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<meta name="description" content="Scientists funded by the National Eye Institute (NEI) report a novel gene therapy that halts vision loss in a canine model of a blinding condition called autosomal dominant retinitis pigmentosa (adRP)." />
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<title>Researchers find potential new gene therapy for blinding disease | National Eye Institute</title>
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Researchers find potential new gene therapy for blinding disease
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<span>Researchers find potential new gene therapy for blinding disease</span>
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Scientists funded by NIH preserve vision in dogs with a disease similar to retinitis pigmentosa in humans
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<div class="c-item__date">
August 20, 2018
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<div class="c-item__tag c-item__tag--topic">
<a href="/about/news-and-events/news?topic=401" hreflang="en">Gene Therapy</a>
<a href="/about/news-and-events/news?topic=402" hreflang="en">Genetics</a>
<a href="/about/news-and-events/news?topic=56" hreflang="en">Rare Diseases</a>
<a href="/about/news-and-events/news?topic=364" hreflang="en">Regenerative Medicine</a>
<a href="/about/news-and-events/news?topic=7" hreflang="en">Retina</a>
<a href="/about/news-and-events/news?topic=57" hreflang="en">Retinitis Pigmentosa</a>
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<a href="/about/news-and-events/news?research=25" hreflang="en">Basic Research</a>
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<img src="https://www.nei.nih.gov/sites/default/files/styles/small/public/news/Cideciyan_pressrelease_v4.jpg?itok=0RCsd8jC" alt="Illustration of icosahedral virus capsid, containing circular AAV vector. Arrows point from green and blue colored regions of the vector to shRNA and rhodopsin protein, respectively. " width="1174" height="1174">
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<p>Gene therapy adeno-associated viral (AAV) vector includes sequences that encode both the shRNA knockdown element and the replacement rhodopsin protein. Image credit: Lesley Earl, National Eye Institute</p>
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<p>Scientists funded by the National Eye Institute (NEI) report a novel gene therapy that halts vision loss in a canine model of a blinding condition called autosomal dominant retinitis pigmentosa (adRP). The strategy could one day be used to slow or prevent vision loss in people with the disease. NEI is part of the National Institutes of Health.</p><p>“Weve developed and shown proof-of-concept for a gene therapy for one of the most common forms of retinitis pigmentosa,” said William Beltran, D.V.M., Ph.D., of the University of Pennsylvania School of Veterinary Medicine, Philadelphia, a lead author of the study, which appears online today in the Proceedings of the National Academy of Sciences.</p><p>Retinitis pigmentosa refers to a group of rare genetic disorders that damage light-sensing cells in the retina known as photoreceptors. Rod photoreceptor cells enable vision in low light and require a protein called rhodopsin for their light-sensing ability. People with adRP caused by mutations in the rhodopsin gene usually have one good copy of the gene and a second, mutated copy that codes for an abnormal rhodopsin protein. The abnormal rhodopsin is often toxic, slowly killing the rod cells. As the photoreceptors die, vision deteriorates over years or decades. Scientists have identified more than 150 rhodopsin mutations that cause adRP, challenging efforts to develop effective therapies.</p><p>Beltran, in collaboration with Artur Cideciyan, Ph.D. and Samuel Jacobson, M.D., Ph.D., University of Pennsylvania Scheie Eye Institute, Gustavo Aguirre, V.M.D., Ph.D., University of Pennsylvania School of Veterinary Medicine, and Alfred Lewin, Ph.D., and William Hauswirth, Ph.D., University of Florida, Gainesville, generated a gene therapy construct that knocks down the rod cells ability to produce rhodopsin using a technology known as shRNA (short-hairpin RNA) interference.</p><p>Gene therapy introduces genetic material, like shRNA, into cells to compensate for abnormal genes or to make a beneficial protein. Often adapted from viruses, vectors are engineered to effectively deliver this genetic material into cells without causing disease.</p><p>The researchers tested their gene therapy construct on dogs with a rhodopsin mutation. As in people with adRP, these dogs slowly lose their rod photoreceptors. In the dogs retinas, the construct knocked down about 98-99 percent of rhodopsin (both mutated and normal). But because normal rhodopsin is required for the rods to detect light, the researchers added a “hardened” shRNA-resistant rhodopsin gene to the same vector.</p><p>Initially, the researchers tried using two separate vectors to deliver the shRNA and rhodopsin replacement, but getting the right amount of each into all the cells without overloading the retina with viral vector was challenging.</p><p>“The problem is balance,” said Lewin. “We wanted to be sure that every cell that got the shRNA also got the replacement, so we made a single adeno-associated viral vector that did both.”</p><p>When treated with the combined vector, the dogs maintained healthy, functional photoreceptors, and because the vector was designed to produce human rhodopsin, it could potentially work in humans as well.</p><p>“This all-in-one, remove-and-replace approach needed a lot of fine-tuning,” Beltran said. “The naturally-occurring dog model of adRP was critical. Only in a model where you have natural levels of both the mutant and wild-type copies can you actually test that fine-tuning and see whether youre knocking down sufficiently; whether youre replacing sufficiently,” he added.</p><p>The team hopes to start pre-clinical safety studies within the next year or two, with the goal of eventual human trials. Because the treatment prevents photoreceptor loss rather than regenerating photoreceptors, it could be helpful for patients who have slowly progressing forms of adRP, and whose retinas include areas with living rod cells that can be treated.</p><p>“The beauty of this novel gene therapy product is in its elegant vector design. I hope it works as well in humans, too,” said Neeraj Agarwal, Ph.D., translational research program director at NEI.</p><p>This work was supported in part by a multi-institution NEI R24 grant aimed at developing novel translational therapies for the treatment of visual system disorders.</p><p>For more information about retinitis pigmentosa, visit the NEI website at <a href="/learn-about-eye-health/eye-conditions-and-diseases/retinitis-pigmentosa">https://nei.nih.gov/health/pigmentosa/pigmentosa_facts</a>.</p><p><strong>Reference:</strong> Cideciyan A.V., et al. “Mutation-independent rhodopsin gene therapy by knockdown and replacement with a single AAV vector.” Aug 20, 2018. Proceedings of the National Academy of Sciences. doi: 10.1073/pnas.18055115 <a href="https://pubmed.ncbi.nlm.nih.gov/30127005">Pubmed</a></p><p>&nbsp;</p><p>NEI leads the federal governments research on the visual system and eye diseases. NEI supports basic and clinical science programs to develop sight-saving treatments and address special needs of people with vision loss. For more information, visit <a href="/">https://www.nei.nih.gov</a>.</p><p>About the National Institutes of Health (NIH): NIH, the nations medical research agency, includes 27 Institutes and Centers and is a component of the U.S. Department of Health and Human Services. NIH is the primary federal agency conducting and supporting basic, clinical, and translational medical research, and is investigating the causes, treatments, and cures for both common and rare diseases. For more information about NIH and its programs, visit <a href="https://www.nih.gov/">https://www.nih.gov/</a>.</p><p>NIH…Turning Discovery Into Health®</p>
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