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首页> 外文期刊>Life sciences >Antioxidant properties of Krebs cycle intermediates against malonate pro-oxidant activity in vitro: a comparative study using the colorimetric method and HPLC analysis to determine malondialdehyde in rat brain homogenates.
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Antioxidant properties of Krebs cycle intermediates against malonate pro-oxidant activity in vitro: a comparative study using the colorimetric method and HPLC analysis to determine malondialdehyde in rat brain homogenates.

机译:Krebs循环中间体在体外对丙二酸前氧化活性的抗氧化性能:使用比色法和HPLC分析确定大鼠脑匀浆中丙二醛的比较研究。

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摘要

A variety of Krebs cycle intermediaries has been shown to possess antioxidant properties in different in vivo and in vitro systems. Here we examined whether citrate, succinate, malate, oxaloacetate, fumarate and alpha-ketoglutarate could modulate malonate-induced thiobarbituric acid-reactive species (TBARS) production in rat brain homogenate. The mechanisms involved in their antioxidant activity were also determined using two analytical methods: 1) a popular spectrophotometric method (Ohkawa, H., Ohishi, N., Yagi, K., 1979. Assay for lipid peroxides in animal tissues by thiobarbituric acid reaction. Analytical Biochemistry 95, 351-358.) and a high performance liquid chromatographic (HPLC) procedure (Grotto, D., Santa Maria, L. D., Boeira, S., Valentini, J., Charao, M. F., Moro, A. M., Nascimento, P. C., Pomblum, V. J., Garcia, S. C., 2006. Rapid quantification of malondialdehyde in plasma by high performance liquid chromatography-visible detection. Journal of Pharmaceutical and Biomedical Analysis 43, 619-624.). Citrate, malate, and oxaloacetate reduced both basal and malonate-induced TBARS production. Their effects were not changed by pre-treatment of rat brain homogenates at 100 degrees C for 10 min. alpha-Ketoglutarate increased basal TBARS without changing malonate-induced TBARS production in fresh and heat-treated homogenates. Succinate reduced basal--without altering malonate-induced TBARS production. Its antioxidant activity was abolished by KCN or heat treatment. Fumarate reduced malonate-induced TBARS production in fresh homogenates; however, its effect was completely abolished by heat treatment. There were minimal differences among the studied methods. Citrate, oxaloacetate, malate, alpha-ketoglutarate and malonate showed iron-chelating activity. We suggest that antioxidant properties of citrate, malate and oxaloacetate were due to their ability to cancel iron redox activity by forming inactive complexes, whereas alpha-ketoglutarate and malonate pro-oxidant activity can be due to formation of active complexes with iron. In contrast, succinate and fumarate antioxidant activity was probably due to some enzymatic system.
机译:各种克雷布斯循环中间体已显示在不同的体内和体外系统中均具有抗氧化特性。在这里,我们检查了柠檬酸,琥珀酸,苹果酸,草酰乙酸,富马酸和α-酮戊二酸是否可以调节丙二酸诱导的大鼠脑匀浆中的硫代巴比妥酸反应性物种(TBARS)的产生。还使用两种分析方法确定了其抗氧化活性的机制:1)一种流行的分光光度法(Ohkawa,H.,Ohishi,N.,Yagi,K.,1979。通过硫代巴比妥酸反应测定动物组织中的脂质过氧化物)分析生物化学95,351-358。)和高效液相色谱(HPLC)程序(Grotto,D.,Santa Maria,LD,Boeira,S.,Valentini,J.,Charao,MF,Moro,AM,Nascimento ,PC,Pomblum,VJ,Garcia,SC,2006。通过高效液相色谱-可见检测法快速定量测定血浆中的丙二醛,药物与生物医学分析杂志43,619-624。)。柠檬酸,苹果酸和草酰乙酸减少了基础和丙二酸诱导的TBARS产生。通过在100摄氏度下预处理大鼠脑匀浆10分钟,其作用不会改变。在新鲜和热处理的匀浆中,α-酮戊二酸可增加基础TBARS,而不会改变丙二酸诱导的TBARS产生。琥珀酸降低了基础-不会改变丙二酸诱导的TBARS产生。通过KCN或热处理消除了其抗氧化活性。富马酸酯减少了新鲜匀浆中丙二酸酯诱导的TBARS产生;但是,通过热处理,其效果完全消失了。研究方法之间的差异很小。柠檬酸,草酰乙酸,苹果酸,α-酮戊二酸和丙二酸显示出铁螯合活性。我们认为柠檬酸,苹果酸和草酰乙酸的抗氧化特性是由于它们通过形成非活性复合物而取消铁氧化还原活性的能力,而α-酮戊二酸和丙二酸酯的抗氧化剂活性可能是由于与铁形成了活性复合物。相反,琥珀酸盐和富马酸盐的抗氧化活性可能是由于某些酶系统造成的。

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