2009-08-03
Stimulation of homology-directed gene targeting at an endogenous human locus by a nicking endonuclease
Publication
Publication
Nucleic Acids Research , Volume 37 - Issue 17 p. 5725- 5736
Homologous recombination (HR) is a highly accurate mechanism of DNA repair that can be exploited for homology-directed gene targeting. Since in most cell types HR occurs very infrequently (̃10.-6to 10.-8), its practical application has been largely restricted to specific experimental systems that allow selection of the few cells that become genetically modified. HR-mediated gene targeting has nonetheless revolutionized genetics by greatly facilitating the analysis of mammalian gene function. Recent studies showed that generation of double-strand DNA breaks at specific loci by designed endonucleases greatly increases the rate of homology-directed gene repair. These findings opened new perspectives for HR-based genome editing in higher eukaryotes. Here, we demonstrate by using donor DNA templates together with the adeno-associated virus (AAV) Rep78 and Rep68 proteins that sequence-and strand-specific cleavage at a native, predefined, human locus can also greatly enhance homology-directed gene targeting. Our findings argue for the development of other strategies besides direct induction of double-strand chromosomal breaks to achieve efficient and heritable targeted genetic modification of cells and organisms. Finally, harnessing the cellular HR pathway through Rep-mediated nicking expands the range of strategies that make use of AAV elements to bring about stable genetic modification of human cells.
Additional Metadata | |
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doi.org/10.1093/nar/gkp643, hdl.handle.net/1765/24692 | |
Nucleic Acids Research | |
Organisation | Erasmus MC: University Medical Center Rotterdam |
van Nierop, G., de Vries, A., Holkers, M., Vrijsen, K., & Gonçalves, M. (2009). Stimulation of homology-directed gene targeting at an endogenous human locus by a nicking endonuclease. Nucleic Acids Research, 37(17), 5725–5736. doi:10.1093/nar/gkp643 |