EFFECT OF ALKYL CHAIN-LENGTH ON INHIBITION OF N-NITROSOMETHYLBENZYLAMINE-INDUCED ESOPHAGEAL TUMORIGENESIS AND DNA METHYLATION BY ISOTHIOCYANATES

This study was undertaken to evaluate the inhibitory effects of benzyl isothiocyanate (BITC), phenethyl isothiocyanate (PEITC), 3-phenylprop yl isothiocyanate (PPITC) or 4-phenylbutyl isothiocyanate (PBITC) on N -nitrosomethylbenzylamine (NMBA)-induced esophageal tumorigenesis in m ale Fischer 344 rats. Groups of 15 male rats were fed modified AIN-76A diet or diet containing the four isothiocyanates at concentrations of 2.5, 1.0 and 0.4 mu mol/g) diet for 25 weeks. After two weeks, rats w ere administered 0.5 mg/kg NMBA s.c. once weekly for 15 weeks, Additio nal controls received modified AIN-76A diet only or diet containing th e high concentration of isothiocyanates (2.5 mu mol/g) only. No tumors were found in any of the groups that were not administered NMBA, Rats treated with NMBA only developed 6.7+/-0.8 tumors/animal. Tumor incid ences in rats treated with 2.5 and 1.0 mu mol PEITC/g diet, and with a ll three dietary concentrations of PPITC were inhibited by 60-100% com pared to controls. Tumor multiplicities were inhibited by 83-100% by P EITC or PPITC at all dietary concentrations tested, PPITC clearly had a stronger inhibitory effect on NMBA tumorigenesis than did PEITC. Com pared to PEITC and PPITC, BITC and PBITC had little inhibitory effect on tumor multiplicity and no effect on NMBA tumor incidence. In genera l, the occurrence of preneoplastic lesions (acanthoses, hyperkeratoses , leukoplakias and leukokeratoses) was inhibited in a similar manner a s tumor incidence and multiplicity, except that no experimental diet r esulted in a significant reduction of the incidence of acanthoses and hyperkeratoses. As with their effects on tumorigenicity and formation of premalignant lesions, the inhibitory effects of the isothiocyanates on NMBA-induced DNA methylation 24 h after administration followed th e order: PPITC > PEITC > PBITC > BITC.