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Homologous recombination-mediated targeted integration in monkey embryos using TALE nucleases

机译:使用TALE核酸酶的同源重组介导的猴胚靶向整合

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摘要

BackgroundNon-human primate (NHP) models can closely mimic human physiological functions and are therefore highly valuable in biomedical research. Genome editing is now developing rapidly due to the precision and efficiency offered by engineered site-specific endonuclease-based systems, such as transcription activator-like effector nucleases (TALENs) and the clustered regularly interspaced short palindromic repeats (CRISPR)/CRISPR-associated protein-9 nuclease (Cas9) system. It has been demonstrated that these programmable nucleases can introduce genetic changes in embryos from many species including NHPs. In 2014, we reported the first genetic editing of macaques using TALENs and CRISPR/Cas9. Subsequently, we characterized the phenotype of a methyl CpG binding protein 2 (MECP2)-mutant cynomolgus monkey model of Rett syndrome generated using the TALEN approach. These efforts not only accelerated the advance of modeling genetic diseases in NHPs, but also encouraged us to develop specific gene knock-in monkeys. In this study, we assess the possibility of homologous recombination (HR)-mediated gene replacement using TALENs in monkeys, and generate preimplantation embryos carrying an EmGFP fluorescent reporter constructed in the OCT4 gene.
机译:背景非人类灵长类动物(NHP)模型可以紧密模仿人类的生理功能,因此在生物医学研究中具有很高的价值。由于工程化的基于位点的特定内切核酸酶的系统(例如转录激活因子样效应核酸酶(TALENs)和成簇的规则间隔的短回文重复序列(CRISPR)/ CRISPR相关蛋白)的精确性和效率,基因组编辑现在正在迅速发展。 -9核酸酶(Cas9)系统。已经证明这些可编程核酸酶可以在包括NHP在内的许多物种的胚胎中引入遗传变化。在2014年,我们报告了使用TALENs和CRISPR / Cas9对猕猴进行的首次遗传编辑。随后,我们表征了使用TALEN方法生成的Rett综合征的甲基CpG结合蛋白2(MECP2)突变猕猴模型的表型。这些努力不仅加速了NHP中遗传疾病建模的进展,而且还鼓励我们开发特定的基因敲入猴子。在这项研究中,我们评估了在猴中使用TALENs进行同源重组(HR)介导的基因替代的可能性,并生成了携带在OCT4基因中构建的EmGFP荧光报告基因的植入前胚胎。

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