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首页> 外文期刊>Angewandte Chemie >Discovery of Small Molecule Ligands for MALAT1 by Tuning an RNA-Binding Scaffold
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Discovery of Small Molecule Ligands for MALAT1 by Tuning an RNA-Binding Scaffold

机译:通过调整RNA装订支架来发现MALAT1的小分子配体

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摘要

Structural studies of the 3-end of the oncogenic long non-coding RNA metastasis-associated lung adenocarcinoma transcript 1 (MALAT1) confirmed a unique triple-helix structure. This structure enables accumulation of the transcript, and high levels of MALAT1 are found in several cancers. Here, we synthesize a small molecule library based on an RNA-binding scaffold, diphenylfuran (DPF), screen it against a variety of nucleic acid constructs, and demonstrate for the first time that the MALAT1 triple helix can be selectively targeted with small molecules. Computational analysis revealed a trend between subunit positioning and composition on DPF shape and intramolecular interactions, which in turn generally correlated with selectivity and binding strengths. This work thus provides design strategies toward chemical probe development for the MALAT1 triple helix and suggests that comprehensive analyses of RNA-focused libraries can generate insights into selective RNA recognition.
机译:致癌长非编码RNA转移相关肺腺癌转录1(MALAT1)的三端的结构研究证实了独特的三螺旋结构。 该结构能够积累转录物,并且在几种癌症中发现高水平的Malat1。 在此,我们基于RNA结合支架,二苯基呋喃(DPF),筛选出各种核酸构建体的基于RNA结合支架,并首次证明MALAT1三螺旋可以选择性地靶向小分子。 计算分析揭示了亚基定位与DPF形状和分子内相互作用的组成之间的趋势,其又与选择性和结合强度相关。 因此,这项工作为Malat1三螺旋的化学探测开发提供了设计策略,并表明RNA的综合分析可以产生对选择性RNA识别的见解。

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