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美国卫生研究院文献>Chemical Science
>Oxidation triggers extensive conjugation and unusual stabilization of two di-heme dication diradical intermediates: role of bridging group for electronic communication
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Oxidation triggers extensive conjugation and unusual stabilization of two di-heme dication diradical intermediates: role of bridging group for electronic communication
MauG is a diheme enzyme that utilizes two covalently bound c-type hemes to catalyse the biosynthesis of the protein-derived cofactor tryptophan tryptophylquinone. The two hemes are physically separated by 14.5 Å and a hole-hopping mechanism is proposed in which a tryptophan residue located between the hemes undergoes reversible oxidation and reduction to increase the effective electronic coupling element and enhance the rate of reversible electron transfer between the hemes in bis-Fe(iv) MauG. The present work describes the structure and spectroscopic investigation of 2e-oxidations of the synthetic diheme analogs in which two heme centers are covalently connected through a conjugated ethylene bridge that leads to the stabilization of two unusual trans conformations (U and P′ forms) with different and distinct spectroscopic and geometric features. Unlike in MauG, where the two oxidizing equivalents are distributed within the diheme system giving rise to the bis-Fe(iv) redox state, the synthetic analog stabilizes two ferric hemes, each coupled with a porphyrin cation radical, a scenario resembling the binuclear dication diradical complex. Interestingly, charge resonance-transition phenomena are observed here both in 1e and 2e-oxidised species from the same system, which are also clearly distinguishable by their relative position and intensity. Detailed UV-vis-NIR, X-ray, Mössbauer, EPR and 1H NMR spectroscopic investigations as well as variable temperature magnetic studies have unraveled strong electronic communications between two porphyrin π-cation radicals through the bridging ethylene group. The extensive π-conjugation also allows antiferromagnetic coupling between iron(iii) centers and porphyrin radical spins of both rings. DFT calculations revealed extended π-conjugation and H-bonding interaction as the major factors in controlling the stability of the conformers.
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机译:MauG是一种双血红素酶,它利用两个共价结合的c型血红素来催化蛋白质衍生的辅因子色氨酸色氨酸醌的生物合成。两个血红素之间的物理距离为14.5Å,并提出了一种空穴跳跃机制,其中位于血红素之间的色氨酸残基经历可逆的氧化和还原,以增加有效的电子耦合元素并提高血红素之间可逆的电子转移速率。双-Fe(iv)MauG。本工作描述了合成的二血红素类似物的2e-氧化的结构和光谱学研究,其中两个血红素中心通过共轭乙烯桥共价连接,从而导致两个不同的不同反式构象(U和P'形式)稳定化。以及独特的光谱和几何特征。与MauG不同,在MauG中,两个氧化当量分布在双血红素系统中,从而产生双-Fe(iv)氧化还原态,合成的类似物稳定了两个铁血红素,每个血红素都带有卟啉阳离子自由基,这种情况类似于双核指示。双基复杂。有趣的是,在同一系统的1e和2e氧化物种中都观察到了电荷共振跃迁现象,它们的相对位置和强度也可以清楚地区分。详细的UV-vis-NIR,X射线,Mössbauer,EPR和 1 H NMR光谱研究以及可变温度磁研究已经揭示了通过桥联乙烯在两个卟啉π阳离子自由基之间的强电子通信组。广泛的π共轭还允许两个环的铁(iii)中心与卟啉自由基自旋之间发生反铁磁耦合。 DFT计算表明,扩展的π共轭和H键相互作用是控制构象异构体稳定性的主要因素。
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