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肿瘤选择性细胞溶解仅由CD45R + CTL执行,而异种特异性细胞毒性也可由CD45R - CTL执行。

Tumor-selective cytolysis is executed exclusively by CD45R+ CTL whereas allo-specific cytotoxicity can be executed also by CD45R- CTL.

作者信息

Ericsson P O, Hedlund G, Hansson J, Dohlsten M, Sjögren H O

机构信息

Department of Tumor Immunology, University of Lund, Sweden.

出版信息

Cell Immunol. 1990 Mar;126(1):69-79. doi: 10.1016/0008-8749(90)90301-7.

Abstract

Naive and memory CD4+ T helper cells can be distinguished on the basis of expression of the CD45R molecule. Whether this dichotomy applies also to CD8+ T cells has not yet been established. In the present investigation the cytolytic activity of peritoneal CD8+CD45R+ and CD8+CD45R- T cells from tumor- and allo-immunized rats has been studied. More than 90% of the CD8+ peripheral blood T lymphocytes expressed the CD45R molecule, whereas in the peritoneal cavity about 60% of the CD8+ T cells displayed the CD45R+ phenotype. Analysis of cytotoxicity of sorted peritoneal cells of W439 tumor-immunized donors demonstrated selective cytolytic activity of the CD5+CD4-CD8+CD45R+ subpopulation to W439 lymphoma target cells but no effect of CD5+CD4-CD8+CD45R- lymphocytes. None of these lymphocyte populations exhibited cytolytic activity to the NK-sensitive cell line YAC-1, whereas the CD5-CD45R+ population showed strong cytotoxicity to YAC-1 cells. In allo-immunized rats both CD5+CD4- CD8+CD45R+ and CD5+CD4-CD8+CD45R- peritoneal cells exhibited strong allo-specific cytolytic activity, but no activity to YAC-1 cells. Both CD5+CD4-CD8+CD45R+ and CD5+CD4-CD8+CD45R- cells from tumor-immunized rats proliferated in response to Con A and rIL-2. This is the first study demonstrating that tumor-selective cytolytic CD8+ T cells express the CD45R molecule and that allo-specific cytolytic CD8+ T cells are found in both the CD45R+ and CD45R- populations.

摘要

幼稚型和记忆型CD4+辅助性T细胞可根据CD45R分子的表达加以区分。这种二分法是否也适用于CD8+T细胞尚未确定。在本研究中,对来自肿瘤免疫和同种异体免疫大鼠的腹膜CD8+CD45R+和CD8+CD45R-T细胞的细胞溶解活性进行了研究。超过90%的CD8+外周血T淋巴细胞表达CD45R分子,而在腹腔中,约60%的CD8+T细胞表现为CD45R+表型。对W439肿瘤免疫供体的分选腹膜细胞的细胞毒性分析表明,CD5+CD4-CD8+CD45R+亚群对W439淋巴瘤靶细胞具有选择性细胞溶解活性,但CD5+CD4-CD8+CD45R-淋巴细胞则无此作用。这些淋巴细胞群体对NK敏感细胞系YAC-1均无细胞溶解活性,而CD5-CD45R+群体对YAC-1细胞表现出较强的细胞毒性。在同种异体免疫大鼠中,CD5+CD4-CD8+CD45R+和CD5+CD4-CD8+CD45R-腹膜细胞均表现出较强的同种异体特异性细胞溶解活性,但对YAC-1细胞无活性。来自肿瘤免疫大鼠的CD5+CD4-CD8+CD45R+和CD5+CD4-CD8+CD45R-细胞在接触刀豆蛋白A和重组白细胞介素-2后均发生增殖。这是第一项表明肿瘤选择性细胞溶解CD8+T细胞表达CD45R分子且在CD45R+和CD45R-群体中均发现同种异体特异性细胞溶解CD8+T细胞的研究。

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