Lu P, Zhou X D, Chen S J, Moorman M, Schoneveld A, Morris S, Finkelman F D, Linsley P, Claassen E, Gause W C
Department of Microbiology, Uniformed Services University of the Health Sciences, Bethesda, MD 20814.
J Immunol. 1995 Feb 1;154(3):1078-87.
The CD28/CTLA-4 costimulatory signal is required for TCR-mediated T cell activation resulting in increased IL-2 production in vitro, but its role in IL-4 production is unclear and few studies have examined the function of CTLA-4/CD28 in the in vivo immune response. We have examined the in vivo effects of blocking the interaction of B7 with its ligands, CTLA-4 and CD28, in an IL-4 dominant in vivo immune response to goat anti-mouse IgD. This response is characterized by elevations in serum Igs preceded by elevations in IL-2 and the Th2 cytokines: IL-4, IL-9, and IL-10. The fusion protein CTLA4-Ig administered during the in vivo immune response to goat anti-mouse IgD caused an inhibition in elevations of IL-2, IL-4, and IL-9 gene expression at both day 3 and day 6 after immunization. In contrast, IL-10 cytokine gene expression as late as day 6 after immunization was not decreased. Cell sorting analysis demonstrated that TCR-alpha beta +, CD4+ T cells were the primary source of the elevated IL-10, suggesting that T cell activation leading to IL-10 gene expression may not require CTLA-4 ligand interactions. Similarly CTLA4-Ig completely blocked elevations in the number of IL-4- but not IL-10-secreting cells, as measured by ELISPOT, in both unsorted splenic cells and sorted CD4+, TCR-alpha beta+ T cells. In situ staining of spleen sections also showed inhibition of IL-4-producing cells. These results suggest that, with the notable exception of IL-10, interaction, of B7 with its ligands is required for elevated Th2 cytokine gene expression and secretion during a primary systemic IL-4-dominant response.
CD28/CTLA-4共刺激信号是TCR介导的T细胞活化所必需的,可导致体外IL-2产生增加,但其在IL-4产生中的作用尚不清楚,很少有研究探讨CTLA-4/CD28在体内免疫反应中的功能。我们研究了在对山羊抗小鼠IgD的体内IL-4主导免疫反应中,阻断B7与其配体CTLA-4和CD28相互作用的体内效应。该反应的特征是血清Ig升高,之前是IL-2和Th2细胞因子(IL-4、IL-9和IL-10)升高。在对山羊抗小鼠IgD的体内免疫反应期间给予融合蛋白CTLA4-Ig,在免疫后第3天和第6天,IL-2、IL-4和IL-9基因表达的升高均受到抑制。相比之下,直到免疫后第6天,IL-10细胞因子基因表达并未降低。细胞分选分析表明,TCR-αβ+、CD4+ T细胞是IL-10升高的主要来源,这表明导致IL-10基因表达的T细胞活化可能不需要CTLA-4配体相互作用。同样,通过ELISPOT检测,CTLA4-Ig完全阻断了未分选的脾细胞和分选的CD4+、TCR-αβ+ T细胞中IL-4分泌细胞数量的增加,但未阻断阻断IL-10分泌细胞数量不受影响。脾脏切片的原位染色也显示IL-4产生细胞受到抑制。这些结果表明,在原发性全身性IL-4主导反应期间,除IL-10外,B7与其配体的相互作用是Th2细胞因子基因表达和分泌升高所必需的。
