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首页> 外文期刊>Biochimica et biophysica acta. Molecular cell research >TrxR1 and GPx2 are potently induced by isothiocyanates and selenium, and mutually cooperate to protect Caco-2 cells against free radical-mediated cell death
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TrxR1 and GPx2 are potently induced by isothiocyanates and selenium, and mutually cooperate to protect Caco-2 cells against free radical-mediated cell death

机译:TrxR1和GPx2被异硫氰酸盐和硒强烈诱导,并相互协作以保护Caco-2细胞免受自由基介导的细胞死亡

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Currently, there is significant interest in the field of diet-gene interactions and the mechanisms by which food compounds regulate gene expression to modify cancer susceptibility. From a nutrition perspective, two key components potentially exert cancer chemopreventive effects: isothiocyanates (ITCs), present in cruciferous vegetables, and selenium (Se) which, as selenocysteine, is an integral part of selenoproteins. However, the role of these compounds in the expression of key selenoenzymes once the cancer process has been initiated still needs elucidation. Therefore, this investigation examined the effect of two forms of selenium, selenium-methylselenocysteine and sodium selenite, both individually and in combination with two ITCs, sulforaphane or iberin, on the expression of the two selenoenzymes, thioredoxin reductase 1 (TrxR1) and gastrointestinal glutathione peroxidase (GPx2), which are targets of ITCs, in Caco-2 cells. Co-treatment with both ITCs and Se induced expression of TrxR1 and GPx2 more than either compound alone. Moreover, pre-treatment of cells with ITC+Se enhanced cytoprotection against H 2O 2-induced cell death through a ROS-dependent mechanism. Furthermore, a single and double knockdown of TrxR1 and/or GPx2 suggested that both selenoproteins were responsible for protecting against H 2O 2-induced cell death. Together, these data shed new light on the mechanism of interactions between ITC and Se in which translational expression of the enhanced transcripts by the former is dependent on an adequate Se supply, resulting in a cooperative antioxidant protective effect against cell death.
机译:当前,在饮食-基因相互作用和食物化合物调节基因表达以改变癌症易感性的机制领域中,引起了极大的兴趣。从营养学的角度来看,两个关键成分可能发挥癌症化学预防作用:十字花科蔬菜中存在的异硫氰酸盐(ITC)和硒硒(硒硒)是硒蛋白不可或缺的一部分。但是,一旦癌症过程开始,这些化合物在关键硒酶表达中的作用仍然需要阐明。因此,这项研究检查了两种形式的硒,即硒-甲基-硒代半胱氨酸和亚硒酸钠,分别单独或与两种ITC萝卜硫烷或iberin组合,对两种硒代酶硫氧还蛋白还原酶1(TrxR1)和胃肠道谷胱甘肽的表达的影响。过氧化物酶(GPx2)是Caco-2细胞中ITC的靶标。与ITC和Se共同处理比单独使用任何一种化合物诱导的TrxR1和GPx2表达更多。此外,用ITC + Se预处理细胞可通过ROS依赖性机制增强针对H 2O 2诱导的细胞死亡的细胞保护作用。此外,TrxR1和/或GPx2的一次和两次敲低表明这两种硒蛋白都负责防止H 2O 2诱导的细胞死亡。总之,这些数据为ITC和Se之间的相互作用机制提供了新的思路,其中前者增强转录本的翻译表达依赖于充足的Se供应,从而导致了针对细胞死亡的协同抗氧化保护作用。

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