TY - JOUR
T1 - Syntheses and identification of benzo[c]chrysene metabolites
AU - Desai, Dhimant
AU - Krzeminski, Jacek
AU - Lin, Jyh Ming
AU - Chadha, Anju
AU - Miyata, Naoki
AU - Yagi, Haruhiko
AU - Jerina, Donald M.
AU - Amin, Shantu
PY - 2000
Y1 - 2000
N2 - Like other PAHs, chiysenes are thought to exert their carcimogenicity via metabolic activation of proximally carcinogenic dihydrodiols to diol epoxides as ultimate carcinogens. Benzo[c] chrysene (B[c]C) is structurally intriguing among the PAH because it features both a bay region and a fjord region. Although B[c]C is carcinogenic and mutagenic, few data are available on its metabolic activation or the nature of its metabolites. We have synthesized the B[c]C trans-1,2-, 7,8-, and 9,10-dihydrodiols from the appropriate methoxy-substituted bisnaphthyl olefins by photochemical cyclization. B[c]C was metabolized with S9 liver fraction from phenobarbital/β-naphthoflavone-treated rats. Dihydrodiols were formed on both terminal rings as well as in the K-region. 2-, 3-, and 10-HydroxyB[c]C were also identified as metabolites. In mutagenicity studies toward S. typhimurium TA100, 1,2-dihydrodiol was more mutagenic than B[c]C at doses above 1.25 μg/plate, whereas 9,10-dihydrodiol was toxic at doses above 1.25 μg/plate.
AB - Like other PAHs, chiysenes are thought to exert their carcimogenicity via metabolic activation of proximally carcinogenic dihydrodiols to diol epoxides as ultimate carcinogens. Benzo[c] chrysene (B[c]C) is structurally intriguing among the PAH because it features both a bay region and a fjord region. Although B[c]C is carcinogenic and mutagenic, few data are available on its metabolic activation or the nature of its metabolites. We have synthesized the B[c]C trans-1,2-, 7,8-, and 9,10-dihydrodiols from the appropriate methoxy-substituted bisnaphthyl olefins by photochemical cyclization. B[c]C was metabolized with S9 liver fraction from phenobarbital/β-naphthoflavone-treated rats. Dihydrodiols were formed on both terminal rings as well as in the K-region. 2-, 3-, and 10-HydroxyB[c]C were also identified as metabolites. In mutagenicity studies toward S. typhimurium TA100, 1,2-dihydrodiol was more mutagenic than B[c]C at doses above 1.25 μg/plate, whereas 9,10-dihydrodiol was toxic at doses above 1.25 μg/plate.
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U2 - 10.1080/10406639908020592
DO - 10.1080/10406639908020592
M3 - Article
AN - SCOPUS:0033264869
SN - 1040-6638
VL - 16
SP - 255
EP - 264
JO - Polycyclic Aromatic Compounds
JF - Polycyclic Aromatic Compounds
IS - 1-4
ER -