The Effects of Atrazine on Female Wistar Rats: An Evaluation of the Protocol for Assessing Pubertal Development and Thyroid Function

doi:10.1093/toxsci/58.2.366

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Toxicological Sciences 58, 366-376 (2000)
Copyright © 2000 by the Society of Toxicology

Reproductive and Developmental Toxicology

The Effects of Atrazine on Female Wistar Rats: An Evaluation of the Protocol for Assessing Pubertal Development and Thyroid Function

Susan C. Laws^*^,1, Janet M. Ferrell^*, Tammy E. Stoker, Judith Schmid and Ralph L. Cooper^*

^* Endocrinology Branch, Gamete and Early Embryo Biology Branch, and Biostatistics and Research Support Staff, Reproductive Toxicology Division, National Health and Environmental Effects Research Laboratory, U.S. Environmental Protection Agency, Research Triangle Park, North Carolina 27711

The effects of atrazine (ATR), a chlorotriazine herbicide, onthe onset of puberty were evaluated in Wistar rats. Female ratswere dosed by oral gavage from postnatal day(s) (PND) 22 throughPND 41 with 0, 12.5, 25, 50, 100, or 200 mg ATR/kg. Vaginalopening (VO) was significantly delayed 3.4, 4.5, or greaterthan 6.8 days by 50, 100, and 200 mg/kg, respectively. VO hadnot occurred in 4 of 15 females in the 200 mg/kg group by thetime of necropsies (PND 41). Body weight (bw) at necropsy wasreduced in the 200 mg/kg group by 11.6%, but was not differentfrom the control (0) in the 50 and 100 mg/kg groups. To examinethe influence of reduced bw on pubertal development, a groupof pair-fed controls was included whose daily food intake wasdependent upon the amount consumed by their counterpart in the200 mg/kg group. Although necropsy bw was reduced to the sameextent as the ATR females, VO in the pair-fed controls was notsignificantly delayed. Adrenal, kidney, pituitary, ovary, anduterine weights were reduced by 200 mg/kg ATR. Serum T₃, T₄,and TSH were unaltered by ATR, which was consistent with nohistopathologic/morphologic changes in the thyroid. Estrouscyclicity was monitored in a second group of females from VOto PND 149. The number of females displaying regular 4- or 5-dayestrous cycles during the first 15-day interval after VO waslower in the 100 and 200 mg/kg ATR and pair-fed controls. Irregularcycles were characterized by extended periods of diestrus. Bythe end of the second 15-day interval (PND 57–71), noeffects on estrous cyclicity were observed. These data showthat ATR can delay the onset of puberty and alter estrous cyclicityin the female Wistar rat ( NOAEL of 25 mg/kg). Reduced foodconsumption and bw did not account for the delay in VO, becausethis effect was not observed in the pair-fed controls. In addition,the effect on estrous cyclicity was observed in the 100 mg/kgATR group where no significant reduction in bw was observed.

Key Words: female reproductive toxicology; puberty; rat; atrazine; vaginal opening; estrous cyclicity.

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