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David L. McCormick, Fredric J. Bums, Roy E. Albert, Inhibition of Benzo[a]pyrene-Induced Mammary Carcinogenesis by Retinyl Acetate, JNCI: Journal of the National Cancer Institute, Volume 66, Issue 3, March 1981, Pages 559–564, https://doi.org/10.1093/jnci/66.3.559
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Abstract
The administration of a 250-ppm retinyl acetate dietary supplement for various periods relative to intragastric administration of 50 mg benzo[a]pyrene (BP) significantly inhibited the induction of mammary cancers in virgin female inbred LEW/Mai rats. With day of BP administration taken as time 0, groups receiving the retinoid from weeks −2 to +1, +1 to +90, +20 to +90, and −p2 to +90 showed a significant reduction in tumor response as compared to controls. The inhibition of carcinogenesis achieved by a +1 to +20 administration schedule was temporary; the tumor yield was suppressed initially but returned to control levels by week 60. Autoradiographic analysis of mammary glands from 50-day-old rats indicated that a 2-week exposure to supplemental retinyl acetate significantly reduced the mammary gland parenchymal cell labeling index in ductal, alveolar, and terminal end bud structures. Beginning the retinyl acetate supplement 1 week after the administration of BP significantly reduced the number of terminal ductal hyperplasias. The inhibition of carcinogenesis achieved by a short period of retinyl acetate administration before and during the period of carcinogen availability as well as the inhibition achieved by longterm postcarcinogen retinoid exposure may involve an antiproliferative effect on the rat mammary gland.
