Tumor initiating activity of 9- and 10-fluoro-7,12-dimethylbenz[a]-anthracene (DMBA) and the effect of 2,3,7,8-tetrachlorodibenzo-p-dioxin on tumor initiation by monofluoro derivatives of DMBA in SENCAR mice

Carcinogenesis
J DiGiovanniL Diamond

Abstract

We have determined the skin tumor initiating activity in SENCAR mice of 6 monofluoro derivatives of 7,12-dimethylbenz[a]anthracene (DMBA). 9-Fluoro-DMBA (9-F-DMBA) was approximately as active, and 10-F-DMBA was more active than the parent hydrocarbon, DMBA. The difference between DMBA and 10-F-DMBA was most dramatic at the highest initiating doses of 10-F-DMBA tested. 4-F-DMBA, which was only weakly active as an initiator, was also tested as a complete carcinogen on mouse skin; after 30 weeks of treatment, 50- and 100-nmol weekly doses failed to elicit papillomas or carcinomas. Animals treated with 50 nmol of DMBA weekly exhibited a 100% papilloma incidence and a 42% carcinoma incidence. Pretreatment with 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD) effectively inhibited tumor initiation with all of the monofluoro derivatives of DMBA tested. The ED50 (dose of TCDD producing half-maximal inhibition) for the inhibition of DMBA initiation in SENCAR mice was determined to be 1.8 X 10(-3) micrograms/mouse (5.6 pmol). The results indicate that the introduction of a fluorine atom in ring D of DMBA has no effect (positions 9 and 11) or enhances (position 10) tumor initiating activity. We believe 10-F-DMBA to be the first example of a hyd...Continue Reading

Citations

Sep 14, 1992·Chemico-biological Interactions·E H WeyandE J LaVoie
Jan 1, 1990·Free Radical Research Communications·E L Cavalieri, E G Rogan
Feb 22, 2018·Chemical Record : an Official Publication of the Chemical Society of Japan ... [et Al.]·Dinabandhu SarDipanjan Pan
Jun 1, 1996·Chemical Research in Toxicology·W Baer-DubowskaJ DiGiovanni

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