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精氨酸生物合成调节铜绿假单胞菌中绿脓菌素的产生和释放,是其适应氧化应激机制的一部分。

Arginine Biosynthesis Modulates Pyoverdine Production and Release in Pseudomonas putida as Part of the Mechanism of Adaptation to Oxidative Stress.

机构信息

Department of Environmental Protection, Estación Experimental del Zaidín, CSIC, Granada, Spain.

Department of Environmental Protection, Estación Experimental del Zaidín, CSIC, Granada, Spain

出版信息

J Bacteriol. 2019 Oct 21;201(22). doi: 10.1128/JB.00454-19. Print 2019 Nov 15.

Abstract

Iron is essential for most life forms. Under iron-limiting conditions, many bacteria produce and release siderophores-molecules with high affinity for iron-which are then transported into the cell in their iron-bound form, allowing incorporation of the metal into a wide range of cellular processes. However, free iron can also be a source of reactive oxygen species that cause DNA, protein, and lipid damage. Not surprisingly, iron capture is finely regulated and linked to oxidative-stress responses. Here, we provide evidence indicating that in the plant-beneficial bacterium KT2440, the amino acid l-arginine is a metabolic connector between iron capture and oxidative stress. Mutants defective in arginine biosynthesis show reduced production and release of the siderophore pyoverdine and altered expression of certain pyoverdine-related genes, resulting in higher sensitivity to iron limitation. Although the amino acid is not part of the siderophore side chain, addition of exogenous l-arginine restores pyoverdine release in the mutants, and increased pyoverdine production is observed in the presence of polyamines (agmatine and spermidine), of which arginine is a precursor. Spermidine also has a protective role against hydrogen peroxide in , whereas defects in arginine and pyoverdine synthesis result in increased production of reactive oxygen species. The results of this study show a previously unidentified connection between arginine metabolism, siderophore turnover, and oxidative stress in Although the precise molecular mechanisms involved have yet to be characterized in full detail, our data are consistent with a model in which arginine biosynthesis and the derived pathway leading to polyamine production function as a homeostasis mechanism that helps maintain the balance between iron uptake and oxidative-stress response systems.

摘要

铁是大多数生命形式所必需的。在缺铁条件下,许多细菌会产生并释放铁载体——与铁具有高亲和力的分子——然后将其以铁结合的形式运入细胞内,从而将金属纳入广泛的细胞过程中。然而,游离铁也可能成为活性氧物质的来源,这些物质会导致 DNA、蛋白质和脂质损伤。毫不奇怪,铁的捕获受到精细调节,并与氧化应激反应相关联。在这里,我们提供的证据表明,在对植物有益的细菌 KT2440 中,氨基酸 l-精氨酸是铁捕获和氧化应激之间的代谢连接物。精氨酸生物合成缺陷的突变体显示出降低的铁载体绿脓菌素的产生和释放,以及某些绿脓菌素相关基因的表达改变,导致对铁限制的敏感性增加。尽管氨基酸不是铁载体侧链的一部分,但外源性 l-精氨酸的添加可在突变体中恢复绿脓菌素的释放,并且在多胺(胍丁胺和亚精胺)存在的情况下观察到绿脓菌素产量增加,其中精氨酸是前体。亚精胺在 中也具有对抗过氧化氢的保护作用,而精氨酸和绿脓菌素合成的缺陷导致活性氧物质的产生增加。这项研究的结果表明,在 中,精氨酸代谢、铁载体周转和氧化应激之间存在以前未被识别的联系。尽管涉及的确切分子机制尚未被充分描述,但我们的数据与这样一种模型一致,即精氨酸生物合成和导致多胺产生的途径作为一种动态平衡机制,有助于维持铁摄取和氧化应激反应系统之间的平衡。

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