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Identification and Analysis of the Biosynthetic Gene Cluster Encoding the Thiopeptide Antibiotic Cyclothiazomycin in Streptomyces hygroscopicus 10-22

机译:吸水链霉菌中编码硫肽抗生素胞嘧菌霉素的生物合成基因簇的鉴定和分析10-22

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Thiopeptide antibiotics are an important class of natural products resulting from posttranslational modifications of ribosomally synthesized peptides. Cyclothiazomycin is a typical thiopeptide antibiotic that has a unique bridged macrocyclic structure derived from an 18-amino-acid structural peptide. Here we reported cloning, sequencing, and heterologous expression of the cyclothiazomycin biosynthetic gene cluster from Streptomyces hygroscopicus 10-22. Remarkably, successful heterologous expression of a 22.7-kb gene cluster in Streptomyces lividans 1326 suggested that there is a minimum set of 15 open reading frames that includes all of the functional genes required for cyclothiazomycin production. Six genes of these genes, cltBCDEFG flanking the structural gene cltA , were predicted to encode the enzymes required for the main framework of cyclothiazomycin, and two enzymes encoded by a putative operon, cltMN , were hypothesized to participate in the tailoring step to generate the tertiary thioether, leading to the final cyclization of the bridged macrocyclic structure. This rigorous bioinformatics analysis based on heterologous expression of cyclothiazomycin resulted in an ideal biosynthetic model for us to understand the biosynthesis of thiopeptides.
机译:硫肽抗生素是核糖体合成肽的翻译后修饰产生的重要一类天然产物。环z霉素是一种典型的硫肽抗生素,具有独特的桥接大环结构,该结构衍生自18个氨基酸的结构肽。在这里,我们报道了来自吸水链霉菌10-22的环噻唑霉素生物合成基因簇的克隆,测序和异源表达。值得注意的是,在Lividans链霉菌1326中成功地异源表达了22.7-kb的基因簇,这表明至少有15个开放阅读框,其中包括生产环噻唑霉素所需的所有功能基因。这些基因的六个基因,即位于结构基因cltA两侧的cltBCDEFG,预计将编码环噻唑霉素主框架所需的酶,并假定由假定的操纵子cltMN编码的两种酶将参与剪裁步骤以生成第三级硫醚,导致桥连的大环结构的最终环化。基于环噻唑霉素异源表达的这种严格的生物信息学分析为我们理解硫肽的生物合成提供了理想的生物合成模型。

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