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小鼠CD4 T细胞生长的共刺激:B7与热稳定抗原之间的协同作用。

Co-stimulation of murine CD4 T cell growth: cooperation between B7 and heat-stable antigen.

作者信息

Liu Y, Jones B, Brady W, Janeway C A, Linsley P S

机构信息

Section of Immunobiology, Yale University School of Medicine, New Haven.

出版信息

Eur J Immunol. 1992 Nov;22(11):2855-9. doi: 10.1002/eji.1830221115.

Abstract

The B cell activation antigen B7/BB1 has been shown to co-stimulate growth of human T cells by binding the T cell molecule CD28. In mice, the heat-stable antigen (HSA) has also been shown to act as a co-stimulator for T cell growth. In this study, we have evaluated the contributions of B7 and HSA to the co-stimulatory activity of antigen-presenting cells (APC). Mouse B7 provides co-stimulatory activity for murine CD4 T cells in anti-CD3-induced proliferation. Human CTLA4Ig, a chimeric molecule comprising the extracellular region of CTLA-4 fused to an immunoglobulin C gamma fragment, binds to murine B7. We, therefore, use human CTLA4Ig and the hamster anti-HSA monoclonal antibody 20C9 to analyze the relative contributions of B7 and HSA to the co-stimulatory activity of murine spleen APC. Our data reveal that both murine B7 and HSA are expressed by dendritic cells and by low-density spleen B cells. Either CTLA4Ig alone or anti-HSA alone inhibited CD4 T cell proliferation to anti-CD3 by > 90%, while CTLA4Ig and anti-HSA together were far more efficient in inhibiting clonal expansion of CD4 T cells. These results demonstrate that functionally defined co-stimulation involves at least B7 and HSA and suggest that signals delivered by B7 and HSA synergize in promoting T cell growth.

摘要

B细胞活化抗原B7/BB1已被证明可通过与T细胞分子CD28结合来共刺激人类T细胞的生长。在小鼠中,热稳定抗原(HSA)也已被证明可作为T细胞生长的共刺激因子。在本研究中,我们评估了B7和HSA在抗原呈递细胞(APC)共刺激活性中的作用。小鼠B7在抗CD3诱导的增殖中为鼠CD4 T细胞提供共刺激活性。人CTLA4Ig是一种嵌合分子,由与免疫球蛋白Cγ片段融合的CTLA-4细胞外区域组成,可与鼠B7结合。因此,我们使用人CTLA4Ig和仓鼠抗HSA单克隆抗体20C9来分析B7和HSA在鼠脾脏APC共刺激活性中的相对作用。我们的数据显示,鼠B7和HSA均由树突状细胞和低密度脾脏B细胞表达。单独使用CTLA4Ig或单独使用抗HSA均可使CD4 T细胞对抗CD3的增殖抑制>90%,而CTLA4Ig和抗HSA联合使用在抑制CD4 T细胞克隆扩增方面效率更高。这些结果表明,功能上定义的共刺激至少涉及B7和HSA,并表明B7和HSA传递的信号在促进T细胞生长方面具有协同作用。

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