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首页> 外文期刊>Transplantation Proceedings >Hepatic artery reconstruction prevents ischemic graft injury, inhibits graft rejection, and mediates long-term graft acceptance in rat liver transplantation
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Hepatic artery reconstruction prevents ischemic graft injury, inhibits graft rejection, and mediates long-term graft acceptance in rat liver transplantation

机译:肝动脉重建可防止缺血性移植物损伤,抑制移植物排斥并介导大鼠肝移植中的长期移植物接受

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Background: Hepatic artery (HA) reconstruction is performed in the clinical liver transplantation. Methods: We assessed the importance of HA reconstruction in the success of liver transplantation. Orthotopic liver transplantation was performed without immunosspression from Lewis (RT1l) to Lewis rats (syngeneic transplantation) as well as Lewis to BN (RT1n) rats (allogeneic transplantation) with or without HA reconstruction. We examined graft function, pathology, and mRNA levels using DNA arrays in both arterialized and nonarterialized liver grafts. Results: In Lewis-to-Lewis syngeneic grafts, both the arterialized and nonarterialized grafts survived 120 days with normal graft function. lnfiltration of CD3+ T cells and CD68+ macrophages, marked bile duct proliferation with apoptotic epithelial cells, and expansion and increasing fibrosis of portal areas were evident in the nonarterialized grafts at day 120, although preservation of architecture was noted in the arterialized grafts. DNA array analysis of nonarterialized syngeneic grafts demonstrated the upregulation of mRNA of cell death-related proteins, cell cycle-related proteins, and inflammation-related proteins than those in arterialized grafts. Moreover, the arterialized Lewis-to-BN allogeneic grafts could survive for a long time with less severe graft dysfunction than those in non-arterialized allogeneic grafts. Conclusions: HA reconstruction in liver transplantation inhibited hypoxic injury and subsequent inflammation and bile duct proliferation, prevented the augmentation of T-cell-and antibody-mediated rejection, and mediated long-term graft acceptance. HA reconstruction is essential factor in the success of liver transplantation.
机译:背景:在临床肝移植​​中进行肝动脉(HA)重建。方法:我们评估了HA重建在肝移植成功中的重要性。进行原位肝移植时,Lewis(RT11)不对Lewis大鼠进行免疫抑制(同基因移植),Lewis对BN(RT1n)大鼠进行同种异体移植(同种异体移植),无论是否进行HA重建。我们在动脉和非动脉肝移植物中均使用DNA阵列检查了移植物的功能,病理学和mRNA水平。结果:在Lewis-Lewis同基因移植物中,动脉化和非动脉化移植物均存活> 120天,且移植物功能正常。在第120天时,未动脉化的移植物中可见CD3 + T细胞和CD68 +巨噬细胞的浸润,明显的胆管增殖与凋亡的上皮细胞,以及门静脉区域的扩张和纤维化增加,尽管在动脉化移植物中注意到了结构的保留。非动脉化同系移植物的DNA阵列分析表明,与动脉化移植物相比,细胞死亡相关蛋白,细胞周期相关蛋白和炎症相关蛋白的mRNA上调。此外,动脉化的Lewis-BN同种异体移植物可以存活较长时间,而移植功能障碍的严重程度要低于非动脉化的同种异体移植物。结论:肝移植中的HA重建可抑制缺氧损伤及其后的炎症和胆管增殖,阻止T细胞和抗体介导的排斥反应的增强以及长期移植物的接受。 HA重建是肝移植成功的关键因素。

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