A METABOLITE OF CARCINOGENIC 2-ACETYLAMINOFLUORENE, 2-NITROSOFLUORENE, INDUCES REDOX CYCLING IN MITOCHONDRIA

The present study was designed to confirm the recent proposal that 2-nitrosofluorene (2-NOF) as well as N-hydroxy-2-aminofluorene (N-OH-AF) induce a redox-cycle in rat liver mitochondria as part of the chronic toxic effects of the carcinogen 2-acetylaminofluorene (2-AAF). The formation of O-2(-) was demonstrated in submitochondrial particles by the formation of adrenochrome with NADH and succinate as respiratory substrates. 2-NOF was as effective as paraquat, a known redox-cycler, the lowest effective concentration being 0.4 nmol 2-NOF/mg protein. Experiments with isolated mitochondria showed that 2-NOF, in contrast to N-OH-AF, induces cyanide-resistant O-2 consumption only in the presence of respiratory substrates, indicating that the reduction, but not the reoxidation, depends on a continuous flow of electrons through the respiratory chain of the mitochondrial membrane. Lipid peroxidation was estimated by the formation of thiobarbituric-acid-reactive substances. In comparison to the well-known prooxidant tert-butylhydroperoxide, 2-NOF was not significantly active. The results support the notion that 2-NOF induces oxidative stress by mitochondrial redox-cycling in vivo. Effects other than lipid peroxidation seem to be important for the chronic toxicity of 2-AAF.