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Targeting the Osmotic Stress Response for Strain Improvement of an Industrial Producer of Secondary Metabolites

机译:针对渗透应激反应,以改善次生代谢产物工业生产者的菌株

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摘要

The transition from primary to secondary metabolism in antibiotic-producing Streptomyces correlates with expression of genes involved in stress responses. Consequently, regulatory pathways that regulate specific stress responses are potential targets to manipulate to increase antibiotic titers. In this study, genes encoding key proteins involved in regulation of the osmotic stress response in Streptomyces avermitilis, the industrial producer of avermectins, are investigated as targets. Disruption of either osaB(Sa), encoding a response regulator protein, or osaC(Sa), encoding a multidomain regulator of the alternative sigma factor SigB, led to increased production of both oligomycin, by up to 200%, and avermectin, by up to 37%. The mutations also conditionally affected morphological development; under osmotic stress, the mutants were unable to erect an aerial mycelium. In addition, we demonstrate the delivery of DNA into a streptomycete using biolistics. The data reveal that information on stress regulatory responses can be integrated in rational strain improvement to improve yields of bioactive secondary metabolites.
机译:产生抗生素的链霉菌从初级代谢到次级代谢的转变与参与应激反应的基因的表达有关。因此,调节特定应激反应的调节途径是操纵以增加抗生素效价的潜在目标。在本研究中,以编码参与阿维链霉菌素的工业生产者阿维链霉菌的渗透应激反应调控的关键蛋白的基因为目标。编码应答调节蛋白的osaB(Sa)或编码替代sigma因子SigB的多域调节剂的osaC(Sa)的破坏导致寡聚霉素和阿维菌素的产量增加多达200%至37%。突变也有条件地影响形态发育。在渗透胁迫下,突变体无法建立气生菌丝体。此外,我们证明了使用生物弹药将DNA输送到链霉菌中。数据表明,有关压力调节反应的信息可以整合到合理的菌株改良中,以提高生物活性次生代谢产物的产量。

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