非标准三向和四向DNA连接的分析。

IF 4.2 3区 生物学 Q1 BIOCHEMICAL RESEARCH METHODS Methods Pub Date : 2023-11-01 DOI:10.1016/j.ymeth.2023.09.002
Bríonna McGorman , Simon Poole , Miguel Vázquez López , Andrew Kellett
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引用次数: 0

摘要

近年来,可以选择性地与非经典DNA结构结合的化合物的开发已经扩大。连接DNA,包括三向连接(3WJs)和四向Holliday连接(HJs),为发育治疗提供了一个有趣的靶点,因为3WJ和HJs都参与DNA复制和修复过程。然而,可用于分析连接DNA结合的测定方法数量有限。在这里,我们描述了多重荧光聚丙烯酰胺凝胶电泳(PAGE)和微尺度热泳(MST)分析的设计和执行,这些分析能够评估连接结合化合物。两种表征良好的连接结合化合物——C6连接的双吖啶配体和铁(II)结合的肽螺旋体,分别识别HJs和3WJs,被用作MST和PAGE实验的探针。多重PAGE分析扩展了先前报道的荧光PAGE,因为它使用了四个单独的荧光团,这些荧光团可以组合起来可视化3WJ和HJ形成过程中存在的单链、假双链和连接DNA。据我们所知,使用MST来鉴定连接结合剂的结合亲和力是该技术的第一个报道例子。PAGE和MST的联合使用为3WJ和HJ的形成以及这些试剂的直接结合亲和力(Kd和EC50)的可视化提供了互补的结果。这些测定可用于帮助发现和设计靶向非经典核酸结构的新疗法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Analysis of non-canonical three- and four-way DNA junctions

The development of compounds that can selectively bind with non-canonical DNA structures has expanded in recent years. Junction DNA, including three-way junctions (3WJs) and four-way Holliday junctions (HJs), offer an intriguing target for developmental therapeutics as both 3WJs and HJs are involved in DNA replication and repair processes. However, there are a limited number of assays available for the analysis of junction DNA binding. Here, we describe the design and execution of multiplex fluorescent polyacrylamide gel electrophoresis (PAGE) and microscale thermophoresis (MST) assays that enable evaluation of junction-binding compounds. Two well characterised junction-binding compounds—a C6 linked bis-acridine ligand and an iron(II)-bound peptide helicate, which recognise HJs and 3WJs, respectively—were employed as probes for both MST and PAGE experiments. The multiplex PAGE assay expands beyond previously reported fluorescent PAGE as it uses four individual fluorophores that can be combined to visualise single-strands, pseudo-duplexes, and junction DNA present during 3WJ and HJ formation. The use of MST to identify the binding affinity of junction binding agents is, to our knowledge, first reported example of this technique. The combined use of PAGE and MST provides complementary results for the visualisation of 3WJ and HJ formation and the direct binding affinity (Kd and EC50) of these agents. These assays can be used to aid the discovery and design of new therapeutics targeting non-canonical nucleic acid structures.

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来源期刊
Methods
Methods 生物-生化研究方法
CiteScore
9.80
自引率
2.10%
发文量
222
审稿时长
11.3 weeks
期刊介绍: Methods focuses on rapidly developing techniques in the experimental biological and medical sciences. Each topical issue, organized by a guest editor who is an expert in the area covered, consists solely of invited quality articles by specialist authors, many of them reviews. Issues are devoted to specific technical approaches with emphasis on clear detailed descriptions of protocols that allow them to be reproduced easily. The background information provided enables researchers to understand the principles underlying the methods; other helpful sections include comparisons of alternative methods giving the advantages and disadvantages of particular methods, guidance on avoiding potential pitfalls, and suggestions for troubleshooting.
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