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根据 overnight 记录的光谱集完成蛋白质分配。 (注:“overnight”在这里结合语境推测可能是指“一整夜”地记录光谱,但单独这个词翻译为“通宵”等更符合日常语境,而在这里结合专业内容,直接保留英文更合适,因为不清楚具体专业上这个词的准确含义,如果有专业背景知识,可根据实际情况调整翻译使其更准确专业。)

Complete protein assignment from sets of spectra recorded overnight.

作者信息

Fredriksson Jonas, Bermel Wolfgang, Billeter Martin

机构信息

Department of Chemistry and Molecular Biology, University of Gothenburg, 40530, Gothenburg, Sweden.

Bruker BioSpin GmbH, 76287, Rheinstetten, Germany.

出版信息

J Biomol NMR. 2019 Feb;73(1-2):59-70. doi: 10.1007/s10858-019-00226-8. Epub 2019 Feb 15.

DOI:10.1007/s10858-019-00226-8
PMID:30771052
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6441399/
Abstract

A flexible and scalable approach for protein NMR is introduced that builds on rapid data collection via projection spectroscopy and analysis of the spectral input data via joint decomposition. Input data may originate from various types of spectra, depending on the ultimate goal: these may result from experiments based on triple-resonance pulse sequences, or on TOCSY or NOESY sequences, or mixtures thereof. Flexible refers to the free choice of spectra for the joint decompositions depending on the purpose: assignments, structure, dynamics, interactions. Scalable means that the approach is open to the addition of similar or different experiments, e.g. larger proteins may require a wider selection of triple-resonance based experiments. Central to the proposed approach is the mutual support among the different spectra during the spectral analysis: for example, sparser triple-resonance spectra may help decomposing (separating) spin systems in a TOCSY or identifying unique NOEs. In the example presented, backbone plus side chain assignments of ubiquitin were obtained from the combination of either two or three of the following projection experiments: a 4D HCCCONH, a 4D HNCACO and a 3D HNCACB. In all cases, TOCSY data (4D HCCCONH) proved crucial not only for the side chain assignments, but also for the sequential assignment. Even when total recording time was reduced to about 10 h, nearly complete assignments were obtained, with very few missing assignments and even fewer differences to a reference.

摘要

本文介绍了一种灵活且可扩展的蛋白质核磁共振方法,该方法基于通过投影光谱进行快速数据采集,并通过联合分解对光谱输入数据进行分析。输入数据可能源自各种类型的光谱,这取决于最终目标:这些光谱可能来自基于三共振脉冲序列、TOCSY或NOESY序列或它们的混合序列的实验。灵活性是指根据目的自由选择用于联合分解的光谱:归属、结构、动力学、相互作用。可扩展性意味着该方法对添加相似或不同的实验开放,例如,更大的蛋白质可能需要更广泛地选择基于三共振的实验。所提出方法的核心是光谱分析过程中不同光谱之间的相互支持:例如,更稀疏的三共振光谱可能有助于在TOCSY中分解(分离)自旋系统或识别独特的核Overhauser效应(NOE)。在给出的示例中,泛素的主链加侧链归属是通过以下投影实验中的两个或三个的组合获得的:一个4D HCCCONH、一个4D HNCACO和一个3D HNCACB。在所有情况下,TOCSY数据(4D HCCCONH)不仅被证明对侧链归属至关重要,而且对序列归属也至关重要。即使总记录时间减少到约10小时,也获得了几乎完整的归属,缺失的归属很少,与参考文献的差异甚至更少。

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本文引用的文献

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Non-Uniform Sampling for All: More NMR Spectral Quality, Less Measurement Time.面向所有人的非均匀采样:更高的核磁共振光谱质量,更短的测量时间。
Am Pharm Rev. 2017 May/Jun;20(4). Epub 2017 Jun 30.
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C APSY-NMR for sequential assignment of intrinsically disordered proteins.用于内在无序蛋白质序列归属的CAPSY-NMR
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Current NMR Techniques for Structure-Based Drug Discovery.基于结构的药物发现的当前 NMR 技术。
Molecules. 2018 Jan 12;23(1):148. doi: 10.3390/molecules23010148.
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Non-uniform sampling in biomolecular NMR.生物分子核磁共振中的非均匀采样
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Recent advances in measuring the kinetics of biomolecules by NMR relaxation dispersion spectroscopy.利用核磁共振弛豫分散光谱法测量生物分子动力学的最新进展。
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Modern Technologies of Solution Nuclear Magnetic Resonance Spectroscopy for Three-dimensional Structure Determination of Proteins Open Avenues for Life Scientists.用于蛋白质三维结构测定的溶液核磁共振光谱现代技术为生命科学家开辟了道路。
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DIADECOMP: A new approach to analyze decompositions from projection spectroscopy.DIADECOMP:一种分析投影光谱分解的新方法。
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Highly efficient NMR assignment of intrinsically disordered proteins: application to B- and T cell receptor domains.高效的 NMR 分配固有无序蛋白:在 B 细胞和 T 细胞受体结构域的应用。
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Automated protein backbone assignment using the projection-decomposition approach.利用投影分解方法进行自动蛋白质主链赋值。
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Structural characterisation of a histone domain by projection-decomposition.通过投影分解对组蛋白结构域进行结构分析。
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