| Literature DB >> 34273276 |
Georgia Zarkada1, Joel P Howard2, Xue Xiao3, Hyojin Park1, Mathilde Bizou3, Severine Leclerc2, Steffen E Künzel1, Blanche Boisseau2, Jinyu Li1, Gael Cagnone2, Jean Sebastien Joyal2, Gregor Andelfinger2, Anne Eichmann4, Alexandre Dubrac5.
Abstract
Endothelial tip cells guiding tissue vascularization are primary targets for angiogenic therapies. Whether tip cells require differential signals to develop their complex branching patterns remained unknown. Here, we show that diving tip cells invading the mouse neuroretina (D-tip cells) are distinct from tip cells guiding the superficial retinal vascular plexus (S-tip cells). D-tip cells have a unique transcriptional signature, including high TGF-β signaling, and they begin to acquire blood-retina barrier properties. Endothelial deletion of TGF-β receptor I (Alk5) inhibits D-tip cell identity acquisition and deep vascular plexus formation. Loss of endothelial ALK5, but not of the canonical SMAD effectors, leads to aberrant contractile pericyte differentiation and hemorrhagic vascular malformations. Oxygen-induced retinopathy vasculature exhibits S-like tip cells, and Alk5 deletion impedes retina revascularization. Our data reveal stage-specific tip cell heterogeneity as a requirement for retinal vascular development and suggest that non-canonical-TGF-β signaling could improve retinal revascularization and neural function in ischemic retinopathy.Entities:
Keywords: ALK5; SMAD-independent signaling; TGF-β signaling; blood-retina barrier; retina angiogenesis; single-cell RNA sequencing; sprouting angiogenesis; tip cell
Year: 2021 PMID: 34273276 DOI: 10.1016/j.devcel.2021.06.021
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270