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首页> 外文期刊>Dalton transactions: An international journal of inorganic chemistry >Towards [NiFe]-hydrogenase biomimetic models that couple H2 binding with functionally relevant intramolecular electron transfers: A quantum chemical study
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Towards [NiFe]-hydrogenase biomimetic models that couple H2 binding with functionally relevant intramolecular electron transfers: A quantum chemical study

机译:迈向[NiFe]-氢化酶仿生模型,将H2结合与功能相关的分子内电子转移耦合:量子化学研究

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[FeFe]- and [NiFe]-hydrogenases are dihydrogen-evolving metalloenzymes that share striking structural and functional similarities, despite being phylogenetically unrelated. Most notably, they are able to combine substrate binding and redox functionalities, which has important bearings on their efficiency. Model complexes of [FeFe]-hydrogenases that are able to couple H_2 binding with a substrate-dependent intramolecular electron transfer promoting dihydrogen activation were recently shown to reproduce the complex redox chemistry of the all-iron enzyme. Notably, coupling of H_2 binding and intramolecular redox events was proposed to have a key role also in [NiFe]-hydrogenases, but this feature is not reproduced in currently available nickel-iron biomimetic compounds. In the present study, we exploit dedicated density functional theory approaches to show that H_2 binding and activation on a NiFe core can be favored by the installment of conveniently substituted isocyanoferrocenes, thanks to their ability to undergo intramolecular reduction upon substrate binding. Our results support the concept that a unified view on hydrogenase chemistry is a key element to direct future efforts in the modeling of microbial H_2 metabolism.
机译:[FeFe]-和[NiFe]-加氢酶是进化二氢的金属酶,尽管在系统发育上不相关,但它们具有惊人的结构和功能相似性。最值得注意的是,它们能够将底物粘合和氧化还原功能结合在一起,这对它们的效率具有重要的意义。最近显示,能够将H_2结合与依赖底物的分子内电子转移促进二氢活化的[FeFe]氢化酶模型复合物可重现全铁酶的复合物氧化还原化学。值得注意的是,H_2结合和分子内氧化还原事件的耦合也被认为在[NiFe]-氢化酶中也起着关键作用,但是这一特征在目前可用的镍铁仿生化合物中没有再现。在本研究中,我们利用专用的密度泛函理论方法表明,在NiFe核上的H_2结合和活化可通过安装方便取代的异氰基二茂铁而受到青睐,这是由于它们具有在与底物结合时进行分子内还原的能力。我们的结果支持这样一个概念,即对氢化酶化学的统一看法是指导未来微生物H_2代谢建模的关键因素。

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