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黄素在2型异戊烯基二磷酸异构酶中作为无氧化还原功能的一般酸碱催化剂的新作用。

New role of flavin as a general acid-base catalyst with no redox function in type 2 isopentenyl-diphosphate isomerase.

作者信息

Unno Hideaki, Yamashita Satoshi, Ikeda Yosuke, Sekiguchi Shin-Ya, Yoshida Norie, Yoshimura Tohru, Kusunoki Masami, Nakayama Toru, Nishino Tokuzo, Hemmi Hisashi

机构信息

Department of Applied Chemistry, Faculty of Engineering, Nagasaki University, Bunkyo-machi, Nagasaki, Nagasaki 852-8521, Japan.

出版信息

J Biol Chem. 2009 Apr 3;284(14):9160-7. doi: 10.1074/jbc.M808438200. Epub 2009 Jan 21.

Abstract

Using FMN and a reducing agent such as NAD(P)H, type 2 isopentenyl-diphosphate isomerase catalyzes isomerization between isopentenyl diphosphate and dimethylallyl diphosphate, both of which are elemental units for the biosynthesis of highly diverse isoprenoid compounds. Although the flavin cofactor is expected to be integrally involved in catalysis, its exact role remains controversial. Here we report the crystal structures of the substrate-free and complex forms of type 2 isopentenyl-diphosphate isomerase from the thermoacidophilic archaeon Sulfolobus shibatae, not only in the oxidized state but also in the reduced state. Based on the active-site structures of the reduced FMN-substrate-enzyme ternary complexes, which are in the active state, and on the data from site-directed mutagenesis at highly conserved charged or polar amino acid residues around the active site, we demonstrate that only reduced FMN, not amino acid residues, can catalyze proton addition/elimination required for the isomerase reaction. This discovery is the first evidence for this long suspected, but previously unobserved, role of flavins just as a general acid-base catalyst without playing any redox roles, and thereby expands the known functions of these versatile coenzymes.

摘要

利用黄素单核苷酸(FMN)和一种还原剂(如NAD(P)H),2型异戊烯基二磷酸异构酶催化异戊烯基二磷酸和二甲基烯丙基二磷酸之间的异构化反应,这两种物质都是高度多样化的类异戊二烯化合物生物合成的基本单元。尽管黄素辅因子预计会整体参与催化过程,但其确切作用仍存在争议。在此,我们报道了嗜热嗜酸古菌柴田硫化叶菌(Sulfolobus shibatae)中2型异戊烯基二磷酸异构酶的无底物形式和复合物形式的晶体结构,不仅包括氧化态,还包括还原态。基于处于活性状态的还原型FMN-底物-酶三元复合物的活性位点结构,以及活性位点周围高度保守的带电荷或极性氨基酸残基的定点突变数据,我们证明只有还原型FMN而非氨基酸残基能够催化异构酶反应所需的质子添加/消除。这一发现首次证实了黄素长期以来被怀疑但此前未被观察到的作用,即仅作为一般酸碱催化剂而不发挥任何氧化还原作用,从而扩展了这些多功能辅酶的已知功能。

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