Michael James Gilhooley scite author profile

Optogenetic strategies to restore vision in patients blind from end-stage retinal degenerations aim to render remaining retinal neurons light-sensitive. We present an innovative combination of multi-electrode array recordings together with a complex pattern-generating light source as a toolset to determine the extent to which neural retinal responses to complex light stimuli can be restored following viral delivery of red-shifted channelrhodopsin in the retinally degenerated mouse. Our data indicate that retinal output level spatiotemporal response characteristics achieved by optogenetic gene therapy closely parallel those observed for normal mice but equally reveal important limitations, some of which could be mitigated using bipolarcell targeted gene-delivery approaches. As clinical trials are commencing, these data provide important new information on the capacity and limitations of channelrhodopsin-based gene therapies. The toolset we established enables comparing optogenetic constructs and stem-cell-based techniques, thereby providing an efficient and sensitive starting point to identify future approaches for vision restoration.

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Optogenetics for visual restoration: From proof of principle to translational challenges

Lindner

Gilhooley

Hughes

et al. 2022

Progress in Retinal and Eye Research

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ON-bipolar cell gene expression during retinal degeneration: Implications for optogenetic visual restoration

Gilhooley

Hickey

Lindner

et al. 2021

Experimental Eye Research

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