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高通量 X 射线吸收光谱法对金属蛋白的特性分析。

Characterization of metalloproteins by high-throughput X-ray absorption spectroscopy.

机构信息

New York SGX Research Center for Structural Genomics (NYSGXRC), Case Western Reserve University, Center for Proteomics and Bioinformatics, Case Center for Synchrotron Biosciences, Upton, New York 11973, USA.

出版信息

Genome Res. 2011 Jun;21(6):898-907. doi: 10.1101/gr.115097.110. Epub 2011 Apr 11.

DOI:10.1101/gr.115097.110
PMID:21482623
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3106322/
Abstract

High-throughput X-ray absorption spectroscopy was used to measure transition metal content based on quantitative detection of X-ray fluorescence signals for 3879 purified proteins from several hundred different protein families generated by the New York SGX Research Center for Structural Genomics. Approximately 9% of the proteins analyzed showed the presence of transition metal atoms (Zn, Cu, Ni, Co, Fe, or Mn) in stoichiometric amounts. The method is highly automated and highly reliable based on comparison of the results to crystal structure data derived from the same protein set. To leverage the experimental metalloprotein annotations, we used a sequence-based de novo prediction method, MetalDetector, to identify Cys and His residues that bind to transition metals for the redundancy reduced subset of 2411 sequences sharing <70% sequence identity and having at least one His or Cys. As the HT-XAS identifies metal type and protein binding, while the bioinformatics analysis identifies metal- binding residues, the results were combined to identify putative metal-binding sites in the proteins and their associated families. We explored the combination of this data with homology models to generate detailed structure models of metal-binding sites for representative proteins. Finally, we used extended X-ray absorption fine structure data from two of the purified Zn metalloproteins to validate predicted metalloprotein binding site structures. This combination of experimental and bioinformatics approaches provides comprehensive active site analysis on the genome scale for metalloproteins as a class, revealing new insights into metalloprotein structure and function.

摘要

高通量 X 射线吸收光谱法用于测量过渡金属含量,方法是对来自纽约 SGX 结构基因组学研究中心的几百种不同蛋白质家族的 3879 种纯化蛋白质进行 X 射线荧光信号的定量检测。分析的蛋白质中约有 9%以化学计量的方式存在过渡金属原子(Zn、Cu、Ni、Co、Fe 或 Mn)。该方法高度自动化,高度可靠,其依据是将结果与源自同一蛋白质组的晶体结构数据进行比较。为了利用实验金属蛋白注释,我们使用基于序列的从头预测方法 MetalDetector 来识别 Cys 和 His 残基,这些残基与过渡金属结合,用于具有 <70%序列同一性和至少一个 His 或 Cys 的 2411 个序列的冗余减少子集。由于 HT-XAS 可识别金属类型和蛋白质结合,而生物信息学分析可识别金属结合残基,因此将结果结合起来可鉴定蛋白质及其相关家族中的潜在金属结合位点。我们探索了将此数据与同源模型相结合,以生成具有代表性蛋白质的金属结合位点的详细结构模型。最后,我们使用两种纯化的 Zn 金属蛋白的扩展 X 射线吸收精细结构数据来验证预测的金属蛋白结合位点结构。这种实验和生物信息学方法的结合为金属蛋白这一类提供了全面的基因组规模的活性位点分析,揭示了金属蛋白结构和功能的新见解。

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本文引用的文献

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