PLoS Pathogens (Oct 2020)

IL-27 signalling regulates glycolysis in Th1 cells to limit immunopathology during infection.

  • Marcela Montes de Oca,
  • Fabian de Labastida Rivera,
  • Clay Winterford,
  • Teija C M Frame,
  • Susanna S Ng,
  • Fiona H Amante,
  • Chelsea L Edwards,
  • Luzia Bukali,
  • Yulin Wang,
  • Jude E Uzonna,
  • Rachel D Kuns,
  • Ping Zhang,
  • Agnieszka Kabat,
  • Ramon I Klein Geltink,
  • Edward J Pearce,
  • Geoffrey R Hill,
  • Christian R Engwerda

DOI
https://doi.org/10.1371/journal.ppat.1008994
Journal volume & issue
Vol. 16, no. 10
p. e1008994

Abstract

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Inflammation is critical for controlling pathogens, but also responsible for symptoms of infectious diseases. IL-27 is an important regulator of inflammation and can limit development of IFNγ-producing Tbet+ CD4+ T (Th1) cells. IL-27 is thought to do this by stimulating IL-10 production by CD4+ T cells, but the underlying mechanisms of these immunoregulatory pathways are not clear. Here we studied the role of IL-27 signalling in experimental visceral leishmaniasis (VL) caused by infection of C57BL/6 mice with the human pathogen Leishmania donovani. We found IL-27 signalling was critical for the development of IL-10-producing Th1 (Tr1) cells during infection. Furthermore, in the absence of IL-27 signalling, there was improved control of parasite growth, but accelerated splenic pathology characterised by the loss of marginal zone macrophages. Critically, we discovered that IL-27 signalling limited glycolysis in Th1 cells during infection that in turn attenuated inflammation. Furthermore, the modulation of glycolysis in the absence of IL-27 signalling restricted tissue pathology without compromising anti-parasitic immunity. Together, these findings identify a novel mechanism by which IL-27 mediates immune regulation during disease by regulating cellular metabolism.