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均匀 13C 标记蛋白质结构测定中的同核双共振偶联技术。

Homonuclear dipolar recoupling techniques for structure determination in uniformly 13C-labeled proteins.

机构信息

Department of Physics, University of Guelph, 50 Stone Road East, Guelph, Ontario, Canada.

出版信息

Solid State Nucl Magn Reson. 2009 Nov;36(3):119-28. doi: 10.1016/j.ssnmr.2009.07.003. Epub 2009 Aug 5.

Abstract

In solid-state NMR magic angle spinning is often used to remove line broadening associated with anisotropic interactions, such as chemical shift anisotropy and dipolar couplings. Dipolar recoupling refers to sequences of pulses designed to reintroduce dipolar interactions that are otherwise averaged by magic angle spinning. One of the key applications of homonuclear (and heteronuclear) dipolar recoupling is for the purpose of protein structure determination. Recoupling experiments, originally designed for applications in spin-pair labeled samples, have been revised in recent years for applications in samples with extensive or uniform incorporation of isotopic labels. In these samples multiple internuclear distances can in principle be probed simultaneously, but the dipolar truncation effects (i.e. attenuation of the effects of weak couplings by strong ones) circumvent such measurements. In this article we review some of the recent developments in homonuclear recoupling methods that allow overcoming this problem.

摘要

在固态 NMR 中,魔角旋转(magic angle spinning)通常用于消除与各向异性相互作用(如化学位移各向异性和偶极耦合)相关的谱线展宽。偶极重聚指的是一系列脉冲序列,旨在重新引入偶极相互作用,否则这些偶极相互作用会因魔角旋转而被平均化。同核(和异核)偶极重聚的一个主要应用是用于蛋白质结构测定。最初设计用于自旋对标记样品应用的重聚实验,近年来已针对广泛或均匀掺入同位素标记的样品的应用进行了修订。在这些样品中,原则上可以同时探测多个核间距离,但偶极截断效应(即强耦合对弱耦合的影响的衰减)会规避这些测量。在本文中,我们回顾了一些同核重聚方法的最新进展,这些方法可以克服这个问题。

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