| Literature DB >> 29559470 |
Nicolas Gourdin1,2,3, Marion Bossennec1,2, Céline Rodriguez1,2,3, Selena Vigano4, Christelle Machon5,6, Camilla Jandus4, David Bauché2,7,8, Julien Faget1,2,3, Isabelle Durand2,9, Nicolas Chopin10, Olivier Tredan10, Julien C Marie2,7,8, Bertrand Dubois1,2, Jérôme Guitton5,11, Pedro Romero4, Christophe Caux1,2,3, Christine Ménétrier-Caux12,2,3.
Abstract
The production of CD73-derived adenosine (Ado) by Tregs has been proposed as a resistance mechanism to anti-PD-1 therapy in murine tumor models. We reported that human Tregs express the ectonucleotidase CD39, which generates AMP from ATP, but do not express the AMPase CD73. In contrast, CD73 defined a subset of effector CD4+ T cells (Teffs) enriched in polyfunctional Th1.17 cells characterized by expression of CXCR3, CCR6, and MDR1, and production of IL17A/IFNγ/IL22/GM-CSF. CD39+ Tregs selectively targeted CD73+ Teffs through cooperative degradation of ATP into Ado inhibiting and restricting the ability of CD73+ Teffs to secrete IL17A. CD73+ Teffs infiltrating breast and ovarian tumors were functionally blunted by Tregs expressing upregulated levels of CD39 and ATPase activity. Moreover, tumor-infiltrating CD73+ Teffs failed to express inhibitory immune checkpoints, suggesting that CD73 might be selected under pressure from immune checkpoint blockade therapy and thus may represent a nonredundant target for restoring antitumor immunity.Significance: Polyfunctional CD73+ T-cell effectors lacking other immune checkpoints are selectively targeted by CD39 overexpressing Tregs that dominate the breast tumor environment. Cancer Res; 78(13); 3604-18. ©2018 AACR. ©2018 American Association for Cancer Research.Entities:
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Year: 2018 PMID: 29559470 DOI: 10.1158/0008-5472.CAN-17-2405
Source DB: PubMed Journal: Cancer Res ISSN: 0008-5472 Impact factor: 12.701