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激发波长依赖性光循环起始动力学解析嗜盐嗜盐红螺菌光活性黄色蛋白的异质性

Excitation-Wavelength-Dependent Photocycle Initiation Dynamics Resolve Heterogeneity in the Photoactive Yellow Protein from Halorhodospira halophila.

作者信息

Mix L Tyler, Carroll Elizabeth C, Morozov Dmitry, Pan Jie, Gordon Wendy Ryan, Philip Andrew, Fuzell Jack, Kumauchi Masato, van Stokkum Ivo, Groenhof Gerrit, Hoff Wouter D, Larsen Delmar S

机构信息

Department of Chemistry , University of California, Davis , One Shields Avenue , Davis , California 95616 , United States.

Department of Chemistry and NanoScience Center , University of Jyväskylä , P.O. Box 35, 40014 Jyväskylä , Finland.

出版信息

Biochemistry. 2018 Mar 20;57(11):1733-1747. doi: 10.1021/acs.biochem.7b01114. Epub 2018 Mar 6.

Abstract

Photoactive yellow proteins (PYPs) make up a diverse class of blue-light-absorbing bacterial photoreceptors. Electronic excitation of the p-coumaric acid chromophore covalently bound within PYP results in triphasic quenching kinetics; however, the molecular basis of this behavior remains unresolved. Here we explore this question by examining the excitation-wavelength dependence of the photodynamics of the PYP from Halorhodospira halophila via a combined experimental and computational approach. The fluorescence quantum yield, steady-state fluorescence emission maximum, and cryotrapping spectra are demonstrated to depend on excitation wavelength. We also compare the femtosecond photodynamics in PYP at two excitation wavelengths (435 and 475 nm) with a dual-excitation-wavelength-interleaved pump-probe technique. Multicompartment global analysis of these data demonstrates that the excited-state photochemistry of PYP depends subtly, but convincingly, on excitation wavelength with similar kinetics with distinctly different spectral features, including a shifted ground-state beach and altered stimulated emission oscillator strengths and peak positions. Three models involving multiple excited states, vibrationally enhanced barrier crossing, and inhomogeneity are proposed to interpret the observed excitation-wavelength dependence of the data. Conformational heterogeneity was identified as the most probable model, which was supported with molecular mechanics simulations that identified two levels of inhomogeneity involving the orientation of the R52 residue and different hydrogen bonding networks with the p-coumaric acid chromophore. Quantum calculations were used to confirm that these inhomogeneities track to altered spectral properties consistent with the experimental results.

摘要

光活性黄色蛋白(PYPs)构成了一类多样的吸收蓝光的细菌光感受器。共价结合在PYP内的对香豆酸发色团的电子激发导致三相猝灭动力学;然而,这种行为的分子基础仍未得到解决。在这里,我们通过结合实验和计算方法研究嗜盐嗜盐红螺菌PYP光动力学的激发波长依赖性来探讨这个问题。荧光量子产率、稳态荧光发射最大值和低温捕获光谱被证明取决于激发波长。我们还使用双激发波长交错泵浦探测技术比较了PYP在两个激发波长(435和475nm)下的飞秒光动力学。对这些数据的多隔室全局分析表明,PYP的激发态光化学微妙但令人信服地取决于激发波长,具有相似的动力学但光谱特征明显不同,包括基态海滩的移动以及受激发射振子强度和峰值位置的改变。提出了三种涉及多个激发态、振动增强的势垒穿越和不均匀性的模型来解释观察到的数据的激发波长依赖性。构象异质性被确定为最可能的模型,分子力学模拟支持了这一模型,该模拟确定了两种不均匀性水平,涉及R52残基的取向以及与对香豆酸发色团不同的氢键网络。量子计算用于确认这些不均匀性与实验结果一致地跟踪到改变的光谱特性。

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