Macrophage IFN-I signaling promotes autoreactive T cell infiltration into islets in type 1 diabetes model
Brett S. Marro, … , Brian C. Ware, Michael B.A. Oldstone
Brett S. Marro, … , Brian C. Ware, Michael B.A. Oldstone
Published January 24, 2019
Citation Information: JCI Insight. 2019;4(2):e125067. https://doi.org/10.1172/jci.insight.125067.
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Research Article Immunology

Macrophage IFN-I signaling promotes autoreactive T cell infiltration into islets in type 1 diabetes model

Abstract

Here, we report a pathogenic role for type I IFN (IFN-I) signaling in macrophages, and not β cells in the islets, for the development of type 1 diabetes (T1D). Following lymphocytic choriomeningitis (LCMV) infection in the Rip-LCMV-GP T1D model, macrophages accumulated near islets and in close contact to islet-infiltrating GP-specific (autoimmune) CD8+ T cells. Depletion of macrophages with clodronate liposomes or genetic ablation of Ifnar in macrophages aborted T1D, despite proliferation of GP-specific (autoimmune) CD8+ T cells. Histopathologically, disrupted IFNα/β receptor (IFNAR) signaling in macrophages resulted in restriction of CD8+ T cells entering into the islets with significant lymphoid accumulation around the islet. Collectively, these results provide evidence that macrophages via IFN-I signaling, while not entering the islets, are directly involved in interacting, directing, or restricting trafficking of autoreactive-specific T cells into the islets as an important component in causing T1D.

Authors

Brett S. Marro, Sarah Legrain, Brian C. Ware, Michael B.A. Oldstone

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Figure 5

Diminished GP-specific CD8+ effector T cell responses in Rip-LysM-Ifnarfl/fl mice.

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Diminished GP-specific CD8+ effector T cell responses in Rip-LysM-Ifnarf...
(A) Frequencies of LCMV-GP33–41 tetramer–positive CD8+ T cells in the spleens and PLNs at day 11 p.i. (B) Median fluorescence intensity (MFI) of PD-1 and KLRG1 at the surface of LCMV-GP33–41 tetramer–positive CD8+ T cells at day 11 p.i. (C) Detection of IFN-γ, TNF-α, and IL-2 in CD8+ T cells following ex vivo restimulation of splencoytes from Rip-LysM-Ifnarfl/fl mice with LCMV-GP33–41 peptide at day 11 p.i. (D) Specific lysis of target splenocytes loaded with CellTrace violet (CTV) and LCMV-GP33–41 (H-2b, CTVhi population) or NP118–126 (H-2d, CTVlo population) peptides. Statistical significance was measured using an unpaired 2-tailed Student t test, one-way ANOVA analysis or 2-way ANOVA analysis. Data presented as average ± SEM. ***P < 0.001, ****P < 0.0001.