A small-molecule P2RX7 activator promotes anti-tumor immune responses and sensitizes lung tumor to immunotherapy

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Douguet, Laetitia | Janho Dit Hreich, Serena | Benzaquen, Jonathan | Seguin, Laetitia | Juhel, Thierry | Dezitter, Xavier | Duranton, Christophe | Ryffel, Bernhard | Kanellopoulos, Jean | Delarasse, Cecile | Renault, Nicolas | Furman, Christophe | Homerin, Germain | Féral, Chloé | Cherfils-Vicini, Julien | Millet, Régis | Adriouch, Sahil | Ghinet, Alina | Hofman, Paul | Vouret-Craviari, Valérie

Edité par HAL CCSD ; Nature Publishing Group

International audience. Only a subpopulation of non-small cell lung cancer (NSCLC) patients responds to immunotherapies, highlighting the urgent need to develop therapeutic strategies to improve patient outcome. We develop a chemical positive modulator (HEI3090) of the purinergic P2RX7 receptor that potentiates αPD-1 treatment to effectively control the growth of lung tumors in transplantable and oncogene-induced mouse models and triggers long lasting antitumor immune responses. Mechanistically, the molecule stimulates dendritic P2RX7-expressing cells to generate IL-18 which leads to the production of IFN-γ by Natural Killer and CD4+ T cells within tumors. Combined with immune checkpoint inhibitor, the molecule induces a complete tumor regression in 80% of LLC tumor-bearing mice. Cured mice are also protected against tumor re-challenge due to a CD8-dependent protective response. Hence, combination treatment of small-molecule P2RX7 activator followed by immune checkpoint inhibitor represents a strategy that may be active against NSCLC.

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