Development of a multi-organ rat model for evaluating chemopreventive agents: efficacy of indole-3-carbinol

doi:10.1093/carcin/23.2.265

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Carcinogenesis, Vol. 23, No. 2, 265-272, February 2002
© 2002 Oxford University Press

MOLECULAR EPIDEMIOLOGY

Development of a multi-organ rat model for evaluating chemopreventive agents: efficacy of indole-3-carbinol

Gary Stoner¹^,5, Bruce Casto¹, Sherry Ralston¹, Bill Roebuck², Clifford Pereira³ and George Bailey⁴

¹ Division of Environmental Health Sciences, School of Public Health, College of Medicine and Public Health, The Ohio State University, Columbus, OH,
² Department of Pharmacology and Toxicology, Dartmouth Medical School, Hanover, NH,
³ Statistics Department, Oregon State University, Corvallis, OR and
⁴ Medical Biochemistry Department, MFBS Center, Oregon State University, Corvallis, OR, USA

Abstract

Indole-3-carbinol (I-3-C) is among the most widely and popularlyknown antiestrogens. Due to its putative chemopreventive action,I-3-C is being marketed to the general public in health foodestablishments. Although it has been demonstrated to preventcancer in animal bioassays, I-3-C also acts as a promoter inthe liver and colon. Because of this potential dual biologicalactivity, it is important to investigate both the inhibitoryand promotional activities of I-3-C in multi-organ tumorigenesisanimal models. 7,12-Dimethylbenz[a]anthracene, aflatoxin B₁and azoxymethane were used to initiate mammary, liver and coloncarcinogenesis, respectively in female Sprague–Dawleyrats. The rats were fed continuously on a diet containing I-3-Cfor 25 weeks after initiation. I-3-C treatment was begun oneweek after the last carcinogen treatment had been administered.I-3-C treatment resulted in a delay in latency of mammary tumorformation, but did not alter tumor incidence or multiplicityamong survivors. In the colon, the protocol produced a 40% decreasein aberrant colon crypt foci. However, in the liver, it strongly-inducedGST-P foci in carcinogen-treated (a four-fold increase in volumepercent foci) and in the vehicle controls (a 69-fold increase).These data support previous findings in other rodent and fishtumor models that I-3-C both inhibits and promotes carcinogenesis.The results of this study clearly demonstrate that I-3-C isnot an appropriate chemoprotective agent for human use, in spiteof its effects in the breast and colon in this rat animal model.

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