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A step toward the prediction of the fluorescence lifetimes of tryptophan residues in proteins based on structural and spectral data.

机译:根据结构和光谱数据预测蛋白质中色氨酸残基的荧光寿命的步骤。

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摘要

A method is presented that allows the calculation of the lifetimes of tryptophan residues on the basis of spectral and structural data. It is applied to two different proteins. The calcium binding protein from the sarcoplasm of the muscles of the sand worm Nereis diversicolor (NSCP) changes its conformation upon binding of Ca2+ or Mg2+. NSCP contains three tryptophan residues at position 4, 57, and 170, respectively. The fluorescence lifetimes of W57 are investigated in a mutant in which W4 and W170 have been replaced. The time resolved fluorescence properties of W57 are linked to its different microconformations, which were determined by a molecular dynamics simulation map. Together with the determination of the radiative rate constant from the wavelength of maximum intensity of the decay associated spectra, it was possible to determine an exponential relation between the nonradiative rate constant and the distance between the indole CE3 atom and the carbonyl carbon of the peptide bond reflecting a mechanism of electron transfer as the main determinant of the value for the nonradiative rate constant. This result allows the calculation of the fluorescence lifetimes from the protein structure and the spectra. This method was further tested for the tryptophan of Ha-ras p21 (W32) and for W43 of the Tet repressor, which resulted in acceptable values for the predicted lifetimes.
机译:提出了一种允许基于光谱和结构数据计算色氨酸残基寿命的方法。它适用于两种不同的蛋白质。沙虫多样性神经(NSCP)肌肉的肌质中的钙结合蛋白在结合Ca2 +或Mg2 +后会改变其构象。 NSCP在位置4、57和170分别包含三个色氨酸残基。在其中W4和W170已被替换的突变体中研究W57的荧光寿命。 W57的时间分辨荧光特性与其不同的微构象有关,这是通过分子动力学模拟图确定的。与根据衰变相关光谱的最大强度的波长确定辐射速率常数一起,可以确定非辐射速率常数与吲哚CE3原子与肽键羰基碳之间的距离之间的指数关系。反映了电子转移的机制,它是非辐射速率常数值的主要决定因素。该结果允许从蛋白质结构和光谱计算荧光寿命。对该方法的Ha-ras p21色氨酸(W32)和Tet阻遏物的W43进行了进一步测试,得出了预期寿命的可接受值。

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