| Literature DB >> 33548171 |
Sergio Crespo-Garcia1, Pamela R Tsuruda2, Agnieszka Dejda3, Rathi D Ryan4, Frederik Fournier1, Shawnta Y Chaney4, Frederique Pilon3, Taner Dogan4, Gael Cagnone5, Priyanka Patel4, Manuel Buscarlet1, Sonali Dasgupta4, Gabrielle Girouard1, Surabhi R Rao4, Ariel M Wilson3, Robert O'Brien4, Rachel Juneau3, Vera Guber3, Alexandre Dubrac5, Christian Beausejour5, Scott Armstrong4, Frederick A Mallette1, Christopher B Yohn4, Jean-Sebastien Joyal5, Dan Marquess4, Pedro J Beltran4, Przemyslaw Sapieha6.
Abstract
Attenuating pathological angiogenesis in diseases characterized by neovascularization such as diabetic retinopathy has transformed standards of care. Yet little is known about the molecular signatures discriminating physiological blood vessels from their diseased counterparts, leading to off-target effects of therapy. We demonstrate that in contrast to healthy blood vessels, pathological vessels engage pathways of cellular senescence. Senescent (p16INK4A-expressing) cells accumulate in retinas of patients with diabetic retinopathy and during peak destructive neovascularization in a mouse model of retinopathy. Using either genetic approaches that clear p16INK4A-expressing cells or small molecule inhibitors of the anti-apoptotic protein BCL-xL, we show that senolysis suppresses pathological angiogenesis. Single-cell analysis revealed that subsets of endothelial cells with senescence signatures and expressing Col1a1 are no longer detected in BCL-xL-inhibitor-treated retinas, yielding a retina conducive to physiological vascular repair. These findings provide mechanistic evidence supporting the development of BCL-xL inhibitors as potential treatments for neovascular retinal disease.Entities:
Keywords: BCL-xL; UBX1967; aging; angiogenesis; cellular senescence; diabetes; p16(INK4A); retina; retinopathy; senolytic
Mesh:
Substances:
Year: 2021 PMID: 33548171 DOI: 10.1016/j.cmet.2021.01.011
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 27.287