Synergy of IL-12 and IL-18 for IFN-γ Gene Expression: IL-12-Induced STAT4 Contributes to IFN-γ Promoter Activation by Up-Regulating the Binding Activity of IL-18-Induced Activator Protein 1

Nakahira, Masakiyo; Ahn, Hyung Joon; Park, Woong Ryeon; Gao, Ping; Tomura, Michio; Park, Cheung Seog; Hamaoka, Toshiyuki; Ohta, Toshio; Kurimoto, Masashi; Fujiwara, Hiromi

doi:10.4049/jimmunol.168.3.1146

Cited by 231 publications

(186 citation statements)

References 37 publications

(39 reference statements)

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“…By using pharmacological inhibitors of these pathways (SB203580 for p38 and U0126 for Erk), we completely blocked the synergistic expression of IFNg [11], thus demonstrating that both pathways are critical for the synergistic increase in gene expression. These results are most consistent with the model proposed by Nakahira and colleagues [13] where increased pSTAT4 (resulting from the IL-12 treatment) results in increased recruitment of AP-1 to the IFNg promoter [note that in our model, cross-linking LY49D results in increased AP-1 activity, (McVicar DW personal communication)]…”

Section: Resultssupporting

confidence: 92%

Cytokines as critical co-stimulatory molecules in modulating the immune response of natural killer cells

Young

Ortaldo

2006

Cell Res

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Cytokines are involved in directing the activation of natural killer (NK) cells. NK cells are involved in the recognition of cells that have been altered; thus they do not recognize specific insults to the host, but when activated, are capable of destroying infected cells directly, as well as promoting the recruitment and response of the other components of the immune system by the release of cytokines and chemokines. It is these properties that have made NK cells a critical part of innate immunity and adaptive immunity, and they play a principal role linking innate and adaptive immunity by the recruitment of an adaptive immune response to an innate immune reaction.

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Section: Resultssupporting

confidence: 92%

Cytokines as critical co-stimulatory molecules in modulating the immune response of natural killer cells

Young

Ortaldo

2006

Cell Res

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“…CD40LT elicited production of the c-Jun, but not the c-Fos, component of AP-1. The combination of IL-12 and IL-18 markedly increases production and phosphorylation of c-Jun, enhancing binding to AP-1 sites of the IFN-␥ promoter (25). Because we found that the capacity of CD40LT to enhance IFN-␥ production by CD8 ϩ T cells was dependent on the presence of IL-12 and IL-18, we speculate that this effect is mediated in part through c-Jun.…”

Section: Discussionmentioning

confidence: 63%

“…Binding of CD40L on T cells to CD40 on APCs elicits production of IL-12 and IL-18 (22)(23)(24), and IL-12 and IL-18 enhance production of IFN-␥ by CD4 ϩ T cells (25,26). IL-15 also contributes to IFN-␥ production by CD8 ϩ cells in response to mycobacteria (27).…”

Section: Contribution Of Monokines To the Capacity Of Cd40lt To Incrementioning

confidence: 99%

“…The transcription factor AP-1 is composed of dimers of members of the Jun and Fos families, and IL-12 and IL-18 markedly increase production and phosphorylation of c-Jun, enhancing binding to the IFN-␥ promoter (25). Because the experiments above suggested that CD40LT enhanced IFN-␥ production through production of IL-12 and IL-18, we studied the effect of CD40LT on expression of c-Jun in CD8 ϩ T cells from five healthy tuberculin reactors cultured with M. tuberculosis-infected monocytes.…”

Section: Effect Of Cd40lt On Transcription Factors That Activate the mentioning

confidence: 99%

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CD40 Ligand Trimer Enhances the Response of CD8+ T Cells to Mycobacterium tuberculosis

Samten

Wizel

Shams

et al. 2003

The Journal of Immunology

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We investigated the effect of recombinant CD40 ligand trimer (CD40LT) on the functional capacity of peripheral blood CD8+ T cells from healthy tuberculin reactors that were cultured with Mycobacterium tuberculosis-infected autologous monocytes. CD40LT enhanced the capacity of M. tuberculosis-responsive CD8+ T cells to produce IFN-γ by increasing the number of IFN-γ-producing CD8+ T cells and the amount of IFN-γ produced per cell. CD40LT-induced IFN-γ production was dependent on production of IL-12 and IL-18, but did not require IL-15. CD40LT up-regulated expression of the transcription factors phosphorylated CREB and c-Jun, both of which have been previously shown to stimulate IFN-γ mRNA transcription by binding to the IFN-γ promoter. CD40LT also enhanced the capacity of CD8+ T cells to lyse M. tuberculosis-infected monocytes, and increased CTL activity was associated with higher expression of perforin and granulysin, but not of Fas ligand. We conclude that CD40LT can enhance CD8+ T cell effector function in response to M. tuberculosis.

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“…IL12 cooperation with IL18 has been speculated to function via IL18 receptor upregulation and STAT4 activation. 17,20 Apart from interferon gamma expression, little is known about other genes regulated by IL18 alone or in combination with other cytokines.…”

Section: Introductionmentioning

confidence: 99%

cis-Element clustering correlates with dose-dependent pro- and antisignaling effects of IL18

et al. 2004

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We examine the effects of IL18 on monocytes by performing microarray experiments using cell line KG1. Based on sensitivity to IL18, we identified three functionally distinct gene expression clusters (EC). We see little proinflammatory gene induction at low IL18 concentrations, but instead observe induction of diverse NFkB signaling inhibitors. Conversely, intermediate concentrations of IL18 induced proinflammatory genes including the activating subunits of NFkB. At the highest IL18 concentration, we observe a third gene cluster containing the proapoptotic Fas gene among others. Clustering of IL18-responsive genes based on cis-elements in their promoters agreed well with the ECs. We conclude that IL18 produces a dosedependent transcriptional response that can in part be attributed to the composition of cis-elements in the promoters of IL18-responsive genes. These results also support a model for regulatory mechanisms that prevent spurious immune response due to weak cytokine fluctuations and a separate mechanism enabling induction of proinflammatory functions by higher levels of cytokine.

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Synergy of IL-12 and IL-18 for IFN-γ Gene Expression: IL-12-Induced STAT4 Contributes to IFN-γ Promoter Activation by Up-Regulating the Binding Activity of IL-18-Induced Activator Protein 1

Cited by 231 publications

References 37 publications

Cytokines as critical co-stimulatory molecules in modulating the immune response of natural killer cells

Cytokines as critical co-stimulatory molecules in modulating the immune response of natural killer cells

CD40 Ligand Trimer Enhances the Response of CD8+ T Cells to Mycobacterium tuberculosis

cis-Element clustering correlates with dose-dependent pro- and antisignaling effects of IL18

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