Coupled strategy based on regulator manipulation and medium optimization empowers the biosynthetic overproduction of lincomycin

IF 4.4 2区 生物学 Q1 BIOTECHNOLOGY & APPLIED MICROBIOLOGY
Xinlu Cai , Wanlian Xu , Yang Zheng , Sendi Wu , Rundong Zhao , Nian Wang , Yaqian Tang , Meilan Ke , Qianjin Kang , Linquan Bai , Buchang Zhang , Hang Wu
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Abstract

The biosynthesis of bioactive secondary metabolites, specifically antibiotics, is of great scientific and economic importance. The control of antibiotic production typically involves different processes and molecular mechanism. Despite numerous efforts to improve antibiotic yields, joint engineering strategies for combining genetic manipulation with fermentation optimization remain finite. Lincomycin A (Lin-A), a lincosamide antibiotic, is industrially fermented by Streptomyces lincolnensis. Herein, the leucine-responsive regulatory protein (Lrp)-type regulator SLCG_4846 was confirmed to directly inhibit the lincomycin biosynthesis, whereas indirectly controlled the transcription of SLCG_2919, the first reported repressor in S. lincolnensis. Inactivation of SLCG_4846 in the high-yield S. lincolnensis LA219X (LA219XΔ4846) increases the Lin-A production and deletion of SLCG_2919 in LA219XΔ4846 exhibits superimposed yield increment. Given the effect of the double deletion on cellular primary metabolism of S. lincolnensis, Plackett-Burman design, steepest ascent and response surface methodologies were utilized and employed to optimize the seed medium of this double mutant in shake flask, and Lin-A yield using optimal seed medium was significantly increased over the control. Above strategies were performed in a 15-L fermenter. The maximal yield of Lin-A in LA219XΔ4846-2919 reached 6.56 g/L at 216 h, 55.1 % higher than that in LA219X at the parental cultivation (4.23 g/L). This study not only showcases the potential of this strategy to boost lincomycin production, but also could empower the development of high-performance actinomycetes for other antibiotics.

基于调节器操作和培养基优化的耦合策略促进了林可霉素的生物合成过量生产
生物活性次级代谢物(特别是抗生素)的生物合成具有重要的科学和经济意义。抗生素生产的控制通常涉及不同的过程和分子机制。尽管为提高抗生素产量做出了许多努力,但将遗传操作与发酵优化相结合的联合工程策略仍然有限。林可霉素 A(Lin-A)是一种林可酰胺类抗生素,由林肯链霉菌(Streptomyces lincolnensis)进行工业化发酵。研究证实,亮氨酸反应调节蛋白(Lrp)型调节因子 SLCG_4846 可直接抑制林可霉素的生物合成,同时间接控制 SLCG_2919 的转录,SLCG_2919 是首次报道的林肯链霉菌抑制因子。在高产的林肯菌 LA219X(LA219XΔ4846)中,SLCG_4846 失活会增加 Lin-A 的产量,而在 LA219XΔ4846 中缺失 SLCG_2919 则会叠加增产。鉴于双基因缺失对林肯菌细胞初级代谢的影响,研究人员利用普拉克特-伯曼设计法、最陡坡上升法和响应面法对该双突变体在摇瓶中的种子培养基进行了优化,使用最佳种子培养基的麟甲产量比对照组显著增加。上述策略在 15 升发酵罐中进行。216 h时,LA219XΔ4846-2919的Lin-A最高产量达到6.56 g/L,比亲本培养时LA219X的产量(4.23 g/L)高55.1%。这项研究不仅展示了这一策略在提高林可霉素产量方面的潜力,还有助于开发用于其他抗生素的高性能放线菌。
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来源期刊
Synthetic and Systems Biotechnology
Synthetic and Systems Biotechnology BIOTECHNOLOGY & APPLIED MICROBIOLOGY-
CiteScore
6.90
自引率
12.50%
发文量
90
审稿时长
67 days
期刊介绍: Synthetic and Systems Biotechnology aims to promote the communication of original research in synthetic and systems biology, with strong emphasis on applications towards biotechnology. This journal is a quarterly peer-reviewed journal led by Editor-in-Chief Lixin Zhang. The journal publishes high-quality research; focusing on integrative approaches to enable the understanding and design of biological systems, and research to develop the application of systems and synthetic biology to natural systems. This journal will publish Articles, Short notes, Methods, Mini Reviews, Commentary and Conference reviews.
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