Restoration of Vision with Ectopic Expression of Human Rod Opsin

Cehajic-Kapetanovic, Jasmina; Eleftheriou, Cyril G.; Allen, Annette E.; Milosavljevic, Nina; Pienaar, Abigail; Bedford, Robert A.; Davis, Kyle; Bishop, Paul N.; Lucas, Robert J.

doi:10.1016/j.cub.2015.07.029

Cited by 157 publications

(198 citation statements)

References 35 publications

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“…Finally, for patients who still have an intact bipolar cell layer, new viral technologies might also grant access to the bipolar cells of the primate retina for circuit-specific insertion of G proteincoupled vertebrate opsins. [50][51][52] Our study provides evidence that the choice of an appropriate promoter is essential in obtaining high-level microbial opsin expression compatible with illumination safety. A promoter that can drive strong gene expression in designated cells is crucial in the clinical development of a strategy using a protein of foreign origin, which requires high-level expression for functional activation.…”

Section: Discussionmentioning

confidence: 85%

A New Promoter Allows Optogenetic Vision Restoration with Enhanced Sensitivity in Macaque Retina

et al. 2017

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The majority of inherited retinal degenerations converge on the phenotype of photoreceptor cell death. Second-and third-order neurons are spared in these diseases, making it possible to restore retinal light responses using optogenetics. Viral expression of channelrhodopsin in the third-order neurons under ubiquitous promoters was previously shown to restore visual function, albeit at light intensities above illumination safety thresholds. Here, we report (to our knowledge, for the first time) activation of macaque retinas, up to 6 months post-injection, using channelrhodopsin-Ca 2+ -permeable channelrhodopsin (CatCh) at safe light intensities. High-level CatCh expression was achieved due to a new promoter based on the regulatory region of the gamma-synuclein gene (SNCG) allowing strong expression in ganglion cells across species. Our promoter, in combination with clinically proven adeno-associated virus 2 (AAV2), provides CatCh expression in peri-foveolar ganglion cells responding robustly to light under the illumination safety thresholds for the human eye. On the contrary, the threshold of activation and the proportion of unresponsive cells were much higher when a ubiquitous promoter (cytomegalovirus [CMV]) was used to express CatCh. The results of our study suggest that the inclusion of optimized promoters is key in the path to clinical translation of optogenetics.

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Section: Discussionmentioning

confidence: 85%

A New Promoter Allows Optogenetic Vision Restoration with Enhanced Sensitivity in Macaque Retina

et al. 2017

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“…This suggests that the most viscous portion of the vitreous is still firmly implanted into the ILM and may necessitate several hours of aCSF perfusion to dissolve away. One approach to improve implantation of a retinal prosthetic device would be to digest portions of the vitreous and ILM prior to implantation with glycosidic enzymes [71].…”

Section: Discussionmentioning

confidence: 99%

Carbon nanotube electrodes for retinal implants: A study of structural and functional integration over time

et al. 2017

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The choice of electrode material is of paramount importance in neural prosthetic devices. Electrodes must be biocompatible yet able to sustain repetitive current injections in a highly corrosive environment. We explored the suitability of carbon nanotube (CNT) electrodes to stimulate retinal ganglion cells (RGCs) in a mouse model of outer retinal degeneration. We investigated morphological changes at the bio-hybrid interface and changes in RGC responses to electrical stimulation following prolonged in vitro coupling to CNT electrodes.We observed gradual remodelling of the inner retina to incorporate CNT assemblies. Electrophysiological recordings demonstrate a progressive increase in coupling between RGCs and the CNT electrodes over three days, characterized by a gradual decrease in stimulation thresholds and increase in cellular recruitment. These results provide novel evidence for time-dependent formation of viable bio-hybrids between CNTs and the retina, demonstrating that CNTs are a promising material for inclusion in retinal prosthetic devices.

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“…In parallel, the unnaturally high light intensities required for ChR2 activation have spurred the development of novel optogenetic tools based on more light-sensitive mammalian proteins (Cehajic-Kapetanovic et al, 2015; van Wyk et al, 2015a). These next-generation optogenetic therapies target the OBCs and re-activate the native OBC signaling cascade.…”

Section: Introductionmentioning

confidence: 99%

Present Molecular Limitations of ON-Bipolar Cell Targeted Gene Therapy

et al. 2017

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Recent studies have demonstrated the safety and efficacy of ocular gene therapy based on adeno-associated viral vectors (AAVs). Accordingly, a surge in promising new gene therapies is entering clinical trials, including the first optogenetic therapy for vision restoration. To date, optogenetic therapies for vision restoration target either the retinal ganglion cells (GCs) or presynaptic ON-bipolar cells (OBCs). Initiating light responses at the level of the OBCs has significant advantages over optogenetic activation of GCs. For example, important neural circuitries in the inner retina, which shape the receptive fields of GCs, remain intact when activating the OBCs. Current drawbacks of AAV-mediated gene therapies targeting OBCs include (1) a low transduction efficiency, (2) off-target expression in unwanted cell populations, and (3) a poor performance in human tissue compared to the murine retina. Here, we examined side-by-side the performance of three state-of-the art AAV capsid variants, AAV7m8, AAVBP2, and AAV7m8(Y444F) in combination with the 4xGRM6-SV40 promoter construct in the healthy and degenerated mouse retina and in human post-mortem retinal explants. We find that (1) the 4xGRM6-SV40 promoter is not OBC specific, (2) that all AAV variants possess broad cellular transduction patterns, with differences between the transduction patterns of capsid variants AAVBP2 and AAV7m8 and, most importantly, (3) that all vectors target OBCs in healthy tissue but not in the degenerated rd1 mouse model, potentially limiting the possibilities for an OBC-targeted optogenetic therapy for vision restoration in the blind.

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Restoration of Vision with Ectopic Expression of Human Rod Opsin

Cited by 157 publications

References 35 publications

A New Promoter Allows Optogenetic Vision Restoration with Enhanced Sensitivity in Macaque Retina

A New Promoter Allows Optogenetic Vision Restoration with Enhanced Sensitivity in Macaque Retina

Carbon nanotube electrodes for retinal implants: A study of structural and functional integration over time

Present Molecular Limitations of ON-Bipolar Cell Targeted Gene Therapy

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