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A proton delivery pathway in the soluble fumarate reductase from Shewanella frigidimarina.来自嗜冷希瓦氏菌的可溶性延胡索酸还原酶中的质子传递途径。
J Biol Chem. 2006 Jul 21;281(29):20589-97. doi: 10.1074/jbc.M603077200. Epub 2006 May 12.
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3-nitropropionic acid is a suicide inhibitor of mitochondrial respiration that, upon oxidation by complex II, forms a covalent adduct with a catalytic base arginine in the active site of the enzyme.3-硝基丙酸是一种线粒体呼吸的自杀性抑制剂,在被复合物II氧化后,会与该酶活性位点上的催化性碱基精氨酸形成共价加合物。
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8
A third crystal form of Wolinella succinogenes quinol:fumarate reductase reveals domain closure at the site of fumarate reduction.琥珀酸沃林氏菌醌:延胡索酸还原酶的第三种晶体形式揭示了延胡索酸还原位点处的结构域闭合。
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10
Structure of fumarate reductase from Wolinella succinogenes at 2.2 A resolution.嗜琥珀酸沃林氏菌中延胡索酸还原酶在2.2埃分辨率下的结构
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配体与复合物II二羧酸位点结合的晶体学研究,以及“草酰乙酸抑制”状态下配体的身份。

Crystallographic studies of the binding of ligands to the dicarboxylate site of Complex II, and the identity of the ligand in the "oxaloacetate-inhibited" state.

作者信息

Huang Li-Shar, Shen John T, Wang Andy C, Berry Edward A

机构信息

Physical Biosciences Division, Lawrence Berkeley National Lab., MS 64-0121, 1 Cyclotron Road, Berkeley CA 94720, USA.

出版信息

Biochim Biophys Acta. 2006 Sep-Oct;1757(9-10):1073-83. doi: 10.1016/j.bbabio.2006.06.015. Epub 2006 Jul 12.

DOI:10.1016/j.bbabio.2006.06.015
PMID:16935256
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1586218/
Abstract

Mitochondrial Complex II (succinate:ubiquinone oxidoreductase) is purified in a partially inactivated state, which can be activated by removal of tightly bound oxaloacetate (E.B. Kearney, et al., Biochem. Biophys. Res. Commun. 49 1115-1121). We crystallized Complex II in the presence of oxaloacetate or with the endogenous inhibitor bound. The structure showed a ligand essentially identical to the "malate-like intermediate" found in Shewanella Flavocytochrome c crystallized with fumarate (P. Taylor, et al., Nat. Struct. Biol. 6 1108-1112) Crystallization of Complex II in the presence of excess fumarate also gave the malate-like intermediate or a mixture of that and fumarate at the active site. In order to more conveniently monitor the occupation state of the dicarboxylate site, we are developing a library of UV/Vis spectral effects induced by binding different ligands to the site. Treatment with fumarate results in rapid development of the fumarate difference spectrum and then a very slow conversion into a species spectrally similar to the OAA-liganded complex. Complex II is known to be capable of oxidizing malate to the enol form of oxaloacetate (Y.O. Belikova, et al., Biochim. Biophys. Acta 936 1-9). The observations above suggest it may also be capable of interconverting fumarate and malate. It may be useful for understanding the mechanism and regulation of the enzyme to identify the malate-like intermediate and its pathway of formation from oxaloacetate or fumarate.

摘要

线粒体复合物II(琥珀酸:泛醌氧化还原酶)是以部分失活状态纯化得到的,这种失活状态可通过去除紧密结合的草酰乙酸而被激活(E.B. 科尔尼等人,《生物化学与生物物理研究通讯》49 1115 - 1121)。我们在草酰乙酸存在的情况下或结合内源性抑制剂时使复合物II结晶。其结构显示出一种配体,该配体与在与富马酸结晶的希瓦氏菌黄素细胞色素c中发现的“苹果酸样中间体”基本相同(P. 泰勒等人,《自然结构生物学》6 1108 - 1112)。在过量富马酸存在的情况下使复合物II结晶,在活性位点也得到了苹果酸样中间体或其与富马酸的混合物。为了更方便地监测二羧酸位点的占据状态,我们正在开发一个由不同配体结合到该位点所诱导的紫外/可见光谱效应库。用富马酸处理会导致富马酸差异光谱迅速出现,然后非常缓慢地转化为一种光谱上类似于草酰乙酸配体复合物的物质。已知复合物II能够将苹果酸氧化为草酰乙酸的烯醇形式(Y.O. 贝利科娃等人,《生物化学与生物物理学报》936 1 - 9)。上述观察结果表明它可能也能够使富马酸和苹果酸相互转化。鉴定苹果酸样中间体及其从草酰乙酸或富马酸形成的途径,可能有助于理解该酶的作用机制和调控。