Fermentation Optimization of Loonamycin Production by Marine Nocardiopsis flavescens

IF 3.5 4区 生物学 Q2 MICROBIOLOGY
Tianyu Zhou, Yuan Cao, Zhicheng Zhang, Jing Shi, Huiming Ge, Faliang An, Jiang Ye, Ruida Wang, Haizhen Wu
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引用次数: 0

Abstract

The antitumor drug candidate, loonamycin, was isolated from Nocardiopsis flavescens NA01583 and exerts its antitumor activity by inhibiting topoisomerase I activity. However, the current production levels of loonamycin are insufficient for further research. To address this limitation, a liquid fermentation method was developed, optimizing both fermentation conditions and medium components. This optimization increased loonamycin production from 1 mg/mL on agar plate to 602.32 mg/mL in shake flask and ultimately 532.51 mg/mL in a 5-L bioreactor. Exogenous addition experiments revealed that sea salt and metal ions significantly inhibit loonamycin synthesis. Multi-temporal transcriptomic analyses indicated that the reduced expression levels of genes involved in the shikimate pathway and L-tryptophan biosynthesis pathway were the limiting factors for increased loonamycin yield. Overall, an effective fermentation method for rare marine actinomycetes was established, significantly enhancing loonamycin production and providing a foundation for the development of this novel antitumor prodrug.

海洋 Nocardiopsis flavescens 生产卢安霉素的发酵优化。
从黄芽孢杆菌NA01583中分离到抗肿瘤候选药物卢纳霉素,通过抑制拓扑异构酶I活性发挥其抗肿瘤活性。然而,目前卢纳霉素的生产水平不足以进行进一步的研究。为了解决这一限制,开发了一种液体发酵方法,优化了发酵条件和培养基成分。优化后的卢纳霉素产量从琼脂平板上的1 mg/mL提高到摇瓶中的602.32 mg/mL,最终在5-L生物反应器中提高到532.51 mg/mL。外源添加实验表明,海盐和金属离子显著抑制卢纳霉素的合成。多时间转录组学分析表明,莽草酸途径和l -色氨酸生物合成途径相关基因的表达水平降低是卢纳霉素产量增加的限制因素。总之,建立了一种有效的海洋稀有放线菌发酵方法,显著提高了卢纳霉素的产量,为开发这种新型抗肿瘤前药奠定了基础。
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来源期刊
Journal of Basic Microbiology
Journal of Basic Microbiology 生物-微生物学
CiteScore
6.10
自引率
0.00%
发文量
134
审稿时长
1.8 months
期刊介绍: The Journal of Basic Microbiology (JBM) publishes primary research papers on both procaryotic and eucaryotic microorganisms, including bacteria, archaea, fungi, algae, protozoans, phages, viruses, viroids and prions. Papers published deal with: microbial interactions (pathogenic, mutualistic, environmental), ecology, physiology, genetics and cell biology/development, new methodologies, i.e., new imaging technologies (e.g. video-fluorescence microscopy, modern TEM applications) novel molecular biology methods (e.g. PCR-based gene targeting or cassettes for cloning of GFP constructs).
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