oral (po), intraperitoneal (ip), or subcutaneous(sc) doses of either 10 or 100 mg/kg to Fischer 344 rats. Resultsindicated a marked route dependency in the pharmacokineticsof BPA. The relative bioavailability of BPA and plasma radioactivitywas markedly lower following oral administration as comparedto sc or ip administration. The major fraction of plasma radioactivityfollowing oral dosing was the monoglucuronide conjugate of BPA(68–100% of plasma radioactivity). BPA was the major componentin plasma at Cmax following sc or ip administration exceededonly by BPA-monoglucuronide in females dosed ip. Up to fouradditional unidentified metabolites were present only in theplasma of animals dosed ip or sc. One of these, found only followingip administration, was tentatively identified as the monosulfateconjugate of BPA. The monoglucuronide conjugate was the majorurinary metabolite; unchanged BPA was the principal componentexcreted in feces. These results demonstrated a route dependencyof BPA bioavailability in rats, with oral administration resultingin the lowest bioavailability, and offer an explanation forthe apparent route differences in estrogenic potency observedfor BPA.

Key Words: bisphenol A; bioavailability; absorption; metabolism; rats; route dependency.

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				H. Inoue, G. Yuki, H. Yokota, and S. Kato Bisphenol A Glucuronidation and Absorption in Rat Intestine Drug Metab. Dispos., January 1, 2003; 31(1): 140 - 144. [Abstract] [Full Text] [PDF]

				J. J. Pritchett, R. K. Kuester, and I. G. Sipes Metabolism of Bisphenol A in Primary Cultured Hepatocytes from Mice, Rats, and Humans Drug Metab. Dispos., November 1, 2002; 30(11): 1180 - 1185. [Abstract] [Full Text] [PDF]

				Y. Ikezuki, O. Tsutsumi, Y. Takai, Y. Kamei, and Y. Taketani Determination of bisphenol A concentrations in human biological fluids reveals significant early prenatal exposure Hum. Reprod., November 1, 2002; 17(11): 2839 - 2841. [Abstract] [Full Text] [PDF]

				H. Kurebayashi, R. Harada, R. K. Stewart, H. Numata, and Y. Ohno Disposition of a Low Dose of Bisphenol A in Male and Female Cynomolgus Monkeys Toxicol. Sci., July 1, 2002; 68(1): 32 - 42. [Abstract] [Full Text] [PDF]

				R. W. Tyl, C. B. Myers, M. C. Marr, B. F. Thomas, A. R. Keimowitz, D. R. Brine, M. M. Veselica, P. A. Fail, T. Y. Chang, J. C. Seely, et al. Three-Generation Reproductive Toxicity Study of Dietary Bisphenol A in CD Sprague-Dawley Rats Toxicol. Sci., July 1, 2002; 68(1): 121 - 146. [Abstract] [Full Text] [PDF]

				C. M. Markey, E. H. Luque, M. Munoz de Toro, C. Sonnenschein, and A. M. Soto In Utero Exposure to Bisphenol A Alters the Development and Tissue Organization of the Mouse Mammary Gland Biol Reprod, October 1, 2001; 65(4): 1215 - 1223. [Abstract] [Full Text] [PDF]

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				S.'i. Yoshihara, M. Makishima, N. Suzuki, and S. Ohta Metabolic Activation of Bisphenol A by Rat Liver S9 Fraction Toxicol. Sci., August 1, 2001; 62(2): 221 - 227. [Abstract] [Full Text] [PDF]

				R. Elsby, J. L. Maggs, J. Ashby, and B. K. Park Comparison of the Modulatory Effects of Human and Rat Liver Microsomal Metabolism on the Estrogenicity of Bisphenol A: Implications for Extrapolation to Humans J. Pharmacol. Exp. Ther., April 1, 2001; 297(1): 103 - 113. [Abstract] [Full Text]

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