A molecular orbital study of the metabolism and carcinogenicity of the phenols of benzo(a)pyrene

## Abstract Metabolism of the carcinogenic hydrocarbon benzo(a)pyrene (BP) to water and alkali‐soluble products was measured in cultured fibroblast and epithelial cells from human embryos. The alkali‐soluble products represented only a small fraction of BP metabolism. Fibroblasts from different org

## Abstract The metabolism of tritiated benzo[a]pyrene (B[a]P) by primary mouse embryo cells in culture was studied. At concentrations of B[a]P in the medium below about 2–3 mμ moles/ml, metabolism was exponential with time, but at higher concentrations a period of rapid metabolism was followed by

## Abstract Benzo[a]pyrene (B[a]P) and 6‐methylbenzo[a]pyrene ( 6‐MeB[a]P) are metabolized by fortified rat‐liver homogenates to a number of metabolites including one which is indistinguishable from 6‐hydroxymethylbenzo[a]pyrene (6–OHMeB[a]P) by either thin‐layer chromatography or ultra‐violet abso

## Abstract A rat liver microsome‐mediated bacterial mutagenicity test showed 9‐hydroxybenzo (__a__) pyrene to be significantly more effective as a pre‐mutagen than benzo (__a__) pyrene. Experiments measuring the ability of these compounds to be metabolically activated to moieties that alky late ex