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一种包含自身反应性细胞的不寻常的α/β T细胞谱系。

An unusual lineage of alpha/beta T cells that contains autoreactive cells.

作者信息

von Boehmer H, Kirberg J, Rocha B

机构信息

Basel Institute for Immunology, Switzerland.

出版信息

J Exp Med. 1991 Nov 1;174(5):1001-8. doi: 10.1084/jem.174.5.1001.

Abstract

In male mice that express a transgenic alpha/beta T cell receptor (TCR) specific for a male-specific peptide presented by class I Db major histocompatibility complex (MHC) molecules, we describe an unusual lineage of alpha/beta T cells that are thymus dependent but do not require selection by Db MHC molecules on thymic epithelium in the absence of the specific peptide (positive selection). These cells express the transgenic alpha/beta TCR and have the CD4-8- or CD4-8low phenotype. Cells with the latter phenotype are only detected when hemopoietic cells express both the male-specific peptide as well as Db MHC molecules. In fact, these cells are autoreactive, as they expand relatively slowly after transfer into male nude mice. Also in male but not female alpha/beta TCR transgenic mice, the CD8+ cells with the transgenic TCR bear the Pgp1 marker characteristic of mature T cells activated by antigen. CD4-8- as well as CD4-8low cells do not respond significantly when cultured with male stimulator cells but proliferate vigorously when stimulated by TCR antibodies. By this latter criterion, cells in the periphery of male alpha/beta TCR transgenic mice differ from mature male-specific T cells from female alpha/beta TCR transgenic, which become intrinsically anergic when transferred into male nude mice and cannot be stimulated significantly by TCR antibodies. Thus, intrathymic deletion does not eliminate all autoreactive T cells and it is possible that cells with an apparently "benign" autoreactivity may be involved in certain forms of autoimmunity.

摘要

在表达针对由I类Db主要组织相容性复合体(MHC)分子呈递的雄性特异性肽的转基因α/βT细胞受体(TCR)的雄性小鼠中,我们描述了一种不寻常的α/βT细胞谱系,它们依赖胸腺,但在没有特异性肽(阳性选择)的情况下不需要胸腺上皮细胞上的Db MHC分子进行选择。这些细胞表达转基因α/βTCR,具有CD4 - 8 - 或CD4 - 8low表型。只有当造血细胞同时表达雄性特异性肽和Db MHC分子时,才会检测到具有后一种表型的细胞。事实上,这些细胞是自身反应性的,因为它们在转移到雄性裸鼠后增殖相对缓慢。同样在雄性而非雌性α/βTCR转基因小鼠中,带有转基因TCR的CD8 + 细胞带有被抗原激活的成熟T细胞特有的Pgp1标记。CD4 - 8 - 以及CD4 - 8low细胞在用雄性刺激细胞培养时反应不明显,但在用TCR抗体刺激时会大量增殖。根据后一个标准,雄性α/βTCR转基因小鼠外周的细胞与雌性α/βTCR转基因小鼠的成熟雄性特异性T细胞不同,后者转移到雄性裸鼠后会内在性无反应,并且不能被TCR抗体显著刺激。因此,胸腺内缺失并不能消除所有自身反应性T细胞,并且具有明显“良性”自身反应性的细胞可能参与某些形式的自身免疫。

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