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Gene expression analysis on biochemical networks using the Potts spin model.

机译:使用Potts自旋模型对生化网络进行基因表达分析。

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MOTIVATION: Microarray technology allows us to profile the expression of a large subset or all genes of a cell. Biochemical research over the last three decades has elucidated an increasingly complete image of the metabolic architecture. For less complex organisms, such as Escherichia coli, the biochemical network has been described in much detail. Here, we investigate the clustering of such networks by applying gene expression data that define edge lengths in the network. RESULTS: The Potts spin model is used as a nearest neighbour based clustering algorithm to discover fragmentation of the network in mutants or in biological samples when treated with drugs. As an example, we tested our method with gene expression data from E.coli treated with tryptophan excess, starvation and trpyptophan repressor mutants. We observed fragmentation of the tryptophan biosynthesis pathway, which corresponds well to the commonly known regulatory response of the cells.
机译:动机:微阵列技术使我们能够分析细胞的大部分或全部基因的表达。在过去的三十年中,生物化学研究已经阐明了新陈代谢结构的完整图像。对于不太复杂的生物,例如大肠杆菌,已经详细描述了生化网络。在这里,我们通过应用定义网络边缘长度的基因表达数据来研究此类网络的聚类。结果:Potts自旋模型被用作基于最近邻的聚类算法,以发现用药物处理后的突变体或生物样品中网络的碎片。举例来说,我们使用来自大肠杆菌的基因表达数据测试了我们的方法,该基因经过色氨酸过量,饥饿和三磷酸色氨酸阻遏物突变体处理。我们观察到色氨酸生物合成途径的片段化,这与细胞众所周知的调节反应非常吻合。

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