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与奥替普拉相比,2-(烯丙硫基)吡嗪诱导大鼠肝脏解毒酶的分子基础:对促氧化剂生成和DNA降解的影响

Molecular basis for hepatic detoxifying enzyme induction by 2-(allylthio)pyrazine in rats in comparison with oltipraz: effects on prooxidant production and DNA degradation.

作者信息

Kim S G, Cho M K, Choi S H, Kim H J, Kwak M K, Kim N D

机构信息

College of Pharmacy, Seoul National University, Seoul, Korea.

出版信息

Drug Metab Dispos. 1999 Jun;27(6):667-73.

PMID:10348795
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-kappaB, which is associated with the altered cellular redox state, was not activated by the agents. Effects of these agents on the breakage of phix-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-kappaB 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.

摘要

在大鼠中研究了实验性化学预防剂2-(烯丙硫基)吡嗪(2-AP)对肝微粒体环氧化物水解酶(mEH)和谷胱甘肽S-转移酶(GSTs)表达的影响。Northern印迹分析显示,2-AP可使mEH、rGSTA2/3/5和rGSTM1/2的mRNA水平升高。mEH和rGSTA2蛋白也被诱导。与奥替普拉(Olt)相比,研究了2-AP诱导酶的分子基础。在用2-AP或Olt处理前,用谷胱甘肽消耗剂丁硫氨酸亚砜胺处理的大鼠,其mRNA水平的升高幅度大于单独处理。相反,半胱氨酸处理可阻止mRNA的升高,表明半胱氨酸可还原由这些试剂产生的代谢中间体或活性氧。凝胶迁移分析显示,与细胞氧化还原状态改变相关的核因子-κB未被这些试剂激活。在体外比较了这些试剂对phix-174 DNA断裂的影响。2-AP有效地减少了苯三醇诱导的超螺旋DNA向开环形式的转化,并防止了苯三醇和铁催化的DNA降解,而Olt未能阻止DNA链断裂。这些结果证明:1)2-AP可有效提高大鼠肝脏中mEH和GST基因的表达,这可能与活性氧的产生有关;2)尽管2-AP和Olt在体内产生活性氧,但核因子-κB的激活与它们诱导解毒酶无关;3)2-AP在体外的抗氧化作用与Olt不同。

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