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Aptazyme-embedded guide RNAs enable ligand-responsive genome editing and transcriptional activation

机译:嵌入了Aptazyme的指导RNA使配体响应基因组编辑和转录激活成为可能

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摘要

Programmable sequence-specific genome editing agents such as CRISPR-Cas9 have greatly advanced our ability to manipulate the human genome. Although canonical forms of genome-editing agents and programmable transcriptional regulators are constitutively active, precise temporal and spatial control over genome editing and transcriptional regulation activities would enable the more selective and potentially safer use of these powerful technologies. Here, by incorporating ligand-responsive self-cleaving catalytic RNAs (aptazymes) into guide RNAs, we developed a set of aptazyme-embedded guide RNAs that enable small molecule-controlled nuclease-mediated genome editing and small molecule-controlled base editing, as well as small molecule-dependent transcriptional activation in mammalian cells.
机译:可编程序列特异性基因组编辑剂,例如CRISPR-Cas9,极大地提高了我们操纵人类基因组的能力。尽管基因组编辑剂和可编程转录调节剂的规范形式具有组成性活性,但是对基因组编辑和转录调节活动的精确时空控制将使这些强大技术的选择性和安全性更高。在这里,通过将配体反应性自裂解催化RNA(aptazymes)掺入到指导RNA中,我们开发了一套嵌入有酶的,可进行小分子控制的核酸酶介导的基因组编辑和小分子控制的碱基编辑的指导RNA。作为哺乳动物细胞中依赖小分子的转录激活。

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