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从异位大鼠心脏同种异体移植物中分离的淋巴细胞的热休克蛋白反应性

Heat shock protein reactivity of lymphocytes isolated from heterotopic rat cardiac allografts.

作者信息

Moliterno R, Valdivia L, Pan F, Duquesnoy R J

机构信息

Division of Transplantation Pathology, Pittsburgh Transplant Institute, University of Pittsburgh Medical Center, Pennsylvania 15261.

出版信息

Transplantation. 1995 Feb 27;59(4):598-604.

PMID:7878764
Abstract

Although it is well known that cellular rejection is mediated by alloreactive lymphocytes, several investigators, including our group, have shown that such cells are a rather small proportion of the T cell infiltrate of the alolograft. We have therefore postulated that graft-infiltrating lymphocytes must recognize other antigens. Since heat shock protein (hsp)-specific lymphocytes have been shown to participate in several autoimmune diseases and in tumor immunity, we hypothesized that hsp-reactive lymphocytes are involved with allograft rejection. This hypothesis was tested with a rat model of heterotopic MHC-incompatible cardiac allografts (ACI into Lewis), whereby graft-infiltrating lymphocytes and spleen cells were tested in vitro with different recombinant mycobacterial hsp preparations. As expected, allograft lymphocytes showed proliferative responses to irradiated spleen cells from the donor. This proliferation was markedly augmented by hsp65 (3-fold) and hsp70 (5-fold), whereas hsp10 and the protein control ovalbumin had no effect. Proliferation of allograft lymphocytes to hsp in context with syngeneic splenocytes as antigen-presenting cells (APC) was seen primarily if small quantities of IL-2 had been added to the cultures. In contrast, hsp-specific proliferation was never observed with syngraft lymphocytes, even after addition of IL-2. Spleen cells from allograft and syngraft recipients showed hsp augmentation of alloproliferation, but the magnitude was less than that with allograft lymphocytes. Kinetic studies showed that hsp-reactive lymphocytes first appeared in the allograft on day 3 posttransplant. Tacrolimus immunosuppression of transplant rejection prevented the appearance of hsp-reactive lymphocytes in allografts. Culture conditions have been established to generate hsp65- and hsp70-specific T lymphocyte lines and clones from allograft-infiltrating cells. These cultured cells exhibited hsp reactivity only in context with self-APC, and this was augmented by small amounts of IL-2. These data provide strong evidence for the involvement of hsp-reactive lymphocytes in allograft rejection. We propose the concept that during rejection tissue stress induced by alloreactive effector lymphocytes promotes the recruitment and activation of hsp-reactive lymphocytes, especially in the presence of IL-2 released into the allogeneic environment of the transplant. These hsp-reactive T cells may play a role in the immune cascade of the inflammatory process of transplant rejection.

摘要

尽管众所周知细胞排斥是由同种异体反应性淋巴细胞介导的,但包括我们小组在内的一些研究人员已经表明,这类细胞在同种异体移植的T细胞浸润中只占相当小的比例。因此,我们推测移植浸润淋巴细胞必定识别其他抗原。由于热休克蛋白(hsp)特异性淋巴细胞已被证明参与多种自身免疫性疾病和肿瘤免疫,我们假设hsp反应性淋巴细胞与同种异体移植排斥有关。我们用异位MHC不相容心脏同种异体移植大鼠模型(ACI品系大鼠心脏移植到Lewis品系大鼠)对这一假设进行了验证,在此模型中,体外使用不同的重组分枝杆菌hsp制剂对移植浸润淋巴细胞和脾细胞进行检测。正如预期的那样,同种异体移植淋巴细胞对来自供体的经辐照脾细胞表现出增殖反应。hsp65(3倍)和hsp70(5倍)能显著增强这种增殖,而hsp10和蛋白质对照卵清蛋白则没有作用。当以同基因脾细胞作为抗原呈递细胞(APC)时,同种异体移植淋巴细胞对hsp的增殖反应主要出现在向培养物中添加少量白细胞介素-2之后。相比之下,即使添加白细胞介素-2,同基因移植淋巴细胞也从未出现hsp特异性增殖。同种异体移植和同基因移植受体的脾细胞均显示hsp增强了同种异体增殖,但增强幅度小于同种异体移植淋巴细胞。动力学研究表明,hsp反应性淋巴细胞在移植后第3天首次出现在同种异体移植中。他克莫司对移植排斥的免疫抑制作用可阻止同种异体移植中hsp反应性淋巴细胞的出现。现已建立培养条件,从移植浸润细胞中生成hsp65和hsp70特异性T淋巴细胞系和克隆。这些培养细胞仅在与自身APC共同作用时表现出hsp反应性,并且少量白细胞介素-2可增强这种反应性。这些数据为hsp反应性淋巴细胞参与同种异体移植排斥提供了有力证据。我们提出这样一个概念,即在排斥反应过程中,同种异体反应性效应淋巴细胞诱导的组织应激促进了hsp反应性淋巴细胞的募集和激活,特别是在移植的异基因环境中释放白细胞介素-2的情况下。这些hsp反应性T细胞可能在移植排斥炎症过程的免疫级联反应中发挥作用。

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