Publication | Open Access
Regulation of Angiogenic Functions by Angiopoietins through Calcium-Dependent Signaling Pathways
22
Citations
30
References
2015
Year
Signal TransductionAngiogenesisSignaling PathwayCalcium-dependent Signaling PathwaysMedicineVascular AdaptationPhysiologyIntracellular Calcium MobilizationEndothelial DysfunctionBlood Vessel AssemblyVascular BiologyCellular PhysiologyHuvecs MonolayerNeovascularizationPharmacologyCell BiologyCell SignalingTumor Microenvironment
Angiopoietins are vascular factors essential for blood vessel assembly and correct organization and maturation. This study describes a novel calcium-dependent machinery activated through Angiopoietin-1/2-Tie receptor system in HUVECs monolayer. Both cytokines were found to elicit intracellular calcium mobilization. Targeting intracellular Ca(2+) signaling, antagonizing IP3 with 2-APB or cADPR with 8Br-cADPR, was found to modulate in vitro angiogenic responses to Angiopoietins in a specific way. 2-APB and 8Br-cADPR impaired the phosphorylation of AKT and FAK induced by Ang-1 and Ang-2. On the other hand, phosphorylation of ERK1/2 and p38, as well as cell proliferation, was not affected by either inhibitor. The ability of ECs to migrate following Angs stimulation, evaluated by "scratch assay," was reduced by either 2-APB or 8Br-cADPR following Ang-2 stimulation and only slightly affected by 2-APB in cells stimulated with Ang-1. These results identify a novel calcium-dependent machinery involved in the complex interplay regulating angiogenic processes showing that IP3- and cADPR-induced Ca(2+) release specifically regulates distinct Angs-mediated angiogenic steps.
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