Nitric oxide does not mediate but inhibits transformation and tumor phenotype

Although inducible nitric oxide synthase (iNOS) and nitric oxide (NO) are implicated in tumor pathology, their role in the early stages of carcinogenesis is not well defined. Tumor necrosis factor alpha (TNFot) induces NOS and NO production in transformation-sensitive 1136 P+, but not in transformation- resistant JB6 P-, mouse epidermal cells. We tested the hypothesis that NOS, by generating NO and reactive nitrogen species, mediates tumor promoter-induced transformation. Specific [N-[3(aminomethyl)benzyllacetamidine (1400W)] and non- specific (N-omega-methyl-L-arginine) NOS inhibitors significantly reduced TNFalpha-induced NO production in P+ cells but both NOS inhibitors enhanced TNFalpha-induced anchorage-independent transformation, thus ruling out a mediator role and suggesting an inhibitor role for NO. Independent support for an inhibitor role came from the observation that the NO donor [(Z)-1-[N-(2-aminoethyl)-N-(2- ammonioethyl)amino]diazen-1-ium-1,2-diolate (DETA/NO)] inhibited TNFalpha- and 12-0-tetradecanoylphorbol-13-acetate- induced transformation. DETA/NO treatment also suppressed tumor phenotype in tumorigenic JB6 RT101 (Tx) cells. Higher concentrations of DETA/NO induced apoptosis. The transformation inhibitory effect of lower DETA/NO concentrations may be attributable in part to inhibition by NO of NF-kappaB-dependent but not of AP-1-dependent transcription. In conclusion: (a) induction of NOS and NO production does not mediate but actually prevents tumor promotion; (b) NOS inhibitors enhance the transformation response, and therefore appear not to be appropriate as chemoprevention agents; and (c) NO has both chemopreventive and tumoricidal effects, suggesting promise in cancer chemoprevention and therapy

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