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Derivation of a Biomass Proxy for Dynamic Analysis of Whole Genome Metabolic Models

机译:用于全基因组代谢模型动态分析的生物量代理的推导

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A whole genome metabolic model (GEM) is essentially a reconstruction of a network of enzyme-enabled chemical reactions representing the metabolism of an organism, based on information present in its genome. Such models have been designed so that flux balance analysis (FBA) can be applied in order to analyse metabolism under steady state. For this purpose, a biomass function is added to these models as an overall indicator of the model's viability. Our objective is to develop dynamic models based on these FBA models in order to observe new and complex behaviours, including transient behaviour. There is however a major challenge in that the biomass function does not operate under dynamic simulation. An appropriate biomass function would enable the estimation under dynamic simulation of the growth of both wild-type and genetically modified bacteria under different, possibly dynamically changing growth conditions. Using data analytics techniques, we have developed a dynamic biomass function which acts as a faithful proxy for the FBA equivalent for a reduced GEM for E. coli. This involved consolidating data for reaction rates and metabolite concentrations generated under dynamic simulation with gold standard target data for biomass obtained by steady state analysis using FBA. It also led to a number of interesting insights regarding biomass fluxes for pairs of conditions. These findings were reproduced in our dynamic proxy function.
机译:整个基因组代谢模型(GEM)本质上是基于生物体基因组中存在的信息的,代表生物体代谢的酶促化学反应网络的重建。设计了这样的模型,以便可以应用通量平衡分析(FBA)来分析稳态下的代谢。为此,将生物量功能添加到这些模型中,作为模型生存能力的总体指标。我们的目标是基于这些FBA模型开发动态模型,以观察新的复杂行为,包括瞬态行为。然而,主要挑战在于生物量功能不能在动态模拟下运行。适当的生物量功能将能够在动态模拟下估算野生型和转基因细菌在不同,可能动态变化的生长条件下的生长情况。使用数据分析技术,我们开发了动态生物量功能,可充当FBA等效物的忠实代理,从而降低大肠杆菌的GEM。这涉及将在动态模拟下生成的反应速率和代谢物浓度的数据与通过使用FBA进行稳态分析而获得的生物量的金标准目标数据进行合并。这也带来了许多关于成对条件下生物量通量的有趣见解。这些发现被复制到我们的动态代理功能中。

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