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Functional Dissection of Regulatory Models Using Gene Expression Data of Deletion Mutants

机译:利用缺失突变体的基因表达数据对调控模型进行功能剖析

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摘要

Genome-wide gene expression profiles accumulate at an alarming rate, how to integrate these expression profiles generated by different laboratories to reverse engineer the cellular regulatory network has been a major challenge. To automatically infer gene regulatory pathways from genome-wide mRNA expression profiles before and after genetic perturbations, we introduced a new Bayesian network algorithm: Deletion Mutant Bayesian Network (DM_BN). We applied DM_BN to the expression profiles of 544 yeast single or double deletion mutants of transcription factors, chromatin remodeling machinery components, protein kinases and phosphatases in S. cerevisiae. The network inferred by this method identified causal regulatory and non-causal concurrent interactions among these regulators (genetically perturbed genes) that are strongly supported by the experimental evidence, and generated many new testable hypotheses. Compared to networks reconstructed by routine similarity measures or by alternative Bayesian network algorithms, the network inferred by DM_BN excels in both precision and recall. To facilitate its application in other systems, we packaged the algorithm into a user-friendly analysis tool that can be downloaded at .
机译:全基因组范围内的基因表达谱以惊人的速度积累,如何整合不同实验室产生的这些表达谱以逆向工程化细胞调节网络一直是一个重大挑战。为了在遗传扰动之前和之后从全基因组mRNA表达谱自动推断基因调控途径,我们引入了一种新的贝叶斯网络算法:缺失突变贝叶斯网络(DM_BN)。我们将DM_BN应用于酿酒酵母中544个酵母单或双缺失突变体的转录因子,染色质重塑机器组件,蛋白激酶和磷酸酶的表达谱。通过这种方法推断出的网络在实验证据的强烈支持下,确定了这些调节因子之间的因果调节和非因果相互作用(遗传扰动的基因),并产生了许多新的可检验的假设。与通过常规相似性度量或通过替代贝叶斯网络算法重建的网络相比,由DM_BN推断的网络在精度和召回率方面均出色。为了方便其在其他系统中的应用,我们将该算法打包到一个易于使用的分析工具中,可以从下载该工具。

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