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APG: an Active Protein-Gene Network Model to Quantify Regulatory Signals in Complex Biological Systems

机译:APG:一种活跃的蛋白质基因网络模型用于量化复杂生物系统中的调节信号

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摘要

Synergistic interactions among transcription factors (TFs) and their cofactors collectively determine gene expression in complex biological systems. In this work, we develop a novel graphical model, called Active Protein-Gene (APG) network model, to quantify regulatory signals of transcription in complex biomolecular networks through integrating both TF upstream-regulation and downstream-regulation high-throughput data. Firstly, we theoretically and computationally demonstrate the effectiveness of APG by comparing with the traditional strategy based only on TF downstream-regulation information. We then apply this model to study spontaneous type 2 diabetic Goto-Kakizaki (GK) and Wistar control rats. Our biological experiments validate the theoretical results. In particular, SP1 is found to be a hidden TF with changed regulatory activity, and the loss of SP1 activity contributes to the increased glucose production during diabetes development. APG model provides theoretical basis to quantitatively elucidate transcriptional regulation by modelling TF combinatorial interactions and exploiting multilevel high-throughput information.
机译:转录因子(TFs)及其辅因子之间的协同相互作用共同决定了复杂生物系统中的基因表达。在这项工作中,我们开发了一种新型的图形化模型,称为活性蛋白质基因(APG)网络模型,通过整合TF上游调控和下游调控高通量数据来量化复杂生物分子网络中转录的调控信号。首先,我们通过与仅基于TF下游调控信息的传统策略进行比较,从理论上和计算上证明了APG的有效性。然后,我们将这种模型应用于研究自发2型糖尿病后藤崎崎(GK)和Wistar对照大鼠。我们的生物学实验验证了理论结果。特别地,发现SP1是具有改变的调节活性的隐藏的TF,并且SP1活性的丧失有助于糖尿病发展期间葡萄糖生成的增加。 APG模型通过为TF组合相互作用建模并利用多级高通量信息为定量阐明转录调控提供理论基础。

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