Human Tolerogenic Dendritic Cells Regulate Immune Responses through Lactate Synthesis

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Marín, Eros | Bouchet-Delbos, Laurence | Renoult, Ophélie | Louvet, Cédric | Nerriere-Daguin, Véronique | Managh, Amy | Even, Amandine | Giraud, Matthieu | Vu Manh, Thien-Phong | Aguesse, Audrey | Bériou, Gaëlle | Chiffoleau, Elise | Alliot-Licht, Brigitte | Prieur, Xavier | Croyal, Mickael | Hutchinson, James, A | Obermajer, Natasa | Geissler, Edward, K. | Vanhove, Bernard | Blancho, Gilles | Dalod, Marc | Josien, Régis | Pecqueur, Claire | Cuturi, Maria Cristina | Moreau, Aurélie

Edité par CCSD ; Elsevier -

International audience. Cell therapy is a promising strategy for treating patients suffering from autoimmune or inflammatory diseases or receiving a transplant. Based on our preclinical studies, we have generated human autologous tolerogenic dendritic cells (ATDCs), which are being tested in a first-in-man clinical trial in kidney transplant recipients. Here, we report that ATDCs represent a unique subset of monocyte-derived cells based on phenotypic, transcriptomic, and metabolic analyses. ATDCs are characterized by their suppression of T cell proliferation and their expansion of Tregs through secreted factors. ATDCs produce high levels of lactate that shape T cell responses toward tolerance. Indeed, T cells take up ATDCsecreted lactate, leading to a decrease of their glycolysis. In vivo, ATDCs promote elevated levels of circulating lactate and delay graft versus host disease by reducing T cell proliferative capacity. The suppression of T cell immunity through lactate production by ATDCs is a novel mechanism that distinguishes ATDCs from other cell-based immunotherapies.

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