Litcius/Paper detail

Wnt-Dependent Oligodendroglial-Endothelial Interactions Regulate White Matter Vascularization and Attenuate Injury

Manideep Chavali, María José Ulloa-Navas, Pedro Pérez-Borredá, José Manuel García‐Verdugo, Patrick S. McQuillen, Eric J. Huang, David H. Rowitch

2020Neuron95 citationsDOIOpen Access PDF

Abstract

Recent studies have indicated oligodendroglial-vascular crosstalk during brain development, but the underlying mechanisms are incompletely understood. We report that oligodendrocyte precursor cells (OPCs) contact sprouting endothelial tip cells in mouse, ferret, and human neonatal white matter. Using transgenic mice, we show that increased or decreased OPC density results in cognate changes in white matter vascular investment. Hypoxia induced increases in OPC numbers, vessel density and endothelial cell expression of the Wnt pathway targets Apcdd1 and Axin2 in white matter, suggesting paracrine OPC-endothelial signaling. Conditional knockout of OPC Wntless resulted in diminished white matter vascular growth in normoxia, whereas loss of Wnt7a/b function blunted the angiogenic response to hypoxia, resulting in severe white matter damage. These findings indicate that OPC-endothelial cell interactions regulate neonatal white matter vascular development in a Wnt-dependent manner and further suggest this mechanism is important in attenuating hypoxic injury.

Topics & Concepts

Wnt signaling pathwayWhite matterNeuroscienceBiologyCell biologyMedicineSignal transductionMagnetic resonance imagingRadiologyNeuroinflammation and Neurodegeneration MechanismsBarrier Structure and Function StudiesNeurological Disease Mechanisms and Treatments