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Molecular variation of the nonribosomal peptide-polyketide siderophore yersiniabactin through biosynthetic and metabolic engineering

机译:通过生物合成和代谢工程改造非核糖体肽-聚酮化合物铁载体耶尔西菌素的分子变异

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The production of the mixed nonribosomal peptide-polyketide natural product yersiniabactin (Ybt) has been established using E. coli as a heterologous host. In this study, precursor-directed biosynthesis was used to generate five new analogs of Ybt, demonstrating the flexibility of the heterologous system and the biosynthetic process in allowing compound diversity. A combination of biosynthetic and cellular engineering was then used to influence the production metrics of the resulting analogs. First, the cellular levels and activity of FadL, a hydrocarbon transport protein, were tested for subsequent influence upon exogenous precursor uptake and Ybt analog production with a positive correlation observed between FadL over-production and analog formation. Next, a Ybt biosynthetic editing enzyme was removed from the heterologous system which decreased native compound production but increased analog formation. A final series of experiments enhanced endogenous anthranilate towards complete pathway formation of the associated analog which showed a selective ability to bind gold. Biotechnol. Bioeng. 2016;113: 1067-1074. (c) 2015 Wiley Periodicals, Inc.
机译:已经使用大肠杆菌作为异源宿主建立了混合的非核糖体肽-聚酮天然产物耶尔西菌素(Yersiniabactin)(Ybt)的生产。在这项研究中,前体定向的生物合成被用来生成五个新的Ybt类似物,证明了异源系统的灵活性和生物合成过程在允许化合物多样性方面的优势。然后使用生物合成和细胞工程学的组合来影响所得类似物的生产指标。首先,测试了FadL(一种烃转运蛋白)的细胞水平和活性,以确定其对外源前体摄取和Ybt类似物产生的后续影响,并观察到FadL过量产生与类似物形成之间存在正相关。接下来,从异源系统中除去Ybt生物合成编辑酶,这减少了天然化合物的产生但增加了类似物的形成。最后一系列实验增强了内源邻氨基苯甲酸朝向相关类似物的完整途径形成,这显示出结合金的选择性能力。生物技术。生恩2016; 113:1067-1074。 (c)2015年威利期刊有限公司

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