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Research ArticleArticle

Role of Induction of Specific Hepatic Cytochrome P450 Isoforms in Epoxidation of 4-Vinylcyclohexene

S. M. Fontaine, P. B. Hoyer, J. R. Halpert and I. G. Sipes
Drug Metabolism and Disposition September 2001, 29 (9) 1236-1242;
S. M. Fontaine
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P. B. Hoyer
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J. R. Halpert
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I. G. Sipes
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Abstract

4-Vinyl-1-cyclohexene (VCH) is ovotoxic in B6C3F1 mice but not in Fischer-344 rats, which can be partially attributed to greater formation of toxic epoxides from VCH in mice compared with rats. Since repeated exposure to VCH is necessary to cause ovotoxicity in mice, it is important to determine whether repeated exposure results in induction of cytochrome P450 (CYP) enzymes involved in its bioactivation. Hepatic microsomes prepared from mice or rats treated repeatedly with VCH demonstrated significantly increased VCH bioactivation in vitro, as assessed by VCH-1,2-epoxide, VCH-7,8-epoxide, or vinylcyclohexene diepoxide (VCD) formation. Mice and rats were then dosed with VCH, VCH-1,2-epoxide, or VCD for 10 days and measured for increases in hepatic microsomal CYP levels or activities. Total hepatic CYP levels were elevated only in microsomes from mice pretreated with VCH or VCH-1,2-epoxide. Immunoblotting analysis of microsomes from VCH-treated rodents revealed elevated levels of CYP2A and CYP2B in mice but not rats. VCH-1,2-epoxide pretreatment also increased CYP2B levels in the mouse. Activities toward specific substrates for CYP2A and CYP2B (coumarin and pentoxyresorufin, respectively) confirmed that VCH and VCH-1,2-epoxide pretreatments resulted in increased catalytic activities of CYP2A and CYP2B in the mouse but not the rat. Pretreatment with phenobarbital, a known inducer of CYP2A and CYP2B, increased VCH bioactivation in both species. Interestingly, metabolism studies with human CYP “Supersomes” reveal that, of eight isoforms tested, only human CYP2E1 and CYP2B6 were capable of significantly catalyzing VCH epoxidation, whereas CYP2B6, CYP2A6, CYP2E1, and CYP3A4 were capable of catalyzing the epoxidation of the monoepoxides.

Footnotes

  • This research was supported in part by the National Institute of Environmental Health Sciences Training Grant T32 ES07091, the Southwest Environmental Health Sciences Center Grant P30 ES06694, National Institutes of Health Grant R01-ES08979, National Institute of Environmental Health Sciences Grant ES03619, the Chemical Manufacturers' Association, and the Procter and Gamble Fellowship.

  • Abbreviations used are::
    VCH
    4-vinyl-1-cyclohexene
    VCD
    vinylcyclohexene diepoxide
    CYP
    cytochrome P450
    PB
    phenobarbital
    • Received December 21, 2000.
    • Accepted May 11, 2001.
  • The American Society for Pharmacology and Experimental Therapeutics
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Drug Metabolism and Disposition: 29 (9)
Drug Metabolism and Disposition
Vol. 29, Issue 9
1 Sep 2001
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Research ArticleArticle

Role of Induction of Specific Hepatic Cytochrome P450 Isoforms in Epoxidation of 4-Vinylcyclohexene

S. M. Fontaine, P. B. Hoyer, J. R. Halpert and I. G. Sipes
Drug Metabolism and Disposition September 1, 2001, 29 (9) 1236-1242;

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Research ArticleArticle

Role of Induction of Specific Hepatic Cytochrome P450 Isoforms in Epoxidation of 4-Vinylcyclohexene

S. M. Fontaine, P. B. Hoyer, J. R. Halpert and I. G. Sipes
Drug Metabolism and Disposition September 1, 2001, 29 (9) 1236-1242;
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