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Toxicity of organochalcogens in human leukocytes is associated, but not directly related with reactive species production, apoptosis and changes in antioxidant gene expression

机译:人白细胞中有机粒细胞的毒性是相关的,但与反应性物种生产,凋亡和抗氧化基因表达的变化没有直接相关

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Selenium (Se) containing organic compounds, such as ebselen (Ebs) and diphenyl diselenide [(PhSe)(2)], have been used as pharmacological agents due to their antioxidant properties. Tellurium (Te) does not have any biological function in mammals, but Te-containing organic compounds, such as diphenyl ditelluride [(PhTe)(2)], has been used both as an antioxidant or neurotoxic agent. At high concentrations, these compounds cause toxicity by oxidising thiol and selenol groups of proteins. Here, we analysed whether these compounds could modulate reactive species (RS) production, apoptosis and antioxidant gene expression profile of some selenoproteins and antioxidant enzymes or transcription factors in leukocytes isolated from human blood. Since no data is available about their accumulation in isolated leukocytes, we determine their concentration in the cells by CG-MS. Apoptosis (propidium iodide) and RS production (dichloro fluorescein) were determined by flow cytometry. The expression of CAT, SOD1, GPX3, GPX4, TRXR1, and NFLE2L2 genes were analysed by RT-PCR. (PhTe)(2) was the only compound able to increase apoptosis rate. (PhSe)(2) altered the expression of CAT and SOD1, and this was associated with a high RS production. All compounds decreased the expression of GPX3 but did not alter GPX4 and TRXR1 expression. All compounds decreased NFE2L2 expression (Ebs>(PhTe)(2)>(PhSe)(2)). We hypothesise that the toxicity induced by these organochalcogens is not directly related to their ability of inducing RS production.
机译:含硒(SE)的有机化合物,例如EBSELEN(EBS)和二苯基(PHSE)[(PHSE)(2)],已被用作由于其抗氧化性能而被用作药理剂。碲(TE)在哺乳动物中没有任何生物学功能,但是含有TE的有机化合物,例如二苯基DITLELURE [(PHTE)(2)],其既用作抗氧化剂或神经毒剂。在高浓度下,这些化合物通过氧化硫醇和硒醇的蛋白质引起毒性。在这里,我们分析了这些化合物是否可以调节一些硒蛋白和抗氧化酶的反应性物质(RS)生产,细胞凋亡和抗氧化剂基因表达谱或从人类血液中分离的白细胞中的转录因子。由于没有数据在孤立的白细胞中的积累中可以获得,因此我们通过CG-MS确定它们在细胞中的浓度。通过流式细胞术测定细胞凋亡(碘化钛)和RS生产(二氯荧光素)。通过RT-PCR分析CAT,SOD1,GPX3,GPX4,TRXR1和NFLE2L2基因的表达。 (PHTE)(2)是唯一能增加凋亡率的化合物。 (PHSE)(2)改变了猫和SOD1的表达,这与高RS生产相关。所有化合物都降低了GPX3的表达,但没有改变GPX4和TRXR1表达。所有化合物均降低NFE2L2表达(EBS>(PHTE)(2)>(PHSE)(2))。我们假设这些有机能诱导的毒性与其诱导RS生产的能力没有直接相关。

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