Normal Sexual Development of Two Strains of Rat Exposed in Utero to Low Doses of Bisphenol A

doi:10.1093/toxsci/68.2.339

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Toxicological Sciences 68, 339-348 (2002)
Copyright © 2002 by the Society of Toxicology

ENDOCRINE TOXICOLOGY

Normal Sexual Development of Two Strains of Rat Exposed in Utero to Low Doses of Bisphenol A

H. Tinwell^*, J. Haseman, P. A. Lefevre^*, N. Wallis^* and J. Ashby^*^,1

^* Syngenta Central Toxicology Laboratory, Alderley Park, Cheshire, SK10 4TJ, United Kingdom; and National Institute of Environmental Health Sciences, Alexander Drive, Research Triangle Park, North Carolina 27709

Pregnant Sprague-Dawley (SD) and Alderley Park (Wistar derived)rats were exposed by gavage during gestation days 6–21to 20 µg/kg, 100 µg/kg, or 50 mg/kg body weightof BPA with ethinylestradiol (EE; 200 µg/kg) acting asa positive control agent. The sexual development of the derivedpups was monitored until termination at postnatal day 90–98.The endpoints evaluated were litter size and weight, anogenitaldistance at birth, days of vaginal opening, first estrus andprepuce separation, weights of the liver, seminal vesicles,epididimydes, testes, ventral prostate, uterus, vagina, cervixand ovaries, and daily sperm production. Males were terminatedat postnatal day 90 and females at postnatal day 98. The onlystatistically significant effects observed for any dose of BPAwere a decrease in daily sperm production and an increase inthe age of vaginal opening for the Alderley Park animals atthe highest dose evaluated (50 mg/kg). The dose of EE evaluatedproved to be maternally toxic in our laboratory, but providedgross evidence of endocrine disruption in the treated dams.These results diverge from those of Chahoud and his colleagueswho indicated disturbances to the sexual development of bothmale and female SD rat pups administered the same 3 doses ofBPA. This failure to confirm low dose endocrine effects forBPA is discussed within the context of similar divergent conclusionsderived from other assessments of the endocrine toxicity ofthis agent to rats.

Key Words: bisphenol A; Sprague-Dawley rats; Alderley Park rats; sexual development; in utero exposure.

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