Publication:

Blue light-induced retinal lesions, intraretinal vascular leakage and edema formation in the all-cone mouse retina

Date

Date

Date
2015
Journal Article
Published version
cris.lastimport.scopus2025-08-07T03:40:22Z
cris.lastimport.wos2025-08-13T01:33:35Z
dc.contributor.institutionUniversity of Zurich
dc.date.accessioned2015-11-27T12:58:28Z
dc.date.available2015-11-27T12:58:28Z
dc.date.issued2015
dc.description.abstract

Little is known about the mechanisms underlying macular degenerations, mainly for the scarcity of adequate experimental models to investigate cone cell death. Recently, we generated R91W;Nrl(-/-) double-mutant mice, which display a well-ordered all-cone retina with normal retinal vasculature and a strong photopic function that generates useful vision. Here we exposed R91W;Nrl(-/-) and wild-type (wt) mice to toxic levels of blue light and analyzed their retinas at different time points post illumination (up to 10 days). While exposure of wt mice resulted in massive pyknosis in a focal region of the outer nuclear layer (ONL), the exposure of R91W;Nrl(-/-) mice led to additional cell death detected within the inner nuclear layer. Microglia/macrophage infiltration at the site of injury was more pronounced in the all-cone retina of R91W;Nrl(-/-) than in wt mice. Similarly, vascular leakage was abundant in the inner and outer retina in R91W;Nrl(-/-) mice, whereas it was mild and restricted to the subretinal space in wt mice. This was accompanied by retinal swelling and the appearance of cystoid spaces in both inner and ONLs of R91W;Nrl(-/-) mice indicating edema in affected areas. In addition, basal expression levels of tight junction protein-1 encoding ZO1 were lower in R91W;Nrl(-/-) than in wt retinas. Collectively, our data suggest that exposure of R91W;Nrl(-/-) mice to blue light not only induces cone cell death but also disrupts the inner blood-retinal barrier. Macular edema in humans is a result of diffuse capillary leakage and microaneurysms in the macular region. Blue light exposure of the R91W;Nrl(-/-) mouse could therefore be used to study molecular events preceding edema formation in a cone-rich environment, and thus potentially help to develop treatment strategies for edema-based complications in macular degenerations.

dc.identifier.doi10.1038/cddis.2015.333
dc.identifier.issn2041-4889
dc.identifier.scopus2-s2.0-84989332495
dc.identifier.urihttps://www.zora.uzh.ch/handle/20.500.14742/112320
dc.identifier.wos000367155300021
dc.language.isoeng
dc.subject.ddc610 Medicine & health
dc.title

Blue light-induced retinal lesions, intraretinal vascular leakage and edema formation in the all-cone mouse retina

dc.typearticle
dcterms.accessRightsinfo:eu-repo/semantics/openAccess
dcterms.bibliographicCitation.journaltitleCell Death and Disease
dcterms.bibliographicCitation.originalpublishernameNature Publishing Group
dcterms.bibliographicCitation.pagestarte1985
dcterms.bibliographicCitation.pmid26583326
dcterms.bibliographicCitation.volume6
dspace.entity.typePublicationen
uzh.contributor.affiliationUniversity of Zurich
uzh.contributor.affiliationUniversity of Zurich
uzh.contributor.affiliationUniversity of Zurich
uzh.contributor.affiliationUniversity of Zurich
uzh.contributor.authorGeiger, P
uzh.contributor.authorBarben, M
uzh.contributor.authorGrimm, C
uzh.contributor.authorSamardzija, M
uzh.contributor.correspondenceNo
uzh.contributor.correspondenceNo
uzh.contributor.correspondenceNo
uzh.contributor.correspondenceYes
uzh.document.availabilitypublished_version
uzh.eprint.datestamp2015-11-27 12:58:28
uzh.eprint.lastmod2025-08-13 01:39:53
uzh.eprint.statusChange2015-11-27 12:58:28
uzh.harvester.ethYes
uzh.harvester.nbNo
uzh.identifier.doi10.5167/uzh-115031
uzh.jdb.eprintsId22974
uzh.oastatus.unpaywallgold
uzh.oastatus.zoraGold
uzh.publication.citationGeiger, P; Barben, M; Grimm, C; Samardzija, M (2015). Blue light-induced retinal lesions, intraretinal vascular leakage and edema formation in the all-cone mouse retina. Cell Death and Disease, 6:e1985.
uzh.publication.freeAccessAtpubmedid
uzh.publication.originalworkoriginal
uzh.publication.publishedStatusfinal
uzh.scopus.impact50
uzh.scopus.subjectsImmunology
uzh.scopus.subjectsCellular and Molecular Neuroscience
uzh.scopus.subjectsCell Biology
uzh.scopus.subjectsCancer Research
uzh.workflow.doajuzh.workflow.doaj.true
uzh.workflow.eprintid115031
uzh.workflow.fulltextStatuspublic
uzh.workflow.revisions52
uzh.workflow.rightsCheckkeininfo
uzh.workflow.statusarchive
uzh.wos.impact50
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