Stadlbauer T H, Schaub M, Korom S, Onodera K, Sayegh M H, Kupiec-Weglinski J W
Harvard Medical School, and Department of Surgery, Brigham and Women's Hospital, Boston, Massachusetts 02115, USA.
Transplantation. 1997 Dec 27;64(12):1816-22. doi: 10.1097/00007890-199712270-00032.
Peripheral and central immune mechanisms contribute to the induction of tolerance in acute rejection rodent transplant models after systemic administration of CTLA4Ig and intrathymic infusion of donor alloantigen, respectively. We have investigated the effects of CTLA4Ig-induced blockade of CD28-B7 T-cell co-stimulation in conjunction with intrathymic immunomodulation on cellular and humoral immune responses leading to accelerated rejection of cardiac allografts in presensitized rats.
Lewis rats were challenged with Wistar-Furth (WF) skin transplants, followed 7 days later by transplantation of WF hearts. These cardiac allografts were rejected in a fulminant manner in <24 hr. A single infusion of human CTLA4Ig (0.5 mg/rat i.v.) at the time of cardiac engraftment (day 0) did not affect accelerated rejection. Intrathymic injection of WF spleen cells (2x10[7]) at the time of skin transplantation (day -7) abrogated <24-hr rejection and extended cardiac allograft survival to 6.6+/-0.6 days. Moreover, intrathymic host immunomodulation combined with administration of human CTLA4Ig (days 0-14, every other day) extended cardiac allograft survival synergistically to 27.7+/-7.5 days, and immunomodulation combined with murine CTLA4Ig extended survival to >42.5+/-4.8 days. The prolongation of allograft survival required the blockade of both B7-1 and B7-2 ligands and was accompanied by reduction of host proliferative responses (mixed lymphocyte response) and depression of anti-donor cytotoxic T-cell generation/function (lymphocyte-mediated cytotoxicity). CTLA4Ig therapy did not affect the strong systemic IgM and IgG alloantibody response seen otherwise after intrathymic immunomodulation.
CTLA4Ig enhances the effects of intrathymic donor-type cell infusion in sensitized rat recipients of cardiac allografts, indicating that "peripheral" blockade of CD28-B7 T-cell co-stimulation synergizes with the "central" immunosuppressive effects of intrathymic immunomodulation.
在急性排斥反应的啮齿动物移植模型中,外周和中枢免疫机制分别在全身给予CTLA4Ig和胸腺内输注供体同种异体抗原后诱导免疫耐受。我们研究了CTLA4Ig诱导的CD28 - B7 T细胞共刺激阻断联合胸腺内免疫调节对致敏大鼠心脏同种异体移植加速排斥反应中细胞和体液免疫反应的影响。
用Wistar - Furth(WF)皮肤移植对Lewis大鼠进行攻击,7天后进行WF心脏移植。这些心脏同种异体移植在不到24小时内以暴发性方式被排斥。在心脏植入时(第0天)单次静脉注射人CTLA4Ig(0.5mg/大鼠)不影响加速排斥反应。在皮肤移植时(第 - 7天)胸腺内注射WF脾细胞(2×10⁷)消除了不到24小时的排斥反应,并将心脏同种异体移植存活期延长至6.6±0.6天。此外,胸腺内宿主免疫调节联合人CTLA4Ig给药(第0 - 14天,隔日一次)协同将心脏同种异体移植存活期延长至27.7±7.5天,免疫调节联合鼠CTLA4Ig将存活期延长至>42.5±4.8天。同种异体移植存活期的延长需要同时阻断B7 - 1和B7 - 2配体,并伴有宿主增殖反应(混合淋巴细胞反应)的降低和抗供体细胞毒性T细胞生成/功能(淋巴细胞介导的细胞毒性)的抑制。CTLA4Ig治疗不影响胸腺内免疫调节后出现的强烈全身IgM和IgG同种异体抗体反应。
CTLA4Ig增强了致敏大鼠心脏同种异体移植受体胸腺内供体类型细胞输注的效果,表明CD28 - B7 T细胞共刺激的“外周”阻断与胸腺内免疫调节的“中枢”免疫抑制作用协同。
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