Development and degeneration of retina in <i>rds</i> mutant mice: Light microscopy

Sanyal, S.; Ruiter, Arno; Hawkins, Richard K.

doi:10.1002/cne.901940110

Cited by 207 publications

(116 citation statements)

References 42 publications

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“…Such patterns of hypopigmentation, due to a variety of causes including but not limited to RPE cell dropout, have been seen in fundus photographs of most of the known murine inherited retinal degenerations~Hawes et al, 1999;Chang et al, 2002;Mehalow et al, 2003;Pang et al, 2005!. As we have reported here, several studies correlate areas of RPE cell thinning with the apposing and localized loss of photoreceptor cell bodies comprising the ONL~Caley et al, 1972;Sanyal & Bal, 1973;Sanyal et al, 1980;LaVail et al, 1982LaVail et al, , 1993Blanks et al, 1982;Messer et al, 1993!. As in other photoreceptor degenerations, Müller cells fill in space left by these dying photoreceptors. Though immunocytochemistry shows that there is some upregulation of GFAP in these cells, as has been seen in other retinal degenerations~Eisenfeld et al, 1984;Lewis et al, 1994!, we , there is an increase in apoptotic profiles though they are still restricted to the inner retinal layers.…”

Section: Discussionsupporting

confidence: 68%

“…data showed a strong correlation between the time course of photoreceptor loss in each strain and the gradual extinction of the a-wave in each~Chang et al, 1993a; Heckenlively et al, 1993b; Nusinowitz et al, 1997!. These results indicated that the time course of the rd-3 rod0cone degeneration is of intermediate duration when compared to other retinal degenerations in micẽ Carter-Dawson et al, 1978;Messer et al, 1993;Mullen & LaVail, 1975;Sanyal et al, 1980!. Photoreceptor degeneration begins at the time of outer segment differentiation, reaching completion in 2-4 months.…”

Section: Introductionmentioning

confidence: 96%

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Morphological characterization of the retinal degeneration in three strains of mice carrying the rd-3 mutation

Fariss

Heckenlively

Farber³

et al. 2005

Vis Neurosci

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Retinal development in 3 strains of rd-3/rd-3 mutant mice, previously shown to have different rates of degeneration, was studied using light, electron, and immunofluorescence microscopy. The time course and phenotype of the degeneration as well as details on the mechanism of massive photoreceptor cell loss are compared with other known retinal degenerations in mice. Up until postnatal day (P) 10, the retinas of all three strains (RBF, 4Bnr, In-30) develop similarly to those of pigmented and nonpigmented controls. TUNEL-positive cells appear in the outer nuclear layer (ONL) by P14, and reach a maximum in all three mutant strains around P21. Scattered rods and cones form a loose, monolayered ONL by 8 weeks in the albino RBF strain, by 10 weeks in the albino 4Bnr strain, and by 16 weeks in the pigmented In-30 strain. Though the initial degeneration begins in the central retina, there is no preferred gradient of cell death between central and peripheral photoreceptors. Rods and cones are present at all ages examined. During development, stacks of outer segments (OS) form in all three strains though they never achieve full adult lengths, and often have disorganized, atypical OS. Rod opsin is expressed in the developing OS but is redistributed into plasma membrane as OS degeneration proceeds. Retinal pigment epithelial (RPE) cells of all mutant strains contain packets of phagocytosed OS, and their apical processes associate with the distal ends of the OS. At their synaptic sites, photoreceptor terminals contain ribbons apposed to apparently normal postsynaptic triads. As photoreceptors are lost, Müller cells fill in space in the ONL but they do not appear to undergo significant hypertrophy or migration, though during the degeneration, glial fibrillary acidic protein (GFAP) expression is gradually upregulated. Macrophage-like cells are found frequently in the subretinal space after the onset of photoreceptor apoptosis. As OS disappear, the RPE apical processes revert to simple microvilli. Late in the degeneration, some RPE cells die and neighboring cells appear to flatten as if to maintain confluence. In regions of RPE cell loss that happen to lie above retina where the ONL is gone, cells of the inner nuclear layer (INL), wrapped by Müller cell processes, may front directly on Bruch's membrane.

