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带有自身反应性克隆的中间型TCR细胞是在小鼠中诱导同基因移植物抗宿主病的效应细胞。

Intermediate TCR cells with self-reactive clones are effector cells which induce syngeneic graft-versus-host disease in mice.

作者信息

Osman Y, Watanabe T, Kawachi Y, Sato K, Ohtsuka K, Watanabe H, Hashimoto S, Moriyama Y, Shibata A, Abo T

机构信息

Department of Immunology, Niigata University School of Medicine, Japan.

出版信息

Cell Immunol. 1995 Dec;166(2):172-86. doi: 10.1006/cimm.1995.9980.

Abstract

It has been established that, even after syngeneic bone marrow transplantation, animals treated with immunosuppressive drugs may suffer from graft-versus-host disease, showing autoimmune-like symptoms. Although the major effector cells are known to be T-cell subsets, detailed characterization of such T cells remains to be investigated. In the present study, we characterized them, especially as to whether they are thymus-derived T cells or extrathymic T cells, and how self-reactive clones were distributed among the above T-cell subsets. BALB/c mice (Mls-1b2a) were irradiated (9 Gy), subjected to bone marrow transplantation, and then treated with cyclosporin A (CsA) for 6 weeks. From 2 weeks after the cessation of CsA, these mice displayed signs of GVH disease. The major target organs included the liver and colon. Two-color staining for CD3 and IL-2R beta was applied to identify CD3-IL-2R beta+ NK cells, CD3-intermediate +IL-2R beta+ cells (i.e., intermediate CD3 or TCR cells of extrathymic origin) and CD3-high+IL-2R beta- cells (i.e., high CD3 cells of thymic origin). It was demonstrated that the major expanding lymphocytes were intermediate TCR cells and that self-reactive clones (V beta 3+ and V beta 11+ cells in this strain of mice) were confined to this population. Interestingly, these self-reactive clones had ability to respond to immobilized anti-V beta 3 and anti-V beta 11 mAbs. Liver MNC in mice with GVH disease which contained the highest proportion of intermediate TCR cells were able to mediate the adoptive transfer of GVH disease to other irradiated (6.5 Gy) mice. Intermediate TCR cells also showed potent cytotoxic activity against syngeneic leukemia cells. These results suggest that intermediate TCR cells are the major effector cells for the induction of syngeneic GVH disease.

摘要

已经确定,即使在同基因骨髓移植后,用免疫抑制药物治疗的动物仍可能患移植物抗宿主病,表现出自身免疫样症状。虽然已知主要效应细胞是T细胞亚群,但此类T细胞的详细特征仍有待研究。在本研究中,我们对它们进行了表征,特别是关于它们是胸腺来源的T细胞还是胸腺外T细胞,以及自身反应性克隆如何在上述T细胞亚群中分布。对BALB/c小鼠(Mls-1b2a)进行9 Gy照射,进行骨髓移植,然后用环孢素A(CsA)治疗6周。从停止使用CsA后2周起,这些小鼠表现出移植物抗宿主病的症状。主要靶器官包括肝脏和结肠。应用CD3和IL-2Rβ的双色染色来鉴定CD3-IL-2Rβ+NK细胞、CD3中间+IL-2Rβ+细胞(即胸腺外来源的中间CD3或TCR细胞)和CD3高+IL-2Rβ-细胞(即胸腺来源的高CD3细胞)。结果表明,主要扩增的淋巴细胞是中间TCR细胞,并且自身反应性克隆(该品系小鼠中的Vβ3+和Vβ11+细胞)局限于该群体。有趣的是,这些自身反应性克隆能够对固定化的抗Vβ3和抗Vβ11单克隆抗体作出反应。患有移植物抗宿主病的小鼠肝脏单个核细胞中中间TCR细胞比例最高,能够将移植物抗宿主病过继转移给其他经6.5 Gy照射的小鼠。中间TCR细胞对同基因白血病细胞也表现出强大的细胞毒活性。这些结果表明,中间TCR细胞是诱导同基因移植物抗宿主病的主要效应细胞。

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