Abstract 1605: α-cryptoxanthin supplementation inhibits the carcinogen-initiated and nicotine-promoted lung carcinogenesis in AJ mice by suppression of AKT activation

A pooled analysis from well-implemented cohort studies reported that increased dietary α-cryptoxanthin (BCX) intake, rather than α-carotene used in earlier human trials, is associated with reduced risk of lung cancer. Nonetheless, BCX efficacy on lung carcinogenesis has not been reported. In these studies, we examined the protective effects of BCX at different doses against lung carcinogenesis at the initiation and the promotion stages of the cancer development in male AJ mice. In the tobacco carcinogen 4-(methylnitrosamino)- 1-(3-pyridyl)-1-butanone [NNK]-initiated lung carcinogenesis model, we found a 52-63% reduction of lung tumor multiplicity in mice pre-treated with BCX at 0.2 and 2 mg kg BW-1 d-1, as compared to the NNK group (P