Interleukin-6 induces hepcidin expression through STAT3

Wrighting, Diedra M.; Andrews, Nancy C.

doi:10.1182/blood-2006-06-027631

Cited by 797 publications

(628 citation statements)

References 30 publications

(29 reference statements)

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“…7 This study underlines the Iron regulation during acute-phase reaction N Sheikh et al differences between the two animal models and indirectly confirms that IL-6 is the major player in modifying iron metabolism under acute-phase condition. 13,[38][39][40][41][42][43][44] Most studies to date have shown that the transcriptional changes in the Hepc gene expression parallel the changes in serum iron concentration; however, limited studies have been performed to show the changes in the concentration of this important hormone in the serum. [45][46][47][48] Intramuscular TO injection induced significant decrease of the serum iron concentration without a significant change in serum proHepc concentration.…”

Section: Discussionmentioning

confidence: 99%

Changes of gene expression of iron regulatory proteins during turpentine oil-induced acute-phase response in the rat

Sheikh

Dudás

Ramadori

2007

Laboratory Investigation

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Section: Discussionmentioning

confidence: 99%

Changes of gene expression of iron regulatory proteins during turpentine oil-induced acute-phase response in the rat

Sheikh

Dudás

Ramadori

2007

Laboratory Investigation

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“…Recent findings have provided information regarding the part of the promoter required for IL-6 to induce hepcidin expression through the mediation of STAT3 [11]. However, the mechanism by which iron stimulates hepcidin expression still remains unclear.…”

Section: Discussionmentioning

confidence: 99%

In vivo imaging of hepcidin promoter stimulation by iron and inflammation

Flanagan¹,

Truksa²,

Peng³

et al. 2007

Blood Cells, Molecules, and Diseases

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Hepcidin is an acute-phase response antimicrobial peptide that has emerged as a central regulator of iron absorption. Circulating hepcidin levels have been shown to affect iron uptake, release and storage. Hepcidin is mainly liver-derived and regulated, at least in part, transcriptionally. Hypoxia, erythroid demand, iron content and inflammation each have been shown to influence hepcidin mRNA expression in intact animals. In vitro, regulation of hepcidin by cytokines and by hypoxia is readily demonstrated in primary hepatocytes or in hepatocyte lines, but incubating the same cell lines with iron does not increase transcription of hepcidin. Thus, how iron excess stimulates hepcidin production in hepatocytes remains unknown. In addition, there is no current technique available that can investigate how iron induces hepcidin expression. To provide a better understanding of hepcidin gene expression in response to these regulatory stimuli, we have established a whole animal in vivo bioluminescence imaging assay to measure the activity of hepcidin promoter constructs in the animals liver after hydrodynamic transfection of hepcidin promoter/luciferase constructs into mice. Transfected hepcidin promoter constructs were shown to respond to both inflammatory and increasing iron stimuli in vivo. This work highlights the ability of this new imaging technique to investigate the key regions of the hepcidin promoter involved in iron induction of hepcidin expression.

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“…2A, inset). Earlier studies concentrated on the regulation of HAMP expression at the transcriptional level (12)(13)(14)(15). The effect of fatty acids on HAMP transcription was examined by luciferase reporter assays in HepG2 cells transfected with pGL-3 Basic vector harboring the 1.5-kbp HAMP promoter (HAMP PromLuc).…”

Section: Regulation Of Hamp Mrna Expression By Fatty Acids Inmentioning

confidence: 99%

“…Inflammatory cyto-kines, serum transferrin, erythropoiesis, and hepatic iron stores have all been shown to stimulate the promoter activities of both human and mouse hepcidin genes via the activation of specific transcription factors (12)(13)(14)(15). It should, however, be noted that other iron-regulatory proteins, transferrin receptor 1 and ferritin, are regulated at the post-transcriptional and translational level, respectively, by iron-regulatory RNA-binding proteins (IRPs), IRP1 and IRP2 (16).…”

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confidence: 99%