首页> 外文会议>2010 4th International Conference on Bioinformatics and Biomedical Engineering >Robustness and Nonlinear Dynamic Analysis for Trp Operon and Optimization of Tryptophan Production: An Integrated Model Considering Gene Regulation, Genes Interaction and Product Excretion
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Robustness and Nonlinear Dynamic Analysis for Trp Operon and Optimization of Tryptophan Production: An Integrated Model Considering Gene Regulation, Genes Interaction and Product Excretion

机译:Trp操纵子的鲁棒性和非线性动力学分析以及色氨酸的生产优化:考虑基因调控,基因相互作用和产物排泄的集成模型

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The tryptophan operon (trp operon), paradigm for repressible operons, is regulated by three different negative-feedback mechanisms of repression, transcription attenuation and enzyme inhibition. Initiation of transcription is controlled by the interaction of the tryptophan repressor with its target site on the operator. Moreover, the interaction among the regulator genes, the operator genes and the structure genes and excretion of tryptophan play an important factor according to previous works. In this study, an expended mathematical model for the tryptophan operon regulation on the effects of repression, feedback enzyme inhibition, attenuation, interaction among genes and excretion of tryptophan is presented. The new model is first translated into the corresponding S-system version. The robustness of this model is then discussed by using the S-system model and the sensitivity analysis shows that the model is robust enough. The influences of cell growth rate on the biosynthesis of tryptophan, stability and dynamic behavior of the trp operon are also well investigated. The transportation of tryptophan through cytoplasmic membranes, especially the inhibition of tryptophan transport can influence the level of intracellular tryptophan significantly. The theoretical analysis indicates that an increase of inhibition constant of tryptophan transport is favorable for the biosynthesis of tryptophan. Furthermore, a steady-state optimization model is established based on trp operon models. The optimization results indicate that it is possible to attain a stable and robust steady state with a rate of tryptophan production increased more than 4.8 times in which the growth rate is kept as 0.00624h-1 and some key parameters is modulated.
机译:色氨酸操纵子(trp操纵子)是可抑制操纵子的范式,受三种不同的抑制,转录衰减和酶抑制的负反馈机制调节。转录的起始受色氨酸阻遏物与其操纵基因上靶位点相互作用的控制。此外,根据以前的工作,调节基因,操纵基因和结构基因之间的相互作用以及色氨酸的排泄起着重要的作用。在这项研究中,提出了一种用于色氨酸操纵子调节的数学模型,该模型对阻抑,反馈酶抑制,衰减,基因间相互作用和色氨酸排泄的影响。首先将新模型转换为相应的S系统版本。然后,使用S系统模型讨论该模型的鲁棒性,敏感性分析表明该模型足够鲁棒。还充分研究了细胞生长速率对色氨酸生物合成,trp操纵子稳定性和动态行为的影响。色氨酸通过细胞质膜的运输,尤其是色氨酸运输的抑制,可以显着影响细胞内色氨酸的水平。理论分析表明,色氨酸转运抑制常数的增加有利于色氨酸的生物合成。此外,基于trp操纵子模型建立了稳态优化模型。优化结果表明,可以实现稳定,稳定的稳态,其中色氨酸的产生速率增加4.8倍以上,其中色散的增长率保持为0.00624h-1,并调节了一些关键参数。

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