Vascular endothelial growth factor increases Rana vascular permeability and compliance by different signalling pathways

Vascular endothelial growth factor (VEGF) chronically increases microvascular permeability, compliance and vessel diameter. To determine the signalling pathways by which VEGF exerts these effects, we investigated the role of Ca 2+ influx and mitogen-activated protein kinase (MAPK) phosphorylation on the increase in hydraulic conductivity ( L p ), diameter and compliance in mesenteric microvessels in the anaesthetised frog ( Rana species). The VEGF-mediated chronically increased permeability was attenuated by co-perfusion of VEGF with 5 m m NiCl 2 , previously shown to inhibit Ca 2+ influx. MAPK phosphorylation inhibition by PD98059 did not affect the chronic increase in L p . To determine whether other agonists which increased Ca 2+ influx also chronically increased L p , the effect of ATP perfusion on chronic L p was measured. ATP perfusion also chronically increased L p . The chronic increase in L p was therefore dependent on an initial transient Ca 2+ influx, and not MAPK activation, and was not unique to VEGF stimulation. Inhibition of Ca 2+ influx did not inhibit the increase in microvascular diameter or compliance brought about by VEGF. Both these increases were inhibited by PD98059. The VEGF-mediated increase in compliance and diameter was therefore dependent on MAPK activation, not on Ca 2+ influx. The chronic increase in L p stimulated by VEGF perfusion 24 h previously was reduced when the vessel was perfused with 5 m m NiCl 2 . The sustained, high L p was therefore dependent on Ca 2+ influx. The endothelial cell calcium concentration ([Ca 2+ ] i ) of vessels previously perfused with VEGF or ATP, and with a chronically increased L p , was not significantly increased compared to [Ca 2+ ] i of endothelial cells in vessels before agonist perfusion These experiments show that VEGF acts through different pathways to stimulate increased permeability and compliance. The data are consistent with the hypothesis that VEGF chronically increases L p through an acute stimulation of Ca 2+ influx, but increases compliance and diameter by acute stimulation of the MAPK signalling pathway. They also suggest that the increase in L p is dependent on a sustained Ca 2+ influx, even though the endothelial [Ca 2+ ] i is not raised.