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Extraction of transcription regulatory signals from genome-wide DNA - protein interaction data

机译:从全基因组DNA-蛋白质相互作用数据中提取转录调控信号

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Deciphering gene regulatory network architecture amounts to the identification of the regulators, conditions in which they act, genes they regulate, cis-acting motifs they bind, expression profiles they dictate and more complex relationships between alternative regulatory partnerships and alternative regulatory motifs that give rise to sub-modalities of expression profiles. The 'location data' in yeast is a comprehensive resource that provides transcription factor-DNA interaction information in vivo. Here, we provide two contributions: first, we developed means to assess the extent of noise in the location data, and consequently for extracting signals from it. Second, we couple signal extraction with better characterization of the genetic network architecture. We apply two methods for the detection of combinatorial associations between transcription factors (TFs), the integration of which provides a global map of combinatorial regulatory interactions. We discover the capacity of regulatory motifs and TF partnerships to dictate fine-tuned expression patterns of subsets of genes, which are clearly distinct from those displayed by most genes assigned to the same TF. Our findings provide carefully prioritized, high-quality assignments between regulators and regulated genes and as such should prove useful for experimental and computational biologists alike.
机译:破译基因调控网络架构的过程包括鉴定调控因子,它们发挥作用的条件,它们调控的基因,它们所结合的顺式作用基序,它们所决定的表达谱以及替代性调控伙伴关系与替代性调控基序之间的更复杂的关系。表达谱的子模式。酵母中的“位置数据”是一种综合的资源,可在体内提供转录因子与DNA的相互作用信息。在此,我们提供了两个方面的贡献:首先,我们开发了一种方法来评估位置数据中的噪声程度,从而从中提取信号。其次,我们将信号提取与遗传网络架构的更好表征相结合。我们应用两种方法来检测转录因子(TF)之间的组合关联,其整合提供了组合调控相互作用的全局图。我们发现调节基序和TF伙伴关系的能力决定了基因子集的微调表达模式,这与指定给同一TF的大多数基因所显示的明显不同。我们的发现为调节剂和被调节基因之间提供了精心安排的高质量优先级分配,因此对于实验和计算生物学家均应证明是有用的。

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