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Lipid engineering combined with systematic metabolic engineering of Saccharomyces cerevisiae for high-yield production of lycopene

机译:脂质工程与酿酒酵母酿酒酵母的系统代谢工程相结合,高产番茄红素生产

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摘要

Saccharomyces cerevisiae is an efficient host for natural-compound production and preferentially employed in academic studies and bioindustries. However, S. cerevisiae exhibits limited production capacity for lipophilic natural products, especially compounds that accumulate intracellularly, such as polyketides and carotenoids, with some engineered compounds displaying cytotoxicity. In this study, we used a nature-inspired strategy to establish an effective platform to improve lipid oil-triacylglycerol (TAG) metabolism and enable increased lycopene accumulation. Through systematic traditional engineering methods, we achieved relatively high-level production at 56.2 mg lycopene/g cell dry weight (cdw). To focus on TAG metabolism in order to increase lycopene accumulation, we overexpressed key genes associated with fatty acid synthesis and TAG production, followed by modulation of TAG fatty acyl composition by overexpressing a fatty acid desaturase (OLE1) and deletion of Seipin (FLD1), which regulates lipid-droplet size. Results showed that the engineered strain produced 70.5 mg lycopene/g cdw, a 25% increase relative to the original high-yield strain, with lycopene production reaching 2.37 g/L and 73.3 mg/g cdw in fed-batch fermentation and representing the highest lycopene yield in S. cerevisiae reported to date. These findings offer an effective strategy for extended systematic metabolic engineering through lipid engineering.
机译:Saccharomyces Cerevisiae是用于自然复合生产的有效主持人,优先用于学术研究和生物行业。然而,S.Cerevisiae对亲脂性天然产物具有有限的生产能力,特别是聚细胞内酯和类胡萝卜素积聚的化合物,其中一些工程化合物显示细胞毒性。在这项研究中,我们利用自然启发策略来建立一种有效的平台,以改善脂质油 - 三酰基甘油(标签)代谢并实现番茄红素积累。通过系统的传统工程方法,我们在56.2毫克番茄红素/ g细胞干重(CDW)上实现了相对高级别的产量。为了重点关注标签代谢以增加番茄红素积累,我们通过过表达脂肪酸去饱和酶(OLE1)和缺失Seipin(FLD1),过度表达与脂肪酸合成和标签生产相关的关键基因。调节脂质液滴尺寸。结果表明,工程菌株产生70.5mg番茄红素/克CdW,相对于原始的高产菌株增加25%,番茄红素产量达到2.37克/升和73.3mg / g CdW,进料批量发酵,代表最高塞西维亚岛的番茄红素产量达到日期。这些调查结果通过脂质工程提供了扩展系统代谢工程的有效策略。

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  • 来源
    《Metabolic engineering》 |2019年第2019期|共9页
  • 作者单位

    Wuhan Univ Minist Educ Key Lab Combinatorial Biosynth &

    Drug Discovery Wuhan 430072 Peoples R;

    Wuhan Univ Minist Educ Key Lab Combinatorial Biosynth &

    Drug Discovery Wuhan 430072 Peoples R;

    J1 Biotech Co Ltd Wuhan 430075 Hubei Peoples R China;

    Wuhan Univ Minist Educ Key Lab Combinatorial Biosynth &

    Drug Discovery Wuhan 430072 Peoples R;

    Wuhan Univ Minist Educ Key Lab Combinatorial Biosynth &

    Drug Discovery Wuhan 430072 Peoples R;

    Chalmers Univ Technol Dept Biol &

    Biol Engn SE-41296 Gothenburg Sweden;

    Chinese Univ Hong Kong Dept Chem Shatin Hong Kong Peoples R China;

    Chalmers Univ Technol Dept Biol &

    Biol Engn SE-41296 Gothenburg Sweden;

    Wuhan Univ Minist Educ Key Lab Combinatorial Biosynth &

    Drug Discovery Wuhan 430072 Peoples R;

    Wuhan Univ Minist Educ Key Lab Combinatorial Biosynth &

    Drug Discovery Wuhan 430072 Peoples R;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 蛋白质;
  • 关键词

    Saccharomyces cerevisiae; Systematic metabolic engineering; Lipid engineering; Triacylglycerol; Lycopene;

    机译:Saccharomyces酿酒酵母;系统代谢工程;脂质工程;三酰基甘油;番茄红素;

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