Role of Müller cells in cone mosaic rearrangement in a rat model of retinitis pigmentosa

Lee, Eun-Jin; Ji, Yerina; Zhu, Colleen L.; Grzywacz, Norberto M.

doi:10.1002/glia.21183

Cited by 36 publications

(74 citation statements)

References 53 publications

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“…Strettoi and co-workers proposed that neurons in retinal degeneration undergo dendritic pruning and later, sprouting due to loss of their afferent synapses (Strettoi and Pignatelli, 2000;Strettoi et al, 2002Strettoi et al, , 2003. This is supported by Lee et al (2011), who showed Müller cell processes remodel to match photoreceptor rearrangement in a rat model for retinitis pigmentosa. Altered glutamate signaling during retinal degeneration may also play an indirect role.…”

Section: Anatomical Remodelingmentioning

confidence: 85%

Early remodeling of müller cells in the rd/rd mouse model of retinal dystrophy

Chua

Nivison‐Smith

Fletcher

et al. 2013

J of Comparative Neurology

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We studied the anatomical remodeling and gliosis of retinal Müller cells in the rd/rd mouse model of photoreceptor degeneration. A computational calculation of glutamine synthetase immunoreactivity was developed so we could specifically quantify changes in Müller cell anatomy between control mice (C57Bl/6) and the dystrophic strain. We found no change in the number of Müller cell somata between mice strains, indicating no cell proliferation as a function of development and degeneration. The retinal area occupied by the total Müller cell body (soma and processes) was significantly less in the rd/rd mouse retina compared with control mice. When only the outer retina was considered, we found rd/rd Müller cell processes were dramatically reduced during the cone phase of photoreceptor degeneration. However, at older ages an increase in Müller cell processes was seen. Conversely, glial fibrillary acidic protein (GFAP) expression showed a significant increase during cone degeneration followed by a reduction in older ages. Müller cell electrophysiology, particularly K(+) currents and membrane potential, was similar between rd/rd and control Müller cells during cone degeneration. Together, these results show that glial remodeling in the rd/rd retina follows separate phases-an initial conservative glial response involving the loss of Müller cells processes, hyperexpression of GFAP, and preservation of normal electrophysiology followed by an active growth of Müller cell processes, glial seal formation, and attenuation of GFAP expression after complete photoreceptor loss.

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Section: Anatomical Remodelingmentioning

confidence: 85%

Early remodeling of müller cells in the rd/rd mouse model of retinal dystrophy

Chua

Nivison‐Smith

Fletcher

et al. 2013

J of Comparative Neurology

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“…5,9 However, it is still unclear why the cone mosaic is reorganized into rings after photoreceptor loss. It has been suggested that cone rings could be the result of cone migration through processes of Müller cells 81 ; whereas other authors have proposed that it is due to cone death, 68 these studies indicated that rods die in the ''center of the rings'' and photoreceptor (cones and rods) loss expands outward, 27,68 suggesting an interdependence between neighboring photoreceptors. 82,83 Thus, it is likely that rings of cone degeneration could be the result of both cone death and migration.…”

Section: Taurine Depletion Increases Retinal Degenerationmentioning

confidence: 88%

Taurine Depletion Causes ipRGC Loss and Increases Light-Induced Photoreceptor Degeneration

García‐Ayuso

Pierdomenico

Hadj-Saïd

et al. 2018

Invest. Ophthalmol. Vis. Sci.

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METHODS. Albino rats received b-alanine in the drinking water to induce taurine depletion. One month later, half of the animals were exposed to white light (3000 lux) continuously for 48 hours and the rest remained in normal environmental conditions. A control group of animals nontreated with b-alanine also was prepared, and half of them were exposed to light using the same protocol. All the animals were processed 2 months after the beginning of the experiment. Retinas were dissected as wholemounts and immunodetected with antibodies against Brn3a, melanopsin, S-opsin, and L-opsin to label different retinal populations: Brn3a þ retinal ganglion cells (RGCs) (image-forming RGCs), m þ RGCs (non-image-forming RGCs), and S-and L/M-cones, respectively. RESULTS. Light exposure did not affect the numbers of Brn3aþ RGCs or m þ RGCs but diminished the numbers of S-and L/M-cones and caused the appearance of rings devoid of cones, mainly in an ''arciform'' area in the superotemporal retina. Taurine depletion caused a diminution of all the studied populations, with m þ RGCs the most affected, followed by Scones. Light exposure under taurine depletion increased photoreceptor degeneration but did not seem to increase Brn3a þ RGCs or m þ RGCs loss. CONCLUSIONS.Our results document that taurine is necessary for cell survival in the rat retina and even more under light-induced photoreceptor degeneration. Thus, taurine supplementation may help to prevent retinal degenerations, especially those that commence with S-cone degeneration or in which light may be an etiologic factor, such as inherited retinal degenerations, AMD, or glaucoma.

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“…After preliminary testing, 25 ug/ml was used throughout this study. The developmental stage for the injection of SB-3CT was either P15, when there was peak rod death [52] and formation of dying rod clusters [31, 32], or P40, when cone rings were observed throughout the retina [36]. One eye was injected with SB-3CT and the other eye was injected with PBS with 0.05–0.1% DMSO for comparison for each animal.…”

Section: Methodsmentioning

confidence: 99%

Inhibition of Matrix Metalloproteinase 9 Enhances Rod Survival in the S334ter-line3 Retinitis Pigmentosa Model

et al. 2016

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Retinitis Pigmentosa (RP) is one of the most common forms of inherited visual loss with the initial degeneration of rod photoreceptors, followed by a progressive cone photoreceptor deterioration. Coinciding with this visual loss, the extracellular matrix (ECM) is reorganized, which alters matrix metalloproteinase (MMP) activity levels. A potential pathological role of MMPs, MMP-9 in particular, involves an excitotoxicity-mediated physiological response. In the current study, we examine the MMP-9 and MMP-2 expression levels in the rhodopsin S334ter-line3 RP rat model and investigate the impact of treatment with SB-3CT, a specific MMP-9 and MMP-2 inhibitor, on rod cell survival was tested. Retinal MMP-9 and MMP-2 expression levels were quantified by immunoblot analysis from S334ter-line3 rats compared to controls. Gelatinolytic activities of MMP-9 and MMP-2 by zymography were examined. The geometry of rod death was further evaluated using Voronoi analysis. Our results revealed that MMP-9 was elevated while MMP-2 was relatively unchanged when S334ter-line 3 retinas were compared to controls. With SB-3CT treatment, we observed gelatinolytic activity of both MMPs was decreased and diminished clustering associated with rod death, in addition to a robust preservation of rod photoreceptors. These results demonstrate that up-regulation of MMP-9 in retinas of S334ter-line3 are associated with rod death. The application of SB-3CT dramatically interferes with mechanisms leading to apoptosis in an MMP-9-dependent manner. Future studies will determine the feasibility of using SB-3CT as a potential therapeutic strategy to slow progression of vision loss in genetic inherited forms of human RP.

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Role of Müller cells in cone mosaic rearrangement in a rat model of retinitis pigmentosa

Cited by 36 publications

References 53 publications

Early remodeling of müller cells in the rd/rd mouse model of retinal dystrophy

Early remodeling of müller cells in the rd/rd mouse model of retinal dystrophy

Taurine Depletion Causes ipRGC Loss and Increases Light-Induced Photoreceptor Degeneration

Inhibition of Matrix Metalloproteinase 9 Enhances Rod Survival in the S334ter-line3 Retinitis Pigmentosa Model

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