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Increased Effector Memory Insulin-Specific CD4 T Cells Correlate With Insulin Autoantibodies in Patients With Recent-Onset Type 1 Diabetes

Overview
Journal Diabetes
Specialty Endocrinology
Date 2017 Aug 27
PMID 28842400
Citations 32
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Abstract

Type 1 diabetes (T1D) results from T cell-mediated destruction of insulin-producing β-cells. Insulin represents a key self-antigen in disease pathogenesis, as recent studies identified proinsulin-responding T cells from inflamed pancreatic islets of organ donors with recent-onset T1D. These cells respond to an insulin B-chain (InsB) epitope presented by the HLA-DQ8 molecule associated with high T1D risk. Understanding insulin-specific T-cell frequency and phenotype in peripheral blood is now critical. We constructed fluorescent InsB:DQ8 tetramers, stained peripheral blood lymphocytes directly ex vivo, and show DQ8 patients with T1D have increased tetramer CD4 T cells compared with HLA-matched control subjects without diabetes. Patients with a shorter disease duration had higher frequencies of insulin-reactive CD4 T cells, with most of these cells being antigen experienced. We also demonstrate that the number of insulin tetramer effector memory cells is directly correlated with insulin antibody titers, suggesting insulin-specific T- and B-cell interactions. Notably, one of four control subjects with tetramer cells was a first-degree relative who had insulin-specific cells with an effector memory phenotype, potentially representing an early marker of T-cell autoimmunity. Our results suggest that studying InsB:DQ8 reactive T-cell frequency and phenotype may provide a biomarker of disease activity in patients with T1D and those at risk.

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