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Short-term alanyl-glutamine dipeptide pretreatment in liver ischemia-reperfusion model: Effects on microcirculation and antioxidant status in rats.

机译:肝缺血-再灌注模型中短期丙氨酰-谷氨酰胺二肽预处理:对大鼠微循环和抗氧化状态的影响。

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BACKGROUND & AIMS: Ischemia-reperfusion (I-R) injury is responsible for the morbidity associated with liver surgery. Production of toxic free radicals influences the microcirculation. The aim of our study was to examine the effect of glutamine (Gln) supplementation-adminstered in alanyl-glutamine dipeptide form-on liver function, immuno/histopathology and the oxidative state of the liver after injury. METHODS: Two-hundred and fifty grams male Wistar rats underwent normothermic, 60min, segmental liver ischemia followed by 6h of reperfusion. The animals (n=45) were divided into three groups: sham operated, I-R and parenteral Gln pretreatment. Hepatic microcirculation was monitored by laser Doppler flowmetry. At the 6h of reperfusion, histological alterations, TUNEL reaction, active caspase-3 reaction, serum and liver tissue antioxidant levels, serum ALAT, ASAT and TNF-alpha levels were measured. RESULTS: Upon reperfusion, the Gln group had significantly (p<0.05) higher flow rates than the I-R group and, at the end of the 6h of reperfusion, significantly (p<0.05) lower serum ALAT and ASAT levels. The liver chemiluminescent intensity was lower, free SH-groups were elevated, while the reducing power was decreased in the Gln-pretreated group. Positive staining for caspase-3 after Gln pretreatment was significantly increased in contrast to the control tissues. CONCLUSION: Glutamine pretreatment is beneficial in supporting hepatic microcirculation and can prevent hepatocellular necrosis in liver reperfusion injury.
机译:背景与目的:缺血再灌注(I-R)损伤是与肝脏手术相关的发病率的原因。有毒自由基的产生影响微循环。我们研究的目的是研究以谷氨酰胺-谷氨酰胺二肽形式补充谷氨酰胺(Gln)对肝功能,免疫/组织病理学和损伤后肝脏氧化状态的影响。方法:250只雄性Wistar大鼠在60min的节段性肝缺血中进行常温放疗,然后再灌注6h。将动物(n = 45)分为三组:假手术,IR和肠胃外Gln预处理。通过激光多普勒血流仪监测肝微循环。在再灌注的6h,测量组织学改变,TUNEL反应,活性caspase-3反应,血清和肝组织抗氧化剂水平,血清ALAT,ASAT和TNF-α水平。结果:再灌注后,Gln组的血流量显着高于(p <0.05)I-R组,在再灌注6h结束时,血清ALAT和ASAT水平显着降低(p <0.05)。 Gln预处理组的肝脏化学发光强度较低,游离SH-基团升高,而还原能力降低。与对照组织相比,Gln预处理后caspase-3的阳性染色显着增加。结论:谷氨酰胺预处理有利于支持肝微循环,可预防肝再灌注损伤中的肝细胞坏死。

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