Stimulation of endothelial cell migration by vascular permeability factor/vascular endothelial growth factor through cooperative mechanisms involving the alphavbeta3 …

DR Senger, SR Ledbetter, KP Claffey… - The American journal …, 1996 - ncbi.nlm.nih.gov
DR Senger, SR Ledbetter, KP Claffey, A Papadopoulos-Sergiou, CA Peruzzi, M Detmar
The American journal of pathology, 1996ncbi.nlm.nih.gov
We have identified several mechanisms by which the angiogenic cytokine vascular
permeability factor/vascular endothelial growth factor (VPF/VEGF) likely regulates
endothelial cells (EC) migration. VPF/VEGF induced dermal microvascular EC expression of
mRNAs encoding the alphav and beta3 integrin subunits resulting in increased levels of the
alphavbeta3 heterodimer at the cell surface, and VPF/VEGF also induced mRNA encoding
osteopontin (OPN), an alphavbeta3 ligand. OPN promoted EC migration in vitro; and …
Abstract
We have identified several mechanisms by which the angiogenic cytokine vascular permeability factor/vascular endothelial growth factor (VPF/VEGF) likely regulates endothelial cells (EC) migration. VPF/VEGF induced dermal microvascular EC expression of mRNAs encoding the alphav and beta3 integrin subunits resulting in increased levels of the alphavbeta3 heterodimer at the cell surface, and VPF/VEGF also induced mRNA encoding osteopontin (OPN), an alphavbeta3 ligand. OPN promoted EC migration in vitro; and VPF/VEGF induction of alphavbeta3 was accompanied by increased EC migration toward OPN. Because thrombin cleavage of OPN results in substantial enhancement of OPN's adhesive properties, and because VPF/VEGF promotes increased microvascular permeability leading to activation of the extrinsic coagulation pathway, we also investigated whether VPF/VEGF facilitates thrombin cleavage of OPN in vivo. Consistent with this hypothesis, co-injection of VPF/VEGF together with OPN resulted in rapid cleavage of OPN by endogenous thrombin. Furthermore, in comparison with native OPN, thrombin-cleaved OPN stimulated a greater rate of EC migration in vitro, which was additive to the increased migration associated with induction of alpha v beta 3. Thus, these data demonstrate cooperative mechanisms for VPF/VEGF regulation of EC migration involving the alphavbeta3 integrin, the alphavbeta3 ligand OPN, and thrombin cleavage of OPN. These findings also illustrate an operational link between VPF/VEGF induction of EC gene expression and VPF/VEGF enhancement of microvascular permeability, suggesting that these distinct biological activities may act accordingly to stimulate EC migration during angiogenesis.
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