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首页> 外文期刊>Nucleic Acids Research >Optimization of scarless human stem cell genome editing.
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Optimization of scarless human stem cell genome editing.

机译:优化无痕人类干细胞基因组编辑。

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Efficient strategies for precise genome editing in human-induced pluripotent cells (hiPSCs) will enable sophisticated genome engineering for research and clinical purposes. The development of programmable sequence-specific nucleases such as Transcription Activator-Like Effectors Nucleases (TALENs) and Cas9-gRNA allows genetic modifications to be made more efficiently at targeted sites of interest. However, many opportunities remain to optimize these tools and to enlarge their spheres of application. We present several improvements: First, we developed functional re-coded TALEs (reTALEs), which not only enable simple one-pot TALE synthesis but also allow TALE-based applications to be performed using lentiviral vectors. We then compared genome-editing efficiencies in hiPSCs mediated by 15 pairs of reTALENs and Cas9-gRNA targeting CCR5 and optimized ssODN design in conjunction with both methods for introducing specific mutations. We found Cas9-gRNA achieved 7-8x higher non-homologous end joining efficiencies (3%) than reTALENs (0.4%) and moderately superior homology-directed repair efficiencies (1.0 versus 0.6%) when combined with ssODN donors in hiPSCs. Using the optimal design, we demonstrated a streamlined process to generated seamlessly genome corrected hiPSCs within 3 weeks.Registry Number/Name of Substance 0 (Oligodeoxyribonucleotides). 0 (RNA, Guide). EC 3-1 (Deoxyribonucleases).
机译:在人类诱导的多能细胞(hiPSC)中进行精确基因组编辑的有效策略将实现用于研究和临床目的的复杂基因组工程。可编程序列特异性核酸酶(如转录激活因子效应子核酸酶(TALENs)和Cas9-gRNA)的发展使在目标靶点上的遗传修饰更有效。但是,仍然存在许多机会来优化这些工具并扩大其应用范围。我们提出了以下改进:首先,我们开发了功能性重新编码的TALE(reTALE),它不仅可以实现简单的一锅式TALE合成,还可以使用慢病毒载体进行基于TALE的应用。然后,我们比较了针对15种reTALENs和靶向CCR5的Cas9-gRNA介导的hiPSC中的基因组编辑效率,并结合了两种引入特定突变的方法对ssODN进行了优化设计。我们发现,在hiPSC中与ssODN供体结合时,Cas9-gRNA的非同源末端连接效率(3%)比reTALENs(0.4%)高7-8倍,并且由同源性导向的修复效率较高(1.0对0.6%)。使用最佳设计,我们证明了一种简化的过程,可以在3周内无缝生成基因组校正的hiPSC。注册号/物质0的名称(寡脱氧核糖核苷酸)。 0(RNA,指南)。 EC 3-1(脱氧核糖核酸酶)。

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