Ag-presenting CpG-activated pDCs prime Th17 cells that induce tumor regression

Plasmacytoid dendritic cells (pDC) rapidly and massively produce type I IFN and other inflammatory cytokines in response to foreign nucleic acids, thereby indirectly influencing T-cell responses. Moreover, antigen (Ag)-presenting pDCs directly regulate T-cell differentiation. Depending on the immune...

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Detalles Bibliográficos
Autores: Guéry, L. (Leslie)|||/items/0eb28b69-6340-4de0-91f8-3e32e8fbf810, Dubrot-Armendáriz, J. (Juan)|||/items/b42afe78-7095-4682-8c2c-0904580d8d53, Lippens, C. (Carla)|||/items/f617161c-2862-4140-bf35-1405955cc044, Brighouse, D. (Dale)|||/items/b526e470-5918-4ec1-9ef6-cc47fb647515, Malinge, P. (Pauline)|||/items/28e5d332-fbbb-47e9-a532-093d990d3da7, Irla, M. (Magali)|||/items/a7654a7e-fd1c-42d5-a55d-31f76a63957f, Pot, C. (Caroline)|||/items/c727e7e1-19dc-41d7-be5d-ee51d4127059, Reith, W. (Walter)|||/items/ddc6cd9b-c893-4e92-ac21-46e826cefea7, Waldburger, J.M. (Jean-Marc)|||/items/edea8c66-e9a7-4b2a-8c39-8a6d3bd2fcdc, Hugues, S. (Stéphanie)|||/items/437178cd-54c9-41db-b5c9-fa25dea04152
Tipo de recurso: artículo
Fecha de publicación:2014
País:España
Institución:Universidad de Navarra
Repositorio:Dadun. Depósito Académico Digital de la Universidad de Navarra
Idioma:inglés
OAI Identifier:oai:dadun.unav.edu:10171/122980
Acceso en línea:https://hdl.handle.net/10171/122980
Access Level:acceso abierto
Palabra clave:Plasmacytoid dendritic cells
Interferon type I
Antigen presentation
Major histocompatibility complex class II
T helper 17 cells
Tumor-infiltrating lymphocytes
Cytotoxic T lymphocytes
CpG oligodeoxynucleotides
Antitumor immunity
Descripción
Sumario:Plasmacytoid dendritic cells (pDC) rapidly and massively produce type I IFN and other inflammatory cytokines in response to foreign nucleic acids, thereby indirectly influencing T-cell responses. Moreover, antigen (Ag)-presenting pDCs directly regulate T-cell differentiation. Depending on the immune environment, pDCs exhibit either tolerogenic or immunogenic properties. Here, we show that CpG-activated pDCs promote efficient Th17 differentiation. Indeed, Th17 responses are defective in mice selectively lacking MHCII on pDCs upon antigenic challenge. Importantly, in those mice, the frequency of Th17 cells infiltrating solid tumors is impaired. As a result, the recruitment of infiltrating leukocytes in tumors, including tumor-specific cytotoxic T lymphocytes (CTL), is altered and results in increased tumor growth. Importantly, following immunization with tumor Ag and CpG-B, MHCII-restricted Ag presentation by pDCs promotes the differentiation of antitumor Th17 cells that induce intratumor CTL recruitment and subsequent regression of established tumors. Our results highlight a new role for Ag presenting activated pDCs in promoting the development of Th17 cells and impacting on antitumor immunity.