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The Dps protein of Escherichia coli is involved in copper homeostasis

机译:大肠杆菌的Dps蛋白与铜稳态有关

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The DNA-binding protein of starved cells (Dps) has two distinct cellular functions in Escherichia coli. The spherical Dps dodecamer can store iron and, predominantly in the stationary growth phase, high amounts of Dps protein protect the genome by binding non-specifically to DNA. In this study we investigated the role of Dps in copper homeostasis in growing cells of E. coli. Under reductive aerobic growth conditions that favor a redox shift from Cu(II) to Cu(I) or under anaerobiosis, cells deleted in dps were sensitive to tow copper ion concentrations. Deletion of the DNA-binding N-terminus of Dps did not abrogate protection against copper toxicity indicating protection against copper stress is not directly related to DNA binding of Dps. The Dps protein is not a copper-storage protein in vitro or in vivo. In contrast, cells lacking Dps exhibited increased cellular copper concentrations compared to their wild-type parent. Furthermore, overproduction of Dps during growth phase resulted in decreased intracellular copper content under copper stress.
机译:饥饿细胞(Dps)的DNA结合蛋白在大肠杆菌中具有两种不同的细胞功能。球形Dps十二聚体可以储存铁,并且主要在静止生长期,大量Dps蛋白通过与DNA非特异性结合来保护基因组。在这项研究中,我们研究了Dps在大肠杆菌生长细胞中铜稳态中的作用。在有利于从Cu(II)到Cu(I)的氧化还原转变的还原性需氧生长条件下或在厌氧状态下,dps中缺失的细胞对两个铜离子浓度敏感。 Dps DNA结合N末端的删除并没有取消对铜毒性的保护,这表明针对铜胁迫的保护与Dps的DNA结合没有直接关系。 Dps蛋白在体外或体内不是铜存储蛋白。相反,与野生型亲本相比,缺乏Dps的细胞表现出更高的细胞铜浓度。此外,在生长期期间Dps的过量生产导致铜胁迫下细胞内铜含量降低。

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