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Research ArticleArticle

Identification of Urinary Metabolites of Isoprene in Rats and Comparison with Mouse Urinary Metabolites

Lorrene A. Buckley, Donna P. Coleman, Jason P. Burgess, Brian F. Thomas, Leo T. Burka and A. Robert Jeffcoat
Drug Metabolism and Disposition July 1999, 27 (7) 848-854;
Lorrene A. Buckley
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Donna P. Coleman
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Jason P. Burgess
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Brian F. Thomas
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Leo T. Burka
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A. Robert Jeffcoat
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Abstract

Isoprene, a major commodity chemical used in production of polyisoprene elastomers, has been shown to be carcinogenic in rodents. Similar to findings for the structurally related compound butadiene, mice are more susceptible than rats to isoprene-induced toxicity and carcinogenicity. Although differences in uptake, and disposition of isoprene in rats and mice have been described, its in vivo biotransformation products have not been characterized in either species. The purpose of these studies was to identify the urinary metabolites of isoprene in Fischer 344 rats and compare these metabolites with those formed in male B6C3F1mice. After i.p. administration of 64 mg [14C]isoprene/kg to rats and mice, isoprene was excreted unchanged in breath (∼50%) or as urinary metabolites (∼32%). In rats isoprene was primarily excreted in urine as 2-hydroxy-2-methyl-3-butenoic acid (53%), 2-methyl-3-buten-1,2-diol (23%), and the C-1 glucuronide conjugate of 2-methyl-3-buten-1,2-diol (13%). These metabolites are consistent with preferential oxidation of isoprene’s methyl-substituted vinyl group. No oxidation of the unsubstituted vinyl group was observed. In addition to the isoprene metabolites found in rat urine, mouse urine contained numerous other isoprene metabolites with a larger percentage (25%) of total urinary radioactivity associated with an unidentified, polar fraction than in the rat (7%). Unlike butadiene, there was no evidence that glutathione conjugation played a significant role in the metabolism of isoprene in rats. Because of the unidentified metabolites in mouse urine, involvement of glutathione in the metabolism of isoprene in mice cannot be delineated.

Footnotes

  • Send reprint requests to: Dr. A. Robert Jeffcoat, Research Triangle Institute, P.O. Box 12194, Research Triangle Park, NC 27709-2194. E-mail: arj{at}rti.org

  • ↵1 Present address: Lilly Research Laboratories, 2001 West Main Street, Greenfield, Indiana 46140.

  • This work was supported by National Institutes of Health Contract N01-ES-15329.

  • Abbreviations used are::
    GC/MS
    gas chromatography/mass spectroscopy
    COSY
    correlated spectroscopy
    BSTFA
    bis(trimethylsilyl)trifluoroacetamide
    TMS
    trimethylsilyl
    TMSCHN2
    trimethylsilyldiazomethane
    BD-M-1
    1,2-dihydroxy-4-(N-acetylcysteinyl-S-)butane
    AMS
    α-methylstyrene
    • Received April 23, 1998.
    • Accepted April 13, 1999.
  • The American Society for Pharmacology and Experimental Therapeutics
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Drug Metabolism and Disposition: 27 (7)
Drug Metabolism and Disposition
Vol. 27, Issue 7
1 Jul 1999
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Research ArticleArticle

Identification of Urinary Metabolites of Isoprene in Rats and Comparison with Mouse Urinary Metabolites

Lorrene A. Buckley, Donna P. Coleman, Jason P. Burgess, Brian F. Thomas, Leo T. Burka and A. Robert Jeffcoat
Drug Metabolism and Disposition July 1, 1999, 27 (7) 848-854;

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Research ArticleArticle

Identification of Urinary Metabolites of Isoprene in Rats and Comparison with Mouse Urinary Metabolites

Lorrene A. Buckley, Donna P. Coleman, Jason P. Burgess, Brian F. Thomas, Leo T. Burka and A. Robert Jeffcoat
Drug Metabolism and Disposition July 1, 1999, 27 (7) 848-854;
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