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链霉菌中 N-乙酰葡萄糖胺对铁载体产生的意外控制。

Unsuspected control of siderophore production by N-acetylglucosamine in streptomycetes.

机构信息

Centre for Protein Engineering, Université de Liège, Institut de chimie B6a, Liège B-4000, Belgium Walloon Centre for Industrial Biology, Université de Liège/Gembloux Agro-Bio Tech, Gembloux B-5030, Belgium Institute of Biotechnology of Léon, INBIOTEC, Parque Cientifico de Léon, Leon 24006, Spain Microbial Development, Leiden Institute of Chemistry, Leiden University, PO Box 9502, 2300RA Leiden, the Netherlands.

出版信息

Environ Microbiol Rep. 2012 Oct;4(5):512-21. doi: 10.1111/j.1758-2229.2012.00354.x. Epub 2012 May 18.

Abstract

Iron is one of the most abundant elements on earth but is found in poorly soluble forms hardly accessible to microorganisms. To subsist, they have developed iron-chelating molecules called siderophores that capture this element in the environment and the resulting complexes are internalized by specific uptake systems. While biosynthesis of siderophores in many bacteria is regulated by iron availability and oxidative stress, we describe here a new type of regulation of siderophore production. We show that in Streptomyces coelicolor, their production is also controlled by N-acetylglucosamine (GlcNAc) via the direct transcriptional repression of the iron utilization repressor dmdR1 by DasR, the GlcNAc utilization regulator. This regulatory nutrient-metal relationship is conserved among streptomycetes, which indicates that the link between GlcNAc utilization and iron uptake repression, however unsuspected, is the consequence of a successful evolutionary process. We describe here the molecular basis of a novel inhibitory mechanism of siderophore production that is independent of iron availability. We speculate that the regulatory connection between GlcNAc and siderophores might be associated with the competition for iron between streptomycetes and their fungal soil competitors, whose cell walls are built from the GlcNAc-containing polymer chitin. Alternatively, GlcNAc could emanate from streptomycetes' own peptidoglycan that goes through intense remodelling throughout their life cycle, thereby modulating the iron supply according to specific needs at different stages of their developmental programme.

摘要

铁是地球上最丰富的元素之一,但它以微生物难以利用的低溶解度形式存在。为了生存,它们开发了铁螯合分子,称为铁载体,这些分子可以在环境中捕获这种元素,然后通过特定的摄取系统将形成的复合物内化。虽然许多细菌中铁载体的生物合成受铁可用性和氧化应激的调节,但我们在这里描述了一种新的铁载体生产调控方式。我们表明,在变铅青链霉菌中,其生产也受 N-乙酰葡萄糖胺(GlcNAc)的控制,通过 GlcNAc 利用调节剂 DasR 直接转录抑制铁利用阻遏物 dmdR1。这种调节营养物质-金属关系在链霉菌中是保守的,这表明 GlcNAc 利用和铁摄取抑制之间的联系,尽管出乎意料,但却是成功进化过程的结果。我们在这里描述了一种新的、独立于铁可用性的抑制铁载体生产的抑制机制的分子基础。我们推测,GlcNAc 和铁载体之间的调控联系可能与链霉菌与其真菌土壤竞争者之间的铁竞争有关,其细胞壁由含有 GlcNAc 的聚合物几丁质组成。或者,GlcNAc 可能来自链霉菌自身的肽聚糖,在其生命周期中经历了强烈的重塑,从而根据其发育计划不同阶段的特定需求来调节铁供应。

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