Donor template delivery by recombinant adeno-associated virus for the production of knock-in mice.
Graham DuddyKatherine CourtisJuliette HorwoodJessica OlsenHelen HorslerTina HodgsonSunita Varsani-BrownAbdullah AbdullahLaura DentiHollie LaneFabio DelaquaJulia JanzenMolly StromIan RosewellKatharine CrawleyBenjamin DaviesPublished in: BMC biology (2024)
Our results confirm that recombinant adeno-associated virus transduction of zygotes provides a robust and effective delivery route for donor templates for the production of knock-in mice, across a range of insertion sizes (0.9-4.7 kb). We find that the animal cost of this method is considerably less than generating knock-in models via embryonic stem cells and thus constitutes a considerable 3Rs reduction.