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细菌中铁调节基因的信号转导及转录和转录后调控

Signal transduction and transcriptional and posttranscriptional control of iron-regulated genes in bacteria.

作者信息

Crosa J H

机构信息

Department of Molecular Microbiology and Immunology, Oregon Health Sciences University, Portland 97201, USA.

出版信息

Microbiol Mol Biol Rev. 1997 Sep;61(3):319-36. doi: 10.1128/mmbr.61.3.319-336.1997.

Abstract

Iron is an essential element for nearly all living cells. Thus, the ability of bacteria to utilize iron is a crucial survival mechanism independent of the ecological niche in which the microorganism lives, because iron is scarce both in potential biological hosts, where it is bound by high-affinity iron-binding proteins, and in the environment, where it is present as part of insoluble complex hydroxides. Therefore, pathogens attempting to establish an infection and environmental microorganisms must all be able to utilize the otherwise unavailable iron. One of the strategies to perform this task is the possession of siderophore-mediated iron uptake systems that are capable of scavenging the hoarded iron. This metal is, however, a double-edged sword for the cell because it can catalyze the production of deadly free hydroxyl radicals, which are harmful to the cells. It is therefore imperative for the cell to control the concentration of iron at levels that permit key metabolic steps to occur without becoming a messenger of cell death. Early work identified a repressor, Fur, which as a complex with iron repressed the expression of most iron uptake systems as well as other iron-regulated genes when the iron concentration reached a certain level. However, later work demonstrated that this regulation by Fur was not the only answer under low-iron conditions, there was a need for activation of iron uptake genes as well as siderophore biosynthetic genes. Furthermore, it was also realized that in some instances the actual ferric iron-siderophore complex induced the transcription of the cognate receptor and transport genes. It became evident that control of the expression of iron-regulated genes was more complex than originally envisioned. In this review, I analyze the processes of signal transduction, transcriptional control, and posttranscriptional control of iron-regulated genes as reported for the ferric dicitrate system in Escherichia coli; the pyochelin, pyoverdin, and enterobactin systems in Pseudomonas species; the irgB system in Vibrio cholerae; and the plasmid-mediated anguibactin system in Vibrio anguillarum. I hope that by using these diverse paradigms, I will be able to convey a unifying picture of these mechanism and their importance in the maintenance and prosperity of bacteria within their ecological niches.

摘要

铁是几乎所有活细胞所必需的元素。因此,细菌利用铁的能力是一种至关重要的生存机制,与微生物所处的生态位无关,因为铁在潜在生物宿主中稀缺,在生物宿主中它与高亲和力的铁结合蛋白结合,而在环境中,铁以不溶性复合氢氧化物的形式存在。所以,试图建立感染的病原体和环境微生物都必须能够利用原本无法获取的铁。完成这项任务的策略之一是拥有铁载体介导的铁摄取系统,该系统能够清除储存的铁。然而,这种金属对细胞来说是一把双刃剑,因为它能催化产生致命的游离羟基自由基,对细胞有害。因此,细胞必须将铁的浓度控制在允许关键代谢步骤发生的水平,而不会成为细胞死亡的信使。早期研究发现了一种阻遏物Fur,当铁浓度达到一定水平时,它与铁形成复合物,抑制大多数铁摄取系统以及其他铁调节基因的表达。然而,后来的研究表明,在低铁条件下,Fur的这种调节并非唯一的答案,还需要激活铁摄取基因以及铁载体生物合成基因。此外,人们还意识到,在某些情况下,实际的三价铁 - 铁载体复合物会诱导同源受体和转运基因的转录。很明显,铁调节基因表达的控制比最初设想的更为复杂。在这篇综述中,我分析了大肠杆菌中柠檬酸铁系统、假单胞菌属中的绿脓菌素、绿脓杆菌素和肠杆菌素系统、霍乱弧菌中的irgB系统以及鳗弧菌中质粒介导的鳗弧菌素系统所报道的铁调节基因的信号转导、转录控制和转录后控制过程。我希望通过使用这些不同的范例,能够传达这些机制的统一图景以及它们在细菌在其生态位中的维持和繁衍中的重要性。

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