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High production of triterpenoids in Yarrowia lipolytica through manipulation of lipid components

机译:通过操纵脂质组分,在Yarrowia Lipolytica中高生产Triterpenoids

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Lupeol exhibits novel physiological and pharmacological activities, such as anticancer and immunity-enhancing activities. However, cytotoxicity remains a challenge for triterpenoid overproduction in microbial cell factories. As lipophilic and relatively small molecular compounds, triterpenes are generally secreted into the extracellular space. The effect of increasing triterpene efflux on the synthesis capacity remains unknown. In this study, we developed a strategy to enhance triterpene efflux through manipulation of lipid components in Y. lipolytica by overexpressing the enzyme Δ9-fatty acid desaturase (OLE1) and disturbing phosphatidic acid phosphatase (PAH1) and diacylglycerol kinase (DGK1). By this strategy combined with two-phase fermentation, the highest lupeol production reported to date was achieved, where the titer in the organic phase reached 381.67?mg/L and the total production was 411.72?mg/L in shake flasks, exhibiting a 33.20-fold improvement over the initial strain. Lipid manipulation led to a twofold increase in the unsaturated fatty acid (UFA) content, up to 61–73%, and an exceptionally elongated cell morphology, which might have been caused by enhanced membrane phospholipid biosynthesis flux. Both phenotypes accelerated the export of toxic products to the extracellular space and ultimately stimulated the capacity for triterpenoid synthesis, which was proven by the 5.11-fold higher ratio of extra/intracellular lupeol concentrations, 2.79-fold higher biomass accumulation and 2.56-fold higher lupeol productivity per unit OD in the modified strains. This strategy was also highly efficient for the biosynthesis of other triterpenes and sesquiterpenes, including α-amyrin, β-amyrin, longifolene, longipinene and longicyclene. In conclusion, we successfully created a high-yield lupeol-producing strain via lipid manipulation. We demonstrated that the enhancement of lupeol efflux and synthesis capacity was induced by the increased UFA content and elongated cell morphology. Our study provides a novel strategy to promote the biosynthesis of valuable but toxic products in microbial cell factories.
机译:Lupeol表现出新的生理和药理学活动,例如抗癌和免疫增强活动。然而,细胞毒性仍然是微生物细胞工厂中三萜类化合物的挑战。作为亲脂性和相对较小的分子化合物,通常分泌到细胞外空间中的三萜。增加Triterpene Efflux对合成能力的影响仍然是未知的。在这项研究中,我们通过过表达酶δ9-脂肪酸去饱和酶(OLE1)和干扰磷脂酸磷酸酶(PAH1)和二酰基甘油激酶(DGK1)来制定通过在Y. Lipolytica的脂质组分进行脂质组分来提高脂质组分的策略。通过该策略结合两相发酵,实现了迄今为止迄今为止报告的最高卢博尔的产量,其中有机相中的滴度达到381.67〜67. mg / L,总产量为411.72?Mg / L在摇瓶中,表现为33.20 - 对初始应变的改善。脂质操纵导致不饱和脂肪酸(UFA)含量的双重增加,高达61-73%,以及一种异常细长的细胞形态,其可能是由增强膜磷脂生物合成通量引起的。两种表型加速了对细胞外空间的有毒产物的出口,最终刺激了三萜合成的能力,其额外/细胞内碱醇浓度的5.11倍,生物量增长2.79倍,卢普尔高2.56倍修饰菌株中每单位OD的生产率。该策略对其他三萜和酪蛋白的生物合成,包括α-奥霉素,β-淀粉蛋白,长乙烯,稀丙烯烯和环丙烯环。总之,我们通过脂质操作成功地产生了高产卢河生产菌株。我们证明,通过增加的UFA含量和细胞细胞形态来诱导卢博尔流出和合成能力的增强。我们的研究提供了一种新颖的策略,可促进微生物细胞工厂中有价值但有毒产品的生物合成。

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