首页> 外文期刊>The anatomical record: advances in integrative anatomy and evolutionary biology >Protective effect of glutathione against liver warm ischemia-reperfusion injury in rats is associated with regulation of P-selectin and neutrophil infiltration.
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Protective effect of glutathione against liver warm ischemia-reperfusion injury in rats is associated with regulation of P-selectin and neutrophil infiltration.

机译:谷胱甘肽对大鼠肝脏热缺血-再灌注损伤的保护作用与调节P-选择蛋白和中性粒细胞浸润有关。

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摘要

We examined the effects of glutathione (GSH) preconditioning through the portal vein on rat warm liver ischemia reperfusion injury (I/R injury) and investigated the mechanisms involved. In rats with warm liver I/R injury, administration of GSH by means of the portal vein before ischemia increased the 7-day survival rates of rats after liver I/R from 38% to 75%. This effect was correlated with significantly improved liver function, depressed MDA content in the liver and fewer histologic features of hepatocyte injury. Intrahepatic expression of P-selectin and infiltration of neutrophils were increased significantly after liver I/R. GSH pretreatment decreased intrahepatic MPO content and the expression of P-selectin. However, it did not significantly affect the mRNA levels for P-selectin after liver I/R. Thus, preconditioning with GSH protects the liver against I/R injury by a mechanism dependent on free radical species scavenging, down-regulation of adhesion molecule expression and inhibition of neutrophil accumulation. These findings document the potential clinical utility of GSH to improve the overall success of diverse procedures, such as liver surgery and liver transplantation.
机译:我们研究了通过门静脉谷胱甘肽(GSH)预处理对大鼠温暖肝脏缺血再灌注损伤(I / R损伤)的影响,并研究了其中的机制。在温暖的肝I / R损伤大鼠中,缺血前通过门静脉给​​予GSH可将肝I / R后大鼠的7天生存率从38%提高到75%。该作用与肝功能显着改善,肝中MDA含量降低和肝细胞损伤的组织学特征减少有关。肝I / R后,肝内P-选择蛋白的表达和中性粒细胞的浸润明显增加。 GSH预处理可降低肝内MPO含量和P-选择素的表达。但是,它对肝脏I / R后P-选择素的mRNA水平没有明显影响。因此,用GSH进行预处理可通过一种机制来保护肝脏免受I / R损伤,该机制取决于自由基种类的清除,粘附分子表达的下调和嗜中性粒细胞积累的抑制。这些发现证明了GSH在改善各种手术(例如肝脏手术和肝移植)的总体成功率方面的潜在临床效用。

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