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异种胸腺移植后,异常的调节性和效应性T细胞功能易引发自身免疫。

Abnormal regulatory and effector T cell function predispose to autoimmunity following xenogeneic thymic transplantation.

作者信息

Fudaba Yasuhiro, Onoe Takashi, Chittenden Meredith, Shimizu Akira, Shaffer Juanita M, Bronson Roderick, Sykes Megan

机构信息

Department of Surgery, Transplantation Biology Research Center, Massachusetts General Hospital/Harvard Medical School, Boston, MA 02129, USA.

出版信息

J Immunol. 2008 Dec 1;181(11):7649-59. doi: 10.4049/jimmunol.181.11.7649.

Abstract

Porcine thymus grafts support robust murine and human thymopoiesis, generating a diverse T cell repertoire that is deleted of donor and host-reactive cells, achieving specific xenograft tolerance. Positive selection is mediated exclusively by the xenogeneic thymic MHC. Although thymectomized, T cell-depleted normal mice usually remain healthy following xenogeneic thymic transplantation, thymus-grafted congenitally athymic mice frequently develop multiorgan autoimmunity. We investigated the etiology of this syndrome by adoptively transferring lymphocyte populations from fetal pig thymus-grafted BALB/c nude mice to secondary BALB/c nude recipients. Fetal pig thymus-grafted nude mice generated normal numbers of CD25(+)Foxp3(+)CD4 T cells, but these cells lacked the capacity to block autoimmunity. Moreover, thymocytes and peripheral CD4(+)CD25(-) cells from fetal pig thymus-grafted nude mice, but not those from normal mice, induced autoimmunity in nude recipients. Injection of thymic epithelial cells from normal BALB/c mice into fetal pig thymus grafts reduced autoimmunity and enhanced regulatory function of splenocytes. Our data implicate abnormalities in postthymic maturation, expansion, and/or survival of T cells positively selected by a xenogeneic MHC, as well as incomplete intrathymic deletion of thymocytes recognizing host tissue-specific Ags, in autoimmune pathogenesis. Regulatory cell function is enhanced and negative selection of host-specific thymocytes may potentially also be improved by coimplantation of recipient thymic epithelial cells in the thymus xenograft.

摘要

猪胸腺移植可支持强大的小鼠和人类胸腺生成,产生多样化的T细胞库,其中供体和宿主反应性细胞被清除,从而实现特异性异种移植耐受。阳性选择仅由异种胸腺MHC介导。虽然胸腺切除、T细胞耗竭的正常小鼠在异种胸腺移植后通常保持健康,但胸腺移植的先天性无胸腺小鼠经常发生多器官自身免疫。我们通过将来自胎猪胸腺移植的BALB/c裸鼠的淋巴细胞群过继转移到二级BALB/c裸鼠受体中,研究了这种综合征的病因。胎猪胸腺移植的裸鼠产生了正常数量的CD25(+)Foxp3(+)CD4 T细胞,但这些细胞缺乏阻断自身免疫的能力。此外,来自胎猪胸腺移植裸鼠的胸腺细胞和外周CD4(+)CD25(-)细胞,而非正常小鼠的这些细胞,在裸鼠受体中诱导了自身免疫。将正常BALB/c小鼠的胸腺上皮细胞注射到胎猪胸腺移植中可降低自身免疫并增强脾细胞的调节功能。我们的数据表明,在自身免疫发病机制中,异种MHC阳性选择的T细胞在胸腺后成熟、扩增和/或存活方面存在异常,以及识别宿主组织特异性抗原的胸腺细胞在胸腺内的阴性选择不完全。通过在胸腺异种移植中共植入受体胸腺上皮细胞,可增强调节细胞功能,并可能改善宿主特异性胸腺细胞的阴性选择。

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