Publication | Open Access
Synergistic gene editing in human iPS cells via cell cycle and DNA repair modulation
52
Citations
62
References
2020
Year
GeneticsDna Repair ModulationMolecular BiologyCell CycleGenome EngineeringGene TransferGenome InstabilitySynergistic GeneDna ReplicationGenome EditingPrecise GeneCell BiologyFluorescent Dna RepairGene TherapiesNatural SciencesGenetic EngineeringGene EditingSystems BiologyMedicineCrispr
Precise gene editing aims at generating single-nucleotide modifications to correct or model human disease. However, precision editing with nucleases such as CRIPSR-Cas9 has seen limited success due to poor efficiency and limited practicality. Here, we establish a fluorescent DNA repair assay in human induced pluripotent stem (iPS) cells to visualize and quantify the frequency of DNA repair outcomes during monoallelic and biallelic targeting. We found that modulating both DNA repair and cell cycle phase via defined culture conditions and small molecules synergistically enhanced the frequency of homology-directed repair (HDR). Notably, targeting in homozygous reporter cells results in high levels of editing with a vast majority of biallelic HDR outcomes. We then leverage efficient biallelic HDR with mixed ssODN repair templates to generate heterozygous mutations. Synergistic gene editing represents an effective strategy to generate precise genetic modifications in human iPS cells.
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