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环孢素对移植耐受的影响:白细胞介素-2的作用

Effects of cyclosporine on transplant tolerance: the role of IL-2.

作者信息

Kang H G, Zhang D, Degauque N, Mariat C, Alexopoulos S, Zheng X X

机构信息

Harvard Medical School, Transplant Research Center, Beth Israel Deaconess Medical Center, Boston, MA, USA.

出版信息

Am J Transplant. 2007 Aug;7(8):1907-16. doi: 10.1111/j.1600-6143.2007.01881.x.

DOI:10.1111/j.1600-6143.2007.01881.x
PMID:17617853
Abstract

Allograft(dagger) transplant outcome, rejection or tolerance, depends upon striking a balance between the pertinent cytopathic and regulatory T cells. The drug cyclosporine is a widely used immunosuppressive agent among transplant recipients. Previous studies have demonstrated that cyclosporine blocks apoptosis of activated T cells and the ability of costimulation blockade based regimens to create peripheral transplant tolerance. We now test the hypothesis that the mechanism by which cyclosporine blocks tolerance induction is IL-2 dependent, and linked to a detrimental effect upon T(reg) function. Our study demonstrates that cyclosporine blocks IL-2 gene expression and activation induced cell death (AICD) of alloreactive T effector cells. We also show that cyclosporine abolishes the beneficial effects of a donor specific transfusion (DST) plus anti-CD154 monoclonal antibody (alpha CD154) regimen on enhanced T(regs) function and allograft tolerance induction. Interestingly, provision of IL-2/Fc, a long-lived form of IL-2, completely reverses the detrimental effects of this adjunctive cyclosporine treatment on AICD of alloreactive T effectors, T(regs) function and tolerance induction. Furthermore, in a MHC mismatched islet allograft model, the combination of cyclosporine with IL-2/Fc permitted long-term allograft survival and induced alloantigen specific allograft tolerance. The combination of IL-2/Fc and cyclosporine treatment may provide a new clinical strategy to promote transplant tolerance.

摘要

同种异体移植(†)的结果,无论是排斥还是耐受,都取决于在相关的细胞病变性T细胞和调节性T细胞之间取得平衡。环孢素是移植受者中广泛使用的免疫抑制剂。先前的研究表明,环孢素可阻断活化T细胞的凋亡以及基于共刺激阻断方案产生外周移植耐受的能力。我们现在检验以下假设:环孢素阻断耐受诱导的机制是IL-2依赖性的,并且与对Treg功能的有害作用有关。我们的研究表明,环孢素可阻断IL-2基因表达以及同种异体反应性T效应细胞的活化诱导细胞死亡(AICD)。我们还表明,环孢素消除了供体特异性输血(DST)加抗CD154单克隆抗体(αCD154)方案对增强Tregs功能和同种异体移植耐受诱导的有益作用。有趣的是,提供IL-2/Fc(一种长效形式的IL-2)可完全逆转这种辅助性环孢素治疗对同种异体反应性T效应细胞的AICD、Tregs功能和耐受诱导的有害作用。此外,在MHC不匹配的胰岛同种异体移植模型中,环孢素与IL-2/Fc的组合可使同种异体移植长期存活并诱导同种抗原特异性同种异体移植耐受。IL-2/Fc与环孢素治疗的组合可能为促进移植耐受提供一种新的临床策略。

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