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7,12-DMBA-induced rat leukemia: a review with insights into future research |
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| Authors: | Sugiyama Taketoshi Osaka Mitsuhiko Koami Kenichi Maeda Sakan Ueda Norifumi |
| Affiliation: | a Shiga Medical Center Research Institute, Moriyama, Shiga 524, Japan b Department of Pathology and Tumor Biology, Graduate School of Medicine, Kyoto University, Sakyo-ku, Kyoto 606, Japan c Department of Pathology, Kobe University School of Medicine, Chuo-ku, Kobe 758, Japan d Department of Pathology, Ehime University School of Medicine, Matsuyama, Ehime 791, Japan |
| Abstract: | 7,12-Dimethylbenz[a]anthracene (DMBA) elicits leukemia in Long–Evans rats (LE). This leukemia is mostly erythroblastic and 30% of leukemias have total and partial trisomy of #2 chromosome and the rest have diploid karyotype. The common duplication site is in 2q26–q34 and N-ras gene is located in 2q34. 7,8,12-Trimethylbenz[a]anthracene (TMBA) also induces similar leukemias. These leukemias reveal a highly specific mutation of N-ras gene as in human leukemias. N-ras mutation is induced 48 h after DMBA treatment. Wild type N-ras allele is frequently lost in diploid leukemias but not in trisomy type. Therefore, a gene dosage problem related to the mutant N-ras gene is involved in development of leukemia. Some secondary genetic rearrangements involving abl and H-ras are also observed in cultured leukemia cells. DMBA-induced chromosome aberrations as well as leukemia are enhanced by erythropoietin and blocked by Sudan III given prior to DMBA treatment. This leukemia will provide an important tool for chemical carcinogenesis and leukemia studies. |
| Keywords: | DMBA Carcinogenesis Chemical carcinogen Experimental leukemia Leukemia N-ras abl H-ras Rat Long–Evans rat Erythropoietin Huggins DNA-adduct |
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