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Expression of TAM-R in Human Immune Cells and Unique Regulatory Function of MerTK in IL-10 Production by Tolerogenic DC

P Giroud, Sarah Renaudineau, Laura Gudefin, Alexandre Calcei, Thierry Menguy, Caroline Rozan, Jacques Mizrahi, Christophe Caux, Vanessa Duong, Jenny Valladeau‐Guilemond

2020Frontiers in Immunology43 citationsDOIOpen Access PDF

Abstract

Tumor infiltrating myeloid cells are a key component of the immune infiltrate often correlated with a poor prognosis due to their capacities to sustain an immunosuppressive environment. Among membrane receptors implicated in myeloid cell functions, Tyro3, Axl and MerTK which are a family of tyrosine kinase receptor (TAM-R) have been described in the regulation of innate cell functions. Here, we have identified MerTK among TAM-R as the major marker of both human M2 macrophages and tolerogenic DC. In situ, MerTK expression was found within the immune infiltrate in multiple solid tumors, highlighting its potential role in cancer immunity. TAM-R ligands Gas6 and PROS1 were found to be constitutively produced by myeloid cells in vitro. Importantly, we describe a novel function of MerTK/PROS1 axis in the regulation of IL-10 production by tolerogenic DC. Finally, the analysis of TAM-R expression within the lymphoid compartment following activation revealed that MerTK, but not Axl or Tyro3, is expressed on activated B lymphocytes and regulatory T cells, as well as CD4+ and CD8+ T cells. Thus, our findings deepen the implication of MerTK in the regulation of myeloid cells mediated immunosuppression and identified new cellular targets expressing MerTK that could participate in the antitumor immune response.

Topics & Concepts

MERTKGAS6Immune systemCancer researchBiologyMyeloidImmunologyCell biologyReceptor tyrosine kinaseInnate immune systemSignal transductionPhagocytosis and Immune RegulationImmune cells in cancerImmune Cell Function and Interaction