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基于蛋白质纳米孔的三级 RNA 折叠靶向药物筛选策略

Tertiary RNA Folding-Targeted Drug Screening Strategy Using a Protein Nanopore.

机构信息

Disease Target Structure Research Center, KRIBB, Daejeon 34141, Republic of Korea.

College of Pharmacy, Chungbuk National University, Cheongju 28644, Republic of Korea.

出版信息

Anal Chem. 2021 Feb 9;93(5):2811-2819. doi: 10.1021/acs.analchem.0c03941. Epub 2021 Jan 21.

Abstract

Bacterial riboswitch RNAs are attractive targets for novel antibiotics against antibiotic-resistant superbacteria. Their binding to cognate metabolites is essential for the regulation of bacterial gene expression. Despite the importance of RNAs as therapeutic targets, the development of RNA-targeted, small-molecule drugs is limited by current biophysical methods. Here, we monitored the specific interaction between the adenine-sensing riboswitch aptamer domain (ARS) and adenine at the single-molecule level using α-hemolysin (αHL) nanopores. During adenine-induced tertiary folding, adenine-bound ARS intermediates exhibited characteristic nanopore events, including a two-level ionic current blockade and a ∼ 5.6-fold longer dwell time than that of free RNA. In a proof-of-concept experiment, tertiary RNA folding-targeted drug screening was performed using a protein nanopore, which resulted in the discovery of three new ARS-targeting hit compounds from a natural compound library. Taken together, these results reveal that αHL nanopores are a valuable platform for ultrasensitive, label-free, and single-molecule-based drug screening against therapeutic RNA targets.

摘要

细菌核糖体开关 RNA 是针对抗药性超级细菌的新型抗生素的有吸引力的靶标。它们与同源代谢物的结合对于细菌基因表达的调控至关重要。尽管 RNA 作为治疗靶标非常重要,但 RNA 靶向小分子药物的发展受到当前生物物理方法的限制。在这里,我们使用α-hemolysin (αHL) 纳米孔在单分子水平上监测腺嘌呤感应核糖开关适体结构域 (ARS) 与腺嘌呤的特异性相互作用。在腺嘌呤诱导的三级折叠过程中,结合腺嘌呤的 ARS 中间体表现出特征性的纳米孔事件,包括两级离子电流阻断和比游离 RNA 长约 5.6 倍的停留时间。在概念验证实验中,使用蛋白质纳米孔进行了针对三级 RNA 折叠的药物筛选实验,从天然化合物文库中发现了三种新的 ARS 靶向化合物。总之,这些结果表明,αHL 纳米孔是针对治疗性 RNA 靶标进行超灵敏、无标记和基于单分子的药物筛选的有价值平台。

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