The relation of metabolism to macromolecular binding of the carcinogen benzo[a]pyrene, by mouse embryo cells in culture

## Abstract The metabolism and consequent macromolecular binding of dibenz(a,c)anthracene and dibenz(a,h) anthracene by mouse embryo cells in culture was compared at approximately equal, low doses of hydrocarbon in the medium. Both hydrocarbons were metabolized more slowly than other hydrocarbons t

A series of eight tritium-labelled polycyclic hydrocarbons were incubated in the presence of monolayer cultures of primary mouse embryo cells, and the time-course of their metabolism to water-soluble derivatives was studied. All the hydrocarbons, both carcinogenic and non-carcinogenic, were metaboli

## Abstract The marked localization of a carcinogenic polycyclic aromatic hydrocarbon, benzo(__a__)pyrene, and its metabolites and a carcinogenic alkylating agent, N‐methyl‐N'‐nitro‐N‐nitrosoguanidine, to a specific subnuclear fraction (fraction I) from AKR‐2B mouse embryo cells in culture is descr

## 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 DNA of mouse embryo cells was specifically labelled in the purine moieties with (G^3^H)‐deoxyadenosine or in the cytosine moieties with (5^3^H)‐deoxycytidine. These cells were then treated with 7‐methylbenz (__a__) anthracene (__7MBA__) or benzo (__a__)‐pyrene (B(__a__)P) and the DN