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Flux balance analysis with or without molecular crowding fails to predict two thirds of experimentally observed epistasis in yeast

机译:有或没有分子拥挤的通量平衡分析无法预测酵母中实验观察到的上位性的三分之二

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摘要

Computational predictions of double gene knockout effects by flux balance analysis (FBA) have been used to characterized genome-wide patterns of epistasis in microorganisms. However, it is unclear how in silico predictions are related to in vivo epistasis, as FBA predicted only a minority of experimentally observed genetic interactions between non-essential metabolic genes in yeast. Here, we perform a detailed comparison of yeast experimental epistasis data to predictions generated with different constraint-based metabolic modeling algorithms. The tested methods comprise standard FBA; a variant of MOMA, which was specifically designed to predict fitness effects of non-essential gene knockouts; and two alternative implementations of FBA with macro-molecular crowding, which account approximately for enzyme kinetics. The number of interactions uniquely predicted by one method is typically larger than its overlap with any alternative method. Only 20% of negative and 10% of positive interactions jointly predicted by all methods are confirmed by the experimental data; almost all unique predictions appear to be false. More than two thirds of epistatic interactions are undetectable by any of the tested methods. The low prediction accuracies indicate that the physiology of yeast double metabolic gene knockouts is dominated by processes not captured by current constraint-based analysis methods.
机译:通过通量平衡分析(FBA)对双基因敲除作用的计算预测已用于表征微生物上皮的全基因组分布模式。但是,目前尚不清楚计算机模拟的预测与体内上皮的关系如何,因为FBA仅预测了酵母中非必需代谢基因之间的少数实验观察到的遗传相互作用。在这里,我们执行酵母实验上位数据与使用不同基于约束的代谢建模算法生成的预测的详细比较。测试方法包括标准FBA; MOMA的一种变体,专门设计用于预测非必需基因敲除的适应性影响;以及具有大分子拥挤的FBA的两种替代实现方式,这些实现方式大约可以解释酶的动力学。通过一种方法唯一预测的交互作用的数量通常大于其与任何其他方法的重叠。实验数据证实了所有方法共同预测的负相互作用的20%和正相互作用的10%。几乎所有独特的预测似乎都是错误的。通过任何一种测试方法都无法检测到超过三分之二的上位相互作用。较低的预测准确度表明,酵母双代谢基因敲除的生理机制主要受当前基于约束的分析方法未捕获的过程的控制。

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