Structural insight into the substrate- and dioxygen-binding manner in the catalytic cycle of Rieske nonheme iron oxygenase system, carbazole 1,9a-dioxygenase

被引:37
作者
Ashikawa, Yuji [1 ,5 ]
Fujimoto, Zui [2 ]
Usami, Yusuke [1 ]
Inoue, Kengo [3 ]
Noguchi, Haruko [1 ,4 ,6 ]
Yamane, Hisakazu [1 ]
Nojiri, Hideaki [1 ,4 ]
机构
[1] Univ Tokyo, Biotechnol Res Ctr, Bunkyo Ku, Tokyo 1138657, Japan
[2] Natl Inst Agrobiol Sci, Prot Res Unit, Tsukuba, Ibaraki 3058602, Japan
[3] Miyazaki Univ, Interdisciplinary Res Org, Kiyotake, Miyazaki 8891692, Japan
[4] Univ Tokyo, Profess Programme Agr Bioinformat, Bunkyo Ku, Tokyo 1138657, Japan
[5] Waseda Univ, Adm & Technol Management Ctr Sci & Engn, Technol Management Div, Educ & Res Support Sect,Shinjuku Ku, Tokyo 1698555, Japan
[6] Tokyo Univ Agr, Fac Appl Bio Sci, Dept Appl Biol & Chem, Setagaya Ku, Tokyo 1568502, Japan
关键词
RING-HYDROXYLATING DIOXYGENASE; ELECTRON-TRANSFER COMPLEX; FERROUS ACTIVE-SITE; CRYSTAL-STRUCTURE; NAPHTHALENE 1,2-DIOXYGENASE; PHTHALATE DIOXYGENASE; CIS-DIHYDROXYLATION; COMPONENT; FERREDOXIN; DEGRADATION;
D O I
10.1186/1472-6807-12-15
中图分类号
Q6 [生物物理学];
学科分类号
071011 ;
摘要
Background: Dihydroxylation of tandemly linked aromatic carbons in a cis-configuration, catalyzed by multicomponent oxygenase systems known as Rieske nonheme iron oxygenase systems (ROs), often constitute the initial step of aerobic degradation pathways for various aromatic compounds. Because such RO reactions inherently govern whether downstream degradation processes occur, novel oxygenation mechanisms involving oxygenase components of ROs (RO-Os) is of great interest. Despite substantial progress in structural and physicochemical analyses, no consensus exists on the chemical steps in the catalytic cycles of ROs. Thus, determining whether conformational changes at the active site of RO-O occur by substrate and/or oxygen binding is important. Carbazole 1,9a-dioxygenase (CARDO), a RO member consists of catalytic terminal oxygenase (CARDO-O), ferredoxin (CARDO-F), and ferredoxin reductase. We have succeeded in determining the crystal structures of oxidized CARDO-O, oxidized CARDO-F, and both oxidized and reduced forms of the CARDO-O: CARDO-F binary complex. Results: In the present study, we determined the crystal structures of the reduced carbazole (CAR)-bound, dioxygen-bound, and both CAR- and dioxygen-bound CARDO-O: CARDO-F binary complex structures at 1.95, 1.85, and 2.00 angstrom resolution. These structures revealed the conformational changes that occur in the catalytic cycle. Structural comparison between complex structures in each step of the catalytic mechanism provides several implications, such as the order of substrate and dioxygen bindings, the iron-dioxygen species likely being Fe(III)-(hydro)peroxo, and the creation of room for dioxygen binding and the promotion of dioxygen binding in desirable fashion by preceding substrate binding. Conclusions: The RO catalytic mechanism is proposed as follows: When the Rieske cluster is reduced, substrate binding induces several conformational changes (e.g., movements of the nonheme iron and the ligand residue) that create room for oxygen binding. Dioxygen bound in a side-on fashion onto nonheme iron is activated by reduction to the peroxo state [Fe(III)-(hydro)peroxo]. This state may react directly with the bound substrate, or O-O bond cleavage may occur to generate Fe(V)-oxo-hydroxo species prior to the reaction. After producing a cis-dihydrodiol, the product is released by reducing the nonheme iron. This proposed scheme describes the catalytic cycle of ROs and provides important information for a better understanding of the mechanism.
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页数:14
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