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Transcriptional and metabolic data integration and modeling for identification of active pathways

机译:转录和代谢数据集成和建模用于鉴定活性途径

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摘要

With the growing availability of omics data generated to describe different cells and tissues, the modeling and interpretation of such data has become increasingly important. Pathways are sets of reactions involving genes, metabolites, and proteins highlighting functional modules in the cell. Therefore, to discover activated or perturbed pathways when comparing two conditions, for example two different tissues, it is beneficial to use several types of omics data. We present a model that integrates transcriptomic and metabolomic data in order to make an informed pathway-level decision. Since metabolites can be seen as end-points of perturbations happening at the gene level, the gene expression data constitute the explanatory variables in a sparse regression model for the metabolite data. Sophisticated model selection procedures are developed to determine an appropriate model. We demonstrate that the transcript profiles can be used to informatively explain the metabolite data from cancer cell lines. Simulation studies further show that the proposed model offers a better performance in identifying active pathways than, for example, enrichment methods performed separately on the transcript and metabolite data.
机译:随着用于描述不同细胞和组织的组学数据的可用性不断提高,此类数据的建模和解释已变得越来越重要。途径是涉及基因,代谢产物和蛋白质的反应集,突出了细胞中的功能模块。因此,为了在比较两种条件(例如两种不同的组织)时发现激活的或受干扰的途径,使用几种类型的组学数据是有益的。我们提出了一个整合转录组和代谢组学数据的模型,以便做出明智的途径水平的决策。由于代谢物可以看作是在基因水平发生扰动的终点,因此基因表达数据构成了代谢物数据稀疏回归模型中的解释变量。开发了复杂的模型选择程序来确定适当的模型。我们证明了转录物谱可用于信息性地解释癌细胞系的代谢物数据。仿真研究进一步表明,与例如对转录物和代谢物数据分别进行的富集方法相比,所提出的模型在识别活性途径方面具有更好的性能。

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