van Seventer G A, Newman W, Shimizu Y, Nutman T B, Tanaka Y, Horgan K J, Gopal T V, Ennis E, O'Sullivan D, Grey H
Experimental Immunology Branch, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892.
J Exp Med. 1991 Oct 1;174(4):901-13. doi: 10.1084/jem.174.4.901.
Many ligands of adhesion molecules mediate costimulation of T cell activation. The generality of this emerging concept is best determined by using model systems which exploit physiologically relevant ligands. We developed such an "antigen-specific" model system for stimulation of resting CD4+ human T cells using the following purified ligands: (a) major histocompatibility complex class II plus the superantigen Staphylococcus enterotoxin A, to engage the T cell receptor (TCR); (b) adhesion proteins vascular cell adhesion molecule 1 (VCAM-1), intercellular adhesion molecule 1 (ICAM-1), and endothelial leukocyte adhesion molecule 1 (ELAM-1), to provide potential cell surface costimulatory signals; and (c) recombinant interleukin 1 beta (rIL-1 beta)/rIL-6 as costimulatory cytokines. In this biochemically defined system, we find that resting CD4+ T cells require costimulation in order to respond to TCR engagement. This costimulation can be provided by VCAM-1 or ICAM-1; however adhesion alone is not sufficient since ELAM-1 mediates adhesion but not costimulation. The cytokines IL-1 beta and IL-6 by themselves cannot mediate costimulation, but augment the adhesion ligand-mediated costimulation. Direct comparison with the model of TCR/CD3 engagement by CD3 monoclonal antibody demonstrated comparable costimulatory requirements in both systems, thereby authenticating the commonly used CD3 model. The costimulation mediated by the activation-dependent interaction of the VLA-4 and LFA-1 integrins with their respective ligands VCAM-1 and ICAM-1 leads to increased IL-2R alpha (CD25) expression and proliferation in both CD45RA+ CD4+ and CD45RO+ CD4+ T cells. The integrins also regulate the secretion of IL-2, IL-4, and granulocyte/macrophage colony-stimulating factor. In contrast the activation-independent adhesion of CD4+ T cell to ELAM-1 molecules does not lead to T cell stimulation as measured by proliferation, IL-2R alpha expression, or cytokine release. These findings imply that adhesion per se is not sufficient for costimulation, but rather that the costimulation conferred by the VLA-4/VCAM-1 and LFA-1/ICAM-1 interactions reflects specialized accessory functions of these integrin pathways. The new finding that VLA-4/VCAM-1 mediates costimulation adds significance to observations that VCAM-1 is expressed on a unique set of potential antigen-presenting cells in vivo.
许多黏附分子配体介导T细胞活化的共刺激。这个新出现概念的普遍性最好通过使用利用生理相关配体的模型系统来确定。我们开发了这样一个“抗原特异性”模型系统,用于使用以下纯化配体刺激静息的人CD4⁺ T细胞:(a) 主要组织相容性复合体II类加上超抗原金黄色葡萄球菌肠毒素A,以激活T细胞受体(TCR);(b) 黏附蛋白血管细胞黏附分子1(VCAM-1)、细胞间黏附分子1(ICAM-1)和内皮白细胞黏附分子1(ELAM-1),以提供潜在的细胞表面共刺激信号;以及(c) 重组白细胞介素1β(rIL-1β)/rIL-6作为共刺激细胞因子。在这个生物化学定义的系统中,我们发现静息的CD4⁺ T细胞需要共刺激才能对TCR激活作出反应。这种共刺激可以由VCAM-1或ICAM-1提供;然而,单纯的黏附是不够的,因为ELAM-1介导黏附但不介导共刺激。细胞因子IL-1β和IL-6自身不能介导共刺激,但能增强黏附配体介导的共刺激。与CD3单克隆抗体激活TCR/CD3的模型直接比较表明,两个系统中的共刺激需求相当,从而验证了常用的CD3模型。由VLA-4和LFA-1整合素与其各自配体VCAM-1和ICAM-1的激活依赖性相互作用介导的共刺激导致CD45RA⁺ CD4⁺和CD45RO⁺ CD4⁺ T细胞中IL-2Rα(CD25)表达增加和细胞增殖。整合素还调节IL-2、IL-4和粒细胞/巨噬细胞集落刺激因子的分泌。相比之下,CD4⁺ T细胞与ELAM-1分子的非激活依赖性黏附不会导致T细胞刺激,这通过增殖、IL-2Rα表达或细胞因子释放来衡量。这些发现意味着黏附本身不足以提供共刺激,而是由VLA-4/VCAM-1和LFA-1/ICAM-1相互作用赋予的共刺激反映了这些整合素途径的特殊辅助功能。VLA-4/VCAM-1介导共刺激这一新发现增加了对体内VCAM-1在一组独特的潜在抗原呈递细胞上表达的观察结果的重要性。
