CRISPR Corrects Retinal Disease Mutation

Patient-derived stem cells containing a genetic mutation leading to blindness can be successfully edited using CRISPR/Cas9, researchers show.

Written byCatherine Offord
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The interior of an eye in the middle stages of retinosa pigmentosaWIKIMEDIA, CHRISTIAN HAMELRetinitis pigmentosa, an inherited disease causing progressive degeneration of the retina, is repsonsible for blindness in approximately 1.5 million people worldwide. Using patient-derived stem cells, researchers in the U.S. have now used the CRISPR/Cas9 gene-editing technology to correct one of the mutations that commonly leads to the disease. The team’s results were published yesterday (January 27) in Nature.

“Our vision is to develop a personalized approach to treating eye disease,” study coauthor Stephen Tsang of Columbia University Medical Center said in a press release. “We still have some way to go, but we believe that the first therapeutic use of CRISPR will be to treat an eye disease. Here we have demonstrated that the initial steps are feasible.”

The researchers extracted fibroblasts from a patient with X-linked retinitis pigmentosa. This particularly aggressive variant of the disease is often caused by a single mutation, making it a good candidate for precision medicine. The researchers used the fibroblasts to create pluripotent stem cells, which they then edited using CRISPR.

The team reported a 13 percent success rate at converting the mutated allele into the wild-type, ...

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  • After undergraduate research with spiders at the University of Oxford and graduate research with ants at Princeton University, Catherine left arthropods and academia to become a science journalist. She has worked in various guises at The Scientist since 2016. As Senior Editor, she wrote articles for the online and print publications, and edited the magazine’s Notebook, Careers, and Bio Business sections. She reports on subjects ranging from cellular and molecular biology to research misconduct and science policy. Find more of her work at her website.

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