Litcius/Paper detail

Glial type specific regulation of CNS angiogenesis by HIFα-activated different signaling pathways

Sheng Zhang, Bokyung Kim, Xiaoqing Zhu, Xuehong Gui, Yan Wang, Zhaohui Lan, Preeti Prabhu, Kenneth A. Fond, Aijun Wang, Fuzheng Guo

2020Nature Communications63 citationsDOIOpen Access PDF

Abstract

The mechanisms by which oligodendroglia modulate CNS angiogenesis remain elusive. Previous in vitro data suggest that oligodendroglia regulate CNS endothelial cell proliferation and blood vessel formation through hypoxia inducible factor alpha (HIFα)-activated Wnt (but not VEGF) signaling. Using in vivo genetic models, we show that HIFα in oligodendroglia is necessary and sufficient for angiogenesis independent of CNS regions. At the molecular level, HIFα stabilization in oligodendroglia does not perturb Wnt signaling but rather activates VEGF. At the functional level, genetically blocking oligodendroglia-derived VEGF but not Wnt significantly decreases oligodendroglial HIFα-regulated CNS angiogenesis. Blocking astroglia-derived Wnt signaling reduces astroglial HIFα-regulated CNS angiogenesis. Together, our in vivo data demonstrate that oligodendroglial HIFα regulates CNS angiogenesis through Wnt-independent and VEGF-dependent signaling. These findings suggest an alternative mechanistic understanding of CNS angiogenesis by postnatal glial cells and unveil a glial cell type-dependent HIFα-Wnt axis in regulating CNS vessel formation.

Topics & Concepts

AngiogenesisWnt signaling pathwayBiologyCell biologySignal transductionVascular endothelial growth factorCancer researchVEGF receptorsCancer, Hypoxia, and MetabolismNeurogenesis and neuroplasticity mechanismsAngiogenesis and VEGF in Cancer
Glial type specific regulation of CNS angiogenesis by HIFα-activated different signaling pathways | Litcius