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PubMed articles by:
Medford, A.
Douglas, S.
Godinho, S.
Millar, A.
Respir Res. 2009; 10(1): 27.
Published online 2009 April 9. doi: 10.1186/1465-9921-10-27.
PMCID: PMC2674417
Copyright © 2009 Medford et al; licensee BioMed Central Ltd.
Vascular Endothelial Growth Factor (VEGF) isoform expression and activity in human and murine lung injury
Andrew RL Medford,1 Samantha K Douglas,1 Sofia IH Godinho,1 Kay M Uppington,1 Lynne Armstrong,1 Kathleen M Gillespie,1 Berendine van Zyl,1 Terry D Tetley,2 Nassif BN Ibrahim,3 and Ann B Millarcorresponding author1
1Department of Clinical Science at North Bristol, University of Bristol Paul O'Gorman Lifeline Centre, Southmead Hospital, Westbury-on-Trym, Bristol, BS10 5NB, UK
2Lung Cell Biology, National Heart & Lung Institute, Imperial College, Dovehouse Street, London, SW3 6LY, UK
3Department of Pathology, North Bristol NHS Trust, Frenchay Hospital, Frenchay Park Road, Frenchay, Bristol, BS16 1LE, UK
corresponding authorCorresponding author.
Andrew RL Medford: andrewmedford/at/hotmail.com; Samantha K Douglas: samantha.douglas/at/bristol.ac.uk; Sofia IH Godinho: sofia.godinho/at/bristol.ac.uk; Kay M Uppington: kay.uppington/at/bristol.ac.uk; Lynne Armstrong: lynne.armstrong/at/bristol.ac.uk; Kathleen M Gillespie: K.M.Gillespie/at/bristol.ac.uk; Berendine van Zyl: Berendine.vanZyl/at/bristol.ac.uk; Terry D Tetley: t.tetley/at/imperial.ac.uk; Nassif BN Ibrahim: Nassif.Ibrahim/at/nbt.nhs.uk; Ann B Millar: Ann.Millar/at/bristol.ac.uk
Received September 23, 2008; Accepted April 9, 2009.
This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
 
Abstract
Background
The properties of vascular endothelial growth factor (VEGF) as a potent vascular permogen and mitogen have led to investigation of its potential role in lung injury. Alternate spliced VEGF transcript generates several isoforms with potentially differing functions. The purpose of this study was to determine VEGF isoform expression and source in normal and ARDS subjects and investigate the expression and regulation of VEGF isoforms by human alveolar type 2 (ATII) cells.
Methods
VEGF protein expression was assessed immunohistochemically in archival normal and ARDS human lung tissue. VEGF isoform mRNA expression was assessed in human and murine lung tissue. Purified ATII cells were cultured with proinflammatory cytokines prior to RNA extraction/cell supernatant sampling/proliferation assay.
Measurements and Main Results
VEGF was expressed on alveolar epithelium, vascular endothelium and alveolar macrophages in normal and ARDS human lung tissue. Increases in VEGF expression were detected in later ARDS in comparison to both normal subjects and early ARDS (p < 0.001). VEGF121, VEGF165 and VEGF189 isoform mRNA expression increased in later ARDS (p < 0.05). The ratio of soluble to cell-associated isoforms was lower in early ARDS than normal subjects and later ARDS and also in murine lung injury. ATII cells constitutionally produced VEGF165 and VEGF121 protein which was increased by LPS (p < 0.05). VEGF165 upregulated ATII cell proliferation (p < 0.001) that was inhibited by soluble VEGF receptor 1 (sflt) (p < 0.05).
Conclusion
These data demonstrate that changes in VEGF isoform expression occur in ARDS which may be related to their production by and mitogenic effect on ATII cells; with potentially significant clinical consequences.
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