Frontiers in Immunology (Jan 2019)

CD11c+ Cells Are Gatekeepers for Lymphocyte Trafficking to Infiltrated Islets During Type 1 Diabetes

  • Adam M. Sandor,
  • Adam M. Sandor,
  • Robin S. Lindsay,
  • Robin S. Lindsay,
  • Nathan Dyjack,
  • Jennifer C. Whitesell,
  • Jennifer C. Whitesell,
  • Cydney Rios,
  • Brenda J. Bradley,
  • Kathryn Haskins,
  • David V. Serreze,
  • Aron M. Geurts,
  • Yi-Guang Chen,
  • Max A. Seibold,
  • Max A. Seibold,
  • Max A. Seibold,
  • Jordan Jacobelli,
  • Jordan Jacobelli,
  • Rachel S. Friedman,
  • Rachel S. Friedman

DOI
https://doi.org/10.3389/fimmu.2019.00099
Journal volume & issue
Vol. 10

Abstract

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Type 1 diabetes (T1D) is a T cell mediated autoimmune disease that affects more than 19 million people with incidence increasing rapidly worldwide. For T cells to effectively drive T1D, they must first traffic to the islets and extravasate through the islet vasculature. Understanding the cues that lead to T cell entry into inflamed islets is important because diagnosed T1D patients already have established immune infiltration of their islets. Here we show that CD11c+ cells are a key mediator of T cell trafficking to infiltrated islets in non-obese diabetic (NOD) mice. Using intravital 2-photon islet imaging we show that T cell extravasation into the islets is an extended process, with T cells arresting in the islet vasculature in close proximity to perivascular CD11c+ cells. Antigen is not required for T cell trafficking to infiltrated islets, but T cell chemokine receptor signaling is necessary. Using RNAseq, we show that islet CD11c+ cells express over 20 different chemokines that bind chemokine receptors expressed on islet T cells. One highly expressed chemokine-receptor pair is CXCL16-CXCR6. However, NOD. CXCR6−/− mice progressed normally to T1D and CXCR6 deficient T cells trafficked normally to the islets. Even with CXCR3 and CXCR6 dual deficiency, T cells trafficked to infiltrated islets. These data reinforce that chemokine receptor signaling is highly redundant for T cell trafficking to inflamed islets. Importantly, depletion of CD11c+ cells strongly inhibited T cell trafficking to infiltrated islets of NOD mice. We suggest that targeted depletion of CD11c+ cells associated with the islet vasculature may yield a therapeutic target to inhibit T cell trafficking to inflamed islets to prevent progression of T1D.

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