Zeliszewski D, Gaudebout P, Golvano J J, Dorval I, Prévost A, Borras-Cuesta F, Sterkers G
INSERM CJF90.15 Laboratory, R. Debré Hospital, Paris, France.
Hum Immunol. 1994 Sep;41(1):28-33. doi: 10.1016/0198-8859(94)90080-9.
We report the study of one CD4+ T-cell clone that recognizes peptide HA306-320 in the context of autologous DR1101 molecules as well as of allogeneic DR1301, DR0402, DR1501, and DR1601 molecules. This degenerate T-cell recognition is mediated by a single T-cell receptor (TCR) as judged by both TCR-V beta sequencing and cold-target competition assays. Restriction analysis shows that substitutions of DR residues within the third hypervariable region result in a loss of T-cell reactivity, which is restored by additional substitutions in the first and/or second hypervariable regions. Thus, there is no correlation between antigen presentation abilities of the different allelic DR products and the degree of sequence homology between these products. DR residues whose substitution is compatible with T-cell recognition potentially interact with peptides rather than with TCRs by virtue of their location in the floor of the groove or as previously documented for residues of the alpha-helix. Furthermore, antigen presentation by allogeneic DR molecules occurs independently of their affinity for the peptide, as determined in cell surface-binding assays using biotinylated HA306-320. Altogether these data suggest that degenerate T-cell recognition mainly depends on an influence of polymorphic DR residues on the configuration adopted by the peptide in the DR groove so that the epitope is left intact.
我们报告了对一个CD4 + T细胞克隆的研究,该克隆在自体DR1101分子以及同种异体DR1301、DR0402、DR1501和DR1601分子的背景下识别肽HA306 - 320。通过TCR - Vβ测序和冷靶竞争试验判断,这种简并性T细胞识别是由单个T细胞受体(TCR)介导的。限制性分析表明,第三高变区内DR残基的替换导致T细胞反应性丧失,而在第一和/或第二高变区内的额外替换可恢复这种反应性。因此,不同等位基因DR产物的抗原呈递能力与这些产物之间的序列同源程度之间没有相关性。其替换与T细胞识别相容的DR残基,可能因其位于沟槽底部的位置,或如先前关于α - 螺旋残基的记录,与肽而非TCR相互作用。此外,如使用生物素化的HA306 - 320进行的细胞表面结合试验所确定的,同种异体DR分子的抗原呈递与其对肽的亲和力无关。总之,这些数据表明,简并性T细胞识别主要取决于多态性DR残基对肽在DR沟槽中所采用构象的影响,从而使表位保持完整。
