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作 者:Yunus E Eksi Ahter D Sanlioglu Bahar Akkaya Bilge Esin Ozturk Salih Sanlioglu
机构地区:[1]Department of Gene and Cell Therapy,Akdeniz University Faculty of Medicine,Antalya 07058,Turkey [2]Department of Ophthalmology,University of Pittsburgh,Pittsburgh,PA 15213,United States
出 处:《World Journal of Stem Cells》2021年第6期485-502,共18页世界干细胞杂志(英文版)(电子版)
基 金:the Akdeniz University Scientific Research Commission and the Scientific and Technological Research Council of Turkey,No.TUBITAK-215S820.
摘 要:Targeted genome editing is a continually evolving technology employing programmable nucleases to specifically change,insert,or remove a genomic sequence of interest.These advanced molecular tools include meganucleases,zinc finger nucleases,transcription activator-like effector nucleases and RNA-guided engineered nucleases(RGENs),which create double-strand breaks at specific target sites in the genome,and repair DNA either by homologous recombination in the presence of donor DNA or via the error-prone non-homologous end-joining mechanism.A recently discovered group of RGENs known as CRISPR/Cas9 gene-editing systems allowed precise genome manipulation revealing a causal association between disease genotype and phenotype,without the need for the reengineering of the specific enzyme when targeting different sequences.CRISPR/Cas9 has been successfully employed as an ex vivo gene-editing tool in embryonic stem cells and patient-derived stem cells to understand pancreatic beta-cell development and function.RNA-guided nucleases also open the way for the generation of novel animal models for diabetes and allow testing the efficiency of various therapeutic approaches in diabetes,as summarized and exemplified in this manuscript.
关 键 词:Programmable nucleases CRISPR/Cas9 Stem cells Disease modeling DIABETES Insulin gene therapy
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