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Published in: Inflammation Research 9/2010

01-09-2010 | Original Research Paper

Endotoxin-induced HIF-1α stabilisation in equine endothelial cells: synergistic action with hypoxia

Authors: A. C. Brooks, N. Menzies-Gow, S. R. Bailey, F. M. Cunningham, J. Elliott

Published in: Inflammation Research | Issue 9/2010

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Abstract

Objective and design

Hypoxia may enhance the deleterious effects of lipopolysaccharide (LPS) in the endotoxaemic horse. This study has examined some of the actions of LPS and hypoxia, alone and in combination, on cultured equine digital vein endothelial cells (EDVEC) and the signalling molecules involved.

Methods

EDVEC were exposed to LPS, 5% O2 and LPS then 5% O2 for up to 24 h. HIF-1α stabilisation, neutrophil adhesion and EDVEC permeability were assessed by immunoblotting, measurement of myeloperoxidase and movement of FITC-dextran, respectively. Pharmacological inhibitors were used to assess the roles of p38 MAPK and HIF-1α.

Results

LPS and hypoxia significantly increased HIF-1α stabilisation, neutrophil adhesion and EDVEC permeability and the effects of the two stimuli in combination on HIF-1α stabilisation and neutrophil adhesion were more than additive. The effect of LPS, but not 5% O2, on neutrophil adherence required activation of p38 MAPK, whereas EDVEC permeability in response to both stimuli was dependent on p38 MAPK and HIF-1α.

Conclusions

Exposure of EDVEC to LPS prior to induction of hypoxia up-regulates responses that may enhance LPS-induced tissue damage in the endotoxaemic horse. Inhibitors of p38 MAPK or HIF-1α could reduce such unwanted effects.
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Metadata
Title
Endotoxin-induced HIF-1α stabilisation in equine endothelial cells: synergistic action with hypoxia
Authors
A. C. Brooks
N. Menzies-Gow
S. R. Bailey
F. M. Cunningham
J. Elliott
Publication date
01-09-2010
Publisher
SP Birkhäuser Verlag Basel
Published in
Inflammation Research / Issue 9/2010
Print ISSN: 1023-3830
Electronic ISSN: 1420-908X
DOI
https://doi.org/10.1007/s00011-010-0180-x

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