Literature DB >> 21505421

Virally delivered channelrhodopsin-2 safely and effectively restores visual function in multiple mouse models of blindness.

M Mehdi Doroudchi1, Kenneth P Greenberg, Jianwen Liu, Kimberly A Silka, Edward S Boyden, Jennifer A Lockridge, A Cyrus Arman, Ramesh Janani, Shannon E Boye, Sanford L Boye, Gabriel M Gordon, Benjamin C Matteo, Alapakkam P Sampath, William W Hauswirth, Alan Horsager.   

Abstract

Previous work established retinal expression of channelrhodopsin-2 (ChR2), an algal cation channel gated by light, restored physiological and behavioral visual responses in otherwise blind rd1 mice. However, a viable ChR2-based human therapy must meet several key criteria: (i) ChR2 expression must be targeted, robust, and long-term, (ii) ChR2 must provide long-term and continuous therapeutic efficacy, and (iii) both viral vector delivery and ChR2 expression must be safe. Here, we demonstrate the development of a clinically relevant therapy for late stage retinal degeneration using ChR2. We achieved specific and stable expression of ChR2 in ON bipolar cells using a recombinant adeno-associated viral vector (rAAV) packaged in a tyrosine-mutated capsid. Targeted expression led to ChR2-driven electrophysiological ON responses in postsynaptic retinal ganglion cells and significant improvement in visually guided behavior for multiple models of blindness up to 10 months postinjection. Light levels to elicit visually guided behavioral responses were within the physiological range of cone photoreceptors. Finally, chronic ChR2 expression was nontoxic, with transgene biodistribution limited to the eye. No measurable immune or inflammatory response was observed following intraocular vector administration. Together, these data indicate that virally delivered ChR2 can provide a viable and efficacious clinical therapy for photoreceptor disease-related blindness.

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Year:  2011        PMID: 21505421      PMCID: PMC3129568          DOI: 10.1038/mt.2011.69

Source DB:  PubMed          Journal:  Mol Ther        ISSN: 1525-0016            Impact factor:   11.454


  48 in total

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4.  Differential targeting of optical neuromodulators to ganglion cell soma and dendrites allows dynamic control of center-surround antagonism.

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5.  Cone photoreceptors are the main targets for gene therapy of NPHP5 (IQCB1) or NPHP6 (CEP290) blindness: generation of an all-cone Nphp6 hypomorph mouse that mimics the human retinal ciliopathy.

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Journal:  Hum Mol Genet       Date:  2011-01-18       Impact factor: 6.150

6.  Cone contacts, mosaics, and territories of bipolar cells in the mouse retina.

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Journal:  Proc Biol Sci       Date:  2010-11-03       Impact factor: 5.349

10.  Evaluation of the adeno-associated virus mediated long-term expression of channelrhodopsin-2 in the mouse retina.

Authors:  Elena Ivanova; Zhuo-Hua Pan
Journal:  Mol Vis       Date:  2009-08-21       Impact factor: 2.367

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  116 in total

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Review 3.  AAV-mediated gene therapy in mouse models of recessive retinal degeneration.

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Review 4.  Retinal remodeling.

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Review 5.  Pulse trains to percepts: the challenge of creating a perceptually intelligible world with sight recovery technologies.

Authors:  Ione Fine; Geoffrey M Boynton
Journal:  Philos Trans R Soc Lond B Biol Sci       Date:  2015-09-19       Impact factor: 6.237

6.  Transplantation of human embryonic stem cell-derived retinal tissue in two primate models of retinal degeneration.

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7.  Highly Efficient Delivery of Adeno-Associated Viral Vectors to the Primate Retina.

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8.  Intravitreal delivery of a novel AAV vector targets ON bipolar cells and restores visual function in a mouse model of complete congenital stationary night blindness.

Authors:  Miranda L Scalabrino; Sanford L Boye; Kathryn M H Fransen; Jennifer M Noel; Frank M Dyka; Seok Hong Min; Qing Ruan; Charles N De Leeuw; Elizabeth M Simpson; Ronald G Gregg; Maureen A McCall; Neal S Peachey; Shannon E Boye
Journal:  Hum Mol Genet       Date:  2015-08-26       Impact factor: 6.150

9.  Mutations in RD3 are associated with an extremely rare and severe form of early onset retinal dystrophy.

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10.  Restoration of visual function by expression of a light-gated mammalian ion channel in retinal ganglion cells or ON-bipolar cells.

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