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别嘌醇可改善肝脏在缺血/再灌注损伤后的清除能力。

Allopurinol improves scavenging ability of the liver after ischemia/reperfusion injury.

作者信息

Karwinski W, Søreide O

机构信息

Department of Surgery, Deaconess Hospital, University of Bergen, Norway.

出版信息

Liver. 1997 Jun;17(3):139-43. doi: 10.1111/j.1600-0676.1997.tb00796.x.

Abstract

Deterioration of energy metabolism and oxidative stress represent fundamental mechanisms in ischemia and reperfusion injury. In a normothermic ischemia/reperfusion rat model, we investigated whether allopurinol (ALL) may improve the scavenging ability of the liver after ischemia. ALL was given prior to ischemia and reperfusion (concentration 100 or 50 mg/kg) and controls were given a placebo. After a basal period of 30 min, 1 h normothermic ischemia was induced in the median and left liver lobes followed by 24 h observation. The overall liver function was assessed by bile secretion, and free oxygen production was assessed by glutathione efflux into bile during the first 60 min of reperfusion and at 24 h. Allopurinol (concentration 100 mg/kg) protected hepatocyte function as bile flow improved significantly in this group after 1 and 24 h of reperfusion compared with that of controls. Oxidative stress was also significantly attenuated in this group, as efflux of glutathione into bile was significantly higher in the ALL group (100 mg/kg) after 24 h but not after 1 h of reperfusion compared with that of controls. All given in a concentration 50 mg/kg had some, but a non-significant, effect. We conclude that biliary glutathione is an important marker of oxidative stress and may reflect the scavenging ability of the liver after ischemic injury. Significant correlation of bile flow with biliary glutathione during reperfusion indicates that oxidative stress is an important mechanism attenuating liver function after ischemia/reperfusion injury.

摘要

能量代谢恶化和氧化应激是缺血再灌注损伤的基本机制。在常温缺血/再灌注大鼠模型中,我们研究了别嘌呤醇(ALL)是否可以提高肝脏在缺血后的清除能力。在缺血和再灌注前给予ALL(浓度为100或50mg/kg),对照组给予安慰剂。在30分钟的基础期后,对肝中叶和左叶进行1小时的常温缺血,然后观察24小时。通过胆汁分泌评估肝脏整体功能,通过再灌注最初60分钟和24小时期间谷胱甘肽向胆汁中的流出量评估游离氧的产生。别嘌呤醇(浓度100mg/kg)保护肝细胞功能,因为与对照组相比,该组在再灌注1小时和24小时后胆汁流量显著改善。该组的氧化应激也显著减轻,因为与对照组相比,ALL组(100mg/kg)在再灌注24小时后谷胱甘肽向胆汁中的流出量显著更高,但在再灌注1小时后没有显著差异。浓度为50mg/kg的ALL有一定作用,但不显著。我们得出结论,胆汁中的谷胱甘肽是氧化应激的重要标志物,可能反映缺血性损伤后肝脏的清除能力。再灌注期间胆汁流量与胆汁谷胱甘肽的显著相关性表明,氧化应激是缺血/再灌注损伤后肝脏功能减弱的重要机制。

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