Acute-phase response factor, a nuclear factor binding to acute-phase response elements, is rapidly activated by interleukin-6 at the posttranslational level.

Wegenka, Ursula; Buschmann, Jan; Lütticken, Claudia; Heinrich, Peter C.; Horn, Friedemann

doi:10.1128/mcb.13.1.276

Cited by 520 publications

(388 citation statements)

References 65 publications

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“…Previous several studies identified a highly conserved CTGG(G/A)AA motif in the IL-6-responsive regions of all three fibrinogen genes (10,33,34). This CTGG(G/ A)AA motif was also identified in the IL-6-responsive promoter region of the ␣ 2 -macroglobulin gene (35). Since the discovery of STAT3/APRF (36, 37), which interacts with a consensus element of TT(A/C)(C/T)N(G/A)(G/T)AA sequence, there has been intense effort to verify the role of the putative CTGG(G/A)AA motif and STAT3 in regulating the three fibrinogen genes.…”

Section: Discussionmentioning

confidence: 99%

A SAF Binding Site in the Promoter Region of Human γ-Fibrinogen Gene Functions as an IL-6 Response Element

Ray

2000

The Journal of Immunology

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Expression of fibrinogen is highly induced during inflammation, and such abnormal expression of this protein is considered as a major cardiovascular risk factor. IL-6 is one of the main mediators of abnormal expression of fibrinogen leading to the pathogenic conditions. Transient transfection and EMSA were performed to investigate the molecular mechanism of IL-6-induced γ-fibrinogen gene expression in hepatic cells. Using progressively deleted 5′ fragments of the γ-fibrinogen promoter coupled to chloramphenicol acetyltransferase gene, an IL-6 responsive element located between positions −273 and −259 was identified. Mutation of this element abrogates IL-6 responsiveness of the γ-fibrinogen promoter. Interaction of this promoter with a zinc finger transcription factor, serum amyloid A activating factor (SAF)-1, was demonstrated by EMSA. Furthermore, overexpression of wild-type SAF-1 in transfected liver cells can increase transcription of the γ-fibrinogen promoter. These data show that transcription factor SAF-1 is involved in the regulation of IL-6-mediated induction of the human γ-fibrinogen gene in liver cells.

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Section: Discussionmentioning

confidence: 99%

A SAF Binding Site in the Promoter Region of Human γ-Fibrinogen Gene Functions as an IL-6 Response Element

Ray

2000

The Journal of Immunology

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“…Nuclear proteins of HepG2 cells were extracted as previously described [14]. A double-stranded synthetic oligonucleotide comprising the IL-6RE of the ICAM-1 promoter (upper strand: 5'-AGCTTAG-GTTTCCGGGAAAGCAC-3') was 32p-labelled by filling in the 5'-protruding ends with Klenow enzyme.…”

Section: Gel Retardation Analysismentioning

confidence: 99%

“…We have previously identified a ubiquitous transcription factor, APRF, which, in response to IL-6, transiently associates with gpl30 and then is tyrosine phosphorylated and translocated to the nucleus [12,14]. On the basis of immunological cross-reactivity and DNA-binding specificities we proposed a relationship of APRF to the interferon-),-activated transcription factor Stat 1 [15].…”

Section: Introductionmentioning

confidence: 99%

“…Thus, APRF, now also called Stat 3, belongs to a growing family (the Stat family) of signal transducing and transactivating proteins which all are recruited by tyrosine phosphorylation from latent cytoplasmic forms in response to cytokines, hormones, and growth factors [16,[18][19][20][21]. In the nucleus, APRF bnds to IL-6 response elements (IL-6REs) in the flanking regions of many acute-phase protein genes [14]. Furthermore, we could demonstrate its binding to IL-6REs in the promoters of the immediate-early genes IRF-1, ICAM-I, and junB [22,23].…”

Section: Introductionmentioning

confidence: 99%

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Interleukin‐6‐induced serine phosphorylation of transcription factor APRF: evidence for a role in interleukin‐6 target gene induction

et al. 1995

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The cytokine interleukin-6 (IL-6) rapidly activates a latent cytoplasmic transcription factor, acute-phase response factor (APRF), by tyrosine phosphorylation. Activation and DNA binding of APRF are inhibited by inhibitors of protein tyrosine kinases but not serinelthreonine kinases. However, immediateearly gene induction by IL-6 and, as we show here, stimulaton of the promoters of the genes for az-macroglobulin, Jun-B, and intercellular adhesion molecule-I (ICAM-I) are blocked by the serinelthreonine kinase inhibitor 1-17. We now show that IL-6 triggers a delayed phosphorylation of APRF at serine resudues which can be reversed in vitro by protein phosphatase 2A and is also inhibited by H7. Therefore, APRF serine phosphorylation is likely to represent a crucial event in IL-6 signal transduction leading to target gene induction.

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“…STAT3 was initially identified as an acute phase response factor, an inducible DNA binding protein that binds to the IL-6 responsive element within the promoters of hepatic acute phase protein genes [13] . Subsequent studies indicate that STAT3 becomes activated in response to a wide variety of cytokines and growth factors [4,5,14] .…”

Section: Stat3 and Ibd Patientsmentioning

confidence: 99%

Role of STAT3 in inflammatory bowel disease

Sugimoto¹

2008

WJG

108

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Signal transducers and activators of transcription 3 (STAT3) play an important role in various autoimmune disorders including inflammatory bowel disease (IBD). Recent studies have revealed that STAT3 activation plays distinctly different roles between innate immune responses and acquired immune responses in colitis. STAT3-mediated activation of acquired immune responses plays a pathogenic role in colitis by enhancing the survival of pathogenic T cells. In contrast, STAT3-mediated activation of innate responses contributes to the suppression of colitis. This review will summarize the current understanding of the roles of STAT3 in IBD and the potential of targeting STAT3 for the treatment of IBD, emphasizing recent observations.

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Acute-phase response factor, a nuclear factor binding to acute-phase response elements, is rapidly activated by interleukin-6 at the posttranslational level.

Cited by 520 publications

References 65 publications

A SAF Binding Site in the Promoter Region of Human γ-Fibrinogen Gene Functions as an IL-6 Response Element

A SAF Binding Site in the Promoter Region of Human γ-Fibrinogen Gene Functions as an IL-6 Response Element

Interleukin‐6‐induced serine phosphorylation of transcription factor APRF: evidence for a role in interleukin‐6 target gene induction

Role of STAT3 in inflammatory bowel disease

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