2008
DOI: 10.1016/j.febslet.2008.02.058
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IFNγ enhances IL‐23 production during Francisella infection of human monocytes

Abstract: We previously demonstrated that monocytes produce IL-23 during Francisella infection, and that IL-23 induces IFNc from NK cells. Here, we demonstrate that IFNc-priming of monocytes enhances IL-23 production during Francisella infection. This effect was seen on the IL12/23 p40 subunit. Induction of IL-12/23 p40 is reported to be enhanced by IRF-1 and IRF-8. Consistently, microarray analysis of IFNc-treated monocytes revealed a significant induction of the IRFs. Interestingly, IFNcprimed monocytes produced IL-12… Show more

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Cited by 12 publications
(13 citation statements)
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“…In line with our observations, IFN-γ was recently reported to enhance Francisella tularensis induced IL-23 in human monocytes [24]. IFN-γ allows for the transcription of IL-12p35 in response to LPS [25] and for the induction of IL-12 in response to a PAMP an additional stimulus such as IFN-γ is needed [5].…”
Section: Discussionsupporting
confidence: 86%
“…In line with our observations, IFN-γ was recently reported to enhance Francisella tularensis induced IL-23 in human monocytes [24]. IFN-γ allows for the transcription of IL-12p35 in response to LPS [25] and for the induction of IL-12 in response to a PAMP an additional stimulus such as IFN-γ is needed [5].…”
Section: Discussionsupporting
confidence: 86%
“…This result is in favor of the hypothesis that engagement to IL-23 production may persist in proinflammatory conditions such as natural killer cell activation (Butchar et al, 2007;Kim et al, 2009) or even after the DC-T cell interaction, leading to IFN-g production in the microenvironment. Moreover, IFN-g-priming of human monocytes or human monocytederived macrophages/DCs enhances IL-23 production during Francisella infection (Butchar et al, 2008) lipopolysaccharide treatment, respectively (Roses et al, 2008;Verreck et al, 2004). Interestingly, this increase in IL-23 production in NiSO 4 and IFN-g-activated MoDCs was accompanied with a higher fold induction of IL-12p70 as shown in this study and previously described by Antonios et al (2010), suggesting that IL-12p70 was the master regulatory cytokine in shaping T-cell responses in the case of DCs treated concomitantly with NiSO 4 and IFN-g.…”
Section: Discussionmentioning
confidence: 99%
“…IFN-␥ is important in the activation of macrophages to effectively kill intracellular bacteria and in the induction of CD4 ϩ Th1 and CD8 ϩ cytotoxic T cell responses. IFN-␥ has been demonstrated to suppress Francisella replication inside macrophages, inhibit phagosome escape, and also induce the expression of IL-23 (3,5). Conversely, Francisella infection may suppress activation of STAT1 expression and phosphorylation, possibly through upregulated expression of suppressors of cytokine signaling 3 (SOCS3) (27).…”
Section: Discussionmentioning
confidence: 99%