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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Purified MHC class I and peptide complexes activate naive CD8+ T cells independently of the CD28/B7 and LFA-1/ICAM-1 costimulatory interactions.
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Purified MHC class I and peptide complexes activate naive CD8+ T cells independently of the CD28/B7 and LFA-1/ICAM-1 costimulatory interactions.

机译:纯化的I类MHC和肽复合物可独立于CD28 / B7和LFA-1 / ICAM-1共刺激相互作用激活天然CD8 + T细胞。

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摘要

T cells play a central role in the initiation, maintenance, and regulation of the immune response. Effector responses of T cells are controlled by complex combinations of lymphokines and adhesion/costimulatory molecule signals. To isolate the effects of specific adhesion/costimulatory molecules and to define the minimal molecular requirements of naive CD8+ T cell activation, we have developed an APC-free system for stimulation of naive CD8+ T cells. In this report, we demonstrate that immobilized MHC class I-peptide complexes can activate naive CD8+ T cells from TCR transgenic mice at low cell densities. The CD8+ T cells were stimulated to proliferate and secrete IL-2 independently of the molecular interactions between CD28/B7.1-B7.2 or LFA-1/ICAM-1 surface receptors. Previous reports have shown that CD28 ligation is necessary for late T cell survival of APC-stimulated naive CD8+ T cells. Our data suggest that under certain specific conditions of high intensity T cell signaling, early activation and late cell proliferation can occur independently of APC-derived costimulatory signals.
机译:T细胞在免疫反应的启动,维持和调节中起着核心作用。 T细胞的效应反应是由淋巴因子和粘附/共刺激分子信号的复杂组合控制的。为了隔离特定粘附/共刺激分子的作用并定义幼稚CD8 + T细胞活化的最低分子要求,我们开发了无APC刺激幼稚CD8 + T细胞的系统。在本报告中,我们证明了固定的MHC I类肽复合物可以在低细胞密度下激活来自TCR转基因小鼠的幼稚CD8 + T细胞。不依赖于CD28 / B7.1-B7.2或LFA-1 / ICAM-1表面受体之间的分子相互作用,刺激CD8 + T细胞增殖和分泌IL-2。以前的报道表明,CD28连接对于APC刺激的原始CD8 + T细胞的晚期T细胞存活是必需的。我们的数据表明,在高强度T细胞信号转导的某些特定条件下,早期活化和晚期细胞增殖可独立于APC衍生的共刺激信号而发生。

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