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首页> 外文期刊>Journal of Chemical Technology & Biotechnology >Modelling concentration gradients in fed-batch cultivations of E-coli - towards the flexible design of scale-down experiments
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Modelling concentration gradients in fed-batch cultivations of E-coli - towards the flexible design of scale-down experiments

机译:e-coli综合培养浓度梯度 - 朝向尺度缩放实验的灵活设计

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BACKGROUND The impact of concentration gradients in large industrial-scale bioreactors on microbial physiology can be studied in scale-down bioreactors. However, scale-down systems pose several challenges in construction, operation and footprint. Therefore, it is challenging to implement them in emerging technologies for bioprocess development, such as in high throughput cultivation platforms. In this study, a mechanistic model of a two-compartment scale-down bioreactor is developed. Simulations from this model are then used as bases for a pulse-based scale-down bioreactor suitable for application in parallel cultivation systems. RESULTS As an application, the pulse-based system model was used to study the misincorporation of non-canonical branched-chain amino acids into recombinant pre-proinsulin expressed in Escherichia coli, as a response to oscillations in glucose and dissolved oxygen concentrations. The results show significant accumulation of overflow metabolites, up to 18.3% loss in product yield and up to 10-fold accumulation of the non-canonical amino acids norvaline and norleucine in the product in the pulse-based cultivation, compared with a reference cultivation. CONCLUSIONS Results indicate that the combination of a pulse-based scale-down approach with mechanistic models is a very suitable method to test strain robustness and physiological constraints at the early stages of bioprocess development. (c) 2018 Society of Chemical Industry
机译:背景技术在落下的生物反应器中可以研究大型工业规模生物反应器对微生物生理学的浓度梯度的影响。然而,缩放系统在施工,操作和足迹中构成了几个挑战。因此,在生物过程开发的新兴技术中实现它们是挑战,例如在高吞吐量栽培平台中。在该研究中,开发了一种双隔室缩小生物反应器的机械模型。然后将来自该模型的模拟用作适用于并行培养系统的脉冲缩小生物反应器的基础。结果作为应用,基于脉冲的系统模型用于研究非典型支链氨基酸的MISlincoration在大肠杆菌中表达的重组前胰岛素中,作为葡萄糖振荡的反应和溶解氧浓度的响应。结果显示出溢流代谢物的显着积累,产品产量损失高达18.3%,与参考培养相比,在脉冲培养的产品中,在产物中的非规范氨基酸Norvaline和Norleuline的积累量高达10倍。结论结果表明,机械模型的脉冲缩放方法的组合是一种非常合适的方法,用于测试生物过程开发的早期阶段的应变鲁棒性和生理约束。 (c)2018化学工业协会

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