Abstract

The vascular endothelial growth factor (VEGF) was originally described as vascular permeability factor due to its ability to increase microvascular permeability to plasma proteins. However, the vessel types (arteriolar, venular, and capillary) affected by VEGF and the modification of endothelial morphology in response to increased permeability induced by VEGF in vivo have not been precisely documented. By topical application or intradermal injection of recombinant human VEGF-165 we find that VEGF increases the permeability of postcapillary venules as well as muscular venules and capillaries. Surprisingly, we also find that endothelia of small venules and capillaries become fenestrated within 10 minutes of VEGF application. Fenestrations appeared in vascular beds which do not normally have fenestrated endothelium, namely the cremaster muscle and skin. Histamine, saline, and heat-inactivated VEGF do not cause fenestrations. Increased permeability is completely inhibited when VEGF is cleared by immunoprecipitation with anti-VEGF monoclonal antibodies. The VEGF effect on permeability is unlike that of any other mediator described to date since both muscular venules and capillaries are affected.

Keywords

Vascular permeabilityCremaster muscleVascular endothelial growth factorBiologyMicrocirculationEndotheliumVascular endothelial growth factor CEvans BlueBlood vesselVenuleVascular endothelial growth factor APathologyAnatomyIn vivoVEGF receptorsEndocrinologyInternal medicineMedicineCancer research

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Publication Info

Year
1995
Type
article
Volume
108
Issue
6
Pages
2369-2379
Citations
1024
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W. Gregory Roberts, George E. Palade (1995). Increased microvascular permeability and endothelial fenestration induced by vascular endothelial growth factor. Journal of Cell Science , 108 (6) , 2369-2379. https://doi.org/10.1242/jcs.108.6.2369

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DOI
10.1242/jcs.108.6.2369