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Genome-wide specificity of DNA binding, gene regulation, and chromatin remodeling by TALE- and CRISPR/Cas9-based transcriptional activators

机译:基于TALE和CRISPR / Cas9的转录激活因子对DNA结合,基因调控和染色质重塑的全基因组特异性

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摘要

Genome engineering technologies based on the CRISPR/Cas9 and TALE systems are enabling new approaches in science and biotechnology. However, the specificity of these tools in complex genomes and the role of chromatin structure in determining DNA binding are not well understood. We analyzed the genome-wide effects of TALE-and CRISPR-based transcriptional activators in human cells using ChIP-seq to assess DNA-binding specificity and RNA-seq to measure the specificity of perturbing the transcriptome. Additionally, DNase-seq was used to assess genome-wide chromatin remodeling that occurs as a result of their action. Our results show that these transcription factors are highly specific in both DNA binding and gene regulation and are able to open targeted regions of closed chromatin independent of gene activation. Collectively, these results underscore the potential for these technologies to make precise changes to gene expression for gene and cell therapies or fundamental studies of gene function.
机译:基于CRISPR / Cas9和TALE系统的基因组工程技术正在推动科学和生物技术的新方法。但是,这些工具在复杂基因组中的特异性以及染色质结构在确定DNA结合中的作用尚不清楚。我们使用ChIP-seq评估DNA结合特异性和RNA-seq评估干扰转录组的特异性,分析了TALE和CRISPR基转录激活因子在人细胞中的全基因组效应。此外,DNase-seq用于评估由于其作用而发生的全基因组染色质重塑。我们的结果表明,这些转录因子在DNA结合和基因调控中都具有高度特异性,并且能够独立于基因激活而打开封闭染色质的目标区域。总的来说,这些结果强调了这些技术对基因表达进行精确改变的潜力,以用于基因和细胞疗法或基因功能的基础研究。

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