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Dynamics of Time-Lagged Gene-to-Metabolite Networks of Escherichia coli Elucidated by Integrative Omics Approach

机译:整合组学方法阐明了时间滞后的基因-代谢网络的动力学

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摘要

In the postgenomics era, integrative analysis of several “omics” data is absolutely required for understanding the cell as a system. Integrative analysis of transcriptomics and metabolomics can lead to elucidation of gene-to-metabolite networks. When integrating different time series “omics” data, it is necessary to take into consideration a time lag between those data. In the present study, we conducted an integrative analysis of time series transcriptomics and metabolomics data of Escherichia coli generated by cDNA microarray and Fourier transform ion cyclotron resonance mass spectrometry (FT-ICR/MS), respectively. We identified a 60-min time lag between transition points of transcriptomics and metabolomics data by using a Linear Dynamical System. Furthermore, we investigated gene-to-metabolite correlations in the context of time lag, obtained the maximum number of correlated pairs at transcripts leading 60-min time lag, and finally revealed gene-to-metabolite relations in the phospholipid biosynthesis pathway. Taking into consideration the time lag between transcriptomics and metabolomics data in time series analysis could unravel novel gene-to-metabolite relations. According to gene-to-metabolite correlations, phosphatidylglycerol plays a more critical role for membrane balance than phosphatidylethanolamine in E. coli.
机译:在后基因组学时代,绝对需要对多个“组学”数据进行综合分析,才能将细胞理解为一个系统。转录组学和代谢组学的综合分析可导致阐明基因-代谢网络。在集成不同的时间序列“组学”数据时,有必要考虑这些数据之间的时滞。在本研究中,我们分别对cDNA芯片和傅里叶变换离子回旋共振质谱(FT-ICR / MS)生成的大肠杆菌的时间序列转录组学和代谢组学数据进行了综合分析。我们使用线性动力学系统确定了转录组学和代谢组学数据的转变点之间有60分钟的时间差。此外,我们在时滞的背景下调查了基因与代谢物的相关性,在导致60分钟时滞的转录本上获得了最大的相关对数,并最终揭示了磷脂生物合成途径中的基因与代谢物的关系。在时间序列分析中考虑转录组学和代谢组学数据之间的时间差可以揭示新型的基因-代谢关系。根据基因与代谢物的相关性,磷脂酰甘油对大肠杆菌的膜平衡起着比磷脂酰乙醇胺更重要的作用。

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