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胸腺细胞介导的器官同种异体移植特异性无反应性的转移。胸腺细胞转移导致的特异性无反应性。

Transfer of specific unresponsiveness to organ allografts by thymocytes. Specific unresponsiveness by thymocyte transfer.

作者信息

Hendry W S, Tilney N L, Baldwin W M, Graves M J, Milford E, Strom T B, Carpenter C B

出版信息

J Exp Med. 1979 May 1;149(5):1042-55. doi: 10.1084/jem.149.5.1042.

Abstract

Prolonged survival of vascularized organ allografts has been produced in unmodified inbred rats by transfer of thymocytes from enhanced, engrafted, syngeneic animals. For these thymocytes to increase significantly the survival of test allografts they must be harvested 6-9 d after transplantation. Thymectomy of the enhanced, engrafted animals during the same critical period causes acute rejection of othewise long surviving grafts. For optimal effect, the enhanced thymocyte donor must be actively and passively immunized and receive a cardiac allograft. The necessity for erythrocytes in the initial active immunization regimen is noted. Additionally, the antigenic specificity of the suppressor effect has been established with two histoincompatible donor rat strains. Cellular and humoral host responses mounted by test graft recipients after thymocyte transfer from enhanced, engrafted donors are different from those mounted either by unmodifed animals acutely rejecting their grafts or by enhanced rats bearing well-functioning grafts. Numbers of T lymphocytes are reduced in the grafted hearts and in the spleens of test graft recipients, a finding paralleled by the complete absence of specific direct lymphocyte-mediated cytotoxicity. In contrast, cytotoxic antibody production, although delayed, is increased in magnitude, peaking around the time of graft rejection. These studies provide evidence that different biological manipulations can modify separate pathways in the complex cellular and humoral responses towards organ allografts. They demonstrate that cellular immunity is critically involved in immunological enhancement of vascularized organ allografts, a phenomenon hitherto considered primarily humoral. It seems clear that cells with suppressor activity are present within the thymus during the early phases of immunological enhancement.

摘要

通过移植来自经过增强、移植的同基因动物的胸腺细胞,在未经修饰的近交系大鼠中实现了血管化器官同种异体移植的长期存活。为了使这些胸腺细胞显著提高测试同种异体移植的存活率,必须在移植后6 - 9天收获它们。在同一关键时期对经过增强、移植的动物进行胸腺切除术会导致原本长期存活的移植物急性排斥。为了达到最佳效果,增强的胸腺细胞供体必须进行主动和被动免疫,并接受心脏同种异体移植。注意到在初始主动免疫方案中红细胞的必要性。此外,已用两种组织不相容的供体大鼠品系确定了抑制作用的抗原特异性。从经过增强、移植的供体转移胸腺细胞后,测试移植物受体产生的细胞和体液宿主反应不同于未经修饰的动物急性排斥其移植物时产生的反应,也不同于带有功能良好移植物的增强大鼠产生的反应。移植心脏和测试移植物受体脾脏中的T淋巴细胞数量减少,这一发现与完全不存在特异性直接淋巴细胞介导的细胞毒性情况相似。相比之下,细胞毒性抗体的产生虽然延迟,但幅度增加,在移植物排斥时达到峰值。这些研究提供了证据,表明不同的生物学操作可以改变针对器官同种异体移植的复杂细胞和体液反应中的不同途径。它们表明细胞免疫在血管化器官同种异体移植的免疫增强中起关键作用,这一现象迄今主要被认为是体液性的。显然,在免疫增强的早期阶段,胸腺中存在具有抑制活性的细胞。

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