在代谢网络模型 Halo-ecGEM 的指导下,删除了带有多种转座酶的长期生长稳定的 Halomonas sp.

IF 6.8 1区 生物学 Q1 BIOTECHNOLOGY & APPLIED MICROBIOLOGY Metabolic engineering Pub Date : 2024-06-18 DOI:10.1016/j.ymben.2024.06.004
Lizhan Zhang , Jian-Wen Ye , Gang Li , Helen Park , Hao Luo , Yina Lin , Shaowei Li , Weinan Yang , Yuying Guan , Fuqing Wu , Wuzhe Huang , Qiong Wu , Nigel S. Scrutton , Jens Nielsen , Guo-Qiang Chen
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引用次数: 0

摘要

在基于微生物宿主的生物生产过程中,微生物不稳定性是一个常见问题。蓝光单胞菌(Halomonas bluephagenesis)已被开发为开放和无菌条件下的下一代工业生物技术(NGIB)底盘。然而,隐藏的基因组信息和特殊的新陈代谢极大地阻碍了其在细胞工厂工程中的深度开发。基于最新完成的 H. bluephagenesis TD01 基因组序列,揭示了 1889 个生物过程相关基因,并将其归类为 84 个 GO-slim 术语。构建的酶约束基因组尺度代谢模型Halo-ecGEM显示出很强的模拟饲料批量发酵的能力。通过结合GO-slim术语富集和基于CVT的omics图谱分析,获得了可见的盐胁迫响应图谱,表明当暴露于盐胁迫时,细胞会强制调配大部分蛋白质资源以支持翻译和蛋白质代谢的基本活动。在 Halo-ecGEM 的指导下,8 个转座酶被删除,从而显著提高了其生长和生物生产各种聚羟基烷酸酯(PHA)的稳定性,包括 3-hydroxybutyrate (3HB) 均聚物 PHB、3HB 和 3-hydroxyvalerate (3HV) 共聚物 PHBV 以及 3HB 和 4-hydroxyvalerate (4HB) 共聚物 P34HB。这项研究揭示了蓝藻的新陈代谢特征和应激反应情况,首次构建了一种可用于工业应用的长期稳定生长的底盘。研究首次证明,基因组编码的转座子是烧瓶和发酵罐中微生物生长不稳定的原因。
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A long-term growth stable Halomonas sp. deleted with multiple transposases guided by its metabolic network model Halo-ecGEM

Microbial instability is a common problem during bio-production based on microbial hosts. Halomonas bluephagenesis has been developed as a chassis for next generation industrial biotechnology (NGIB) under open and unsterile conditions. However, the hidden genomic information and peculiar metabolism have significantly hampered its deep exploitation for cell-factory engineering. Based on the freshly completed genome sequence of H. bluephagenesis TD01, which reveals 1889 biological process-associated genes grouped into 84 GO-slim terms. An enzyme constrained genome-scale metabolic model Halo-ecGEM was constructed, which showed strong ability to simulate fed-batch fermentations. A visible salt-stress responsive landscape was achieved by combining GO-slim term enrichment and CVT-based omics profiling, demonstrating that cells deploy most of the protein resources by force to support the essential activity of translation and protein metabolism when exposed to salt stress. Under the guidance of Halo-ecGEM, eight transposases were deleted, leading to a significantly enhanced stability for its growth and bioproduction of various polyhydroxyalkanoates (PHA) including 3-hydroxybutyrate (3HB) homopolymer PHB, 3HB and 3-hydroxyvalerate (3HV) copolymer PHBV, as well as 3HB and 4-hydroxyvalerate (4HB) copolymer P34HB. This study sheds new light on the metabolic characteristics and stress-response landscape of H. bluephagenesis, achieving for the first time to construct a long-term growth stable chassis for industrial applications. For the first time, it was demonstrated that genome encoded transposons are the reason for microbial instability during growth in flasks and fermentors.

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来源期刊
Metabolic engineering
Metabolic engineering 工程技术-生物工程与应用微生物
CiteScore
15.60
自引率
6.00%
发文量
140
审稿时长
44 days
期刊介绍: Metabolic Engineering (MBE) is a journal that focuses on publishing original research papers on the directed modulation of metabolic pathways for metabolite overproduction or the enhancement of cellular properties. It welcomes papers that describe the engineering of native pathways and the synthesis of heterologous pathways to convert microorganisms into microbial cell factories. The journal covers experimental, computational, and modeling approaches for understanding metabolic pathways and manipulating them through genetic, media, or environmental means. Effective exploration of metabolic pathways necessitates the use of molecular biology and biochemistry methods, as well as engineering techniques for modeling and data analysis. MBE serves as a platform for interdisciplinary research in fields such as biochemistry, molecular biology, applied microbiology, cellular physiology, cellular nutrition in health and disease, and biochemical engineering. The journal publishes various types of papers, including original research papers and review papers. It is indexed and abstracted in databases such as Scopus, Embase, EMBiology, Current Contents - Life Sciences and Clinical Medicine, Science Citation Index, PubMed/Medline, CAS and Biotechnology Citation Index.
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