PLoS Pathogens (Jun 2019)

The lectin-specific activity of Toxoplasma gondii microneme proteins 1 and 4 binds Toll-like receptor 2 and 4 N-glycans to regulate innate immune priming.

  • Aline Sardinha-Silva,
  • Flávia C Mendonça-Natividade,
  • Camila F Pinzan,
  • Carla D Lopes,
  • Diego L Costa,
  • Damien Jacot,
  • Fabricio F Fernandes,
  • André L V Zorzetto-Fernandes,
  • Nicholas J Gay,
  • Alan Sher,
  • Dragana Jankovic,
  • Dominique Soldati-Favre,
  • Michael E Grigg,
  • Maria Cristina Roque-Barreira

DOI
https://doi.org/10.1371/journal.ppat.1007871
Journal volume & issue
Vol. 15, no. 6
p. e1007871

Abstract

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Infection of host cells by Toxoplasma gondii is an active process, which is regulated by secretion of microneme (MICs) and rhoptry proteins (ROPs and RONs) from specialized organelles in the apical pole of the parasite. MIC1, MIC4 and MIC6 assemble into an adhesin complex secreted on the parasite surface that functions to promote infection competency. MIC1 and MIC4 are known to bind terminal sialic acid residues and galactose residues, respectively and to induce IL-12 production from splenocytes. Here we show that rMIC1- and rMIC4-stimulated dendritic cells and macrophages produce proinflammatory cytokines, and they do so by engaging TLR2 and TLR4. This process depends on sugar recognition, since point mutations in the carbohydrate-recognition domains (CRD) of rMIC1 and rMIC4 inhibit innate immune cells activation. HEK cells transfected with TLR2 glycomutants were selectively unresponsive to MICs. Following in vitro infection, parasites lacking MIC1 or MIC4, as well as expressing MIC proteins with point mutations in their CRD, failed to induce wild-type (WT) levels of IL-12 secretion by innate immune cells. However, only MIC1 was shown to impact systemic levels of IL-12 and IFN-γ in vivo. Together, our data show that MIC1 and MIC4 interact physically with TLR2 and TLR4 N-glycans to trigger IL-12 responses, and MIC1 is playing a significant role in vivo by altering T. gondii infection competency and murine pathogenesis.