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Comparative Analysis of Yeast Metabolic Network Models Highlights Progress Opportunities for Metabolic Reconstruction

机译:酵母代谢网络模型的比较分析突出了代谢重建的进展和机遇

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摘要

We have compared 12 genome-scale models of the Saccharomyces cerevisiae metabolic network published since 2003 to evaluate progress in reconstruction of the yeast metabolic network. We compared the genomic coverage, overlap of annotated metabolites, predictive ability for single gene essentiality with a selection of model parameters, and biomass production predictions in simulated nutrient-limited conditions. We have also compared pairwise gene knockout essentiality predictions for 10 of these models. We found that varying approaches to model scope and annotation reflected the involvement of multiple research groups in model development; that single-gene essentiality predictions were affected by simulated medium, objective function, and the reference list of essential genes; and that predictive ability for single-gene essentiality did not correlate well with predictive ability for our reference list of synthetic lethal gene interactions (R = 0.159). We conclude that the reconstruction of the yeast metabolic network is indeed gradually improving through the iterative process of model development, and there remains great opportunity for advancing our understanding of biology through continued efforts to reconstruct the full biochemical reaction network that constitutes yeast metabolism. Additionally, we suggest that there is opportunity for refining the process of deriving a metabolic model from a metabolic network reconstruction to facilitate mechanistic investigation and discovery. This comparative study lays the groundwork for developing improved tools and formalized methods to quantitatively assess metabolic network reconstructions independently of any particular model application, which will facilitate ongoing efforts to advance our understanding of the relationship between genotype and cellular phenotype.
机译:我们比较了自2003年以来发布的酿酒酵母代谢网络的12个基因组规模模型,以评估酵母代谢网络重建的进展。我们比较了基因组覆盖率,带注释的代谢物的重叠,对单个基因必需性的预测能力以及一系列模型参数的选择,以及在模拟养分受限条件下的生物量生产预测。我们还比较了其中10个模型的成对基因敲除必需性预测。我们发现模型范围和注释的不同方法反映了多个研究小组在模型开发中的参与。单基因必需性预测受模拟培养基,目标函数和必需基因参考列表的影响;单基因必需性的预测能力与我们合成致死基因相互作用的参考清单的预测能力并没有很好的相关性(R = 0.159)。我们得出结论,通过模型开发的迭代过程,酵母代谢网络的确确实在逐步改善,并且通过继续努力重建构成酵母代谢的完整生化反应网络,仍然有很大的机会增进我们对生物学的理解。此外,我们建议有机会完善从代谢网络重建中导出代谢模型的过程,以促进机理研究和发现。这项比较研究为开发改进的工具和形式化方法奠定了基础,以独立于任何特定的模型应用程序来定量评估代谢网络的重建,这将促进正在进行的工作,以加深我们对基因型和细胞表型之间关系的理解。

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