2005
DOI: 10.1073/pnas.0502751102
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Coevolution of TCR-MHC interactions: Conserved MHC tertiary structure is not sufficient for interactions with the TCR

Abstract: The specificity for self-MHC that is necessary for T cell function is a consequence of intrathymic selection during which T cell antigen receptors (TCRs) expressed by immature thymocytes are tested for their affinity for self-peptide:self-MHC. The germ-line-encoded segments of the TCR, however, are believed to have an innate specificity for structural features of MHC molecules. We directly tested this hypothesis by generating a transgenic mouse system in which the protein HLA-DM is expressed at the surface of … Show more

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Cited by 10 publications
(6 citation statements)
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“…44 The improved CD4 1 T-cell recall response in NSGAb°DR1 mice may result from more effective interactions between DR1-restricted CD4 1 T cells and HLA-DR1/peptide complexes presented by DR1 antigen-presenting cells resulting from coevolution of the human TCR and human MHC II molecules. 45,46 Although we observed a slight but significant increase in T-cell frequency in NSGAb°DR1 mice compared with NSG mice, we did not observe an increase in the frequency of CD4 1 T cells, which is in contrast to the increase in CD4…”
Section: Discussioncontrasting
confidence: 79%
“…44 The improved CD4 1 T-cell recall response in NSGAb°DR1 mice may result from more effective interactions between DR1-restricted CD4 1 T cells and HLA-DR1/peptide complexes presented by DR1 antigen-presenting cells resulting from coevolution of the human TCR and human MHC II molecules. 45,46 Although we observed a slight but significant increase in T-cell frequency in NSGAb°DR1 mice compared with NSG mice, we did not observe an increase in the frequency of CD4 1 T cells, which is in contrast to the increase in CD4…”
Section: Discussioncontrasting
confidence: 79%
“…In favor of the former, there is strong evidence for the existence of an intrinsic affinity of TCRs for MHC molecules. 9,10 Nonetheless, crystallographic structures of TCRpeptide/MHC complexes have so far identified few conserved interactions between TCRs and the MHC a1 and a2 helices through which an intrinsic affinity could be mediated. 8,11,12 We have been addressing the distinction between TCR recognition of peptide and MHC by examining different receptors that recognize peptides presented by the class I MHC HLA-A*0201 (HLA-A2).…”
mentioning
confidence: 99%
“…129 As another test of the germline compatibility of TCRs with MHC, the class II homolog HLA-DM was expressed on the cell surface in MHC-deficient mice, and this could not restore T cell selection. 130 The question remains open, however, whether this failure resulted from the lack of positive evolutionary pressure on the invariant MHC-like features of HLA-DM or the inability of HLA-DM to present a diverse peptide repertoire (just as the monolithic class II pMHC of Ii/H2M-deficient mice failed to select T cells). 125 …”
Section: The Selecting Ligand and The Purpose Of Selectionmentioning
confidence: 99%