CRISPR 介导的协同表观遗传和转录控制。
CRISPR-Mediated Synergistic Epigenetic and Transcriptional Control.
机构信息
Department of Bioengineering, University of Alabama at Birmingham, Birmingham, Alabama, USA.
Cancer Biology Program, University of Alabama at Birmingham, Birmingham, Alabama, USA.
出版信息
CRISPR J. 2022 Apr;5(2):264-275. doi: 10.1089/crispr.2021.0099. Epub 2022 Mar 10.
Abstract
Targeted activation of endogenous genes is an important approach for cell engineering. Here, we report that the nuclease-deactivated dCas9 fused to a transcriptional activator (VPR) and an epigenetic effector (the catalytic domain of histone acetyltransferase p300) simultaneously, sequentially, or as a single quadripartite effector can lead to enhanced activation of target genes. The composite activator, VPRP, behaves more efficiently than individual activators across a set of genes in different cell types. We characterize off-target effects for host chromatin acetylation and transcriptome using the effectors. Our work demonstrates that transcriptional and epigenetic effectors can be used together to enhance gene activation and suggests the need for further optimization of epigenetic effectors to reduce off-targets.
摘要
靶向激活内源性基因是细胞工程的重要方法。在这里,我们报告说,与转录激活剂(VPR)和表观遗传效应物(组蛋白乙酰转移酶 p300 的催化结构域)融合的无核酸酶失活的 dCas9 可以依次或作为单个四部分效应物同时导致靶基因的增强激活。复合激活剂 VPRP 在不同细胞类型中的一组基因中比单个激活剂更有效。我们使用效应物来描述宿主染色质乙酰化和转录组的脱靶效应。我们的工作表明,可以将转录和表观遗传效应物一起用于增强基因激活,并表明需要进一步优化表观遗传效应物以减少脱靶效应。
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