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Section: Discussionsupporting

confidence: 68%

Section: Introductionmentioning

confidence: 96%

Morphological characterization of the retinal degeneration in three strains of mice carrying the rd-3 mutation

Fariss

Heckenlively

Farber³

et al. 2005

Vis Neurosci

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“…The RDS/PRPH2 gene codes for a photoreceptor-specific glycoprotein called retinal degeneration slow (RDS 2 or peripherin-2), which is a member of the tetraspanin family of proteins and is critical for the proper formation of both rod and cone photoreceptor outer segments (OSs) (1)(2)(3)(4)(5)(6)(7)(8). The OS is an organelle comprising a series of flattened opsin-packed discs and is specialized to detect incoming light and initiate phototransduction (9 -11).…”

mentioning

confidence: 99%

“…Over 80 individual mutations of the RDS/PRPH2 gene in humans have been associated with significant diseases of the retina that can range from the rod-dominant retinitis pigmentosa to the cone-dominant diseases cone-rod dystrophy and macular degeneration (12). Additionally, extensive studies in mouse models have clearly demonstrated the importance of the RDS protein to retinal structure and function (2,(13)(14)(15)(16)(17)(18). In mice heterozygous for the Rds gene (rds ϩ/Ϫ ), the OSs become highly disorganized, and the discs adopt a bizarre whorl-like morphology.…”

mentioning

confidence: 99%

Retinal Degeneration Slow (RDS) Glycosylation Plays a Role in Cone Function and in the Regulation of RDS·ROM-1 Protein Complex Formation

Stuck

Conley

Naash

2015

Journal of Biological Chemistry

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Background: Mutations in retinal degeneration slow (RDS) lead to rod and cone-dominant retinal degeneration by mechanisms that remain unknown. Results: Knockin mice carrying unglycosylated RDS have reduced RDS levels and functional defects in cones. Conclusion: RDS glycosylation is important for cone but not rod function. Significance: Differential reliance on glycosylation may help explain why some RDS disease mutations target cones and others target rods.The photoreceptor-specific glycoprotein retinal degeneration slow (RDS, also called PRPH2) is necessary for the formation of rod and cone outer segments. Mutations in RDS cause rod and cone-dominant retinal disease, and it is well established that both cell types have different requirements for RDS. However, the molecular mechanisms for this difference remain unclear. Although RDS glycosylation is highly conserved, previous studies have revealed no apparent function for the glycan in rods. In light of the highly conserved nature of RDS glycosylation, we hypothesized that it is important for RDS function in cones and could underlie part of the differential requirement for RDS in the two photoreceptor subtypes. We generated a knockin mouse expressing RDS without the N-glycosylation site (N229S). Normal levels of RDS and the unglycosylated RDS binding partner rod outer segment membrane protein 1 (ROM-1) were found in N229S retinas. However, cone electroretinogram responses were decreased by 40% at 6 months of age. Because cones make up only 3-5% of photoreceptors in the wild-type background, N229S mice were crossed into the nrl ؊/؊ background (in which all rods are converted to cone-like cells) for biochemical analysis. In N229S/nrl ؊/؊ retinas, RDS and

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“…At 72 hr after MNU treatment, detachment of the pigment epithelial cells from Bruch's membrane was seen, and, at day 7, 21 and 35, migrating pigment-containing cells were present in all layers of the retina. In agreement to inherited retinal degeneration mice [5,47], Müller cells, macrophages and migrated pigment epithelial cells are involved in removal of apoptotic cells. However, the migrated melanincontaining cells were not in contact with blood vessels.…”

Section: Time Course Of Mnu-induced Retinal Degeneration In Ratsmentioning

confidence: 92%

N-Methyl-N-nitrosourea-induced Retinal Degeneration in Animals

Tsubura

Yoshizawa

Kiuchi

et al. 2003

Acta Histochem. Cytochem

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Retinitis pigmentosa (RP) is a human disease characterized by loss of photoreceptor cells leading to visual disturbance and eventually to blindness. Establishment of reliable animal models is essential for better understanding of this disease and approaches to therapeutic intervention. N-Methyl-N-nitrosourea (MNU)-induced retinal degeneration is highly reproducible, and involves photoreceptor cell loss that ends approximately 7 days after a single systemic administration of MNU. Although the triggering mechanisms of pathogenesis are different and the apoptosis cascade may differ from human RP, MNU-induced photoreceptor cell loss is due to apoptosis. Here, we describe disease progression and therapeutic trials of MNU-induced retinal degeneration in animals.

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Development and degeneration of retina in rds mutant mice: Light microscopy

Cited by 207 publications

References 42 publications

Morphological characterization of the retinal degeneration in three strains of mice carrying the rd-3 mutation

Morphological characterization of the retinal degeneration in three strains of mice carrying the rd-3 mutation

Retinal Degeneration Slow (RDS) Glycosylation Plays a Role in Cone Function and in the Regulation of RDS·ROM-1 Protein Complex Formation

N-Methyl-N-nitrosourea-induced Retinal Degeneration in Animals

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