PLoS ONE (Jan 2017)

MIF inhibition interferes with the inflammatory and T cell-stimulatory capacity of NOD macrophages and delays autoimmune diabetes onset.

  • Hannelie Korf,
  • Laura Breser,
  • Jelter Van Hoeck,
  • Janet Godoy,
  • Dana P Cook,
  • Benoit Stijlemans,
  • Elien De Smidt,
  • Carolien Moyson,
  • João Paulo Monteiro Carvalho Mori Cunha,
  • Virginia Rivero,
  • Conny Gysemans,
  • Chantal Mathieu

DOI
https://doi.org/10.1371/journal.pone.0187455
Journal volume & issue
Vol. 12, no. 11
p. e0187455

Abstract

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Macrophages contribute in the initiation and progression of insulitis during type 1 diabetes (T1D). However, the mechanisms governing their recruitment into the islets as well as the manner of retention and activation are incompletely understood. Here, we investigated a role for macrophage migration inhibitory factor (MIF) and its transmembrane receptor, CD74, in the progression of T1D. Our data indicated elevated MIF concentrations especially in long-standing T1D patients and mice. Additionally, NOD mice featured increased MIF gene expression and CD74+ leukocyte frequencies in the pancreas. We identified F4/80+ macrophages as the main immune cells in the pancreas expressing CD74 and showed that MIF antagonism of NOD macrophages prevented their activation-induced cytokine production. The physiological importance was highlighted by the fact that inhibition of MIF delayed the onset of autoimmune diabetes in two different diabetogenic T cell transfer models. Mechanistically, macrophages pre-conditioned with the MIF inhibitor featured a refractory capacity to trigger T cell activation by keeping them in a naïve state. This study underlines a possible role for MIF/CD74 signaling pathways in promoting macrophage-mediated inflammation in T1D. As therapies directed at the MIF/CD74 pathway are in clinical development, new opportunities may be proposed for arresting T1D progression.