首页> 外文期刊>Brain research >Levetiracetam enhances endogenous antioxidant in the hippocampus of rats: in vivo evaluation by brain microdialysis combined with ESR spectroscopy.
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Levetiracetam enhances endogenous antioxidant in the hippocampus of rats: in vivo evaluation by brain microdialysis combined with ESR spectroscopy.

机译:左乙拉西坦增强大鼠海马中的内源性抗氧化剂:通过脑微透析结合ESR光谱进行体内评估。

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We have attempted to explore the neuroprotective effectiveness of levetiracetam (LEV) by measuring its in vivo antioxidant effect in the hippocampus of rats in a freely moving state. Male Wistar rats were used for the estimation of the in vivo antioxidant effect of LEV through microdialysis combined with electron spin resonance spectroscopy. The antioxidant effect was examined using the principle by which a systemically administered blood-brain barrier-permeable nitroxide radical (PCAM) decreases in an exponential decay manner that is correlated with the amount of antioxidant in the brain. The PCAM decay ratio during perfusion with normal Ringer's solution was compared with that during 32 microM and 100 microM LEV co-perfusion. The in vivo antioxidant effect was examined. In addition, the expressions of the cystine/glutamate exchanger (xCT) and the inducible nitric oxide synthase (iNOS) protein related to redox regulation were measured in the hippocampus of rats after 14 days of administration of LEV at a dose of 54 mg/day i.p. The half-life of PCAM was statistically shortened after LEV perfusion compared with the results of the control experiment. While the expression of the pro-oxidant protein iNOS was decreased, that of the antioxidant protein xCT was statistically increased by the administration of LEV. The role of xCT is to transport cystine, the internal material of glutathione, into the cell. The shortened half-life of the nitroxide radical by co-perfusion of LEV with increased xCT and decreased iNOS expression revealed the enhancement of the endogenous antioxidant effect or free-radical scavenging activity. The results of this study suggest that LEV synergistically enhances the basal endogenous antioxidant effect in the hippocampus with ascorbic acid and alpha-tocopherol. Our findings further suggest that LEV exerts a neuroprotective role by 1) modifying the expression of xCT and iNOS in connection with lipid peroxidation, 2) synergistically enhancing the increased basal endogenous antioxidant ability in the hippocampus, and 3) decreasing the basal concentration of glutamate followed by up-regulation of the intake of cystine, an internal material of GSH.
机译:我们已经尝试通过测量左乙拉西坦(LEV)在自由移动状态的大鼠海马中的体内抗氧化作用来探索其神经保护作用。通过微透析结合电子自旋共振光谱法,将雄性Wistar大鼠用于评估LEV的体内抗氧化作用。使用以下原理检查抗氧化作用:通过系统给药的血脑屏障-可渗透氮氧化物自由基(PCAM)以与大脑中抗氧化剂量相关的指数衰减方式降低。比较了使用普通林格氏液灌注时的PCAM衰减率与32 microM和100 microM LEV共灌注时的PCAM衰减率。检查了体内抗氧化作用。另外,以54 mg /天的剂量给予LEV 14天后,在大鼠海马中测量了与氧化还原调节相关的胱氨酸/谷氨酸交换子(xCT)和诱导型一氧化氮合酶(iNOS)蛋白的表达。 ip与对照实验结果相比,LEV灌注后PCAM的半衰期在统计学上缩短了。虽然通过施用LEV,促氧化剂蛋白iNOS的表达降低,但是抗氧化剂蛋白xCT的表达在统计学上增加。 xCT的作用是将谷胱甘肽的内部物质胱氨酸转运到细胞中。通过LEV与xCT的增加和iNOS表达的共同灌注而缩短的氮氧化物自由基的半衰期表明,内源性抗氧化剂作用或自由基清除活性的增强。这项研究的结果表明,LEV与抗坏血酸和α-生育酚协同增强海马的基础内源性抗氧化作用。我们的发现进一步表明,LEV通过以下方式发挥神经保护作用:1)与脂质过氧化有关的修饰xCT和iNOS的表达; 2)协同增强海马基础内源性抗氧化能力的增强; 3)降低谷氨酸的基础浓度通过上调胱氨酸(一种GSH的内部物质)的摄入量。

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