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时间分辨面积归一化发射光谱揭示吲哚化合物的荧光衰减特性。

Fluorescence decay characteristics of indole compounds revealed by time-resolved area-normalized emission spectroscopy.

作者信息

Otosu Takuhiro, Nishimoto Etsuko, Yamashita Shoji

机构信息

Institute of Biophysics, Faculty of Agriculture, Graduate School of Kyushu University, Hakozaki, Fukuoka 812-8581, Japan.

出版信息

J Phys Chem A. 2009 Mar 26;113(12):2847-53. doi: 10.1021/jp8078937.

Abstract

Time-resolved fluorescence spectroscopy of tryptophan residue has been extensively applied to the studies on structure-function relationships of protein. Regardless of this, the fluorescence decay mechanism and kinetics of tryptophan residue in many proteins still remains unclear. Previous studies have demonstrated that conformational heterogeneity and relaxation dynamics are both involved in the peculiar multiexponential decay kinetics in subnanosecond resolution. In the present study, we characterized the fluorescence decay property of six indole compounds in glycerol by resolving the contribution of conformational heterogeneity and relaxation dynamics. We applied the time-resolved area-normalized fluorescence emission spectrum (TRANES) method for the fluorescence decay analysis. The results of TRANES, time-dependent shift of fluorescence spectral center of gravity, and fluorescence decay simulation demonstrated that the dielectric relaxation process independent of intrinsic rotamer/conformer and the individual fluorescence lifetime gives the peculiarity to the fluorescence decay of indole compounds. These results confirmed that TRANES and time-dependent spectral shift analysis are potent methods to resolve the origin of multiexponential decay kinetics of tryptophyl fluorescence in protein.

摘要

色氨酸残基的时间分辨荧光光谱已被广泛应用于蛋白质结构-功能关系的研究。尽管如此,许多蛋白质中色氨酸残基的荧光衰减机制和动力学仍不清楚。先前的研究表明,构象异质性和弛豫动力学都与亚纳秒分辨率下独特的多指数衰减动力学有关。在本研究中,我们通过解析构象异质性和弛豫动力学的贡献,表征了六种吲哚化合物在甘油中的荧光衰减特性。我们应用时间分辨面积归一化荧光发射光谱(TRANES)方法进行荧光衰减分析。TRANES的结果、荧光光谱重心的时间依赖性位移以及荧光衰减模拟表明,与内在旋转异构体/构象异构体和单个荧光寿命无关的介电弛豫过程赋予了吲哚化合物荧光衰减的特殊性。这些结果证实,TRANES和时间依赖性光谱位移分析是解析蛋白质中色氨酸荧光多指数衰减动力学起源的有效方法。

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