Hsu B L, Evavold B D, Allen P M
Center for Immunology, Washington University School of Medicine, St. Louis, Missouri 63110.
J Exp Med. 1995 Feb 1;181(2):805-10. doi: 10.1084/jem.181.2.805.
T cells potentially encounter numerous endogenous peptides during selection in the thymus and in the periphery. We examined the impact of an endogenous peptide on in vivo T cell development, using a TCR transgenic mouse model based on a hemoglobin-specific T cell clone. In these mice, the transgenic beta chains paired with endogenous alpha chains. This led to a serendipitous primary reactivity to Ser69 peptide, an altered peptide ligand of the Hbd (64-76) epitope of the parent clone. Two Ser69-reactive T cell populations were identified. A smaller population of the Ser69-reactive T cells responded both to Ser69 and Hbd (64-76). A majority reacted only to Ser69, and not to Hbd(64-76); in fact, Hbd(64-76) was a specific TCR antagonist for these Ser69-only-reactive T cells. Thus, in this unique experimental system, Ser69 became an agonist, and Hbd (64-76) was an antagonist. Endogenous presentation of the antagonist ligand in the thymus selectively eliminated the high-avidity cells, while sparing low-avidity cells in the Ser69-reactive T cell repertoire. These results highlight how specificity guides developing T cells through a network of ligands and indicate that the endogenous peptide pool has a profound effect on T cell development and repertoire.
T细胞在胸腺和外周进行选择的过程中可能会接触到大量内源性肽段。我们使用基于血红蛋白特异性T细胞克隆的TCR转基因小鼠模型,研究了一种内源性肽对体内T细胞发育的影响。在这些小鼠中,转基因β链与内源性α链配对。这意外地导致了对Ser69肽的初次反应性,Ser69肽是亲本克隆的Hbd(64-76)表位的一种改变的肽配体。我们鉴定出了两个对Ser69有反应的T细胞群体。数量较少的Ser69反应性T细胞群体对Ser69和Hbd(64-76)都有反应。大多数细胞只对Ser69有反应,而对Hbd(64-76)没有反应;事实上,Hbd(64-76)是这些仅对Ser69有反应的T细胞的特异性TCR拮抗剂。因此,在这个独特的实验系统中,Ser69变成了激动剂,而Hbd(64-76)是拮抗剂。胸腺中拮抗剂配体的内源性呈递选择性地消除了高亲和力细胞,同时保留了Ser69反应性T细胞库中的低亲和力细胞。这些结果突出了特异性如何通过配体网络引导发育中的T细胞,并表明内源性肽库对T细胞发育和库有深远影响。
