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Exploring modular reengineering strategies to redesign the teicoplanin non-ribosomal peptide synthetase

机译:探索模块化再造策略重新设计Teicoplanin非核糖体肽合成酶

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Non-ribosomal peptide synthesis is an important biosynthesis pathway in secondary metabolism. In this study we have investigated modularisation and redesign strategies for the glycopeptide antibiotic teicoplanin. Using the relocation or exchange of domains within the NRPS modules, we have identified how to initiate peptide biosynthesis and explored the requirements for the functional reengineering of both the condensation/adenylation domain and epimerisation/condensation domain interfaces. We have also demonstrated strategies that ensure communication between isolated NRPS modules, leading to new peptide assembly pathways. This provides important insights into NRPS reengineering of glycopeptide antibiotic biosynthesis and has broad implications for the redesign of other NRPS systems.
机译:非核糖体肽合成是次生代谢的重要生物合成途径。在这项研究中,我们研究了糖肽抗生素Teicoplanin的模块化和重新设计策略。使用NRPS模块内的域映射或交换,我们已经确定了如何启动肽生物合成并探索缩合/腺苷酸化结构域和凝聚域界面的功能再造的要求。我们还证明了确保孤立的NRPS模块之间的沟通的策略,导致新的肽组装途径。这提供了对糖肽抗生素生物合成的NRPS再造的重要见解,并且对其他NRPS系统的重新设计具有广泛的影响。

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