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本文引用的文献

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Kinetic and Binding Studies of Streptococcus pneumoniae Type 2 Isopentenyl Diphosphate:Dimethylallyl Diphosphate Isomerase.肺炎链球菌2型异戊烯基二磷酸:二甲基烯丙基二磷酸异构酶的动力学及结合研究
Biochemistry. 2016 Apr 19;55(15):2260-8. doi: 10.1021/acs.biochem.6b00087. Epub 2016 Apr 5.
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Determination of kinetics and the crystal structure of a novel type 2 isopentenyl diphosphate: dimethylallyl diphosphate isomerase from Streptococcus pneumoniae.肺炎链球菌新型2型异戊烯基二磷酸:二甲基烯丙基二磷酸异构酶的动力学及晶体结构测定
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Current development in isoprenoid precursor biosynthesis and regulation.异戊烯前体生物合成与调控的最新进展。
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Covalent modification of reduced flavin mononucleotide in type-2 isopentenyl diphosphate isomerase by active-site-directed inhibitors.通过活性位点定向抑制剂对 II 型异戊烯二磷酸异构酶中还原黄素单核苷酸的共价修饰。
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Stereochemical studies of the type II isopentenyl diphosphate-dimethylallyl diphosphate isomerase implicate the FMN coenzyme in substrate protonation.II型异戊烯基二磷酸-二甲基烯丙基二磷酸异构酶的立体化学研究表明,黄素单核苷酸辅酶参与底物的质子化过程。
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Enzymatic chemistry of cyclopropane, epoxide, and aziridine biosynthesis.环丙烷、环氧化物和氮丙啶生物合成的酶化学
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Biosynthesis via carbocations: theoretical studies on terpene formation.通过碳正离子的生物合成:萜类化合物形成的理论研究。
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Linear free energy relationships demonstrate a catalytic role for the flavin mononucleotide coenzyme of the type II isopentenyl diphosphate:dimethylallyl diphosphate isomerase.线性自由能关系表明黄素单核苷酸辅酶在 II 型异戊烯二磷酸:二甲基烯丙基二磷酸异构酶中具有催化作用。
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The lycopene cyclase CrtY from Pantoea ananatis (formerly Erwinia uredovora) catalyzes an FADred-dependent non-redox reaction.泛酸钙不动杆菌(原欧文氏菌)的番茄红素环化酶 CrtY 催化一个 FADred 依赖性的非氧化还原反应。
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Probing the role of active site residues in NikD, an unusual amino acid oxidase that catalyzes an aromatization reaction important in nikkomycin biosynthesis.探究活性位点残基在NikD中的作用,NikD是一种不同寻常的氨基酸氧化酶,催化对尼可霉素生物合成至关重要的芳构化反应。
Biochemistry. 2009 Jul 28;48(29):6951-62. doi: 10.1021/bi9006918.

II型异戊烯基二磷酸:二甲基烯丙基二磷酸异构酶(IDI-2):黄素酶催化中酸碱化学的一个模型。

The type II isopentenyl Diphosphate:Dimethylallyl diphosphate isomerase (IDI-2): A model for acid/base chemistry in flavoenzyme catalysis.

作者信息

Thibodeaux Christopher J, Liu Hung-Wen

机构信息

Department of Chemistry, McGill University, 801Sherbrooke St. West, Montreal, QC, H3A 0B8, Canada.

Department of Medicinal Chemistry, College of Pharmacy, University of Texas, 2409 University Ave, A1915, Austin, TX, 78712-1028, United States.

出版信息

Arch Biochem Biophys. 2017 Oct 15;632:47-58. doi: 10.1016/j.abb.2017.05.017. Epub 2017 May 31.

DOI:10.1016/j.abb.2017.05.017
PMID:28577910
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5650523/
Abstract

The chemical versatility of the flavin coenzyme is nearly unparalleled in enzyme catalysis. An interesting illustration of this versatility can be found in the reaction catalyzed by the type II isopentenyl diphosphate:dimethylallyl diphosphate isomerase (IDI-2) - an enzyme that interconverts the two essential isoprene units (isopentenyl pyrophosphate and dimethylallyl pyrophosphate) that are needed to initiate the biosynthesis of all isoprenoids. Over the past decade, a variety of biochemical, spectroscopic, structural and mechanistic studies of IDI-2 have provided mounting evidence that the flavin coenzyme of IDI-2 acts in a most unusual manner - as an acid/base catalyst to mediate a 1,3-proton addition/elimination reaction. While not entirely without precedent, IDI-2 is by far the most extensively studied flavoenzyme that employs flavin-mediated acid/base catalysis. Thus, IDI-2 serves as an important mechanistic model for understanding this often overlooked, but potentially widespread reactivity of flavin coenzymes. This review details the most pertinent studies that have contributed to the development of mechanistic proposals for this highly unusual flavoenzyme, and discusses future experiments that may be able to clarify remaining uncertainties in the chemical mechanism of IDI-2.

摘要

黄素辅酶在酶催化中的化学多功能性几乎是无与伦比的。这种多功能性的一个有趣例子可以在II型异戊烯基二磷酸:二甲基烯丙基二磷酸异构酶(IDI-2)催化的反应中找到,IDI-2是一种能使启动所有类异戊二烯生物合成所需的两种必需异戊二烯单元(异戊烯基焦磷酸和二甲基烯丙基焦磷酸)相互转化的酶。在过去十年中,对IDI-2进行的各种生物化学、光谱学、结构和机理研究提供了越来越多的证据,表明IDI-2的黄素辅酶以一种非常特殊的方式起作用——作为酸碱催化剂介导1,3-质子加成/消除反应。虽然并非完全没有先例,但IDI-2是迄今为止研究最广泛的利用黄素介导的酸碱催化的黄素酶。因此,IDI-2是理解这种常常被忽视但可能广泛存在的黄素辅酶反应性的重要机理模型。本综述详细介绍了有助于形成这种高度特殊的黄素酶机理假说的最相关研究,并讨论了未来可能能够阐明IDI-2化学机理中尚存不确定性的实验。