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设计细菌细胞工厂以提高商业价值的非核糖体肽的产量。

Designer bacterial cell factories for improved production of commercially valuable non-ribosomal peptides.

机构信息

Department of Biotechnology, Indian Institute of Technology Kharagpur, Kharagpur 721302, West Bengal, India.

Department of Biotechnology, Indian Institute of Technology Kharagpur, Kharagpur 721302, West Bengal, India.

出版信息

Biotechnol Adv. 2022 Nov;60:108023. doi: 10.1016/j.biotechadv.2022.108023. Epub 2022 Jul 22.

Abstract

Non-ribosomal peptides have gained significant attention as secondary metabolites of high commercial importance. This group houses a diverse range of bioactive compounds, ranging from biosurfactants to antimicrobial and cytotoxic agents. However, low yield of synthesis by bacteria and excessive losses during purification hinders the industrial-scale production of non-ribosomal peptides, and subsequently limits their widespread applicability. While isolation of efficient producer strains and optimization of bioprocesses have been extensively used to enhance yield, further improvement can be made by optimization of the microbial strain using the tools and techniques of metabolic engineering, synthetic biology, systems biology, and adaptive laboratory evolution. These techniques, which directly target the genome of producer strains, aim to redirect carbon and nitrogen fluxes of the metabolic network towards the desired product, bypass the feedback inhibition and repression mechanisms that limit the maximum productivity of the strain, and even extend the substrate range of the cell for synthesis of the target product. The present review takes a comprehensive look into the biosynthesis of bacterial NRPs, how the same is regulated by the cell, and dives deep into the strategies that have been undertaken for enhancing the yield of NRPs, while also providing a perspective on other potential strategies that can allow for further yield improvement. Furthermore, this review provides the reader with a holistic perspective on the design of cellular factories of NRP production, starting from general techniques performed in the laboratory to the computational techniques that help a biochemical engineer model and subsequently strategize the architectural plan.

摘要

非核糖体肽作为具有高商业重要性的次生代谢物而备受关注。这一类包含了多种多样的生物活性化合物,从生物表面活性剂到抗菌和细胞毒性剂。然而,细菌合成产量低和纯化过程中损失过大,阻碍了非核糖体肽的工业规模生产,从而限制了它们的广泛应用。虽然已经广泛采用分离高效生产菌株和优化生物工艺来提高产量,但可以通过使用代谢工程、合成生物学、系统生物学和适应性实验室进化的工具和技术来优化微生物菌株,从而进一步改进。这些技术直接针对生产菌株的基因组,旨在将代谢网络中的碳和氮通量重新导向所需的产物,绕过限制菌株最大生产力的反馈抑制和抑制机制,甚至扩展细胞的底物范围以合成目标产物。本综述全面考察了细菌非核糖体肽的生物合成,以及细胞如何对其进行调控,并深入探讨了提高非核糖体肽产量所采用的策略,同时还提供了其他可能进一步提高产量的策略的展望。此外,本综述还为读者提供了关于非核糖体肽生产细胞工厂设计的整体视角,从实验室中进行的一般技术到帮助生化工程师对架构计划进行建模和策略制定的计算技术。

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