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首页> 外文期刊>Synthetic and Systems Biotechnology >Systematic development of biomass overproducing Scheffersomyces stipitis for high-cell-density fermentations
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Systematic development of biomass overproducing Scheffersomyces stipitis for high-cell-density fermentations

机译:用于高细胞密度发酵的生物量过量生产的酿酒酵母的系统开发

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Abstract The development of economically feasible bio-based process requires efficient cell factories capable of producing the desired product at high titer under high-cell-density fermentation. Herein we present a combinatorial approach based on systems metabolic engineering and metabolic evolution for the development of efficient biomass-producing strain. Systems metabolic engineering guided by flux balance analysis (FBA) was first employed to rationally design mutant strains of Scheffersomyces stipitis with high biomass yield. By experimentally implementing these mutations, the biomass yield was improved by 30% in GPD1, 25% in TKL1, 30% in CIT1, and 44% in {ZWF1} overexpressed mutants compared to wild-type. These designed mutants were further fine-tuned through metabolic evolution resulting in the maximal biomass yield of 0.49?g-cdw/g-glucose, which matches well with predicted yield phenotype. The constructed mutants are beneficial for biotechnology applications dealing with high cell titer cultivations. This work demonstrates a solid confirmation of systems metabolic engineering in combination with metabolic evolution approach for efficient strain development, which could assist in rapid optimization of cell factory for an economically viable and sustainable bio-based process.
机译:摘要经济上可行的生物基工艺的发展要求高效的细胞工厂能够在高细胞密度发酵下以高滴度生产所需的产物。本文中,我们提出了一种基于系统代谢工程和代谢进化的组合方法,用于开发有效的生物质生产菌株。首先通过通量平衡分析(FBA)指导的系统代谢工程技术合理设计了高产生物量的拟南芥裂殖酵母突变株。通过实验实现这些突变,与野生型相比,GPD1的生物量产量提高了30%,TKL1的生物量产量提高了25%,CIT1的生物量产量提高了30%,{ZWF1}的生物量产量提高了44%。通过代谢进化对这些设计的突变体进行进一步的微调,以使最大生物量产量达到0.49?g-cdw / g-葡萄糖,与预期的产量表型非常吻合。构建的突变体对于处理高细胞滴度培养的生物技术应用是有益的。这项工作证明了系统代谢工程与代谢进化方法相结合的有效方法,可以有效地开发菌株,从而可以为经济可行和可持续的基于生物的过程快速优化细胞工厂。

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