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首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >Impairment of microcirculation in the early reperfusion period predicts the degree of graft pancreatitis in clinical pancreas transplantation.
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Impairment of microcirculation in the early reperfusion period predicts the degree of graft pancreatitis in clinical pancreas transplantation.

机译:再灌注早期的微循环障碍预示着胰腺移植在临床胰腺移植中的程度。

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BACKGROUND: Graft pancreatitis is thought to be induced by ischemia/reperfusion. Animal experiments have suggested that an impaired microcirculation is crucial in this process. We have therefore studied the relevance of microcirculation in clinical pancreas transplantation. METHODS: In 17 patients undergoing pancreas transplantation, tissue pO2 was monitored continuously by an electrode implanted into the pancreatic tail. A catheter was inserted in the distal part of the splenic vein of the pancreas graft. After reperfusion blood samples were taken from this catheter and blood flow was measured by the venous outflow method. The degree of graft pancreatitis was assessed by peak-C-reactive protein (CRP) defined as highest CRP within 3 days after transplantation. RESULTS: Tissue pO2 increased within 5 min after reperfusion. Thereafter, in most patients a transient decrease was noted, indicating impairment of nutritive perfusion. During this period there was an increasing negative correlation between peak-CRP and tissue pO2 which was highly significant at 60 min after reperfusion (r=-0.70, P<0.002). Also donor age correlated significantly with peak-CRP (r=0.64, P<0.005) and to a somewhat lesser extend with tissue pO2 60 min after reperfusion (r= -0.55, P<0.03). CONCLUSION: These data show that the degree of organ damage in clinical pancreas transplantation is directly related to an impairment of microcirculation in the early reperfusion period. These data also support the idea that grafts from older donors have a higher probability to develop graft pancreatitis and that this might be due to an increased incidence of microcirculatory disturbances in these organs.
机译:背景:移植物胰腺炎被认为是由缺血/再灌注引起的。动物实验表明,微循环障碍在此过程中至关重要。因此,我们研究了微循环在临床胰腺移植中的相关性。方法:在17例接受胰腺移植的患者中,通过植入胰尾的电极连续监测组织中的pO2。将导管插入胰腺移植物脾静脉的远端。再灌注后,从该导管中取血样,并通过静脉流出法测量血流量。移植物胰腺炎的程度通过峰值C反应蛋白(CRP)评估,该蛋白定义为移植后3天内的最高CRP。结果:再灌注后5分钟内组织pO2增加。此后,在大多数患者中注意到短暂的减少,表明营养灌注受损。在此期间,CRP峰值与组织pO2之间的负相关性增加,在再灌注后60分钟时高度显着(r = -0.70,P <0.002)。同样,供体年龄与CRP峰值显着相关(r = 0.64,P <0.005),并且在再灌注后60分钟时,随着组织pO2的延长程度略有降低(r = -0.55,P <0.03)。结论:这些数据表明,临床胰腺移植中器官损伤的程度与再灌注早期微循环的损害直接相关。这些数据也支持这样的想法,即来自较老供体的移植物发生胰腺炎的可能性更高,这可能是由于这些器官中微循环障碍的发生率增加。

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