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A TALEN genome-editing system for generating human stem cell-based disease models

机译:TALEN基因组编辑系统,用于生成基于人类干细胞的疾病模型

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摘要

Transcription activator-like effector nucleases (TALENs) are a new class of engineered nucleases that are easier to design to cleave at desired sites in a genome than previous types of nucleases. We report here the use of TALENs to rapidly and efficiently generate mutant alleles of 15 genes in cultured somatic cells or human pluripotent stem cells, the latter for which we differentiated both the targeted lines and isogenic control lines into various metabolic cell types. We demonstrate cell-autonomous phenotypes directly linked to disease - dyslipidemia, insulin resistance, hypoglycemia, lipodystrophy, motor-neuron death, and hepatitis C infection. We found little evidence of TALEN off-target effects, but each clonal line nevertheless harbors a significant number of unique mutations. Given the speed and ease with which we were able to derive and characterize these cell lines, we anticipate TALEN-mediated genome editing of human cells becoming a mainstay for the investigation of human biology and disease.
机译:转录激活因子样效应核酸酶(TALENs)是一类新型的工程核酸酶,比以前的核酸酶类型更易于设计以在基因组中的所需位点进行裂解。我们在这里报告TALENs的使用,以在培养的体细胞或人多能干细胞中快速有效地产生15个基因的突变等位基因,为此,我们将目标细胞系和等基因控制细胞分化为各种代谢细胞类型。我们证明了与疾病直接相关的细胞自主表型-血脂异常,胰岛素抵抗,低血糖,脂肪营养不良,运动神经元死亡和丙型肝炎感染。我们几乎没有发现TALEN脱靶效应的证据,但是每个克隆系仍然具有大量独特的突变。考虑到我们能够快速简便地衍生和表征这些细胞系,我们预计TALEN介导的人类细胞基因组编辑将成为研究人类生物学和疾病的主要手段。

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