Relationship Between Tumorigenic Potency, Ki-rasCodon 12 Mutations, and DNA Adducts Induced by Cyclopenta[cd]pyrene

Abstract

Abstract Cyclopenta[cd]pyrene (CPP) was examined for its lung tumorigenic activity in strain A/J mice, for the formation and persistence of CPP-induced DNA adducts in lung tissue, and for its induction of mutations in the Ki−ras oncogene from CPP-induced tumors. CPP displayed high tumorigenic activity, inducing 97.7 lung adenomas/mouse at 200 mg/kg. Ki−ras codon 12 mutations in the DNA of induced tumors were: GGT→CGT (50%); GGT→KTT (15%); GGT→TGT (25%); GGT→GAT (10%). All DNA adducts in the lungs of CPP-treated mice were CPP−3,4−oxide derived and most were CPP−3,4−oxide−2′−deoxyguanosine adducts. CPP is highly tumorigenic in the strain A/J mouse lung adenoma model, being 5 times more active than benzo[a]pyrene. The increased activity of CPP may be related to the unique induction of the GGT→CGT, Ki−ras codon 12 mutation.