Galectin-1 expression imprints a neurovascular phenotype in proliferative retinopathies and delineates responses to anti-VEGF

Neovascular retinopathies are leading causes of irreversible blindness. Although vascular endothelial growth factor (VEGF) inhibitors have been established as the mainstay of current treatment, clinical management of these diseases is still limited. As retinal impairment involves abnormal neovascula...

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Detalles Bibliográficos
Autor principal: Croci Russo, Diego Omar
Publicado: 2017
Materias:
Galectin-1
Neovascularization
Neurodegeneration
Retinopathies
Vascular endothelial growth factor
bevacizumab
epitope
galectin 1
glycan
oxygen
vasculotropin
vasculotropin inhibitor
animal experiment
animal model
animal tissue
aqueous humor
Article
cell surface
controlled study
female
human
male
molecular imprinting
mouse
nonhuman
oxygen-induced retinopathy
perinatal period
phenotype
proliferative retinopathy
protein expression
protein localization
protein targeting
retina blood vessel
retina neovascularization
signal transduction
treatment response
upregulation
Acceso en línea:https://bibliotecadigital.exactas.uba.ar/collection/paper/document/paper_19492553_v8_n20_p32505_Ridano
http://hdl.handle.net/20.500.12110/paper_19492553_v8_n20_p32505_Ridano
Aporte de:
Biblioteca Digital - Facultad de Ciencias Exactas y Naturales (UBA) de Universidad de Buenos Aires
Descripción
Sumario:Neovascular retinopathies are leading causes of irreversible blindness. Although vascular endothelial growth factor (VEGF) inhibitors have been established as the mainstay of current treatment, clinical management of these diseases is still limited. As retinal impairment involves abnormal neovascularization and neuronal degeneration, we evaluated here the involvement of galectin-1 in vascular and non-vascular alterations associated with retinopathies, using the oxygen-induced retinopathy (OIR) model. Postnatal day 17 OIR mouse retinas showed the highest neovascular profile and exhibited neuro-glial injury as well as retinal functional loss, which persisted until P26 OIR. Concomitant to VEGF up-regulation, galectin-1 was highly expressed in P17 OIR retinas and it was mainly localized in neovascular tufts. In addition, OIR induced remodelling of cell surface glycophenotype leading to exposure of galectin-1-specific glycan epitopes. Whereas VEGF returned to baseline levels at P26, increased galectin-1 expression persisted until this time period. Remarkably, although anti-VEGF treatment in P17 OIR improved retinal vascularization, neither galectin-1 expression nor non-vascular and functional alterations were attenuated. However, this functional defect was partially prevented in galectin-1-deficient (Lgals1-/-) OIR mice, suggesting the importance of targeting both VEGF and galectin-1 as non-redundant independent pathways. Supporting the clinical relevance of these findings, we found increased levels of galectin-1 in aqueous humor from patients with proliferative diabetic retinopathy and neovascular glaucoma. Thus, using an OIR model and human samples, we identified a role for galectin-1 accompanying vascular and non-vascular retinal alterations in neovascular retinopathies. © Ridano et al.

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