Streptomyces secondary metabolism is strongly affected by oxygen availability. The increased culture aeration enhances pimaricin production in S. natalensis, however the excess of O 2 consumption can lead to an intracellular ROS imbalance that is harmful to the cell. The adaptive physiological response of S. natalensis upon the addition of exogenous H 2O 2 suggested that the modulation of the intracellular ROS levels, through the activation of the H 2O 2 inducible catalase during the late exponential growth phase, can alter the production of pimaricin. With the construction of defective mutants on the H 2O 2 related enzymes SodF, AhpCD and KatA1, an effective and enduring modulation of intracellular ROS was achieved. Characterization of the knock-out strains revealed different behaviours regarding pimaricin production: whilst the superoxide dismutase defective mutant presented low levels of pimaricin production compared to the wild-type, the mutants defective on the H 2O 2-detoxifying enzymes displayed a pimaricin overproducer phenotype. Using physiological and molecular approaches we report a crosstalk between oxidative stress and secondary metabolism regulatory networks. Our results reveal that the redox-based regulation network triggered by an imbalance of the intracellular ROS homeostasis is also able to modulate the biosynthesis of pimaricin in S. natalensis. © 2011 Beites, et al.
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Beites, T., PiresSí, S. D. S., Santos, C. L., Osório, H., Moradas-Ferreira, P., & Mendes, M. V. (2011). Crosstalk between ROS homeostasis and secondary metabolism in s. natalensis atcc 27448: Modulation of pimaricin production by intracellular ros. PLoS ONE, 6(11). https://doi.org/10.1371/journal.pone.0027472