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谷氨酸棒杆菌缬氨酸/亮氨酸合成途径中反应动力学的监测与建模

Monitoring and modeling of the reaction dynamics in the valine/leucine synthesis pathway in Corynebacterium glutamicum.

作者信息

Magnus Jørgen Barsett, Hollwedel Daniel, Oldiges Marco, Takors Ralf

机构信息

Forschungszentrum Jülich, Institute of Biotechnology 2, Germany.

出版信息

Biotechnol Prog. 2006 Jul-Aug;22(4):1071-83. doi: 10.1021/bp060072f.

DOI:10.1021/bp060072f
PMID:16889382
Abstract

The intracellular concentrations of the valine and leucine pathway intermediates in a Corynebacterium glutamicum strain were measured during a transient state. The data were obtained by performing a glucose stimulus-response experiment with the use of a rapid sampling device and advanced mass spectrometry. The glucose stimulus resulted in a 3-fold increase in the intracellular pyruvate concentration within less than a second, demonstrating the very fast interactions in metabolic networks. The samples were taken at subsecond intervals for a time period of 25 s. The time courses of the metabolite concentrations formed the experimental basis of a mathematical model simulating the fluxes and concentrations in the valine/leucine pathway. The implementation of a model selection criterion based on the second law of thermodynamics is demonstrated to be essential for the identification of realistic and unique models. Large differences between the enzyme properties determined in vitro and those determined in vivo by the model were observed with the in vivo maximal rates being almost an order of magnitude larger than the in vitro maximal rates. The transamination of ketoisovalerate (KIV) to valine is carried out mainly by the transaminase B enzyme, with the transaminase C enzyme playing a minor role. The availability of the cofactors NADP and NADPH only has modest influence on the flux through the valine pathway, while the influence of NAD and NADH on the flux through the leucine pathway is negligible.

摘要

在瞬态期间测量了谷氨酸棒杆菌菌株中缬氨酸和亮氨酸途径中间体的细胞内浓度。这些数据是通过使用快速采样装置和先进的质谱技术进行葡萄糖刺激 - 反应实验获得的。葡萄糖刺激在不到一秒的时间内使细胞内丙酮酸浓度增加了3倍,这表明代谢网络中存在非常快速的相互作用。以亚秒级间隔采集样本,持续25秒。代谢物浓度的时间进程构成了模拟缬氨酸/亮氨酸途径通量和浓度的数学模型的实验基础。基于热力学第二定律的模型选择标准的实施被证明对于识别现实且唯一的模型至关重要。观察到体外测定的酶性质与模型在体内测定的酶性质之间存在很大差异,体内最大速率几乎比体外最大速率大一个数量级。α-酮异戊酸(KIV)向缬氨酸的转氨作用主要由转氨酶B酶进行,转氨酶C酶起次要作用。辅因子NADP和NADPH的可用性对通过缬氨酸途径的通量只有适度影响,而NAD和NADH对通过亮氨酸途径的通量影响可忽略不计。

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