CLEC-1 is a death sensor that limits antigen cross-presentation by dendritic cells and represents a target for cancer immunotherapy

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Drouin, Marion | Saenz, Javier | Gauttier, Vanessa | Evrard, Berangere | Teppaz, Geraldine | Pengam, Sabrina | Mary, Caroline | Desselle, Ariane | Thepenier, Virginie | Wilhelm, Emmanuelle | Merieau, Emmanuel | Ligeron, Camille | Girault, Isabelle | Lopez, Maria-Dolores | Fourgeux, Cynthia | Sinha, Debajyoti | Baccelli, Irene | Moreau, Aurelie | Louvet, Cedric | Josien, Regis | Poschmann, Jeremie | Poirier, Nicolas | Chiffoleau, Elise

Edité par CCSD ; American Association for the Advancement of Science (AAAS) -

International audience. Tumors exploit numerous immune checkpoints, including those deployed by myeloid cells to curtail antitumor immunity. Here, we show that the C-type lectin receptor CLEC-1 expressed by myeloid cells senses dead cells killed by programmed necrosis. Moreover, we identified Tripartite Motif Containing 21 (TRIM21) as an endogenous ligand overexpressed in various cancers. We observed that the combination of CLEC-1 blockade with chemotherapy prolonged mouse survival in tumor models. Loss of CLEC-1 reduced the accumulation of immunosuppressive myeloid cells in tumors and invigorated the activation state of dendritic cells (DCs), thereby increasing T cell responses. Mechanistically, we found that the absence of CLEC-1 increased the cross-presentation of dead cellassociated antigens by conventional type-1 DCs. We identified antihuman CLEC-1 antagonist antibodies able to enhance antitumor immunity in CLEC-1 humanized mice. Together, our results demonstrate that CLEC-1 acts as an immune checkpoint in myeloid cells and support CLEC-1 as a novel target for cancer immunotherapy.

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