Long-term restoration of visual function in end-stage retinal degeneration using subretinal human melanopsin gene therapy

Author:

De Silva Samantha R.,Barnard Alun R.ORCID,Hughes Steven,Tam Shu K. E.,Martin Chris,Singh Mandeep S.,Barnea-Cramer Alona O.,McClements Michelle E.,During Matthew J.,Peirson Stuart N.ORCID,Hankins Mark W.,MacLaren Robert E.

Abstract

Optogenetic strategies to restore vision in patients who are blind from end-stage retinal degenerations aim to render remaining retinal cells light sensitive once photoreceptors are lost. Here, we assessed long-term functional outcomes following subretinal delivery of the human melanopsin gene (OPN4) in the rd1 mouse model of retinal degeneration using an adeno-associated viral vector. Ectopic expression of OPN4 using a ubiquitous promoter resulted in cellular depolarization and ganglion cell action potential firing. Restoration of the pupil light reflex, behavioral light avoidance, and the ability to perform a task requiring basic image recognition were restored up to 13 mo following injection. These data suggest that melanopsin gene therapy via a subretinal route may be a viable and stable therapeutic option for the treatment of end-stage retinal degeneration in humans.

Funder

Wellcome Trust

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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