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NfuA,一种在氧化应激和铁饥饿条件下大肠杆菌中成熟铁硫蛋白所需的新因子。

NfuA, a new factor required for maturing Fe/S proteins in Escherichia coli under oxidative stress and iron starvation conditions.

作者信息

Angelini Sandra, Gerez Catherine, Ollagnier-de Choudens Sandrine, Sanakis Yiannis, Fontecave Marc, Barras Frédéric, Py Béatrice

机构信息

Laboratoire de Chimie Bactérienne, CNRS, UPR 9043, Marseille Cedex, France.

出版信息

J Biol Chem. 2008 May 16;283(20):14084-91. doi: 10.1074/jbc.M709405200. Epub 2008 Mar 13.

DOI:10.1074/jbc.M709405200
PMID:18339628
Abstract

Iron/sulfur (Fe/S) proteins are central to the functioning of cells in both prokaryotes and eukaryotes. Here, we show that the yhgI gene, which we renamed nfuA, encodes a two-domain protein that is required for Fe/S biogenesis in Escherichia coli. The N-terminal domain resembles the so-called Fe/S A-type scaffold but, curiously, has lost the functionally important Cys residues. The C-terminal domain shares sequence identity with Nfu proteins. Mössbauer and UV-visible spectroscopic analyses revealed that, upon reconstitution, NfuA binds a [4Fe-4S] cluster. Moreover, NfuA can transfer this cluster to apo-aconitase. Mutagenesis studies indicated that the N- and C-terminal domains are important for NfuA function in vivo. Similarly, the functional importance of Cys residues present in the Nfu-like domain was demonstrated in vivo by introducing Cys-->Ser mutations. In vivo investigations revealed that the nfuA gene is important for E. coli to sustain oxidative stress and iron starvation. Also, combining nfuA with either isc or suf mutations led to additive phenotypic deficiencies, indicating that NfuA is a bona fide new player in Isc- and Suf-dependent Fe/S biogenesis pathways. Taken together, these data demonstrate that NfuA intervenes in the maturation of apoproteins in E. coli, allowing them to acquire Fe/S clusters. By taking into account results from numerous previous transcriptomic studies that had suggested a link between NfuA and protein misfolding, we discuss the possibility that NfuA could act as a scaffold/chaperone for damaged Fe/S proteins.

摘要

铁硫(Fe/S)蛋白对于原核生物和真核生物细胞的功能发挥都至关重要。在此,我们表明我们重新命名为nfuA的yhgI基因编码一种双结构域蛋白,它是大肠杆菌中Fe/S生物合成所必需的。N端结构域类似于所谓的Fe/S A型支架,但奇怪的是,它已经失去了功能上重要的半胱氨酸残基。C端结构域与Nfu蛋白具有序列同一性。穆斯堡尔光谱和紫外可见光谱分析表明,重组后,NfuA结合一个[4Fe-4S]簇。此外,NfuA可以将这个簇转移到脱辅基乌头酸酶上。诱变研究表明,N端和C端结构域对于NfuA在体内的功能很重要。同样,通过引入半胱氨酸到丝氨酸的突变,在体内证明了Nfu样结构域中存在的半胱氨酸残基的功能重要性。体内研究表明,nfuA基因对于大肠杆菌承受氧化应激和铁饥饿很重要。此外,将nfuA与isc或suf突变结合会导致累加的表型缺陷,表明NfuA是Isc和Suf依赖性Fe/S生物合成途径中一个真正的新成员。综上所述,这些数据表明NfuA参与大肠杆菌中脱辅基蛋白的成熟,使其能够获得Fe/S簇。考虑到之前众多转录组学研究的结果表明NfuA与蛋白质错误折叠之间存在联系,我们讨论了NfuA可能作为受损Fe/S蛋白的支架/伴侣蛋白的可能性。

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