Tallquist M D, Weaver A J, Pease L R
Department of Immunology, Mayo Clinic, Rochester, MN 55905, USA.
J Immunol. 1998 Jan 15;160(2):802-9.
The well-defined 2C T cell was used to investigate alloreactive degeneracy. A panel of class I molecules that are known ligands for the 2C TCR were sensitized with three known peptide ligands, p2Ca (LSPFPFDL), dEV-8 (EQYKFYSV), and SIYR-8 (SIYRYYGL). The peptide p2Ca was originally identified as the allopeptide seen in the Ld class I molecule by 2C T cells, 2C recognizes the dEV-8 peptide as the ligand in the Kbm3 class I molecule, and SIYR-8 was recently identified as a peptide ligand for 2C in the context of the Kb class I molecule. Strong recognition of all three Ag-presenting molecules occurred in the context of their respective allopeptides, but 2C recognized all three peptides to a measurable extent in the context of Kb. Molecular modeling of these Kb/peptide complexes revealed a high degree of similarity between dEV-8 and SIYR-8, but very little conformational similarity of either of these peptides with p2Ca. Furthermore, the structural changes in the mutant Kbm3 binding site resulted in generalized changes in the conformation of each of five bound peptides compared with those of the same peptides bound to Kb. The finding that degenerate recognition occurs on Kb, the restriction element responsible for selecting 2C T cells, suggests a unique relationship between a TCR and the Ag-presenting molecule that mediates its positive selection.
利用明确界定的2C T细胞来研究同种异体反应性简并性。一组已知为2C TCR配体的I类分子用三种已知的肽配体p2Ca(LSPFPFDL)、dEV-8(EQYKFYSV)和SIYR-8(SIYRYYGL)进行致敏。肽p2Ca最初被2C T细胞鉴定为在Ld I类分子中出现的别肽,2C将dEV-8肽识别为Kbm3 I类分子中的配体,并且SIYR-8最近被鉴定为在Kb I类分子背景下2C的肽配体。在各自别肽的背景下,对所有三种抗原呈递分子都有强烈的识别,但2C在Kb背景下对所有三种肽都有可测量程度的识别。这些Kb/肽复合物的分子建模显示dEV-8和SIYR-8之间有高度相似性,但这两种肽与p2Ca的构象相似性很小。此外,与结合到Kb上的相同肽相比,突变型Kbm3结合位点的结构变化导致五个结合肽中每个肽的构象发生普遍变化。在负责选择2C T细胞的限制元件Kb上发生简并识别这一发现,表明TCR与介导其阳性选择的抗原呈递分子之间存在独特关系。