Efficient prime editing in two-cell mouse embryos using PEmbryo.
Rebecca P Kim-YipRyan McNultyBradley JoyceAntonio MollicaPeter J ChenPurnima RavisankarBenjamin K LawDavid R LiuJared E ToettcherEvgueni A IvakineEszter PosfaiBritt AdamsonPublished in: Nature biotechnology (2024)
Using transient inhibition of DNA mismatch repair during a permissive stage of development, we demonstrate highly efficient prime editing of mouse embryos with few unwanted, local byproducts (average 58% precise edit frequency, 0.5% on-target error frequency across 13 substitution edits at 8 sites), enabling same-generation phenotyping of founders. Whole-genome sequencing reveals that mismatch repair inhibition increases off-target indels at low-complexity regions in the genome without any obvious phenotype in mice.