Perinatal tolerance to proinsulin is sufficient to prevent autoimmune diabetes
Gaurang Jhala, … , Thomas W.H. Kay, Balasubramanian Krishnamurthy
Gaurang Jhala, … , Thomas W.H. Kay, Balasubramanian Krishnamurthy
Published July 7, 2016
Citation Information: JCI Insight. 2016;1(10):e86065. https://doi.org/10.1172/jci.insight.86065.
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Research Article

Perinatal tolerance to proinsulin is sufficient to prevent autoimmune diabetes

Abstract

High-affinity self-reactive thymocytes are purged in the thymus, and residual self-reactive T cells, which are detectable in healthy subjects, are controlled by peripheral tolerance mechanisms. Breakdown in these mechanisms results in autoimmune disease, but antigen-specific therapy to augment natural mechanisms can prevent this. We aimed to determine when antigen-specific therapy is most effective. Islet autoantigens, proinsulin (PI), and islet-specific glucose-6-phosphatase catalytic subunit-related protein (IGRP) were expressed in the antigen-presenting cells (APCs) of autoimmune diabetes-prone nonobese diabetic (NOD) mice in a temporally controlled manner. PI expression from gestation until weaning was sufficient to completely protect NOD mice from diabetes, insulitis, and development of insulin autoantibodies. Insulin-specific T cells were significantly diminished, were naive, and did not express IFN-γ when challenged. This long-lasting effect from a brief period of treatment suggests that autoreactive T cells are not produced subsequently. We tracked IGRP206–214-specific CD8+ T cells in NOD mice expressing IGRP in APCs. When IGRP was expressed only until weaning, IGRP206–214-specific CD8+ T cells were not detected later in life. Thus, anti-islet autoimmunity is determined during early life, and autoreactive T cells are not generated in later life. Bolstering tolerance to islet antigens in the perinatal period is sufficient to impart lasting protection from diabetes.

Authors

Gaurang Jhala, Jonathan Chee, Prerak M. Trivedi, Claudia Selck, Esteban N. Gurzov, Kate L. Graham, Helen E. Thomas, Thomas W.H. Kay, Balasubramanian Krishnamurthy

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Figure 3

Phenotype of antigen-specific T cells in TIP mice.

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Phenotype of antigen-specific T cells in TIP mice. Insulin B10–23-specif...
Insulin B10–23-specific CD4+ T cells were stained with I-A(g7) tetramer and enriched from pooled peripheral lymphoid organs of 12- to 15-week-old TIP mice in indicated cohorts using magnetic beads and enumerated by flow cytometry. Representative FACS plots (A) and frequency (B) of intracellular IFN-γ–secreting insulin tetramer+ CD4+ T cells in indicated cohorts of TIP mice. Representative FACS plots (C) and frequency (D) of FR4+ CD73+ insulin B10–23 tetramer+ CD4+ T cells in TIP mice. Values in the FACS plots show percentage (A and C) in the indicated gate. Each symbol in the scatter plots (mean ± SEM) represents data from an individual mouse. *P < 0.05, **P < 0.01, ***P < 0.001. Values compared using One-way ANOVA with Tukey’s multiple comparisons test (B) and 2-tailed unpaired t test (D).