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Programmable Sequence-Specific Transcriptional Regulation of Mammalian Genome Using Designer TAL Effectors

机译:使用Designer TaL效应器对哺乳动物基因组进行可编程序列特异性转录调控

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摘要

The ability to direct functional proteins to specific DNA sequences is a long-sought goal in the study and engineering of biological processes. Transcription activator–like effectors (TALEs) from Xanthomonas sp. are site-specific DNA-binding proteins that can be readily designed to target new sequences. Because TALEs contain a large number of repeat domains, it can be difficult to synthesize new variants. Here we describe a method that overcomes this problem. We leverage codon degeneracy and type IIs restriction enzymes to generate orthogonal ligation linkers between individual repeat monomers, thus allowing full-length, customized, repeat domains to be constructed by hierarchical ligation. We synthesized 17 TALEs that are customized to recognize specific DNA-binding sites, and demonstrate that they can specifically modulate transcription of endogenous genes (SOX2 and KLF4) in human cells.
机译:在生物学过程的研究和工程中,将功能蛋白定向到特定DNA序列的能力是一个长期的目标。 Xanthomonas sp。的转录激活因子样效应物(TALE)。是位点特异性DNA结合蛋白,可以很容易地设计为靶向新序列。由于TALE包含大量重复域,因此可能难以合成新的变体。在这里,我们描述了一种克服此问题的方法。我们利用密码子简并和II型限制酶在各个重复单体之间生成正交连接接头,从而允许通过分层连接构建全长,定制的重复结构域。我们合成了17种TALE,这些TALE被定制来识别特定的DNA结合位点,并证明它们可以特异性调节人类细胞中内源基因(SOX2和KLF4)的转录。

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