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Metabolic Activation of Benzo

  1. Author:
    Agarwal, R.
    Coffing, S. L.
    Baird, W. M.
    Kiselyov, A. S.
    Harvey, R. G.
    Dipple, A.
  2. Author Address

    Dipple A NCI FREDERICK CANC RES & DEV CTR ABL BASIC RES PROGRAM POB B FREDERICK, MD 21702 USA NCI FREDERICK CANC RES & DEV CTR ABL BASIC RES PROGRAM FREDERICK, MD 21702 USA PURDUE UNIV CTR CANC W LAFAYETTE, IN 47907 USA BEN MAY INST CHICAGO, IL 60637 USA
    1. Year: 1997
  1. Journal: Cancer Research
    1. 57
    2. 3
    3. Pages: 415-419
  2. Type of Article: Article
  1. Abstract:

    Benzo[g]chrysene (BgC) is an environmental pollutant, and recent studies have demonstrated that anti-BgC-11,12-dihydrodiol 13,14-epoxide (anti-BgCDE) is a potent mammary carcinogen in rats. To determine whether BgC can be metabolically activated to anti-BgCDE in human cells, the human mammary carcinoma cell line MCF-7 was treated with BgC and with the racemic trans-3,4- and 11,12 dihydrodiols. The DNA adducts formed in these experiments were examined using P-32-postlabeling, and specific adducts were identified through comparisons with adducts obtained by the reaction of the racemic syn- and anti-BgCDEs with calf thymus DNA and with purine deoxyribonucleoside-3'-phosphates in vitro. It was found that BgC is metabolically activated in MCF-7 cells to form major DNA adducts through both the syn- and anti-11,12-dihydrodiol 13,14-epoxide metabolites. BgC is therefore a potential environmental risk to humans. The major BgC-DNA adducts formed from both the dihydrodiol-epoxide diastereomers were deoxyadenosine adducts. Thus, BgC has DNA-binding properties that are very similar to those of the potent mammary carcinogens 7,12-dimethylbenz[a]anthracene and dibenzo[a,l]pyrene. [References: 41]

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