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- W1650684965 abstract "Human HLA-B*3501 binds an antigenic peptide of 14-aa length derived from an alternative reading frame of M-CSF with high affinity. Due to its extraordinary length, the exact HLA binding mode was unpredictable. The crystal structure of HLA-B*3501 at 1.5 A shows that the N and C termini of the peptide are embedded in the A and F pockets, respectively, similar to a peptide of normal length. The central part of the 14-meric peptide bulges flexibly out of the groove. Two variants of the alternative reading frame of M-CSF peptide substituted at P2 or P2 and P9 with Ala display weak or no T cell activation. Their structure differs mainly in flexibility and conformation from the agonistic peptide. Moreover, the variants induce subtle changes of MHC alpha-helical regions implicated as critical for TCR contact. The TCR specifically recognizing this peptide/MHC complex exhibits CDR3 length within the normal range, suggesting major conformational adaptations of this receptor upon peptide/MHC binding. Thus, the potential antigenic repertoire recognizable by CTLs is larger than currently thought." @default.
- W1650684965 created "2016-06-24" @default.
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- W1650684965 date "2004-10-19" @default.
- W1650684965 modified "2023-10-17" @default.
- W1650684965 title "Conformational Restraints and Flexibility of 14-Meric Peptides in Complex with HLA-B*3501" @default.
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- W1650684965 doi "https://doi.org/10.4049/jimmunol.173.9.5610" @default.
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