Willis Richard A, Kappler John W, Marrack Philippa C
Integrated Department of Immunology, National Jewish Medical and Research Center, Denver, CO 80206, USA.
Proc Natl Acad Sci U S A. 2006 Aug 8;103(32):12063-8. doi: 10.1073/pnas.0605130103. Epub 2006 Jul 31.
T cell responses against an antigen are often focused on a small fraction of potentially immunogenic determinants, a phenomenon known as immunodominance. Immunodominance can be established at several stages of antigen presentation, including antigen processing, binding of peptides to MHC, and competition between T cells for dendritic cells (DCs). The mechanism of this T cell competition is unclear, but may include competition for physical access to DCs, competition for limiting soluble DC-derived factors, or a suppressive effect of one T cell population on the other(s). To model DC-specific T cell competition, normal mice were injected with one or two T cell receptor transgenic CD8 T cell populations, each with high affinity for different peptides presented by different class I MHC complexes. These mice were immunized with DCs pulsed with peptides that are recognized by the transferred T cells. Competition was detectable when both T cell populations were transferred and their target peptides were present on the same DCs. The competition resulted in fewer cells entering the response, but had no effect on the level of activation of the cells that did respond. The effect was evident very early in the response, and in fact the competing T cells needed to be present in the first 5 h of the response for competition to occur. Thus, some aspect of DCs other than peptide/MHC complexes is limiting in the earliest stages of the CD8 T cell response. These results have implications for the design of multivalent vaccines.
针对一种抗原的T细胞反应通常集中在一小部分潜在的免疫原性决定簇上,这一现象被称为免疫显性。免疫显性可在抗原呈递的多个阶段建立,包括抗原加工、肽与MHC的结合以及T细胞之间对树突状细胞(DC)的竞争。这种T细胞竞争的机制尚不清楚,但可能包括对DC的物理接触竞争、对有限的可溶性DC衍生因子的竞争,或一个T细胞群体对其他T细胞群体的抑制作用。为了模拟DC特异性T细胞竞争,给正常小鼠注射一个或两个T细胞受体转基因CD8 T细胞群体,每个群体对由不同I类MHC复合物呈递的不同肽具有高亲和力。用经转移的T细胞识别的肽脉冲处理的DC对这些小鼠进行免疫。当两个T细胞群体都被转移且它们的靶肽存在于同一DC上时,竞争是可检测到的。竞争导致进入反应的细胞减少,但对有反应的细胞的激活水平没有影响。这种效应在反应的早期就很明显,实际上,竞争的T细胞需要在反应的前5小时内存在才能发生竞争。因此,在CD8 T细胞反应的最早阶段,除了肽/MHC复合物之外,DC的某些方面是有限的。这些结果对多价疫苗的设计具有启示意义。