Identification of autoreactive CD8(+) T cell responses targeting chromogranin A in humanized NOD mice and type 1 diabetes patients.
Clinical Immunology(2015)
摘要
ChgA has recently been identified as the autoantigen for diabetogenic CD4+ T cells in NOD mice and T1D patients. However, autoreactive CD8+ T-cell responses targeting ChgA haven't been studied yet. Here several HLA-A*0201-restricted peptides derived from mChgA and hChgA were selected by an integrated computational prediction approach, followed by an HLA-A*0201 binding assay. MChgA10–19 and mChgA43–52 peptides, which bound well with HLA-A*0201 molecule, induced significant proliferation and IFN-γ-releasing of splenocytes from diabetic NOD.β2mnull.HHD mice. Notably, flow cytometry analysis found that mChgA10–19 and mChgA43–52 stimulated the production of IFN-γ, perforin, and IL-17 by splenic CD8+ T cells of diabetic NOD.β2mnull.HHD mice. Furthermore, hChgA10–19 and hChgA43–52-induced IFN-γ releasing by specific CD8+ T cells were frequently detected in recent-onset HLA-A*0201-positive T1D patients. Thus, this study demonstrated that autoreactive CD8+ T cells targeting ChgA were present in NOD.β2mnull.HHD mice and T1D patients, and might contribute to pathogenesis of T1D through secreting proinflammatory cytokines and cytotoxic molecules.
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关键词
Type 1 diabetes,Epitope,Chronogranin A,Humanized NOD mice
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