Neutrophil extracellular traps target senescent vasculature for tissue remodeling in retinopathy.
François BinetGael CagnoneSergio Crespo-GarciaMasayuki HataMathieu NeaultAgnieszka DejdaAriel Molly WilsonManuel BuscarletGaelle Tagne MawamboJoel P HowardRoberto Diaz-MarinCelia ParinotVera GuberFrédérique PilonRachel JuneauRémi LaflammeChristina SawchynKarine BoulaySeverine LeclercAfnan Abu-ThuraiaJean-François CotéGregor U AndelfingerFlavio A RezendeFlorian SennlaubJean-Sebastien JoyalFrédérick A MallettePrzemyslaw SapiehaPublished in: Science (New York, N.Y.) (2020)
In developed countries, the leading causes of blindness such as diabetic retinopathy are characterized by disorganized vasculature that can become fibrotic. Although many such pathological vessels often naturally regress and spare sight-threatening complications, the underlying mechanisms remain unknown. Here, we used orthogonal approaches in human patients with proliferative diabetic retinopathy and a mouse model of ischemic retinopathies to identify an unconventional role for neutrophils in vascular remodeling during late-stage sterile inflammation. Senescent vasculature released a secretome that attracted neutrophils and triggered the production of neutrophil extracellular traps (NETs). NETs ultimately cleared diseased endothelial cells and remodeled unhealthy vessels. Genetic or pharmacological inhibition of NETosis prevented the regression of senescent vessels and prolonged disease. Thus, clearance of senescent retinal blood vessels leads to reparative vascular remodeling.