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Tailing miniSOG: structural bases of the complex photophysics of a flavin-binding singlet oxygen photosensitizing protein

机译:尾矿miniSOG:黄素结合单线态氧光敏蛋白的复杂光物理的结构基础

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摘要

miniSOG is the first flavin-binding protein that has been developed with the specific aim of serving as a genetically-encodable light-induced source of singlet oxygen (1O2). We have determined its 1.17 Å resolution structure, which has allowed us to investigate its mechanism of photosensitization using an integrated approach combining spectroscopic and structural methods. Our results provide a structural framework to explain the ability of miniSOG to produce 1O2 as a competition between oxygen- and protein quenching of its triplet state. In addition, a third excited-state decay pathway has been identified that is pivotal for the performance of miniSOG as 1O2 photosensitizer, namely the photo-induced transformation of flavin mononucleotide (FMN) into lumichrome, which increases the accessibility of oxygen to the flavin FMN chromophore and makes protein quenching less favourable. The combination of the two effects explains the increase in the 1O2 quantum yield by one order of magnitude upon exposure to blue light. Besides, we have identified several surface electron-rich residues that are progressively photo-oxidized, further contributing to facilitate the production of 1O2. Our results help reconcile the apparent poor level of 1O2 generation by miniSOG and its excellent performance in correlative light and electron microscopy experiments.
机译:miniSOG是第一个黄素结合蛋白,其开发目的是用作可遗传编码的光诱导单线态氧( 1 O2)的来源。我们确定了它的1.17Å分辨率结构,这使我们能够使用结合光谱学和结构方法的集成方法来研究其光敏化机理。我们的结果提供了一个结构框架,以解释miniSOG产生 1 O2的能力,以此作为三态状态的氧和蛋白质淬灭之间的竞争。此外,已经确定了第三条激发态衰变途径,这对于miniSOG作为 1 O2光敏剂的性能至关重要,即黄素单核苷酸(FMN)的光诱导转化为发光色素,并增加氧与黄素FMN发色团的可及性,使蛋白质淬灭作用降低。两种效应的结合说明了 1 O2量子产率在暴露于蓝光后增加了一个数量级。此外,我们发现了几个表面富电子的残基,这些残基逐渐被光氧化,从而进一步促进了 1 O2的产生。我们的结果有助于调和miniSOG产生的 1 O2的明显水平低下及其在相关的光学和电子显微镜实验中的优异性能。

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