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A new conceptual framework for enzyme catalysis: Hydrogen tunneling coupled to enzyme dynamics in flavoprotein and quinoprotein enzymes

机译:酶催化的新概念框架:氢隧道效应与黄素蛋白和醌蛋白酶的酶动力学相结合

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摘要

Recent years have witnessed high levels of activity in identifying enzyme systems that catalyse H-transfer by quantum tunneling. Rather than being restricted to a small number of specific enzymes as perceived initially, it has now become an accepted mechanism for H-transfer in a growing number of enzymes. Furthermore, H-tunneling is driven by the thermally induced dynamics of the enzyme. In some of those enzymes that break stable C-H bonds the reaction proceeds purely by quantum tunneling, without the need to partially ascend the barrier. Enzymes studied that fall into this category include the flavoprotein and quinoprotein amine dehydrogenases, which have proved to be excellent model systems. These enzymes have enabled us to study the relationship between barrier shape and reaction kinetics. This has involved studies with 'slow' and 'fast' substrates and enzymes impaired by mutagenesis. A number of key questions now remain, including the nature of the coupling between protein dynamics and quantum tunneling. The wide-ranging implications of quantum tunneling introduce a paradigm shift in the conceptual framework for enzyme catalysis, inhibition and design.
机译:近年来,在鉴定通过量子隧穿催化H转移的酶系统方面目睹了高水平的活性。如今,它已不再是局限在少数特定酶上的酶,而是已成为一种在越来越多的酶中进行H转移的公认机制。此外,H隧穿是由酶的热诱导动力学驱动的。在某些破坏稳定C-H键的酶中,反应完全是通过量子隧穿进行的,而无需部分提升屏障。属于这一类的研究酶包括黄素蛋白和喹蛋白胺脱氢酶,它们被证明是出色的模型系统。这些酶使我们能够研究屏障形状与反应动力学之间的关系。这涉及对“慢”和“快”底物以及被诱变损害的酶的研究。现在仍然存在许多关键问题,包括蛋白质动力学和量子隧穿之间耦合的性质。量子隧穿的广泛含义为酶催化,抑制和设计的概念框架引入了范式转变。

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