Distortion of the Major Histocompatibility Complex Class I Binding Groove to Accommodate an Insulin-derived 10-Mer Peptide |
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| Authors: | Chihiro Motozono James A. Pearson Evy De Leenheer Pierre J. Rizkallah Konrad Beck Andrew Trimby Andrew K. Sewell F. Susan Wong David K. Cole |
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| Affiliation: | From the ‡Division of Infection and Immunity and ;the ¶Institute of Molecular and Experimental Medicine, Cardiff University School of Medicine, Heath Park, Cardiff CF14 4XN, United Kingdom.;the §Department of Immunology, Kinki University School of Medicine, Osaka 589–8511, Japan, and ;the ‖Cardiff University School of Dentistry, Heath Park, Cardiff CF14 4XY, United Kingdom |
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| Abstract: | The non-obese diabetic mouse model of type 1 diabetes continues to be an important tool for delineating the role of T-cell-mediated destruction of pancreatic β-cells. However, little is known about the molecular mechanisms that enable this disease pathway. We show that insulin reactivity by a CD8+ T-cell clone, known to induce type 1 diabetes, is characterized by weak T-cell antigen receptor binding to a relatively unstable peptide-MHC. The structure of the native 9- and 10-mer insulin epitopes demonstrated that peptide residues 7 and 8 form a prominent solvent-exposed bulge that could potentially be the main focus of T-cell receptor binding. The C terminus of the peptide governed peptide-MHC stability. Unexpectedly, we further demonstrate a novel mode of flexible peptide presentation in which the MHC peptide-binding groove is able to “open the back door” to accommodate extra C-terminal peptide residues. |
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| Keywords: | beta cell insulin T-cell receptor (TCR) type 1 diabetes x-ray crystallography NOD mouse pMHC |
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