Conventional and Neo-Antigenic Peptides Presented by β Cells Are Targeted by Circulating Naïve CD8+ T Cells in Type 1 Diabetic and Healthy Donors

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Gonzalez-Duque, Sergio | Azoury, Marie Eliane | Colli, Maikel | Afonso, Georgia | Turatsinze, Jean-Valery | Nigi, Laura | Lalanne, Ana Inés | Sebastiani, Guido | Carré, Alexia | Pinto, Sheena | Culina, Slobodan | Corcos, Noémie | Bugliani, Marco | Marchetti, Marc | Armanet, Mathieu | Diedisheim, Marc | Kyewski, Bruno | Steinmetz, Lars | Buus, Søren | You, Sylvaine | Dubois-Laforgue, Daniele | Larger, Etienne | Beressi, Jean-Paul | Bruno, Graziella | Dotta, Francesco | Scharfmann, Raphael | Eizirik, Decio | Verdier, Yann | Vinh, Joelle | Mallone, Roberto

Edité par CCSD ; Elsevier -

International audience. Although CD8+ T-cell-mediated autoimmune β cell destruction occurs in type 1 diabetes (T1D), the target epitopes processed and presented by β cells are unknown. To identify them, we combined peptidomics and transcriptomics strategies. Inflammatory cytokines increased peptide presentation in vitro, paralleling upregulation of human leukocyte antigen (HLA) class I expression. Peptide sources featured several insulin granule proteins and all known β cell antigens, barring islet-specific glucose-6-phosphatase catalytic subunit-related protein. Preproinsulin yielded HLA-A2-restricted epitopes previously described. Secretogranin V and its mRNA splice isoform SCG5-009, proconvertase-2, urocortin-3, the insulin gene enhancer protein ISL-1, and an islet amyloid polypeptide transpeptidation product emerged as antigens processed into HLA-A2-restricted epitopes, which, as those already described, were recognized by circulating naive CD8+ T cells in T1D and healthy donors and by pancreas-infiltrating cells in T1D donors. This peptidome opens new avenues to understand antigen processing by β cells and for the development of T cell biomarkers and tolerogenic vaccination strategies.

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