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J Vis Exp. 2013 Dec 16(82):e50747. doi: 10.3791/50747.
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本文引用的文献

1
Coordination chemistry of copper proteins: how nature handles a toxic cargo for essential function.铜蛋白的配位化学:大自然如何处理对基本功能至关重要的有毒物质。
J Inorg Biochem. 2012 Feb;107(1):129-43. doi: 10.1016/j.jinorgbio.2011.11.024. Epub 2011 Dec 3.
2
The MXCXXC class of metallochaperone proteins: model studies.金属伴侣蛋白 MXCXXC 类:模型研究。
Chem Soc Rev. 2011 Nov;40(11):5282-92. doi: 10.1039/c1cs15086c. Epub 2011 Jun 22.
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NMR characterization of a Cu(I)-bound peptide model of copper metallochaperones: insights on the role of methionine.NMR 对铜结合肽模型的铜金属伴侣蛋白的表征:对蛋氨酸作用的深入了解。
Chem Commun (Camb). 2011 Jun 14;47(22):6407-9. doi: 10.1039/c1cc11600b. Epub 2011 May 9.
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Protein epitope mimetics as anti-infectives.蛋白表位模拟物作为抗感染药物。
Curr Opin Chem Biol. 2011 Jun;15(3):379-86. doi: 10.1016/j.cbpa.2011.02.015. Epub 2011 Mar 16.
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Structural biology of copper trafficking.铜转运的结构生物学
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Mechanistic insights into Cu(I) cluster transfer between the chaperone CopZ and its cognate Cu(I)-transporting P-type ATPase, CopA.铜(I)簇在伴侣蛋白 CopZ 与其同源铜(I)转运 P 型 ATP 酶 CopA 之间转移的机制见解。
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A tetranuclear Cu(I) cluster in the metallochaperone protein CopZ.金属伴侣蛋白CopZ中的四核铜(I)簇。
Biochemistry. 2009 Oct 13;48(40):9324-6. doi: 10.1021/bi9011995.
8
UCSF Chimera--a visualization system for exploratory research and analysis.加州大学旧金山分校奇美拉——一个用于探索性研究与分析的可视化系统。
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9
Trace elements in human physiology and pathology. Copper.人体生理与病理学中的微量元素。铜。
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10
Function, structure, and mechanism of intracellular copper trafficking proteins.细胞内铜转运蛋白的功能、结构及机制
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使用一维和二维¹H NMR确定肽-金属配合物的结构和配位情况

Structure and coordination determination of peptide-metal complexes using 1D and 2D ¹H NMR.

作者信息

Shoshan Michal S, Tshuva Edit Y, Shalev Deborah E

机构信息

Department of Chemistry, The Hebrew University of Jerusalem.

出版信息

J Vis Exp. 2013 Dec 16(82):e50747. doi: 10.3791/50747.

DOI:10.3791/50747
PMID:24378924
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4059281/
Abstract

Copper (I) binding by metallochaperone transport proteins prevents copper oxidation and release of the toxic ions that may participate in harmful redox reactions. The Cu (I) complex of the peptide model of a Cu (I) binding metallochaperone protein, which includes the sequence MTCSGCSRPG (underlined is conserved), was determined in solution under inert conditions by NMR spectroscopy. NMR is a widely accepted technique for the determination of solution structures of proteins and peptides. Due to difficulty in crystallization to provide single crystals suitable for X-ray crystallography, the NMR technique is extremely valuable, especially as it provides information on the solution state rather than the solid state. Herein we describe all steps that are required for full three-dimensional structure determinations by NMR. The protocol includes sample preparation in an NMR tube, 1D and 2D data collection and processing, peak assignment and integration, molecular mechanics calculations, and structure analysis. Importantly, the analysis was first conducted without any preset metal-ligand bonds, to assure a reliable structure determination in an unbiased manner.

摘要

金属伴侣转运蛋白对铜(I)的结合可防止铜氧化以及可能参与有害氧化还原反应的有毒离子的释放。通过核磁共振光谱法在惰性条件下于溶液中测定了一种铜(I)结合金属伴侣蛋白的肽模型的铜(I)配合物,该肽模型包含序列MTCSGCSRPG(下划线部分为保守序列)。核磁共振是一种广泛用于测定蛋白质和肽溶液结构的技术。由于难以结晶以提供适合X射线晶体学的单晶,核磁共振技术极具价值,特别是因为它提供的是关于溶液状态而非固态的信息。在此我们描述了通过核磁共振进行完整三维结构测定所需的所有步骤。该方案包括在核磁共振管中进行样品制备、一维和二维数据收集与处理、峰归属与积分、分子力学计算以及结构分析。重要的是,分析首先在没有任何预设金属 - 配体键的情况下进行,以确保以无偏差的方式可靠地确定结构。