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Large-scale mapping of sequence-function relations in small regulatory RNAs reveals plasticity and modularity

机译:小调节RNA中的序列-功能关系的大规模作图揭示了可塑性和模块性

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Two decades into the genomics era the question of mapping sequence to function has evolved from identifying functional elements to characterizing their quantitative properties including, in particular, their specificity and efficiency. Here, we use a large-scale approach to establish a quantitative map between the sequence of a bacterial regulatory RNA and its efficiency in modulating the expression of its targets. Our approach generalizes the sort-seq method, introduced recently to analyze promoter sequences, in order to accurately quantify the efficiency of a large library of sequence variants. We focus on two small RNAs (sRNAs) in E. coli, DsrA and RyhB, and their regulation of both repressed and activated targets. In addition to precisely identifying functional elements in the sRNAs, our data establish quantitative relationships between structural and energetic features of the sRNAs and their regulatory activity, and characterize a large set of direct and indirect interactions between nucleotides. A core of these interactions supports a model where specificity can be enhanced by a rigid molecular structure. Both sRNAs exhibit a modular design with limited cross-interactions, dividing the requirements for structural stability and target binding among modules.
机译:在基因组学时代的二十年间,将序列映射到功能的问题已经从识别功能元件演变为表征其定量特性的方法,尤其包括其特异性和效率。在这里,我们使用大规模的方法来建立细菌调控RNA的序列与其调节其靶标表达效率之间的定量图。我们的方法概括了最近引入的用于分析启动子序列的sort-seq方法,以便准确地量化大型序列变体文库的效率。我们专注于大肠杆菌中的两个小RNA(sRNA),DsrA和RyhB,以及它们对受阻和受激活靶标的调控。除了精确识别sRNA中的功能元件外,我们的数据还建立了sRNA的结构和能量特征与其调节活性之间的定量关系,并表征了核苷酸之间的大量直接和间接相互作用。这些相互作用的核心支持一个模型,在该模型中可以通过刚性分子结构来增强特异性。两种sRNA均具有有限的交叉相互作用的模块化设计,从而在模块之间划分了结构稳定性和靶标结合的要求。

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