DOI: 10.1126/science.adp8179 ISSN: 0036-8075

Ribozyme-activated mRNA trans-ligation enables large gene delivery to treat muscular dystrophies

Sean R. Lindley, Kadiam C. Venkata Subbaiah, Fnu Priyanka, Pornthida Poosala, Yijie Ma, Leila Jalinous, Jason A. West, William A. Richardson, Tamlyn N. Thomas, Douglas M. Anderson

Ribozymes are small catalytic RNA sequences capable of nucleotide-specific self-cleavage found widespread in nature. Ribozyme cleavage generates distinct 2′,3′-phosphate and 5′-hydroxyl termini that resemble substrates for recently characterized RNA repair pathways in cells. We report that ribozyme cleavage of two separate mRNAs activated their scarless trans-ligation and translation into full-length protein in eukaryotic cells, a process that we named StitchR (for Stitch RNA). Optimization of StitchR activity in mammalian cells resulted in a ~900-fold increase in protein expression that approached levels observed for genes expressed from single vectors. We demonstrate that StitchR can be harnessed for effective dual adeno-associated virus gene therapies to correct muscular dystrophies by restoring large functional muscle proteins to endogenous levels in vivo.

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