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Simultaneous characterization of cellular RNA structure and function with in-cell SHAPE-Seq

机译:使用细胞内SHAPE-Seq同时表征细胞RNA结构和功能

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Many non-coding RNAs form structures that interact with cellular machinery to control gene expression. A central goal of molecular and synthetic biology is to uncover design principles linking RNA structure to function to understand and engineer this relationship. Here we report a simple, high-throughput method called in-cell SHAPE-Seq that combines in-cell probing of RNA structure with a measurement of gene expression to simultaneously characterize RNA structure and function in bacterial cells. We use in-cell SHAPE-Seq to study the structure–function relationship of two RNA mechanisms that regulate translation in Escherichia coli. We find that nucleotides that participate in RNA–RNA interactions are highly accessible when their binding partner is absent and that changes in RNA structure due to RNA–RNA interactions can be quantitatively correlated to changes in gene expression. We also characterize the cellular structures of three endogenously expressed non-coding RNAs: 5S rRNA, RNase P and the btuB riboswitch. Finally, a comparison between in-cell and in vitro folded RNA structures revealed remarkable similarities for synthetic RNAs, but significant differences for RNAs that participate in complex cellular interactions. Thus, in-cell SHAPE-Seq represents an easily approachable tool for biologists and engineers to uncover relationships between sequence, structure and function of RNAs in the cell.
机译:许多非编码RNA形成与细胞机器相互作用以控制基因表达的结构。分子生物学和合成生物学的主要目标是揭示将RNA结构与功能联系起来的设计原理,以理解和构建这种关系。在这里,我们报告了一种称为细胞内SHAPE-Seq的简单,高通量方法,该方法将细胞内RNA结构的探测与基因表达的测量相结合,以同时表征细菌细胞中RNA的结构和功能。我们使用细胞内SHAPE-Seq来研究调节大肠杆菌中翻译的两种RNA机制的结构-功能关系。我们发现,当不存在结合伴侣时,参与RNA-RNA相互作用的核苷酸是高度可及的,并且由于RNA-RNA相互作用而引起的RNA结构变化可与基因表达的变化定量相关。我们还表征了三个内源表达的非编码RNA的细胞结构:5S rRNA,RNase P和btuB核糖开关。最后,细胞内和体外折叠RNA结构之间的比较揭示了合成RNA的显着相似性,但参与复杂细胞相互作用的RNA却存在显着差异。因此,细胞内SHAPE-Seq是生物学家和工程师发现细胞中RNA的序列,结构和功能之间关系的一种易于使用的工具。

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