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Dps/Dpr铁蛋白样蛋白:深入了解猪链球菌中铁掺入机制及细胞铁稳态核心作用的证据

Dps/Dpr ferritin-like protein: insights into the mechanism of iron incorporation and evidence for a central role in cellular iron homeostasis in Streptococcus suis.

作者信息

Pulliainen Arto T, Kauko Anni, Haataja Sauli, Papageorgiou Anastassios C, Finne Jukka

机构信息

Department of Medical Biochemistry and Molecular Biology, University of Turku, Kiinamyllynkatu 10, FI-20520 Turku, Finland.

出版信息

Mol Microbiol. 2005 Aug;57(4):1086-100. doi: 10.1111/j.1365-2958.2005.04756.x.

Abstract

The Dps family members constitute a distinct group of multimeric and ferritin-like iron binding proteins (up to 500 iron atoms/12-mer) that are widespread in eubacteria and archaea and implicated in oxidative stress resistance and virulence. Despite the wealth of structural knowledge, the mechanism of iron incorporation has remained elusive. Here, we provide evidence on Dpr of the swine and human pathogen Streptococcus suis that: (i) iron incorporation proceeds by Fe(II) binding, Fe(II) oxidation and subsequent storage as Fe(III); (ii) Fe(II) atoms enter the 12-mer cavity through four hydrophilic pores; and (iii) Fe(II) atoms are oxidized inside the 12-mer cavity at 12 identical inter-subunit sites, which are structurally different but functionally equivalent to the ferroxidase centres of classical ferritins. We also provide evidence, by deleting and ectopically overexpressing Dpr, that Dpr affects cellular iron homeostasis. The key residues responsible for iron incorporation in S. suis Dpr are well conserved throughout the Dps family. A model for the iron incorporation mechanism of the Dps/Dpr ferritin-like protein is proposed.

摘要

Dps家族成员构成了一类独特的多聚体且类似铁蛋白的铁结合蛋白(每个12聚体最多结合500个铁原子),广泛存在于真细菌和古细菌中,并与氧化应激抗性及毒力相关。尽管已有丰富的结构知识,但铁掺入的机制仍不清楚。在此,我们提供了关于猪和人类病原体猪链球菌Dpr的证据,表明:(i)铁掺入通过Fe(II)结合、Fe(II)氧化以及随后以Fe(III)形式储存进行;(ii)Fe(II)原子通过四个亲水孔进入12聚体腔;(iii)Fe(II)原子在12聚体腔内的12个相同亚基间位点被氧化,这些位点在结构上不同,但在功能上等同于经典铁蛋白的铁氧化酶中心。我们还通过删除和异位过表达Dpr提供了证据,表明Dpr影响细胞铁稳态。猪链球菌Dpr中负责铁掺入的关键残基在整个Dps家族中高度保守。本文提出了Dps/Dpr类铁蛋白中铁掺入机制的模型。

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