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T-cell responses to hybrid insulin peptides prior to type 1 diabetes development

Angela M. Mitchell, Aimon A. Alkanani, Kristen A. McDaniel, Laura Pyle, Kathleen Waugh, Andrea K. Steck, Maki Nakayama, Liping Yu, Peter A. Gottlieb, Marian Rewers, Aaron W. Michels

2021Proceedings of the National Academy of Sciences47 citationsDOIOpen Access PDF

Abstract

T-cell responses to posttranslationally modified self-antigens are associated with many autoimmune disorders. In type 1 diabetes, hybrid insulin peptides (HIPs) are implicated in the T-cell-mediated destruction of insulin-producing β-cells within pancreatic islets. The natural history of the disease is such that it allows for the study of T-cell reactivity prior to the onset of clinical symptoms. We hypothesized that CD4 T-cell responses to posttranslationally modified islet peptides precedes diabetes onset. In a cohort of genetically at-risk individuals, we measured longitudinal T-cell responses to native insulin and hybrid insulin peptides. Both proinflammatory (interferon-γ) and antiinflammatory (interluekin-10) cytokine responses to HIPs were more robust than those to native peptides, and the ratio of such responses oscillated between pro- and antiinflammatory over time. However, individuals who developed islet autoantibodies or progressed to clinical type 1 diabetes had predominantly inflammatory T-cell responses to HIPs. Additionally, several HIP T-cell responses correlated to worsening measurements of blood glucose, highlighting the relevance of T-cell responses to posttranslationally modified peptides prior to autoimmune disease development.

Topics & Concepts

PathogenesisImmune systemInsulinImmunologyPancreatic isletsDiabetes mellitusType 1 diabetesEpitopeAutoimmune diseaseDiseaseMedicineIsletAutoimmunityBiologyBioinformaticsAntigenEndocrinologyInternal medicineAntibodyDiabetes and associated disordersPancreatic function and diabetesDiabetes Management and Research
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