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OPTIMIZATION OF BENZYLISOQUINOLINE ALKALOID PRODUCTION IN YEAST

机译:酵母中苄基异喹啉碱的生产工艺优化

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Benzylisoquinoline alkaloids (BIAs) are a large family of plant secondary metabolites. Several members of the BIA family are commercially available as probiotics and Pharmaceuticals. Still more BIAs have been demonstrated to have pharmaceutically relevant properties. Unfortunately, most BIAs do not accumulate in sufficient quantities in planta to merit further study. Microbial synthesis of BIAs could open the door to further commercial development of BIAs. Both Escherichia coli and Saccharomyces cerevisiae have been developed into microbial platforms for BIA synthesis. Currently, E. coli produces significantly higher de novo titers of BIAs (160 mg/L in E. coli vs. 2 mg/L in yeast). However, yeast remain an attractive target for BIA synthesis, as BIA derivatization often requires endomembrane-associated cytochrome P450s that tend to be more easily expressed in eukaryotic hosts. In this work we demonstrate a general improvement of BIA synthesis in yeast by manipulation of multiple areas of yeast metabolism, including increase of precursor synthesis, reduction of precursor catabolism, and balance of flux through pathway branchpoints. This improvement brings yeast titers in line with E. coli titers, establishing yeast as a competitive platform for BIA synthesis.
机译:苄基异喹啉生物碱(BIAs)是植物次生代谢产物的一大家族。 BIA家族的几个成员可以作为益生菌和药品在市场上买到。已经证明更多的BIA具有药学上相关的性质。不幸的是,大多数BIA在植物中的积累量不足,值得进一步研究。 BIA的微生物合成可以为BIA的进一步商业开发打开大门。大肠埃希氏菌和酿酒酵母已被开发成用于BIA合成的微生物平台。目前,大肠杆菌从头产生的BIA滴度要高得多(大肠杆菌中160 mg / L,酵母中2 mg / L)。然而,酵母仍然是BIA合成的诱人靶标,因为BIA衍生化通常需要与膜相关的细胞色素P450,它们在真核宿主中往往更容易表达。在这项工作中,我们证明了通过操纵酵母代谢的多个区域,酵母中BIA合成的总体改善,包括增加前体合成,减少前体分解代谢以及通过途径分支点的通量平衡。这种改进使酵母滴度与大肠杆菌滴度一致,从而将酵母确立为BIA合成的竞争平台。

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