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针对一种细胞内细菌的细胞介导免疫的H-2限制:效应T细胞对与H-21区域编码的自身标记相关的李斯特菌抗原具有特异性。

H-2 restriction of cell-mediated immunity to an intracellular bacterium: effector T cells are specific for Listeria antigen in association with H-21 region-coded self-markers.

作者信息

Zinkernagel R M, Althage A, Adler B, Blanden R V, Davidson W F, Kees U, Dunlop M B, Shreffler D C

出版信息

J Exp Med. 1977 May 1;145(5):1353-67. doi: 10.1084/jem.145.5.1353.

Abstract

The protective activity of anti-Listeria-immune T cells assayed in an adoptive transfer system in H-2 restricted. As shown in the present studies, the demonstration of the restriction is directly dependent on the dose and the relative protective activity of spleen cells. In addition, some H-2-unrestricted protection is conferred predominantly by other than immunoglobulin-negative spleen cells. Thus, the activity of Listeria-immune T cells appears to be 'absolutely' restricted and is in this respect comparable to in vivo T-cell-mediated anti-viral protection. The predominant genetic region of H-2 coding for the structures which are mainly involved in this restriction in T-cell immunity to this prototype intracellular bacterium is the I region. The specificity of Listeria-immune T cells is determined by the H-2 haplotype of the donor. Thus, F1 hybrids seem to possess at least two separable sets of T cells, each specific for one parental haplotype. As is true in the virus model, the results cannot distinguish between an altered-self or a dual recognition model of T-cell recognition to explain H-2 restriction. They are, however, compatible with the idea and I-coded cell surface structures may serve as receptors for cell-specific differentiation signals, which trigger direct or lymphokin-mediated activation of macrophages to manifest increased bactericidal capacity. The interesting parallels in self-marker recognition of T cells in the virus and intracellular bacterium systems, respectively, appear to be reasonably explained by the different types of signals transmitted by T cells to various target cells via the distinctly different self-markers employed (i.e., K or D vs I).

摘要

在过继转移系统中检测的抗李斯特菌免疫T细胞的保护活性受H-2限制。如本研究所示,这种限制的证明直接取决于脾细胞的剂量和相对保护活性。此外,一些H-2非限制保护主要由免疫球蛋白阴性的脾细胞以外的细胞赋予。因此,李斯特菌免疫T细胞的活性似乎受到“绝对”限制,在这方面与体内T细胞介导的抗病毒保护相当。H-2中主要参与对这种原型细胞内细菌的T细胞免疫限制的结构的主要编码遗传区域是I区域。李斯特菌免疫T细胞的特异性由供体的H-2单倍型决定。因此,F1杂种似乎至少拥有两组可分离的T细胞,每组对一种亲本单倍型具有特异性。正如在病毒模型中一样,结果无法区分T细胞识别的改变自身模型或双重识别模型来解释H-2限制。然而,它们与I编码的细胞表面结构可能作为细胞特异性分化信号的受体的观点一致,这些信号触发巨噬细胞的直接或淋巴因子介导的激活,以表现出增强的杀菌能力。分别在病毒和细胞内细菌系统中T细胞对自身标记识别的有趣相似之处,似乎可以通过T细胞通过所使用的明显不同的自身标记(即K或D与I)向各种靶细胞传递的不同类型信号得到合理的解释。

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