Erratum: Ribozyme rescue of photoreceptor cells in a transgenic rat model of autosomal dominant retinitis pigmentosa

Autosomal dominant retinitis pigmentosa (adRP) is frequently caused by mutations in RHO, the gene for rhodopsin. In previous experiments in dogs with the T4R mutation in RHO, an AAV2/5 vector expressing both an shRNA directed to human and dog RHO mRNA and an shRNA-resistant human RHO cDNA (AAV-RHO820-shRNA820) prevented retinal degeneration for more than 8 months following injection. To confirm that this same vector could protect the retinas of a different species and bearing a different RHO mutation, we injected mice transgenic for human P23H RHO at postnatal day 30 in one eye. For nine months, we monitored their retinal structure using spectral-domain optical coherence tomography (SD-OCT) and retinal function using electroretinography (ERG). We compared these to P23H RHO transgenic mice injected with AAV-GFP. Though retinas continued to thin over time, compared to control injected eyes, AAV-RHO820-shRNA820 slowed the loss of photoreceptor cells and decreased ERG amplitudes in AAV-RHO820-shRNA820 eyes during the nine-month study period. Unexpectedly, we also observed preservation of retinal structure and function in the untreated contralateral eyes of AAV-RHO820-shRNA820 treated mice. PCR analysis and western blots provided evidence that a low amount of vector from injected eyes was present in uninjected eyes.

Download Full-text

Astrocytes and Müller Cell Alterations During Retinal Degeneration in a Transgenic Rat Model of Retinitis Pigmentosa

Frontiers in Cellular Neuroscience ◽

10.3389/fncel.2015.00484 ◽

2015 ◽

Vol 9 ◽

Cited By ~ 33

Author(s):

Laura Fernández-Sánchez ◽

Pedro Lax ◽

Laura Campello ◽

Isabel Pinilla ◽

Nicolás Cuenca

Keyword(s):

Retinitis Pigmentosa ◽

Retinal Degeneration ◽

Rat Model ◽

Müller Cell ◽

Transgenic Rat ◽

Muller Cell ◽

Cell Alterations ◽

Transgenic Rat Model

Download Full-text

A rat model for retinitis pigmentosa with rapid retinal degeneration enables drug evaluation in vivo

Biological Procedures Online ◽

10.1186/s12575-021-00150-y ◽

2021 ◽

Vol 23 (1) ◽

Author(s):

Chisato Inoue ◽

Tamaki Takeuchi ◽

Akira Shiota ◽

Mineo Kondo ◽

Yuji Nshizawa

Keyword(s):

Retinitis Pigmentosa ◽

Retinal Degeneration ◽

Rat Model ◽

Photoreceptor Cell ◽

Photoreceptor Cells ◽

Therapeutic Agents ◽

Transgenic Rat ◽

Cell Degeneration ◽

Rat Strain

Abstract Background Although retinitis pigmentosa (RP) is most frequently studied in mouse models, rats, rabbits, and pigs are also used as animal models of RP. However, no studies have reported postnatal photoreceptor cell loss before complete development in these models. Here, we generated a transgenic rat strain, named the P347L rat, in which proline at position 347 in the rhodopsin protein was replaced with leucine. Results A pathological analysis of photoreceptor cells in the P347L rat model was performed, and drugs with potential use as therapeutic agents against RP were investigated. The data clearly showed rapid degeneration and elimination of the outer nuclear layer even before the photoreceptor cells were fully established in P347L rats. To test the usefulness of the P347L rat in the search for new therapeutic agents against RP, the effects of rapamycin on RP were investigated in this rat strain. The findings suggest that rapamycin promotes autophagy and autophagosomal uptake of the rhodopsin that has accumulated abnormally in the cytoplasm, thereby alleviating stress and delaying photoreceptor cell death. Conclusions In this RP model, the time to onset of retinal degeneration was less than that of previously reported RP models with other rhodopsin mutations, enabling quicker in vivo evaluation of drug efficacy. Administration of rapamycin delayed the photoreceptor cell degeneration by approximately 1 day.

Download Full-text