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Mixing and matching genes of marine and terrestrial origin in the biosynthesis of the mupirocin antibiotics

机译:海洋和陆地血管生物合成中的混合和匹配基因综合征抗生素生物合成

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With growing understanding of the underlying pathways of polyketide biosynthesis, along with the continual expansion of the synthetic biology toolkit, it is becoming possible to rationally engineer and fine-tune the polyketide biosynthetic machinery for production of new compounds with improved properties such as stability and/or bioactivity. However, engineering the pathway to the thiomarinol antibiotics has proved challenging. Here we report that genes from a marine Pseudoalternomonas sp. producing thiomarinol can be expressed in functional form in the biosynthesis of the clinically important antibiotic mupirocin from the soil bacterium Pseudomonas fluorescens. It is revealed that both pathways employ the same unusual mechanism of tetrahydropyran (THP) ring formation and the enzymes are cross compatible. Furthermore, the efficiency of downstream processing of 10,11-epoxy versus 10,11-alkenic metabolites are comparable. Optimisation of the fermentation conditions in an engineered strain in which production of pseudomonic acid A (with the 10,11-epoxide) is replaced by substantial titres of the more stable pseudomonic acid C (with a 10,11-alkene) pave the way for its development as a more stable antibiotic with wider applications than mupirocin.
机译:随着对聚酮化合物生物合成的潜在途径不断增长的了解,随着合成生物学工具包的持续扩展,它正在成为可能的工程师和微调聚酮化合物生物合成机械,以生产具有改进的性质,例如稳定性和/的新化合物或生物活性。然而,工程对硫代氨基酚抗生素的途径已经证明了具有挑战性。在这里,我们将该基因从海洋伪本地核苷酸SP报告。生产硫甲醇可以以临床上重要的抗生素Mupirocin的生物合成中的功能形式表达来自土壤菌荧光荧光素的生物合成。据透露,两种途径采用与四氢吡喃(THP)环形成的相同异常机制,并且酶联符合交叉。此外,10,11-环氧树脂的下游加工效率与10,11-烯基代谢物相当。优化在工程菌株中的发酵条件,其中伪肿瘤α(用10,11-环氧化)的生产被更稳定的假蛋白酸C(用10,11-烯烃)铺平道路而替代它的发展是一种更稳定的抗生素,而不是Mupircin的更广泛的应用。

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    《Chemical science》 |2020年第20期|共6页
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  • 正文语种 eng
  • 中图分类 化学;
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