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Orphan spin polarization: A catalyst for high-throughput solid-state NMR spectroscopy of proteins

机译:孤子自旋极化:蛋白质高通量固态NMR光谱的催化剂

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摘要

Magic angle spinning solid-state NMR (MAS ssNMR) spectroscopy is a powerful method for structure determination of biomacromolecules that are recalcitrant to crystallization (membrane proteins and fibrils). Conventional multidimensional ssNMR methods acquire one experiment at a time. This approach is time consuming and discards orphan (unused) spin operators. Relatively low sensitivity and poor resolution of protein samples require long acquisition times for multidimensional ssNMR experiments. Here, we describe our recent progress in the development of multiple acquisition solid-state NMR methods for protein structure determination. A family of experiments called Polarization Optimized Experiments (POE) were designed, in which we utilized the orphan spin operators that are discarded in classical multidimensional NMR experiments, recovering them to allow simultaneous acquisition of multiple 2D and 3D experiments, all while using conventional probes with spectrometers equipped with one receiver. Three strategies namely, DUMAS, MEIOSIS, and MAeSTOSO were used for the concatenation of various 2D and 3D experiments. These methods open up new avenues for reducing the acquisition times of multidimensional experiments for biomolecular ssNMR spectroscopy.
机译:魔角旋转固态NMR(MAS ssNMR)光谱是一种强大的方法,可用于确定对结晶不利的生物大分子(膜蛋白和原纤维)的结构。常规的多维ssNMR方法一次只能进行一次实验。这种方法很耗时,并且会丢弃孤立的(未使用的)自旋运算符。蛋白质样品的相对较低的灵敏度和较差的分辨率需要较长的采集时间才能进行多维ssNMR实验。在这里,我们描述了我们在蛋白质结构确定的多采集固态NMR方法开发中的最新进展。设计了一系列称为极化优化实验(POE)的实验,其中我们利用了在经典多维NMR实验中丢弃的孤立自旋算子,对其进行了回收,以允许同时采集多个2D和3D实验,而同时使用常规探针光谱仪配备一个接收器。 DUMAS,MEIOSIS和MAeSTOSO这三种策略用于各种2D和3D实验的串联。这些方法为减少生物分子ssNMR光谱的多维实验的获取时间开辟了新途径。

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