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Immunology
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- ImmunologyOpen Access
Structural Mechanism Underpinning Cross-reactivity of a CD8+ T-cell Clone That Recognizes a Peptide Derived from Human Telomerase Reverse Transcriptase
Journal of Biological ChemistryVol. 292Issue 3p802–813Published online: November 30, 2016- David K. Cole
- Hugo A. van den Berg
- Angharad Lloyd
- Michael D. Crowther
- Konrad Beck
- Julia Ekeruche-Makinde
- and others
Cited in Scopus: 17T-cell cross-reactivity is essential for effective immune surveillance but has also been implicated as a pathway to autoimmunity. Previous studies have demonstrated that T-cell receptors (TCRs) that focus on a minimal motif within the peptide are able to facilitate a high level of T-cell cross-reactivity. However, the structural database shows that most TCRs exhibit less focused antigen binding involving contact with more peptide residues. To further explore the structural features that allow the clonally expressed TCR to functionally engage with multiple peptide-major histocompatibility complexes (pMHCs), we examined the ILA1 CD8+ T-cell clone that responds to a peptide sequence derived from human telomerase reverse transcriptase.