Literature DB >> 21345987

Use of an adult rat retinal explant model for screening of potential retinal ganglion cell neuroprotective therapies.

Natalie D Bull1, Thomas V Johnson, Guncha Welsapar, Nicholas W DeKorver, Stanislav I Tomarev, Keith R Martin.   

Abstract

PURPOSE. To validate an established adult organotypic retinal explant culture system for use as an efficient medium-throughput screening tool to investigate novel retinal ganglion cell (RGC) neuroprotective therapies. METHODS. Optimal culture conditions for detecting RGC neuroprotection in rat retinal explants were identified. Retinal explants were treated with various recognized, or purported, neuroprotective agents and cultured for either 4 or 7 days ex vivo. The number of cells surviving in the RGC layer (RGCL) was quantified using histologic and immunohistochemical techniques, and statistical analyses were applied to detect neuroprotective effects. RESULTS. The ability to replicate previously reported in vivo RGC neuroprotection in retinal explants was verified by demonstrating that caspase inhibition, brain-derived neurotrophic factor treatment, and stem cell transplantation all reduced RGCL cell loss in this model. Further screening of potential neuroprotective pharmacologic agents demonstrated that betaxolol, losartan, tafluprost, and simvastatin all alleviated RGCL cell loss in retinal explants, supporting previous reports. However, treatment with brimonidine did not protect RGCL neurons from death in retinal explant cultures. Explants cultured for 4 days ex vivo proved most sensitive for detecting neuroprotection. CONCLUSIONS. The current adult rat retinal explant culture model offers advantages over other models for screening potential neuroprotective drugs, including maintenance of neurons in situ, control of environmental conditions, and dissociation from other factors such as intraocular pressure. Verification that neuroprotection by previously identified RGC-protective therapies could be replicated in adult retinal explant cultures suggests that this model could be used for efficient medium-throughput screening of novel neuroprotective therapies for retinal neurodegenerative disease.

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Year:  2011        PMID: 21345987      PMCID: PMC3109030          DOI: 10.1167/iovs.10-6873

Source DB:  PubMed          Journal:  Invest Ophthalmol Vis Sci        ISSN: 0146-0404            Impact factor:   4.799


  66 in total

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Journal:  Invest Ophthalmol Vis Sci       Date:  2000-10       Impact factor: 4.799

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4.  Neuroprotective effects of transcription factor Brn3b in an ocular hypertension rat model of glaucoma.

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5.  Culture of Adult Transgenic Zebrafish Retinal Explants for Live-cell Imaging by Multiphoton Microscopy.

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6.  A mouse ocular explant model that enables the study of living optic nerve head events after acute and chronic intraocular pressure elevation: Focusing on retinal ganglion cell axons and mitochondria.

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7.  Basic fibroblast growth factor expression is implicated in mesenchymal stem cells response to light-induced retinal injury.

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10.  In vivo MRI evaluation of early postnatal development in normal and impaired rat eyes.

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