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Article Dans Une Revue Science Année : 2015

RIPK1 and NF- B signaling in dying cells determines cross-priming of CD8+ T cells

Résumé

Dying cells initiate adaptive immunity by providing both antigens and inflammatory stimuli for dendritic cells, which in turn activate CD8(+) T cells through a process called antigen cross-priming. To define how different forms of programmed cell death influence immunity, we established models of necroptosis and apoptosis, in which dying cells are generated by receptor-interacting protein kinase-3 and caspase-8 dimerization, respectively. We found that the release of inflammatory mediators, such as damage-associated molecular patterns, by dying cells was not sufficient for CD8(+) T cell cross-priming. Instead, robust cross-priming required receptor-interacting protein kinase-1 (RIPK1) signaling and nuclear factor κB (NF-κB)-induced transcription within dying cells. Decoupling NF-κB signaling from necroptosis or inflammatory apoptosis reduced priming efficiency and tumor immunity. Our results reveal that coordinated inflammatory and cell death signaling pathways within dying cells orchestrate adaptive immunity.

Domaines

Immunologie Biologie cellulaire

Marie-Christine Vougny  : Connectez-vous pour contacter le contributeur

https://pasteur.hal.science/pasteur-01380732

Soumis le : jeudi 13 octobre 2016-13:56:45

Dernière modification le : jeudi 23 novembre 2023-10:49:15

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Dates et versions

pasteur-01380732 , version 1 (13-10-2016)

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Citer

N. Yatim, H. Jusforgues-Saklani, S. Orozco, O. Schulz, R. Barreira da Silva, et al.. RIPK1 and NF- B signaling in dying cells determines cross-priming of CD8+ T cells. Science, 2015, 350 (6258), pp.328-334. ⟨10.1126/science.aad0395⟩. ⟨pasteur-01380732⟩

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