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点击化学法对核酸进行位点定向自旋标记:通过电子顺磁共振波谱法检测双链 DNA 中的脱碱基位点。

Site-directed spin-labeling of nucleic acids by click chemistry: detection of abasic sites in duplex DNA by EPR spectroscopy.

机构信息

Department of Physics and Chemistry, University of Southern Denmark, Nucleic Acid Center Campusvej 55, 5230 Odense, Denmark.

出版信息

J Am Chem Soc. 2010 Aug 4;132(30):10424-8. doi: 10.1021/ja102797k.

Abstract

This paper describes a spin label that can detect and identify local structural deformations in duplex DNA, in particular abasic sites. The spin label was incorporated into DNA by a new postsynthetic approach using click-chemistry on a solid support, which simplified both the synthesis and purification of the spin-labeled oligonucleotides. A nitroxide-functionalized azide, prepared by a short synthetic route, was reacted with an oligomer containing 5-ethynyl-2'-dU. The conjugation proceeded in quantitative yield and resulted in a fairly rigid linker between the modified nucleotide and the nitroxide spin label. The spin label was used to detect, for the first time, abasic sites in duplex DNA by X-band CW-EPR spectroscopy and give information about other structural deformations as well as local conformational changes in DNA. For example, reduced mobility of the spin label in a mismatched pair with T was consistent with the spin label displacing the T from the duplex. Addition of mercury(II) to this mispair resulted in a substantial increase in the motion of the spin label, consistent with formation of a metallopair between the T and the spin-labeled base that results in movement of the spin label out of the duplex and toward the solution. Thus, reposition of the spin label, when acting as a mercury(II)-controlled mechanical lever, can be readily detected by EPR spectroscopy. The ease of incorporation and properties of the new spin label make it attractive for EPR studies of nucleic acids and other macromolecules.

摘要

本文描述了一种自旋标记物,它可以检测和识别双链 DNA 中的局部结构变形,特别是碱基缺失。该自旋标记物通过一种新的合成方法被引入 DNA 中,该方法使用点击化学在固体支持物上进行,从而简化了自旋标记寡核苷酸的合成和纯化过程。通过短的合成路线制备的氮氧自由基功能化叠氮化物与含有 5-乙炔基-2'-dU 的寡聚物反应。该反应以定量产率进行,并且在修饰核苷酸和氮氧自由基自旋标记物之间产生了相当刚性的连接体。自旋标记物首次用于通过 X 波段 CW-EPR 光谱检测双链 DNA 中的碱基缺失,并提供有关其他结构变形以及 DNA 局部构象变化的信息。例如,自旋标记物在与 T 不匹配的碱基对中的迁移率降低与自旋标记物从双链体中置换 T 一致。将汞(II)添加到该错配碱基对中,导致自旋标记物的运动大大增加,这与 T 和自旋标记碱基之间形成金属对一致,导致自旋标记物从双链体中移出并向溶液中移动。因此,自旋标记物作为汞(II)控制的机械杠杆重新定位时,很容易通过 EPR 光谱检测到。新自旋标记物的易于掺入和性质使其成为研究核酸和其他大分子的 EPR 的有吸引力的选择。

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