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Kinetic analysis of protein aggregation monitored by real-time 2D solid-state NMR spectroscopy

机译:实时2D固态NMR光谱监测的蛋白质聚集的动力学分析

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摘要

It is shown that real-time 2D solid-state NMR can be used to obtain kinetic and structural information about the process of protein aggregation. In addition to the incorporation of kinetic information involving intermediate states, this approach can offer atom-specific resolution for all detectable species. The analysis was carried out using experimental data obtained during aggregation of the 10.4 kDa Crh protein, which has been shown to involve a partially unfolded intermediate state prior to aggregation. Based on a single real-time 2D 13C–13C transition spectrum, kinetic information about the refolding and aggregation step could be extracted. In addition, structural rearrangements associated with refolding are estimated and several different aggregation scenarios were compared to the experimental data.
机译:结果表明,实时2D固态NMR可用于获得有关蛋白质聚集过程的动力学和结构信息。除了合并涉及中间状态的动力学信息外,该方法还可以为所有可检测的物种提供特定于原子的分辨率。使用在10.4 kDa Crh蛋白聚集过程中获得的实验数据进行分析,该数据已显示在聚集之前涉及部分未折叠的中间状态。基于单个实时2D 13 C– 13 C跃迁谱,可以提取有关重折叠和聚集步骤的动力学信息。另外,估计了与重折叠有关的结构重排,并将几种不同的聚集情况与实验数据进行了比较。

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