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Article Dans Une Revue Journal of Immunology Année : 2017

Cutting Edge: Murine NK Cells Degranulate and Retain Cytotoxic Function without Store-Operated Calcium Entry

Résumé

Sustained Ca2+ signaling, known as store-operated calcium entry (SOCE), occurs downstream of immunoreceptor engagement and is critical for cytotoxic lymphocyte signaling and effector function. CD8(+) T cells require sustained Ca2+ signaling for inflammatory cytokine production and the killing of target cells; however, much less is known about its role in NK cells. In this study, we use mice deficient in stromal interacting molecules 1 and 2, which are required for SOCE, to examine the contribution of sustained Ca2+ signaling to murine NK cell function. Surprisingly, we found that, although SOCE is required for NK cell IFN-gamma production in an NFAT-dependent manner, NK cell degranulation/cytotoxicity and tumor rejection in vivo remained intact in the absence of sustained Ca2+ signaling. Our data suggest that mouse NK cells use different signaling mechanisms for cytotoxicity compared with other cytotoxic lymphocytes.

Domaines

Immunologie

Dates et versions

hal-01765105 , version 1 (12-04-2018)

Identifiants

Citer

Jacquelyn Freund-Brown, Ruth Choa, Brenal K. Singh, Tanner Ford Robertson, Gabrielle M. Ferry, et al.. Cutting Edge: Murine NK Cells Degranulate and Retain Cytotoxic Function without Store-Operated Calcium Entry. Journal of Immunology, 2017, 199 (6), pp.1973-1978. ⟨10.4049/jimmunol.1700340⟩. ⟨hal-01765105⟩

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