Eliminating roles for T-bet and IL-2 but revealing superior activation and proliferation as mechanisms underpinning dominance of regulatory T cells in tumors

نویسندگان

  • Emily J. Colbeck
  • James P. Hindley
  • Kathryn Smart
  • Emma Jones
  • Anja Bloom
  • Hayley Bridgeman
  • Rhoanne C. McPherson
  • Darryl G. Turner
  • Kristin Ladell
  • David A. Price
  • Richard A. O'Connor
  • Stephen M. Anderton
  • Andrew J. Godkin
  • Awen M. Gallimore
چکیده

Foxp3(+) regulatory T cells (Tregs) are often highly enriched within the tumor-infiltrating T cell pool. Using a well-characterised model of carcinogen-induced fibrosarcomas we show that the enriched tumor-infiltrating Treg population comprises largely of CXCR3(+) T-bet(+) 'TH1-like' Tregs which are thymus-derived Helios(+) cells. Whilst IL-2 maintains homeostatic ratios of Tregs in lymphoid organs, we found that the perturbation in Treg frequencies in tumors is IL-2 independent. Moreover, we show that the TH1 phenotype of tumor-infiltrating Tregs is dispensable for their ability to influence tumor progression. We did however find that unlike Tconvs, the majority of intra-tumoral Tregs express the activation markers CD69, CD25, ICOS, CD103 and CTLA4 and are significantly more proliferative than Tconvs. Moreover, we have found that CD69(+) Tregs are more suppressive than their CD69- counterparts. Collectively, these data indicate superior activation of Tregs in the tumor microenvironment, promoting their suppressive ability and selective proliferation at this site.

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عنوان ژورنال:

دوره 6  شماره 

صفحات  -

تاریخ انتشار 2015