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首页> 外文期刊>Biological trace element research >Feeding of selenium alone or in combination with glucoraphanin differentially affects intestinal and hepatic antioxidant and phase II enzymes in growing rats.
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Feeding of selenium alone or in combination with glucoraphanin differentially affects intestinal and hepatic antioxidant and phase II enzymes in growing rats.

机译:单独饲喂硒或与葡萄糖尿素联合饲喂硒,会对成长中的大鼠的肠道和肝脏抗氧化剂和II期酶产生不同的影响。

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The anti-carcinogenic effects of sulforaphane (SFN) are based on the up-regulation of antioxidant enzymes (AE) and phase II enzymes (PIIE) through the transcription factor Nrf2. Current knowledge on the roles of the SFN precursor glucoraphanin (GRA) on these processes is limited. Anti-carcinogenic effects of Se depending on glutathione peroxidase (GPx) activity have also been reported. We studied effects and possible synergisms of Se and GRA on the expression and activity of a broad spectrum of AE and PIIE in jejunum, colon and the liver of rats fed diets differing in Se and GRA concentration. In all organs, GPx1 mRNA expression was 70 % to 90 % lower in Se deficiency than in Se sufficiency. GPx2 expression increased in jejunum and liver under Se deficiency and decreased in the colon. Se deficiency increased most colonic AE and PIIE compared to Se adequacy. Adequate and in particular supranutritive Se combined with GRA increased colonic AE and PIIE expression up to 3.72-fold. In the liver Se deficiency raised the expression of AE and PIIE up to 4.49-fold. GRA attenuated liver AE and PIIE response in Se deficiency. Expression- and correlation analyses revealed that Keap1 mRNA better reflects AE and PIIE gene expression than Nrf2 mRNA. We conclude that: (1) GPx1 sensitively indicates Se deficiency; (2) the influence of Se and Nrf2/Keap1 on GPx2 expression depends on the organ; (3) GRA combined with supranutritive Se may effectively protect against inflammation and colon cancer; (4) future investigations on AE and PIIE expression should consider the role of Keap1 to a higher extent.
机译:萝卜硫烷(SFN)的抗癌作用是基于抗氧化酶(AE)和II期酶(PIIE)通过转录因子Nrf2的上调。目前关于SFN前体糖尿素(GRA)在这些过程中的作用的知识有限。还已经报道了Se依赖于谷胱甘肽过氧化物酶(GPx)活性的抗癌作用。我们研究了硒和GRA对不同饮食和硒浓度的大鼠空肠,结肠和肝脏中多种AE和PIIE的表达和活性的影响以及可能的协同作用。在所有器官中,硒缺乏症患者的GPx1 mRNA表达均比硒缺乏症患者低70%至90%。硒缺乏时,空肠和肝脏中GPx2表达增加,结肠中GPx2表达减少。与硒充足相比,硒缺乏会增加大多数结肠的AE和PIIE。适当的,特别是超营养化的硒与GRA结合可使结肠AE和PIIE的表达增加3.72倍。在肝脏中,硒缺乏症使AE和PIIE的表达提高了4.49倍。 GRA减弱了硒缺乏症患者的肝AE和PIIE反应。表达和相关分析显示,Keap1 mRNA比Nrf2 mRNA更能反映AE和PIIE基因表达。我们得出以下结论:(1)GPx1敏感地表明硒缺乏; (2)Se和Nrf2 / Keap1对GPx2表达的影响取决于器官; (3)GRA联合超营养硒可有效预防炎症和结肠癌; (4)未来有关AE和PIIE表达的研究应更多​​地考虑Keap1的作用。

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