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大肠杆菌中isc操纵子突变对关键厌氧金属酶生物合成和活性的差异影响。

Differential effects of isc operon mutations on the biosynthesis and activity of key anaerobic metalloenzymes in Escherichia coli.

作者信息

Jaroschinsky Monique, Pinske Constanze, Gary Sawers R

机构信息

Institute for Biology/Microbiology, Martin-Luther University Halle-Wittenberg, Kurt-Mothes-Str 3, 06120 Halle (Saale), Germany.

Present address: ICP Analytik GmbH & Co. KG, Brandenburger Platz 1, 24211 Preetz, Germany.

出版信息

Microbiology (Reading). 2017 Jun;163(6):878-890. doi: 10.1099/mic.0.000481. Epub 2017 Jun 26.

DOI:10.1099/mic.0.000481
PMID:28640740
Abstract

Escherichia coli has two machineries for the synthesis of FeS clusters, namely Isc (iron-sulfur cluster) and Suf (sulfur formation). The Isc machinery, encoded by the iscRSUA-hscBA-fdx-iscXoperon, plays a crucial role in the biogenesis of FeS clusters for the oxidoreductases of aerobic metabolism. Less is known, however, about the role of ISC in the maturation of key multi-subunit metalloenzymes of anaerobic metabolism. Here, we determined the contribution of each iscoperon gene product towards the functionality of the major anaerobic oxidoreductases in E. coli, including three [NiFe]-hydrogenases (Hyd), two respiratory formate dehydrogenases (FDH) and nitrate reductase (NAR). Mutants lacking the cysteine desulfurase, IscS, lacked activity of all six enzymes, as well as the activity of fumaratereductase, and this was due to deficiencies in enzyme biosynthesis, maturation or FeS cluster insertion into electron-transfer components. Notably, based on anaerobic growth characteristics and metabolite patterns, the activity of the radical-S-adenosylmethionine enzyme pyruvate formate-lyase activase was independent of IscS, suggesting that FeS biogenesis for this ancient enzyme has different requirements. Mutants lacking either the scaffold protein IscU, the ferredoxin Fdx or the chaperones HscA or HscB had similar enzyme phenotypes: five of the oxidoreductases were essentially inactive, with the exception being the Hyd-3 enzyme, which formed part of the H2-producing formate hydrogenlyase (FHL) complex. Neither the frataxin-homologue CyaY nor the IscX protein was essential for synthesis of the three Hyd enzymes. Thus, while IscS is essential for H2 production in E. coli, the other ISC components are non-essential.

摘要

大肠杆菌有两种合成铁硫簇的机制,即Isc(铁硫簇)和Suf(硫形成)。由iscRSUA-hscBA-fdx-iscX操纵子编码的Isc机制,在有氧代谢氧化还原酶的铁硫簇生物合成中起关键作用。然而,关于ISC在厌氧代谢关键多亚基金属酶成熟中的作用知之甚少。在这里,我们确定了每个isc操纵子基因产物对大肠杆菌中主要厌氧氧化还原酶功能的贡献,包括三种[NiFe] - 氢化酶(Hyd)、两种呼吸型甲酸脱氢酶(FDH)和硝酸还原酶(NAR)。缺乏半胱氨酸脱硫酶IscS的突变体,所有六种酶以及富马酸还原酶均缺乏活性,这是由于酶生物合成、成熟或铁硫簇插入电子传递成分存在缺陷。值得注意的是,基于厌氧生长特性和代谢物模式,自由基S-腺苷甲硫氨酸酶丙酮酸甲酸裂解酶激活酶的活性独立于IscS,这表明这种古老酶的铁硫生物合成有不同的要求。缺乏支架蛋白IscU、铁氧还蛋白Fdx或伴侣蛋白HscA或HscB的突变体具有相似的酶表型:除了形成产氢甲酸氢化酶(FHL)复合物一部分的Hyd-3酶外,五种氧化还原酶基本无活性。铁调素同源物CyaY和IscX蛋白对于三种Hyd酶的合成均不是必需的。因此,虽然IscS对大肠杆菌中产氢至关重要,但其他ISC成分并非必需。

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