PolyI:C plus IL‐2 or IL‐12 induce IFN‐γ production by human NK cells via autocrine IFN‐β |
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Authors: | Dorothée Duluc Fang Tan Mari Scotet Simon Blanchard Isabelle Frémaux Erwan Garo Branka Horvat Pierre Eid Yves Delneste Pascale Jeannin |
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Affiliation: | 1. Institut National de la Santé et de la Recherche Médicale (Inserm), Unité 892, Centre de Recherche en Cancérologie Nantes‐Angers, Angers, France;2. Université d'Angers, Unité Mixte de Recherche‐Santé 892, Angers, France;3. Laboratoire d'immunologie et d'allergologie, Centre Hospitalier Universitaire d'Angers, Angers, France;4. Inserm Unité 758, Lyon, France;5. University of Lyon 1, Lyon France;6. Inserm, Unité 542, Université Paris‐Sud, H?pital Paul Brousse, Villejuif, France |
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Abstract: | NK lymphocytes and type I IFN (IFN‐α/β) are major actors of the innate anti‐viral response that also influence adaptive immune responses. We evaluated type I IFN production by human NK cells in response to polyI:C, a potent type I IFN‐inducing TLR3 agonist. PolyI:C plus IL‐2/IL‐12 induced IFN‐β (but not IFN‐α) mRNA expression and protein production by highly pure human NK cells and by the human NK cell line NK92. Neutralizing anti‐IFNAR1 or anti‐IFN‐β Ab prevented the production of IFN‐γ induced by polyI:C plus IL‐2/IL‐12. Similarly, IFN‐γ production induced by polyI:C plus IL‐12 was reduced in NK cells isolated from IFNAR1?/? compared with WT mice. The ability of polyI:C plus IL‐12 to induce IFN‐γ production was related to an increase of TLR3, Mda5 and IFNAR expression and by an increase of STAT1 and STAT4 phosphorylation. Collectively, these data demonstrate that NK cells, in response to polyI:C plus IL‐2/IL‐12, produce IFN‐β that induce, in an autocrine manner, the production of IFN‐γ and thereby highlight that NK cells may control the outcome of protective or injurious immune responses through type I IFN secretion. |
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Keywords: | IFN‐g NK cells PolyI:C Type I IFN |
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