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首页> 外文期刊>Xenotransplantation >Preconditioning with the prostacyclin analog epoprostenol and cobra venom factor prevents reperfusion injury and hyperacute rejection in discordant liver xenotransplantation.
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Preconditioning with the prostacyclin analog epoprostenol and cobra venom factor prevents reperfusion injury and hyperacute rejection in discordant liver xenotransplantation.

机译:用前列环素类似物前烯醇和眼镜蛇毒因子进行预处理可防止异种肝异种移植中的再灌注损伤和超急性排斥。

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摘要

Liver xenografts transplanted from guinea pig to rat suffer from inadequate organ reperfusion and initial dysfunction, despite sufficient complement depletion using cobra venom factor (CVF). Reperfusion injury is prevented when complement depleted donors are treated with the prostacyclin analog epoprostenol. Histological analysis suggests that epoprostenol preconditioning prevents post-reperfusion spasms of the intrahepatic branches of the portal vein and strongly reduces appearance of hepatocyte apoptosis shortly after transplantation. Cobra-venom-treated rats show breakdown of glucose metabolism and die in acute hypoglycaemia, whereas the additional application of epoprostenol restores gluconeogenesis. Consequently, recipient survival after epoprostenol and CVF treatment is significantly improved compared with animals receiving CVF only (5.1 +/- 2.6 h vs. 17.9 +/- 5.1 h). These data demonstrate that initial dysfunction of discordant liver grafts in the guinea-pig-to-rat species combination, can be overcome by the application of epoprostenol combined with CVF. Using this pharmacologic regimen, the discordant guinea-pig-to-rat model appears useful to study further questions concerning functional and immunological compatibility of a discordant liver xenograft.
机译:尽管使用眼镜蛇毒因子(CVF)充分补充了补体,但从豚鼠向大鼠移植的肝异种移植仍遭受器官再灌注不足和初始功能障碍。当用前列环素类似物依前列烯醇治疗补体耗尽的供体时,可防止再灌注损伤。组织学分析表明,前肾上腺素预处理可以防止移植后不久门静脉肝内分支的再灌注后痉挛,并大大减少肝细胞凋亡的出现。经眼镜蛇毒治疗的大鼠表现出葡萄糖代谢异常,并在急性低血糖症中死亡,而额外应用依泊汀醇可恢复糖异生。因此,与仅接受CVF的动物相比,依泊美汀和CVF治疗后的受体存活率显着提高(5.1 +/- 2.6 h与17.9 +/- 5.1 h)。这些数据表明,豚鼠-大鼠-大鼠物种组合中不协调的肝移植物最初的功能障碍可以通过将依普替诺醇与CVF组合使用来克服。使用这种药理学方案,不一致的豚鼠到大鼠模型似乎对于研究有关不一致的异种肝移植物的功能和免疫相容性的进一步问题很有用。

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