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重组蛋白生产的代谢负荷:大肠杆菌中异源基因诱导后对葡萄糖摄取和呼吸细胞能力的抑制。

Metabolic load of recombinant protein production: inhibition of cellular capacities for glucose uptake and respiration after induction of a heterologous gene in Escherichia coli.

作者信息

Neubauer P, Lin H Y, Mathiszik B

机构信息

Bioprocess Engineering Laboratory, P.O. Box 4300, Department of Process and Environmental Engineering, Biocenter Oulu, University of Oulu, FIN-90014 Oulu, Finland.

出版信息

Biotechnol Bioeng. 2003 Jul 5;83(1):53-64. doi: 10.1002/bit.10645.

Abstract

The strong expression of recombinant proteins in bacteria affects the primary carbon and energy metabolism resulting in growth inhibition and acetate formation. By applying glucose pulses to fed-batch fermentations performed for production of a heterologous (alpha-glucosidase in Escherichia coli, we show that the induction of the recombinant gene strongly inhibits the maximum specific uptake capacities for glucose and the respiration capacity. The accumulation of glucose in the fermentation medium promotes the growth of plasmid-free cells. These inhibition effects are well described by including the kinetics of product formation into a recently published dynamic model (Lin et al. [2001] Biotechnol Bioeng 73:349-357). The new model also includes the population characteristics and gives a good fit to the measured data describing growth, production, substrate consumption, by-product formation, and respiration.

摘要

细菌中重组蛋白的高表达会影响主要的碳和能量代谢,导致生长抑制和乙酸盐生成。通过在用于生产异源蛋白(大肠杆菌中的α-葡萄糖苷酶)的补料分批发酵中施加葡萄糖脉冲,我们发现重组基因的诱导强烈抑制了葡萄糖的最大比摄取能力和呼吸能力。发酵培养基中葡萄糖的积累促进了无质粒细胞的生长。通过将产物形成动力学纳入最近发表的动态模型(Lin等人,[2001]《生物技术与生物工程》73:349 - 357),可以很好地描述这些抑制作用。新模型还包括群体特征,并且与描述生长、生产、底物消耗、副产物形成和呼吸的测量数据拟合良好。

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