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工程改造天蓝色链霉菌以实现硫肽GE2270A的异源表达——一个警示故事

Engineering Streptomyces coelicolor for heterologous expression of the thiopeptide GE2270A-A cautionary tale.

作者信息

Del Carratore Francesco, Hanko Erik K R, Schmidt Kamila, Bilyk Oksana, Ye Huang Suhui, Iorio Marianna, Pérez-Bonilla Mercedes, Pérez-Redondo Rosario, Rudden Michelle, Severi Emmanuele, Tocchetti Arianna, Sosio Margherita, Johnson Emily J, Kirkwood Timothy, Whittall Dominic R, Manousaki Alkisti, Genilloud Olga, Rodríguez-García Antonio, Thomas Gavin H, Donadio Stefano, Breitling Rainer, Takano Eriko

机构信息

Department of Biochemistry, Cell, and Systems Biology, Institute of Integrative, Systems and Molecular Biology, University of Liverpool, Liverpool L69 3BX, UK.

Manchester Institute of Biotechnology, School of Chemistry, Faculty of Science and Engineering, University of Manchester, Manchester M1 7DN, UK.

出版信息

J Ind Microbiol Biotechnol. 2024 Dec 31;52. doi: 10.1093/jimb/kuaf019.

Abstract

The thiopeptide GE2270A is a clinically relevant, ribosomally synthesised, and post-translationally modified peptide naturally produced by Planobispora rosea. Due to the genetically intractable nature of P. rosea, heterologous expression is considered a possible route to yield improvement. In this study, we focused on improving GE2270A production through heterologous expression of the biosynthetic gene cluster (BGC) in the model organism Streptomyces coelicolor M1146. A statistically significant yield improvement was obtained in the S. coelicolor system through the data-driven rational engineering of the BGC, including the introduction of additional copies of key biosynthetic and regulatory genes. However, despite our best efforts, the highest production level observed in the strains generated in this study is 12× lower than published titres achieved in the natural producer and 50× lower than published titres obtained using Nonomuraea ATCC 39727 as expression host. These results suggest that, while using the most genetically amenable strain as host can be the right choice when exploring different BGC designs, the choice of the most suitable host has a major effect on the achievable yield and should be carefully considered. The analysis of the multiomics data obtained in this study suggests an important role of PbtX in GE2270A biosynthesis and provides insights into the differences in production metabolic profiles between the different strains. One Sentence Summary: Data-driven rational engineering of Streptomyces coelicolor for heterologous production of the thiopeptide antibiotic GE2270A resulted in increased production but encountered unexpected challenges compared to production in the natural producer or the alternative host Nonomuraea ATCC 39727.

摘要

硫肽GE2270A是一种与临床相关的、核糖体合成且经过翻译后修饰的肽,由玫瑰双孢放线菌天然产生。由于玫瑰双孢放线菌的遗传难以处理的特性,异源表达被认为是提高产量的一种可能途径。在本研究中,我们专注于通过在模式生物天蓝色链霉菌M1146中对生物合成基因簇(BGC)进行异源表达来提高GE2270A的产量。通过对BGC进行数据驱动的合理工程改造,包括引入关键生物合成和调控基因的额外拷贝,在天蓝色链霉菌系统中获得了具有统计学意义的产量提高。然而,尽管我们尽了最大努力,本研究中产生的菌株中观察到的最高产量水平比天然生产者中公布的滴度低12倍,比使用诺卡氏菌ATCC 39727作为表达宿主获得的公布滴度低50倍。这些结果表明,虽然在探索不同的BGC设计时,使用遗传上最易处理的菌株作为宿主可能是正确的选择,但最合适宿主的选择对可实现的产量有重大影响,应仔细考虑。对本研究中获得的多组学数据的分析表明PbtX在GE2270A生物合成中起重要作用,并提供了对不同菌株生产代谢谱差异的见解。一句话总结:对天蓝色链霉菌进行数据驱动的合理工程改造以异源生产硫肽抗生素GE2270A,产量有所增加,但与天然生产者或替代宿主诺卡氏菌ATCC 39727的生产相比,遇到了意想不到的挑战。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/14d6/12309360/0fa3a77eb683/kuaf019gra.jpg

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