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Research ArticleArticle

Molecular Basis for Hepatic Detoxifying Enzyme Induction by 2-(Allylthio)pyrazine in Rats in Comparison with Oltipraz: Effects on Prooxidant Production and DNA Degradation

Sang Geon Kim, Min Kyung Cho, Sung Hee Choi, Hye Jung Kim, Mi Kyong Kwak and Nak Doo Kim
Drug Metabolism and Disposition June 1999, 27 (6) 667-673;
Sang Geon Kim
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Min Kyung Cho
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Sung Hee Choi
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Hye Jung Kim
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Mi Kyong Kwak
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Nak Doo Kim
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Abstract

The expression of hepatic microsomal epoxide hydrolase (mEH) and glutathione S-transferases (GSTs) by 2-(allylthio)pyrazine (2-AP), an experimental chemopreventive agent, was investigated in rats. Northern blot analysis revealed that 2-AP caused increases in mEH, rGSTA2/3/5, and rGSTM1/2 mRNA levels. mEH and rGSTA2 proteins were also induced. Molecular basis of the enzyme induction by 2-AP was studied in comparison with oltipraz (Olt). Rats exposed to buthionine sulfoximine, a GSH-depleting agent, before treatment with either 2-AP or Olt exhibited greater increases in the mRNA levels than the individual treatment. Conversely, increases of the mRNAs were prevented by cysteine treatment, indicating that metabolic intermediates or reactive oxygens produced from the agents could be reduced by cysteine. Gel shift analysis revealed that nuclear factor-κB, which is associated with the altered cellular redox state, was not activated by the agents. Effects of these agents on the breakage of φx-174 DNA were compared in vitro. 2-AP effectively reduced the conversion of supercoiled DNA to the open circular form induced by benzenetriol and prevented benzenetriol- and iron-catalyzed degradation of DNA, whereas Olt failed to prevent strand breakage of DNA. These results provided evidence that: 1) 2-AP was effective in elevating the hepatic mEH and GST gene expression in rats, which might be mediated with the production of reactive oxygen species; 2) nuclear factor-κB activation was not involved in the induction of the detoxifying enzymes by either 2-AP or Olt in spite of their production of reactive oxygens in vivo; and 3) the antioxidant effect of 2-AP in vitro differed from that of Olt.

Footnotes

  • Send reprint requests to: Dr. Sang Geon Kim, College of Pharmacy, Seoul National University, Silim-dong, Kwanak-gu, Seoul 151-742, South Korea. E-mail: sgk{at}snu.ac.kr

  • This work was supported by the Korea Science and Engineering Foundation (KOSEF) through The Research Center for New Drug Development at Seoul National University.

  • ↵2 Kim and Gates (1997) Olt was dissolved in acetonitrile, as described previously. Comparable result was observed by Olt dissolved in an aqueous solution.

  • Abbreviations used are::
    2-AP
    2-(allylthio)pyrazine
    ARE
    antioxidantresponsive element
    BSO
    buthionine sulfoximine
    BT
    benzenetriol
    GST
    glutathioneS-transferase
    mEH
    microsomal epoxide hydrolase
    LPS
    lipopolysaccharide
    NF-κB
    nuclear factor-κB
    Olt
    oltipraz
    SDS
    sodium dodecylsulfate
    • Received September 10, 1998.
    • Accepted February 19, 1999.
  • The American Society for Pharmacology and Experimental Therapeutics
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Drug Metabolism and Disposition: 27 (6)
Drug Metabolism and Disposition
Vol. 27, Issue 6
1 Jun 1999
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Research ArticleArticle

Molecular Basis for Hepatic Detoxifying Enzyme Induction by 2-(Allylthio)pyrazine in Rats in Comparison with Oltipraz: Effects on Prooxidant Production and DNA Degradation

Sang Geon Kim, Min Kyung Cho, Sung Hee Choi, Hye Jung Kim, Mi Kyong Kwak and Nak Doo Kim
Drug Metabolism and Disposition June 1, 1999, 27 (6) 667-673;

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Research ArticleArticle

Molecular Basis for Hepatic Detoxifying Enzyme Induction by 2-(Allylthio)pyrazine in Rats in Comparison with Oltipraz: Effects on Prooxidant Production and DNA Degradation

Sang Geon Kim, Min Kyung Cho, Sung Hee Choi, Hye Jung Kim, Mi Kyong Kwak and Nak Doo Kim
Drug Metabolism and Disposition June 1, 1999, 27 (6) 667-673;
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