Tumor necrosis factor α decreases aquaporin 3 expression in intestinal epithelial cells through inhibition of constitutive transcription

Tumor necrosis factor α decreases aquaporin 3 expression in intestinal epithelial cells through inhibition of constitutive transcription

Inflammatory diseases of the gut are associated with altered electrolyte and water transport, leading to the development of diarrhea. Epithelially expressed aquaporins (AQPs) are downregulated in inflammation, although the mechanisms involved are not known. We hypothesized that AQP3 expression in in...

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Bibliographic Details
Published in:Physiological reports Vol. 5; no. 19; pp. e13451 - n/a
Main Authors: Peplowski, Michael A., Vegso, Andrew J., Iablokov, Vadim, Dicay, Michael, Zaheer, Raza S., Renaux, Bernard, Proud, David, Hollenberg, Morley D., Beck, Paul L., MacNaughton, Wallace K.
Format: Journal Article
Language:English
Published: United States John Wiley & Sons, Inc 01-10-2017
John Wiley and Sons Inc
Subjects:
Adenocarcinoma
Aquaporin
Aquaporin 3
Aquaporin 3 - genetics
Aquaporin 3 - metabolism
Cellular and Molecular Physiology
Diarrhea
Enterocytes - drug effects
Enterocytes - metabolism
Epithelial cells
Gastrointestinal Tract
Gene expression
Glycerol
HT29 Cells
Humans
Inflammation
inflammatory bowel disease
Inflammatory diseases
intestinal epithelium
Intestine
Intracellular signalling
Ion channels
MAP Kinase Signaling System
Necrosis
NF-kappa B - metabolism
NF-κB protein
Original Research
Promoter Regions, Genetic
RNA, Messenger - genetics
RNA, Messenger - metabolism
Sp3 Transcription Factor - metabolism
transcription regulation
Tumor necrosis factor
Tumor Necrosis Factor-alpha - pharmacology
Tumor necrosis factor-TNF
transcription regulation
tumor necrosis factor (TNF)
intestinal epithelium
Aquaporin
inflammatory bowel disease
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Summary:Inflammatory diseases of the gut are associated with altered electrolyte and water transport, leading to the development of diarrhea. Epithelially expressed aquaporins (AQPs) are downregulated in inflammation, although the mechanisms involved are not known. We hypothesized that AQP3 expression in intestinal epithelial cells is altered in intestinal inflammation and that these changes are driven by tumor necrosis factor (TNF) α. Human colonic adenocarcinoma (HT‐29) cells were treated with TNFα to investigate signaling mechanisms in vitro. AQP3 expression was assessed by real‐time PCR and radiolabeled glycerol uptake, with select inhibitors and a luciferase reporter construct used to further elucidate intracellular signaling. AQP3 expression was downregulated in HT‐29 cells treated with TNFα. Luciferase reporter construct experiments revealed that TNFα downregulated constitutive transcriptional activity of the AQP3 promoter, and inhibition of MEK/ERK and nuclear factor κB (NF‐κB) signaling prevented the decrease in AQP3 mRNA expression. Constitutive AQP3 expression was suppressed by specificity protein (Sp) 3, and knockdown of this transcription factor bound to the AQP3 promoter was able to partially prevent the TNFα‐induced downregulation of AQP3. TNFα signals through MEK/ERK and NF‐κB to enhance the negative transcriptional control of AQP3 expression exerted by Sp3. Similar mechanisms regulate numerous ion channels, suggesting a common mechanism by which both ion and water transport are altered in inflammation. Aquaporins (AQPs) are water channels critical for a variety of functions in epithelia, including water and small solute transport, proliferation, and apoptosis. AQP3 is downregulated in colonic inflammation, with important physiological consequences, but the mechanism underlying this decreased expression remains unknown. We have discovered the signaling mechanisms whereby tumor necrosis factor suppresses AQP3 expression in intestinal epithelium. TNF activation of MAP kinases and NFB to mediate suppression of gene expression via the Sp3 transcription factor.
Bibliography:This work was supported by a grant from Crohn's and Colitis Canada. MAP received salary support in the form of graduate studentships from the Canadian Institutes for Health Research and Alberta Innovates – Health Solutions.
Funding Information
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ISSN:2051-817X
DOI:10.14814/phy2.13451