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Controlled Pore Glass-based oligonucleotide affinity support: towards High Throughput Screening methods for the identification of conformation-selective G-quadruplex ligands

机译:基于孔隙玻璃的寡核苷酸亲和力支持:朝向高通量筛选方法,用于鉴定构象选择性G-四逆转带配体

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摘要

Target selectivity is one of the main challenges in the search for small molecules able to act as effective and non-toxic anticancer and/or antiviral drugs. To achieve this goal, handy, rapid and reliable High Throughput Screening methodologies are needed. We here describe a novel functionalization for the solid phase synthesis of oligonucleotides on Controlled Pore Glass, including a flexible hexaethylene glycol spacer linking the first nucleoside through the nucleobase via a covalent bond stable to the final deprotection step. This allowed us preparing fully deprotected oligonucleotides still covalently attached to their supports. In detail, on this support we performed both the on-line synthesis of different secondary structure-forming oligonucleotides and the affinity chromatography-based screenings of conformation-selective G-quadruplex ligands. By using a fluorescent core-extended naphthalene diimide with different emitting response upon binding to sequences folding into G-quadruplexes of different topologies, we have been able to discriminate not only G-quadruplex vs. duplex DNA structures, but also different G-quadruplex conformations on the glass beads by confocal microscopy. (C) 2018 Elsevier B.V. All rights reserved.
机译:目标选择性是寻找能够充当有效和无毒抗癌和/或抗病毒药物的小分子的主要挑战之一。为了实现这一目标,需要方便,快速可靠的高吞吐量筛选方法。我们在这里描述了对受控孔隙玻璃上的寡核苷酸的固相合成的新官能化,包括通过核碱基通过核碱基与最终脱保护步骤稳定地连接第一核苷的柔性六亚乙二醇间隔物。这允许我们制备完全脱保护的寡核苷酸,仍然共价连接到它们的载体上。详细地,在这种支持下,我们进行了不同二级结构的寡核苷酸的在线合成,以及组合选择性G- Quadreplex配体的基于亲和层析的筛选。通过使用具有不同发光响应的荧光芯延伸的萘二亚胺,在结合到不同拓扑的G-Quadryperes中的序列中,我们能够不仅区分G-QuadRuple与双相DNA结构,而且可以区分不同的G-Quadruplex构象通过共聚焦显微镜在玻璃珠上。 (c)2018 Elsevier B.v.保留所有权利。

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