Molecular profiling of CD8 T cells in autochthonous melanoma identifies Maf as driver of exhaustion.
par Giordano, Marilyn;Henin, Coralie 
;Maurizio, Julien;Imbratta, Claire;Bourdely, Pierre;Buferne, Michel;Baitsch, Lukas;Vanhille, Laurent;Sieweke, Michael MH;Speiser, Daniel;Auphan-Anezin, Nathalie;Schmitt-Verhulst, Anne-Marie;Verdeil, Grégory
Référence EMBO journal, 34, 15, page (2042-2058)
Publication Publié, 2015-08
;Maurizio, Julien;Imbratta, Claire;Bourdely, Pierre;Buferne, Michel;Baitsch, Lukas;Vanhille, Laurent;Sieweke, Michael MH;Speiser, Daniel;Auphan-Anezin, Nathalie;Schmitt-Verhulst, Anne-Marie;Verdeil, GrégoryRéférence EMBO journal, 34, 15, page (2042-2058)
Publication Publié, 2015-08
Article révisé par les pairs
| Résumé : | T cells infiltrating neoplasms express surface molecules typical of chronically virus-stimulated T cells, often termed "exhausted" T cells. We compared the transcriptome of "exhausted" CD8 T cells infiltrating autochthonous melanomas to those of naïve and acutely stimulated CD8 T cells. Despite strong similarities between transcriptional signatures of tumor- and virus-induced exhausted CD8 T cells, notable differences appeared. Among transcriptional regulators, Nr4a2 and Maf were highly overexpressed in tumor-exhausted T cells and significantly upregulated in CD8 T cells from human melanoma metastases. Transduction of murine tumor-specific CD8 T cells to express Maf partially reproduced the transcriptional program associated with tumor-induced exhaustion. Upon adoptive transfer, the transduced cells showed normal homeostasis but failed to accumulate in tumor-bearing hosts and developed defective anti-tumor effector responses. We further identified TGFβ and IL-6 as main inducers of Maf expression in CD8 T cells and showed that Maf-deleted tumor-specific CD8 T cells were much more potent to restrain tumor growth in vivo. Therefore, the melanoma microenvironment contributes to skewing of CD8 T cell differentiation programs, in part by TGFβ/IL-6-mediated induction of Maf. |
