J Clin Invest. 2014 Jun;124(6):2348-54. doi: 10.1172/JCI72273. Epub 2014 Jun 2.
Improvements in clinical care and immunosuppressive medications have positively affected outcomes following kidney transplantation, but graft survival remains suboptimal, with half-lives of approximately 11 years. Late graft loss results from a confluence of processes initiated by ischemia-reperfusion injury and compounded by effector mechanisms of uncontrolled alloreactive T cells and anti-HLA antibodies. When combined with immunosuppressant toxicity, post-transplant diabetes and hypertension, and recurrent disease, among other factors, the result is interstitial fibrosis, tubular atrophy, and graft failure. Emerging evidence over the last decade unexpectedly identified the complement cascade as a common thread in this process. Complement activation and function affects allograft injury at essentially every step. These fundamental new insights, summarized herein, provide the foundation for testing the efficacy of various complement antagonists to improve kidney transplant function and long-term graft survival.
临床护理和免疫抑制药物的改进对肾移植后的结果产生了积极影响,但移植物的存活率仍然不理想,半衰期约为 11 年。晚期移植物丢失是由缺血再灌注损伤引发的一系列过程以及未受控制的同种反应性 T 细胞和抗 HLA 抗体的效应机制共同作用的结果。当与免疫抑制剂毒性、移植后糖尿病和高血压以及复发性疾病等因素相结合时,其结果是间质纤维化、肾小管萎缩和移植物衰竭。过去十年中的新出现的证据出人意料地将补体级联反应确定为这一过程中的共同线索。补体的激活和功能几乎在每个环节都影响同种异体移植物的损伤。本文总结了这些基本的新见解,为测试各种补体拮抗剂的疗效提供了基础,以改善肾移植功能和长期移植物存活率。
