Lin H, Bolling S F, Linsley P S, Wei R Q, Gordon D, Thompson C B, Turka L A
Department of Surgery, University of Michigan, Ann Arbor 48109.
J Exp Med. 1993 Nov 1;178(5):1801-6. doi: 10.1084/jem.178.5.1801.
Allograft rejection is a T cell-dependent process. Productive T cell activation by antigen requires antigen engagement of the T cell receptor as well as costimulatory signals delivered through other T cell surface molecules such as CD28. Engagement of CD28 by its natural ligand B7 can be blocked using a soluble recombinant fusion protein, CTLA4Ig. Administration of CTLA4Ig blocks antigen-specific immune responses in vitro and in vivo, and we have shown that treatment of rats with a 7-d course of CTLA4Ig at the time of transplantation leads to prolonged survival of cardiac allografts (median 30 d), although most grafts are eventually rejected. Here, we have explored additional strategies employing CTLA4Ig in order to achieve long-term allograft survival. Our data indicate that donor-specific transfusion (DST) plus CTLA4Ig can provide effective antigen-specific immunosuppression. When DST is administered at the time of transplantation followed by a single dose of CTLA4Ig 2 d later, all animals had long-term graft survival (> 60 d). These animals had delayed responses to donor-type skin transplants, compared with normal rejection responses to third-party skin transplants. Furthermore, donor-matched second cardiac allografts were well tolerated with minimal histologic evidence of rejection. These data indicate that peritransplant use of DST followed by subsequent treatment with CTLA4Ig can induce prolonged, often indefinite, cardiac allograft acceptance. These results may be clinically applicable for cadaveric organ and tissue transplantation in humans.
同种异体移植排斥是一个T细胞依赖性过程。抗原介导的有效的T细胞激活需要T细胞受体与抗原结合,以及通过其他T细胞表面分子(如CD28)传递的共刺激信号。其天然配体B7与CD28的结合可使用可溶性重组融合蛋白CTLA4Ig来阻断。给予CTLA4Ig可在体外和体内阻断抗原特异性免疫反应,并且我们已经表明,在移植时用CTLA4Ig对大鼠进行为期7天的治疗可使心脏同种异体移植物的存活时间延长(中位数为30天),尽管大多数移植物最终会被排斥。在此,我们探索了采用CTLA4Ig的其他策略以实现同种异体移植物的长期存活。我们的数据表明,供体特异性输血(DST)加CTLA4Ig可提供有效的抗原特异性免疫抑制。在移植时给予DST,随后在2天后给予单剂量的CTLA4Ig,所有动物的移植物均长期存活(> 60天)。与对第三方皮肤移植的正常排斥反应相比,这些动物对供体类型皮肤移植的反应延迟。此外,与供体匹配的第二次心脏同种异体移植耐受性良好,排斥的组织学证据极少。这些数据表明,移植时使用DST随后用CTLA4Ig进行后续治疗可诱导心脏同种异体移植物长期、通常是无限期的接受。这些结果可能在临床上适用于人类尸体器官和组织移植。