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小分子和核仁素靶向 let-7e 前体 miRNA 的 G-四链体

Targeting a G-quadruplex from let-7e pre-miRNA with small molecules and nucleolin.

机构信息

CICS-UBI - Centro de Investigação em Ciências da Saúde, Universidade da Beira Interior, Av. Infante D. Henrique, Covilhã 6200-506, Portugal.

Univ. Grenoble Alpes, CNRS, CEA, Institut de Biologie Structurale (IBS), Grenoble, France; Univ. Grenoble Alpes, CNRS, CEA, EMBL Integrated Structural Biology Grenoble (ISBG), Grenoble, France.

出版信息

J Pharm Biomed Anal. 2022 Jun 5;215:114757. doi: 10.1016/j.jpba.2022.114757. Epub 2022 Apr 7.

DOI:10.1016/j.jpba.2022.114757
PMID:35462282
Abstract

Let-7e precursor microRNA has the potential to adopt a G-quadruplex (rG4) structure and recently, its roles in oncology have been the focus of much attention, as it is now known that let-7e pre-miRNA is frequently dysregulated in cancers. Therefore, it is crucial to unveil and fully characterize its ability to adopt a rG4 structure, which could be stabilized or destabilized by small molecules and proteins such as nucleolin, a protein that is deeply associated with miRNA biogenesis. Herein, by combining a set of different methods such as circular dichroism (CD), nuclear magnetic resonance (NMR), UV spectroscopy (thermal difference spectra (TDS) and isothermal difference spectra (IDS)) and polyacrylamide gel electrophoresis (PAGE), we demonstrate the formation of the rG4 structure found in let-7e pre-miRNA sequence in the presence of K (5'-GGGCUGAGGUAGGAGG-3'). The ability of eight small molecules (or ligands) to bind to and stabilize this rG4 structure was also fully assessed. The dissociation constants for each RNA G-quadruplex/ligand complex, determined by surface plasmon resonance (SPR), ranged in the 10 to 10 M range. Lastly, the binding of the rG4 structure to nucleolin in the presence and absence of ligands was evaluated via CD, SPR, PAGE and confocal microscopy. The small molecules 360 A and PDS demonstrated attractive properties to targetthe rG4 structure of let-7e pre-miRNA and control its biology. Our findings also highlighted that the interaction of TMPyP4 with the G-quadruplex of let-7e precursor miRNA could block the formation of the complex between the rG4 and nucleolin. Overall, this study introduces an approach to target the rG4 found in let-7e pre-miRNA which opens up a new opportunity to control the microRNA biogenesis.

摘要

Let-7e 前体 microRNA 具有形成 G-四链体 (rG4) 结构的潜力,最近,其在肿瘤学中的作用引起了广泛关注,因为现在已知 let-7e 前体 miRNA 在癌症中经常失调。因此,揭示并充分表征其形成 rG4 结构的能力至关重要,小分子和蛋白质(如核仁素)可以稳定或破坏 rG4 结构,核仁素与 miRNA 生物发生密切相关。在此,通过结合一系列不同的方法,如圆二色性 (CD)、核磁共振 (NMR)、紫外光谱 (热差谱 (TDS) 和等度差谱 (IDS)) 和聚丙烯酰胺凝胶电泳 (PAGE),我们证明了在 K (5'-GGGCUGAGGUAGGAGG-3') 存在下,let-7e 前体 miRNA 序列中存在 rG4 结构的形成。还全面评估了八种小分子 (或配体) 结合并稳定这种 rG4 结构的能力。通过表面等离子体共振 (SPR) 测定的每个 RNA G-四联体/配体复合物的离解常数在 10 到 10 M 范围内。最后,通过 CD、SPR、PAGE 和共聚焦显微镜评估了 rG4 结构在存在和不存在配体的情况下与核仁素的结合。小分子 360 A 和 PDS 表现出有吸引力的特性,可以靶向 let-7e 前体 miRNA 的 rG4 结构并控制其生物学。我们的研究结果还强调了 TMPyP4 与 let-7e 前体 miRNA G-四联体的相互作用可以阻止 rG4 与核仁素形成复合物。总的来说,这项研究介绍了一种针对 let-7e 前体 miRNA 中发现的 rG4 的方法,为控制 microRNA 生物发生开辟了新的机会。

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