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链霉菌属白变种和链霉菌属紫色变种在转化含有卡特利链霉菌噻霉素基因簇的质体后,次生代谢产物的激活和沉默。

Activation and silencing of secondary metabolites in Streptomyces albus and Streptomyces lividans after transformation with cosmids containing the thienamycin gene cluster from Streptomyces cattleya.

机构信息

Departamento de Biología Funcional e Instituto Universitario de Oncología del Principado de Asturias, Universidad de Oviedo, 33006, Oviedo, Spain.

出版信息

Arch Microbiol. 2014 May;196(5):345-55. doi: 10.1007/s00203-014-0977-z. Epub 2014 Mar 15.

DOI:10.1007/s00203-014-0977-z
PMID:24633227
Abstract

Activation and silencing of antibiotic production was achieved in Streptomyces albus J1074 and Streptomyces lividans TK21 after introduction of genes within the thienamycin cluster from S. cattleya. Dramatic phenotypic and metabolic changes, involving activation of multiple silent secondary metabolites and silencing of others normally produced, were found in recombinant strains harbouring the thienamycin cluster in comparison to the parental strains. In S. albus, ultra-performance liquid chromatography purification and NMR structural elucidation revealed the identity of four structurally related activated compounds: the antibiotics paulomycins A, B and the paulomenols A and B. Four volatile compounds whose biosynthesis was switched off were identified by gas chromatography-mass spectrometry analyses and databases comparison as pyrazines; including tetramethylpyrazine, a compound with important clinical applications to our knowledge never reported to be produced by Streptomyces. In addition, this work revealed the potential of S. albus to produce many others secondary metabolites normally obtained from plants, including compounds of medical relevance as dihydro-β-agarofuran and of interest in perfume industry as β-patchoulene, suggesting that it might be an alternative model for their industrial production. In S. lividans, actinorhodins production was strongly activated in the recombinant strains whereas undecylprodigiosins were significantly reduced. Activation of cryptic metabolites in Streptomyces species might represent an alternative approach for pharmaceutical drug discovery.

摘要

在引入卡特利链霉菌中的硫霉素簇基因后,白色链霉菌 J1074 和变铅青链霉菌 TK21 实现了抗生素产生的激活和沉默。与亲本菌株相比,携带硫霉素簇的重组菌株表现出明显的表型和代谢变化,涉及多个沉默的次级代谢物的激活和其他通常产生的代谢物的沉默。在白色链霉菌中,通过超高效液相色谱纯化和 NMR 结构解析,鉴定了四种结构相关的激活化合物:抗生素保拉霉素 A、B 和保拉门醇 A、B。通过气相色谱-质谱分析和数据库比较,鉴定了四种生物合成被关闭的挥发性化合物为吡嗪;包括四甲基吡嗪,据我们所知,这种化合物具有重要的临床应用,但从未报道过由链霉菌产生。此外,这项工作揭示了白色链霉菌产生许多其他次级代谢物的潜力,这些代谢物通常来自植物,包括具有医学相关性的二氢-β-agarofuran 和在香水行业具有重要意义的β-石竹烯,表明它可能是其工业生产的替代模型。在变铅青链霉菌中,重组菌株中的放线紫红素的产量被强烈激活,而十一烷吡咯并红菌素的产量则显著降低。链霉菌中隐匿代谢物的激活可能代表了药物发现的一种替代方法。

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