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以单残基空间分辨率和毫秒级时间分辨率跟踪分子跃迁。

Following molecular transitions with single residue spatial and millisecond time resolution.

作者信息

Shcherbakova Inna, Mitra Somdeb, Beer Robert H, Brenowitz Michael

机构信息

Department of Biochemistry, Albert Einstein College of Medicine, Bronx, New York 10461, USA.

出版信息

Methods Cell Biol. 2008;84:589-615. doi: 10.1016/S0091-679X(07)84019-2.

Abstract

"Footprinting" describes assays in which ligand binding or structure formation protects polymers such as nucleic acids and proteins from either cleavage or modification; footprinting allows the accessibility of individual residues to be mapped in solution. Equilibrium and time-dependent footprinting links site-specific structural information with thermodynamic and kinetic transitions, respectively. The hydroxyl radical (*OH) is a uniquely insightful footprinting probe by virtue of it being among the most reactive chemical oxidants; it reports the solvent accessibility of reactive sites on macromolecules with as fine as a single residue resolution. A novel method of millisecond time-resolved *OH footprinting is presented based on the Fenton reaction, Fe(II) + H(2)O(2) --> Fe(III) + *OH + OH(-). It is implemented using a standard three-syringe quench-flow mixer. The utility of this method is demonstrated by its application to the studies on RNA folding. Its applicability to a broad range of biological questions involving the function of DNA, RNA, and proteins is discussed.

摘要

“足迹法”描述的是这样一些分析方法,即配体结合或结构形成可保护诸如核酸和蛋白质等聚合物不被切割或修饰;足迹法能在溶液中绘制出各个残基的可及性图谱。平衡足迹法和时间依赖性足迹法分别将位点特异性结构信息与热力学和动力学转变联系起来。羟基自由基(·OH)是一种极具洞察力的足迹探针,因为它是反应活性最强的化学氧化剂之一;它能以单残基分辨率报告大分子上反应位点的溶剂可及性。基于芬顿反应Fe(II) + H₂O₂ → Fe(III) + ·OH + OH⁻,提出了一种毫秒级时间分辨·OH足迹法的新方法。该方法通过标准的三注射器淬灭流动混合器来实现。通过将其应用于RNA折叠研究,证明了该方法的实用性。还讨论了该方法在涉及DNA、RNA和蛋白质功能的广泛生物学问题中的适用性。

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