4.6 Article

The Role of Heparan Sulfate and Neuropilin 2 in VEGFA Signaling in Human Endothelial Tip Cells and Non-Tip Cells during Angiogenesis In Vitro

CELLS (2021)

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Journal

CELLS
Volume 10, Issue 4, Pages -

Publisher

MDPI
DOI: 10.3390/cells10040926

Keywords

endothelial cells; angiogenesis; VEGFA; tip cells; SULF2; NRP2; HSPG

Categories

Cell Biology

Funding

  1. Landelijke Stichting voor Blinden en Slechtzienden
  2. Algemene Nederlandse Vereniging Ter Voorkoming Van Bindheid
  3. Stichting Blindenpenning
  4. Novartisfonds
  5. ODAS stichting [UitZicht2013-12, UitZicht2018-26]
  6. Stichting tot Verbetering van het Lot der Blinden, Rotterdamse Stichting Blindenbelangen [B20130006, B20180072]
  7. Stichting Nederlands Oogheelkundig Onderzoek [2013-04]
  8. E M Blaauw fonds
  9. Slovenian Research Agency [J3-2526]

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The study found that VEGFA(165) and VEGFA(121) have similar inducing effects on tip cells and sprouting in vitro. Co-binding of NRP2 appears to regulate VEGFA-VEGFR2 induced sprout initiation, but not tip cell formation. VLDL plays a role in sprout formation by providing biomass for stalk cell proliferation.
During angiogenesis, vascular endothelial growth factor A (VEGFA) regulates endothelial cell (EC) survival, tip cell formation, and stalk cell proliferation via VEGF receptor 2 (VEGFR2). VEGFR2 can interact with VEGFR2 co-receptors such as heparan sulfate proteoglycans (HSPGs) and neuropilin 2 (NRP2), but the exact roles of these co-receptors, or of sulfatase 2 (SULF2), an enzyme that removes sulfate groups from HSPGs and inhibits HSPG-mediated uptake of very low density lipoprotein (VLDL), in angiogenesis and tip cell biology are unknown. In the present study, we investigated whether the modulation of binding of VEGFA to VEGFR2 by knockdown of SULF2 or NRP2 affects sprouting angiogenesis, tip cell formation, proliferation of non-tip cells, and EC survival, or uptake of VLDL. To this end, we employed VEGFA splice variant 121, which lacks an HSPG binding domain, and VEGFA splice variant 165, which does have this domain, in in vitro models of angiogenic tip cells and vascular sprouting. We conclude that VEGFA(165) and VEGFA(121) have similar inducing effects on tip cells and sprouting in vitro, and that the binding of VEGFA(165) to HSPGs in the extracellular matrix does not seem to play a role, as knockdown of SULF2 did not alter these effects. Co-binding of NRP2 appears to regulate VEGFA-VEGFR2-induced sprout initiation, but not tip cell formation. Finally, as the addition of VLDL increased sprout formation but not tip cell formation, and as VLDL uptake was limited to non-tip cells, our findings suggest that VLDL plays a role in sprout formation by providing biomass for stalk cell proliferation.

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