| Literature DB >> 30787185 |
Khalil Miloudi1,2, Malika Oubaha3, Catherine Ménard3, Agnieszka Dejda1, Vera Guber1, Gael Cagnone4,5, Ariel M Wilson3, Nicolas Tétreault1, Gaëlle Mawambo3, Francois Binet3, Rony Chidiac5, Chantal Delisle5, Manuel Buscarlet3, Agustin Cerani3, Sergio Crespo-Garcia3, Katie Bentley6, Flavio Rezende1, Jean-Sebastien Joyal4, Frédérick A Mallette3,7, Jean-Philippe Gratton5, Bruno Larrivée1, Przemyslaw Sapieha8,2.
Abstract
Diabetic macular edema is a major complication of diabetes resulting in loss of central vision. Although heightened vessel leakiness has been linked to glial and neuronal-derived factors, relatively little is known on the mechanisms by which mature endothelial cells exit from a quiescent state and compromise barrier function. Here we report that endothelial NOTCH1 signaling in mature diabetic retinas contributes to increased vascular permeability. By providing both human and mouse data, we show that NOTCH1 ligands JAGGED1 and DELTA LIKE-4 are up-regulated secondary to hyperglycemia and activate both canonical and rapid noncanonical NOTCH1 pathways that ultimately disrupt endothelial adherens junctions in diabetic retinas by causing dissociation of vascular endothelial-cadherin from β-catenin. We further demonstrate that neutralization of NOTCH1 ligands prevents diabetes-induced retinal edema. Collectively, these results identify a fundamental process in diabetes-mediated vascular permeability and provide translational rational for targeting the NOTCH pathway (primarily JAGGED1) in conditions characterized by compromised vascular barrier function.Entities:
Keywords: DLL4; JAG1; NOTCH; diabetic macular edema; diabetic retinopathy
Year: 2019 PMID: 30787185 PMCID: PMC6410871 DOI: 10.1073/pnas.1814711116
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205