Sortilin Participates in Light-dependent Photoreceptor Degeneration in Vivo
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Santos Carro, Ana María; López-Sánchez, Noelia; Martín Oliva, David; Villa, Pedro de la; Cuadros Ojeda, Miguel Ángel; Frade, José M.Editorial
Public Library of Science (PLOS)
Materia
Apoptosis Cell death Enzyme-linked immunoassays Eyes Immunohsitochemistry techniques Immunostaining Photoreceptors Retina
Date
2012Referencia bibliográfica
Santos, A.M.; et al. Sortilin Participates in Light-dependent Photoreceptor Degeneration in Vivo. Plos One, 7(4): e36243 (2012). [http://hdl.handle.net/10481/31033]
Sponsorship
This study was supported by grants from the “Ministerio de Ciencia e Innovación” (BFU2009-07671) and from “Fundación Lucha contra la Ceguera” (FUNDALUCE-2008) to JMF, as well as from “Ministerio de Ciencia e Innovación” (BFU2007-61659), from “Junta de Andalucia” (P07-CVI-03008), and from “University of Granada” (2011 GREIB incentive) to MAC.Abstract
Both proNGF and the neurotrophin receptor p75 (p75NTR) are known to regulate photoreceptor cell death caused by exposure of albino mice to intense illumination. ProNGF-induced apoptosis requires the participation of sortilin as a necessary p75NTR co-receptor, suggesting that sortilin may participate in the photoreceptor degeneration triggered by intense lighting. We report here that light-exposed albino mice showed sortilin, p75NTR, and proNGF expression in the outer nuclear layer, the retinal layer where photoreceptor cell bodies are located. In addition, cone progenitor-derived 661W cells subjected to intense illumination expressed sortilin and p75NTR and released proNGF into the culture medium. Pharmacological blockade of sortilin with either neurotensin or the “pro” domain of proNGF (pro-peptide) favored the survival of 661W cells subjected to intense light. In vivo, the pro-peptide attenuated retinal cell death in light-exposed albino mice. We propose that an auto/paracrine proapoptotic mechanism based on the interaction of proNGF with the receptor complex p75NTR/sortilin participates in intense light-dependent photoreceptor cell death. We therefore propose sortilin as a putative target for intervention in hereditary retinal dystrophies.