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Diffractive optics-based heterodyne-detected four-wave mixing signals of protein motion: From “protein quakes” to ligand escape for myoglobin

机译:基于衍射光学的外差检测四波混频 蛋白质运动的信号:从“蛋白质震动”到配体 逃脱肌红蛋白

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摘要

Ligand transport through myoglobin (Mb) has been observed by using optically heterodyne-detected transient grating spectroscopy. Experimental implementation using diffractive optics has provided unprecedented sensitivity for the study of protein motions by enabling the passive phase locking of the four beams that constitute the experiment, and an unambiguous separation of the Real and Imaginary parts of the signal. Ligand photodissociation of carboxymyoglobin (MbCO) induces a sequence of events involving the relaxation of the protein structure to accommodate ligand escape. These motions show up in the Real part of the signal. The ligand (CO) transport process involves an initial, small amplitude, change in volume, reflecting the transit time of the ligand through the protein, followed by a significantly larger volume change with ligand escape to the surrounding water. The latter process is well described by a single exponential process of 725 ± 15 ns at room temperature. The overall dynamics provide a distinctive signature that can be understood in the context of segmental protein fluctuations that aid ligand escape via a few specific cavities, and they suggest the existence of discrete escape pathways.
机译:配体通过肌红蛋白(Mb)的运输已通过使用光学外差检测的瞬态光栅光谱进行了观察。使用衍射光学器件的实验实现通过使构成实验的四个光束实现被动锁相,并明确分离了信号的实部和虚部,为蛋白质运动的研究提供了前所未有的灵敏度。羧基肌红蛋白(MbCO)的配体光解离引发一系列事件,这些事件涉及蛋白质结构的松弛以适应配体逃逸。这些运动显示在信号的实部。配体(CO)的运输过程涉及初始的小幅度变化,其体积变化反映了配体通过蛋白质的时间,随后随着配体逃逸到周围的水中而发生了明显更大的体积变化。后一种过程在室温下通过725±15 ns的单指数过程得到了很好的描述。整体动力学提供了独特的特征,可以在节段蛋白波动的背景下理解该特征,该波动有助于配体通过一些特定的腔逃逸,并且它们表明存在离散的逃逸途径。

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