Overcoming doxorubicin resistance of cancer cells by Cas9-mediated gene disruption

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作者
Jong Seong Ha
Juyoung Byun
Dae-Ro Ahn
机构
[1] The Center for Theragnosis,Department of Biological Chemistry
[2] Biomedical Research Institute,undefined
[3] Korea Institute of Science and Technology,undefined
[4] KIST School,undefined
[5] University of Science and Technology (UST),undefined
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Scientific Reports | / 6卷
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摘要
In this study, Cas9 system was employed to down-regulate mdr1 gene for overcoming multidrug resistance of cancer cells. Disruption of the MDR1 gene was achieved by delivery of the Cas9-sgRNA plasmid or the Cas9-sgRNA ribonucleoprotein complex using a conventional gene transfection agent and protein transduction domain (PTD). Doxorubicin showed considerable cytotoxicity to the drug-resistant breast cancer cells pre-treated with the RNA-guided endonuclease (RGEN) systems, whereas virtually non-toxic to the untreated cells. The potency of drug was enhanced in the cells treated with the protein-RNA complex as well as in those treated with plasmids, suggesting that mutation of the mdr1 gene by intracellular delivery of Cas9-sgRNA complex using proper protein delivery platforms could recover the drug susceptibility. Therefore, Cas9-mediated disruption of the drug resistance-related gene can be considered as a promising way to overcome multidrug resistance in cancer cells.
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