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多目标下的多产品生物合成工厂建模与优化。

Modeling and optimization of a multi-product biosynthesis factory for multiple objectives.

机构信息

Department of Chemical & Biomolecular Engineering, National University of Singapore, 4 Engineering Drive 4, Singapore 117576, Singapore.

出版信息

Metab Eng. 2010 May;12(3):251-67. doi: 10.1016/j.ymben.2009.12.003. Epub 2010 Jan 5.

Abstract

Genetic algorithms and optimization in general, enable us to probe deeper into the metabolic pathway recipe for multi-product biosynthesis. An augmented model for optimizing serine and tryptophan flux ratios simultaneously in Escherichia coli, was developed by linking the dynamic tryptophan operon model and aromatic amino acid-tryptophan biosynthesis pathways to the central carbon metabolism model. Six new kinetic parameters of the augmented model were estimated with considerations of available experimental data and other published works. Major differences between calculated and reference concentrations and fluxes were explained. Sensitivities and underlying competition among fluxes for carbon sources were consistent with intuitive expectations based on metabolic network and previous results. Biosynthesis rates of serine and tryptophan were simultaneously maximized using the augmented model via concurrent gene knockout and manipulation. The optimization results were obtained using the elitist non-dominant sorting genetic algorithm (NSGA-II) supported by pattern recognition heuristics. A range of Pareto-optimal enzyme activities regulating the amino acids biosynthesis was successfully obtained and elucidated wherever possible vis-à-vis fermentation work based on recombinant DNA technology. The predicted potential improvements in various metabolic pathway recipes using the multi-objective optimization strategy were highlighted and discussed in detail.

摘要

遗传算法和优化算法一般来说,可以让我们更深入地研究多产物生物合成的代谢途径配方。通过将动态色氨酸操纵子模型和芳香族氨基酸-色氨酸生物合成途径与中心碳代谢模型相连接,我们为大肠杆菌中的丝氨酸和色氨酸通量比的同时优化建立了一个增强模型。该增强模型的 6 个新动力学参数是在考虑到可用的实验数据和其他已发表的工作的基础上进行估计的。对计算和参考浓度以及通量之间的主要差异进行了解释。根据代谢网络和先前的结果,对碳源通量之间的敏感性和潜在竞争进行了直观的解释。通过同时基因敲除和操作,使用增强模型同时最大化丝氨酸和色氨酸的生物合成速率。使用基于模式识别启发式的精英非支配排序遗传算法 (NSGA-II) 获得了优化结果。成功获得了一系列调节氨基酸生物合成的 Pareto 最优酶活性,并尽可能地阐明了基于重组 DNA 技术的发酵工作。使用多目标优化策略,突出并详细讨论了各种代谢途径配方的潜在改进。

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