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FRET-MC:一种用于体外研究 G4 结构的荧光熔融竞争分析方法。

FRET-MC: A fluorescence melting competition assay for studying G4 structures in vitro.

机构信息

Université Paris Saclay, CNRS UMR9187, INSERM U1196, Institut Curie, Orsay, France.

Laboratoire d'Optique et Biosciences, Ecole Polytechnique, CNRS, Inserm, Institut Polytechnique de Paris, Palaiseau, France.

出版信息

Biopolymers. 2021 Apr;112(4):e23415. doi: 10.1002/bip.23415. Epub 2020 Dec 24.

DOI:10.1002/bip.23415
PMID:33368198
Abstract

G-quadruplexes (G4) play crucial roles in biology, analytical chemistry and nanotechnology. The stability of G4 structures is impacted by the number of G-quartets, the length and positions of loops, flanking motifs, as well as additional structural elements such as bulges, capping base pairs, or triads. Algorithms such as G4Hunter or Quadparser may predict if a given sequence is G4-prone by calculating a quadruplex propensity score; however, experimental validation is still required. We previously demonstrated that this validation is not always straightforward, and that a combination of techniques is often required to unambiguously establish whether a sequence forms a G-quadruplex or not. In this article, we adapted the well-known FRET-melting assay to characterize G4 in batch, where the sequence to be tested is added, as an unlabeled competitor, to a system composed of a dual-labeled probe (F21T) and a specific quadruplex ligand. PhenDC3 was preferred over TMPyP4 because of its better selectivity for G-quadruplexes. In this so-called FRET-MC (melting competition) assay, G4-forming competitors lead to a marked decrease of the ligand-induced stabilization effect (∆T ), while non-specific competitors (e.g., single- or double-stranded sequences) have little effect. Sixty-five known sequences with different typical secondary structures were used to validate the assay, which was subsequently employed to assess eight novel sequences that were not previously characterized.

摘要

四链体(G4)在生物学、分析化学和纳米技术中发挥着关键作用。G4 结构的稳定性受到 G-四联体的数量、环的长度和位置、侧翼基序以及其他结构元素(如凸起、盖帽碱基对或三联体)的影响。G4Hunter 或 Quadparser 等算法可以通过计算四联体倾向性得分来预测给定序列是否易于形成 G4;然而,仍然需要进行实验验证。我们之前已经证明,这种验证并不总是直接的,通常需要结合多种技术才能明确确定一个序列是否形成 G-四联体。在本文中,我们改编了著名的 FRET-融解测定法,以批量方式表征 G4,其中要测试的序列作为未标记的竞争物添加到由双标记探针(F21T)和特定四联体配体组成的系统中。与 TMPyP4 相比,PhenDC3 因其对 G-四联体更好的选择性而被优先选用。在这种所谓的 FRET-MC(融解竞争)测定中,形成 G4 的竞争物会导致配体诱导的稳定化效应(∆T)显著降低,而非特异性竞争物(例如,单链或双链序列)几乎没有影响。使用 65 个具有不同典型二级结构的已知序列对该测定进行了验证,随后该测定被用于评估以前未表征的 8 个新序列。

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