Arginine biosynthesis modulates pyoverdine production and release in pseudomonas putida as part of the mechanism of adaptation to oxidative stress

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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 Pseudomonas putida 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 P. putida, whereas defects in arginine and pyoverdine synthesis result in increased production of reactive oxygen species.

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Barrientos-Moreno, L., Molina-Henares, M. A., Pastor-García, M., Ramos-González, M. I., & Espinosa-Urgel, M. (2019). Arginine biosynthesis modulates pyoverdine production and release in pseudomonas putida as part of the mechanism of adaptation to oxidative stress. Journal of Bacteriology, 201(22). https://doi.org/10.1128/JB.00454-19

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