The effects of promoter treatments prior to initiation on subsequent promotion by
mezerein were examined in SENCAR mice. Groups of mice received two applications of various complete as well as first and second stage promoters given at various time intervals prior to initiation ranging from 3 days to 10 weeks. The mice were then initiated with 2 micrograms of 7,12-dimethylbenz[a]
anthracene (DMBA) followed 2 weeks later by twice-weekly treatments with 2 micrograms of
mezerein. The
papilloma response in mice, receiving pretreatments with 2 micrograms of 12-O-tetradecanoylphorbol-13-acetate (TPA) either 3 days, 1, 2, 3 or 5 weeks before initiation, was similar to that seen when TPA was given after initiation during stage I of promotion followed by stage II of promotion with
mezerein (4-5
papillomas per mouse in all groups). Surprisingly, pretreatment with the stage II promoter,
mezerein (2 micrograms), either 2 or 5 weeks prior to initiation, also gave
papilloma responses similar to that induced with the standard two-stage promotion protocol (4.7 and 6.4
papillomas per mouse, respectively). The
papilloma response was less than that in the standard two-stage promotion protocol when pretreatments with the stage I promoter
A23187 (80 micrograms/mouse) were given either 2 or 5 weeks before initiation (2.6 and 2.3
papillomas per mouse, respectively). However, a repeat experiment (currently in progress) with a higher dose of
A23187 (160 micrograms/mouse) given 2 weeks prior to initiation indicates that it is more effective than the 80 micrograms dose. When the time interval between pretreatment and initiation was increased to 10 weeks, the
papilloma response with TPA and
A23187 pretreatment was reduced to below two
papillomas per mouse and with
mezerein pretreatment to below three
papillomas per mouse, indicating the effect was reversible. Histological changes in epidermis of mice which received two applications of these compounds correlated with the
tumor response. In this regard, treatment with two applications of TPA and
mezerein resulted in an epidermal
hyperplasia of similar magnitude (epidermal thickness of 53.5 +/- 1.5 and 50.0 +/- 1.1 microns, respectively). The
hyperplasia produced by treatment with two applications of 80 micrograms
A23187 (39.4 +/- 1.8 microns) was significantly less. The ability of pretreatments with
benzoyl peroxide (20 mg) and
chrysarobin (50 micrograms) to affect the subsequent promoting activity of
mezerein was also examined.(ABSTRACT TRUNCATED AT 400 WORDS)