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Coupling Endonucleases With Dna End-Processing Enzymes To Drive Gene Disruption.

Nat Methods.. 2012-10;  9(10):973 - 5
MT Certo, KS Gwiazda, R Kuhar, B Sather, G Curinga. Molecular and Cellular Biology Program, University of Washington, Seattle, Washington, USA.
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Abstract

Targeted DNA double-strand breaks introduced by rare-cleaving designer endonucleases can be harnessed for gene disruption applications by engaging mutagenic nonhomologous end-joining DNA repair pathways. However, endonuclease-mediated DNA breaks are often subject to precise repair, which limits the efficiency of targeted genome editing. To address this issue, we coupled designer endonucleases to DNA end-processing enzymes to drive mutagenic break resolution, achieving up to 25-fold enhancements in gene disruption rates.

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