FasLgld(CD95L)突变受体中移植血管硬化明显减轻。同种异体抗体在慢性排斥反应发生中的作用。
Marked mitigation of transplant vascular sclerosis in FasLgld (CD95L) mutant recipients. The role of alloantibodies in the development of chronic rejection.
作者信息
Subbotin V, Sun H, Aitouche A, Salam A, Valdivia L A, Fung J J, Starzl T E, Rao A S
机构信息
Thomas E. Starzl Transplantation Institute and the Department of Pathology, University of Pittsburgh Medical Center, Pennsylvania 15213, USA.
出版信息
Transplantation. 1999 May 27;67(10):1295-300. doi: 10.1097/00007890-199905270-00001.
BACKGROUND
In the acute rejection of allografts, the interaction between Fas (CD95) and its ligand (FasL; CD95L) has been shown to be involved in mediating apoptotic cell death. The role, however, of these molecules in the pathogenesis of transplant vascular sclerosis is as yet undetermined. The present study was therefore designed to address this issue.
MATERIAL
C3H/HEJ FasLgld (FasL-; H2k) spontaneously mutant mice were used either as donors or recipients of aortic allografts; wild-type C57B1/6 (B6; H2b) were used as corresponding recipients or donors (n=6/group), respectively. Controls included aortas transplanted across appropriate allogeneic and syngeneic strain combinations. For histopathological evaluations, the grafts were harvested at day 40 after transplantation, at which time, splenocytes and sera were also obtained for mixed leukocyte reaction and complement-mediated microcytotoxicity assays, respectively.
RESULTS
Similar to aortas obtained from allogeneic controls, allografts harvested from FasL- -->B6 recipients had morphological evidence of chronic rejection characterized by circumferential intimal thickening with partial disruption of the elastic membranes. Correspondingly, heightened antidonor cellular reactivity was also witnessed in these recipients. On the contrary, B6 allografts harvested from the majority of C3H-->FasL- recipients exhibited marked preservation of aortic morphology. Although these recipients had diminished antidonor cellular proliferation, the titers of alloantibodies were markedly elevated.
CONCLUSION
The presence of FasL-expressing functional cytotoxic T cells is required for the pathogenesis of transplant vascular sclerosis. The significant reduction and/or absence of chronic rejection with the concomitant retention of antidonor humoral response in C3H FasL- recipients of B6 aortas prompt us to suggest that perhaps posttransplantation vasculopathy is initiated by cell-mediated cytotoxicity with its perpetuation facilitated by alloantibodies.
背景
在同种异体移植物的急性排斥反应中,Fas(CD95)与其配体(FasL;CD95L)之间的相互作用已被证明参与介导凋亡性细胞死亡。然而,这些分子在移植血管硬化发病机制中的作用尚未确定。因此,本研究旨在解决这一问题。
材料
C3H/HEJ FasLgld(FasL-;H2k)自发突变小鼠用作主动脉同种异体移植物的供体或受体;野生型C57B1/6(B6;H2b)分别用作相应的受体或供体(每组n = 6)。对照组包括跨适当的同种异体和同基因品系组合移植的主动脉。为了进行组织病理学评估,在移植后第40天收获移植物,此时还分别获取脾细胞和血清用于混合淋巴细胞反应和补体介导的微细胞毒性试验。
结果
与同种异体对照获得的主动脉相似,从FasL- -->B6受体收获的同种异体移植物有慢性排斥的形态学证据,其特征为圆周内膜增厚伴弹性膜部分破坏。相应地,在这些受体中也观察到抗供体细胞反应性增强。相反,从大多数C3H-->FasL-受体收获的B6同种异体移植物表现出主动脉形态的显著保留。尽管这些受体的抗供体细胞增殖减少,但同种异体抗体的滴度明显升高。
结论
表达FasL的功能性细胞毒性T细胞的存在是移植血管硬化发病机制所必需的。在B6主动脉的C3H FasL-受体中,慢性排斥反应显著减少和/或不存在,同时保留抗供体体液反应,这促使我们提出,也许移植后血管病变是由细胞介导的细胞毒性引发的,同种异体抗体促进了其持续存在。
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