PolyI:C plus IL‐2 or IL‐12 induce IFN‐γ production by human NK cells via autocrine IFN‐β

Abstract: NK lymphocytes and type I IFN (IFN-a/b) 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-b (but not IFN-a) 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-b Ab prevented the production of IFN-c induced by polyI:C plu… Show more

“…Although IL-12 is considered important for the induction of IFN-␥, it has been shown previously that IFN-␥ may also be induced by alternative pathways, including type I IFNs and IL-15 [35][36][37]. Notably, we found that Myd88 Ϫ/Ϫ ;Trif Lps2/Lps2 mice up-regulate Ifnb to a substantial extent during septic peritonitis and that IFN-regulated genes as well as IL-15 are induced normally.…”

“…5A), and expression of IL-15 was not altered in the absence of MyD88/ TRIF signaling (Fig. 5B), suggesting that these pathways may contribute to IFN-␥ production in septic peritonitis [35][36][37].…”

Improved host defense against septic peritonitis in mice lacking MyD88 and TRIF is linked to a normal interferon response

“…Although IL-12 is considered important for the induction of IFN-␥, it has been shown previously that IFN-␥ may also be induced by alternative pathways, including type I IFNs and IL-15 [35][36][37]. Notably, we found that Myd88 Ϫ/Ϫ ;Trif Lps2/Lps2 mice up-regulate Ifnb to a substantial extent during septic peritonitis and that IFN-regulated genes as well as IL-15 are induced normally.…”

“…5A), and expression of IL-15 was not altered in the absence of MyD88/ TRIF signaling (Fig. 5B), suggesting that these pathways may contribute to IFN-␥ production in septic peritonitis [35][36][37].…”

Improved host defense against septic peritonitis in mice lacking MyD88 and TRIF is linked to a normal interferon response

“…As expected, poly I : C directly induced the secretion of IFN-, as well as pro-inflammatory cytokine IL-6 and IL-8 by NK cells in a dose-dependent manner without the help of other cytokines [44]. And NK cells showed a up-regulation of CD69 expression and enhanced cytotoxicity targeting K562 tumor cells [44,45]. Similarly, poly I : C also directly activated human NK cell lines, NK92, YTCl2 and YTS, which all had a notable TLR3 expression [43].…”

“…Similarly, poly I : C also directly activated human NK cell lines, NK92, YTCl2 and YTS, which all had a notable TLR3 expression [43]. Poly I : C stimulation up-regulated the cytotoxic activity of NK cells targeting K562 and 721.221 cell lines, promoted the secretion of IFN- and induced the CXCL10 mRNA without additional cytokines or cell assist [44,45]. Further study proved that the TLR3 stimulation can directly induce the activation of TRIF/TICAM-1-dependent transcription factor IRF-3 and p38 MAPK in these human NK cell lines, and activation of p38 MAPK was essential for the activation of NK cells [43].…”

Critical role of Toll-like receptor signaling in NK cell activation

“…4B) can also induce NK activity (37). Activated DCs and KCs secrete IL-6, IL-12, and TNF-␣, which stimulate NK (38,39) and NKT (40) cells to produce IFN-␥. In turn, IFN-␥ upregulates NKmediated lysis of HBV-infected cells, enhances the cytokine response of KC, and recruits HBV-specific T cells (41).…”

Poly(I:C) Treatment Leads to Interferon-Dependent Clearance of Hepatitis B Virus in a Hydrodynamic Injection Mouse Model