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Infrared Study of Carbon Monoxide Migration among Internal Cavities of Myoglobin Mutant L29W

机译:一氧化碳在肌红蛋白突变体L29W内部腔之间迁移的红外研究

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摘要

Myoglobin, a small globular heme protein that binds gaseous ligands such asO2, CO and NO reversibly at the heme iron, provides an excellent modelsystem for studying structural and dynamic aspects of protein reactions. Flashphotolysis experiments, performed over wide ranges in time and temperature, reveal a complex ligand binding reaction with multiple kinetic intermediates, resulting from protein relaxation and movements of the ligand within the protein. Our recent studies of carbonmonoxy-myoglobin (MbCO) mutant L29W, using time-resolved infrared spectroscopy in combination with x-ray crystallography, have correlated kinetic intermediates with photoproduct structures that are characterized by the CO residing in different internal protein cavities, so-called xenon holes. Here we have used Fourier transform infrared temperature derivative spectroscopy (FTIR-TDS) to further examine the role of internal cavities in the dynamics. Different cavities can be accessed by the CO ligands at different temperatures, and characteristic infrared absorption spectra have been obtained for the different locations of the CO ligand within the protein, enabling us to monitor ligand migration through the protein as well as conformational changes of the protein.
机译:肌红蛋白是一种小的球状血红素蛋白,可在血红素铁上可逆地结合诸如O2,CO和NO的气态配体,为研究蛋白质反应的结构和动力学方面提供了出色的模型系统。在时间和温度的较宽范围内进行的快速光解实验表明,由于蛋白质松弛和配体在蛋白质中的移动,导致具有多种动力学中间体的复杂配体结合反应。我们最近对碳单氧化肌红蛋白(MbCO)突变体L29W的研究使用时间分辨红外光谱结合X射线晶体学技术,将动力学中间体与光产物结构相关联,这些光产物结构的特征是CO驻留在不同的内部蛋白质腔中,所谓的氙气孔。在这里,我们已经使用傅里叶变换红外温度导数光谱(FTIR-TDS)进一步检查了内腔在动力学中的作用。 CO配体可在不同温度下进入不同的腔,并且已获得蛋白质中CO配体不同位置的特征红外吸收光谱,从而使我们能够监测配体在蛋白质中的迁移以及蛋白质的构象变化。

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