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Structural characterization of NORAD reveals a stabilizing role of spacers and two new repeat units

机译:挪亚的结构表征揭示了垫片的稳定作用和两个新的重复单位

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摘要

Long non-coding RNAs (lncRNAs) can perform a variety of key cellular functions by interacting with proteins and other RNAs. Recent studies have shown that the functions of lncRNAS are largely mediated by their structures. However, our structural knowledge for most lncRNAS is limited to sequence-based computational predictions. Non-coding RNA activated by DNA damage (NORAD) is an atypical lncRNA due to its abundant expression and high sequence conservation. NORAD regulates genomic stability by interacting with proteins and microRNAs. Previous sequence-based characterization has identified a modular organization of NORAD composed of several NORAD repeat units (NRUs). These units comprise the protein-binding elements and are separated by regular spacers. Here, we experimentally determine for the first time the secondary structure of NORAD using the nextPARS approach. Our results suggest that the spacer regions provide structural stability to NRUs. Furthermore, we uncover two previously unreported NRUs, and determine the core structural motifs conserved across NRUs. Overall, these findings will help to elucidate the function and evolution of NORAD.
机译:长期非编码RNA(LNCRNA)可以通过与蛋白质和其他RNA相互作用来执行各种密钥蜂窝功能。最近的研究表明,LNCRNA的功能在很大程度上被其结构介导。然而,我们大多数LNCRNA的结构知识仅限于基于序列的计算预测。由于其丰富的表达和高序列守恒,通过DNA损伤(Norad)激活的非编码RNA是非典型LNCRNA。诺拉德通过与蛋白质和微大罗氏相互作用来调节基因组稳定性。以前的基于序列的表征已经确定了由几个Norad重复单元(NRU)组成的挪拉的模块化组织。这些单元包含蛋白质结合元素,并通过常规间隔物分离。在这里,我们通过Nextpars方法实验首次确定Norad的二级结构。我们的研究结果表明,间隔区为NRU提供了结构稳定性。此外,我们发现了两个先前未报告的NRU,并确定跨越NRU保存的核心结构主题。总体而言,这些调查结果将有助于阐明Norad的功能和演变。

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