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Survivin 在器官移植损伤中的意外作用。

An unanticipated role for survivin in organ transplant damage.

机构信息

Centro Ricerche Trapianti, "Chiara Cucchi de Alessandri e Gilberto Crespi", IRCCS-Istituto di Ricerche Farmacologiche Mario Negri, Ranica, Bergamo, Italy.

出版信息

Am J Transplant. 2014 May;14(5):1046-60. doi: 10.1111/ajt.12677. Epub 2014 Apr 14.

DOI:10.1111/ajt.12677
PMID:24731002
Abstract

Ischemia/reperfusion (I/R) injury is a major determinant of graft survival in kidney transplantation. Survivin, an inhibitor of apoptosis that participates in the control of mitosis and cell cycle progression, has been implicated in renal protection and repair after I/R injury; however, no study has been performed in the transplant setting. We investigated the role of survivin in modulating posttransplant I/R injury in syngeneic and allogeneic kidney grafts, and studied whether protection from I/R injury impacted on the recipient immune system, on chronic allograft nephropathy and rejection. We used genetically engineered mice with survivin haploinsufficiency and WT mice in which survivin over-expression was induced by gene-delivery. Survivin haploinsufficiency in syngeneic grafts was associated with exuberant I/R tissue injury, which triggered inflammation eventually resulting in graft loss. Conversely, survivin over-expression in the grafts minimized I/R injury and dysfunction in syngeneic grafts and in a clinically relevant fully MHC-mismatched allogeneic combination. In the latter, survivin over-expression translated into limited anti-donor adaptive immune response and less long-term allograft injury with protection from renal parenchymal damage. Our data support survivin over-expression in the graft as a novel target for protocols aimed at limiting tissue damage at the time of transplant ultimately modulating the recipient immune system.

摘要

缺血/再灌注 (I/R) 损伤是肾移植中移植物存活的主要决定因素。存活素是一种凋亡抑制剂,参与有丝分裂和细胞周期进程的控制,与 I/R 损伤后的肾脏保护和修复有关;然而,在移植环境中尚未进行研究。我们研究了存活素在调节同种异体和异体肾移植后 I/R 损伤中的作用,并研究了 I/R 损伤的保护是否会影响受者的免疫系统、慢性移植肾肾病和排斥反应。我们使用存活素杂合不足的基因工程小鼠和通过基因传递诱导存活素过表达的 WT 小鼠。同种异体移植物中存活素杂合不足与过度的 I/R 组织损伤相关,这最终引发炎症导致移植物丧失。相反,移植物中存活素的过表达可最大限度地减少同种异体移植物的 I/R 损伤和功能障碍,并且在临床相关的完全 MHC 错配的同种异体组合中也是如此。在后一种情况下,存活素过表达导致对供体的适应性免疫反应有限,并且长期移植物损伤较少,从而保护肾实质免受损伤。我们的数据支持将移植物中的存活素过表达作为旨在限制移植时组织损伤的新靶点,最终调节受者的免疫系统。

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Front Immunol. 2021 Aug 6;12:710904. doi: 10.3389/fimmu.2021.710904. eCollection 2021.
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