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首页> 外文期刊>Nature Communications >RADICL-seq identifies general and cell type–specific principles of genome-wide RNA-chromatin interactions
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RADICL-seq identifies general and cell type–specific principles of genome-wide RNA-chromatin interactions

机译:Radicl-SEQ鉴定了基因组RNA-染色质相互作用的一般和细胞类型特异性原理

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摘要

Mammalian genomes encode tens of thousands of noncoding RNAs. Most noncoding transcripts exhibit nuclear localization and several have been shown to play a role in the regulation of gene expression and chromatin remodeling. To investigate the function of such RNAs, methods to massively map the genomic interacting sites of multiple transcripts have been developed; however, these methods have some limitations. Here, we introduce RNA And DNA Interacting Complexes Ligated and sequenced (RADICL-seq), a technology that maps genome-wide RNA–chromatin interactions in intact nuclei. RADICL-seq is a proximity ligation-based methodology that reduces the bias for nascent transcription, while increasing genomic coverage and unique mapping rate efficiency compared with existing methods. RADICL-seq identifies distinct patterns of genome occupancy for different classes of transcripts as well as cell type–specific RNA-chromatin interactions, and highlights the role of transcription in the establishment of chromatin structure.
机译:哺乳动物基因组编码成千上万的非编码RNA。大多数非编码转录物表现出核定位,并且已经显示出在基因表达和染色质重塑的调节中发挥作用。为了研究这种RNA的功能,已经开发了大规模地图多转录物的基因组相互作用位点的方法;但是,这些方法有一些局限性。在这里,我们引入RNA和DNA相互作用复合物连接并测序(RadicL-SEQ),这是一种映射完整核的基因组RNA-染色质相互作用的技术。 Radicl-SEQ是一种基于接近的连接的方法,其减少了用于新生转录的偏差,同时增加了与现有方法相比的基因组覆盖范围和独特的映射率效率。 Radicl-SEQ鉴定了不同类别转录物以及细胞类型特异性RNA-染色质相互作用的不同模式,并突出了转录在建立染色质结构中的作用。

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