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Estimating binding properties of transcription factors from genome-wide binding profiles

机译:从全基因组结合谱估计转录因子的结合特性

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The binding of transcription factors (TFs) is essential for gene expression. One important characteristic is the actual occupancy of a putative binding site in the genome. In this study, we propose an analytical model to predict genomic occupancy that incorporates the preferred target sequence of a TF in the form of a position weight matrix (PWM), DNA accessibility data (in the case of eukaryotes), the number of TF molecules expected to be bound specifically to the DNA and a parameter that modulates the specificity of the TF. Given actual occupancy data in the form of ChIP-seq profiles, we backwards inferred copy number and specificity for five Drosophila TFs during early embryonic development: Bicoid, Caudal, Giant, Hunchback and Kruppel. Our results suggest that these TFs display thousands of molecules that are specifically bound to the DNA and that whilst Bicoid and Caudal display a higher specificity, the other three TFs (Giant, Hunchback and Kruppel) display lower specificity in their binding (despite having PWMs with higher information content). This study gives further weight to earlier investigations into TF copy numbers that suggest a significant proportion of molecules are not bound specifically to the DNA.
机译:转录因子(TFs)的结合对于基因表达至关重要。一个重要的特征是基因组中假定的结合位点的实际占有。在这项研究中,我们提出了一种分析模型来预测基因组占有率,该模型以位置权重矩阵(PWM),DNA可及性数据(在真核生物的情况下),TF分子的数量的形式结合了TF的优选靶序列。预期与DNA特异性结合,并调节TF特异性的参数。给定ChIP-seq配置文件形式的实际占用数据,我们反向推论了早期胚胎发育过程中五种果蝇TF的拷贝数和特异性:Bicoid,Caudal,Giant,Hunchback和Kruppel。我们的结果表明,这些TF显示出数千种与DNA特异性结合的分子,而Bicoid和Caudal显示出更高的特异性,而其他三个TF(Giant,Hunchback和Kruppel)在其结合中显示出更低的特异性(尽管PWM与较高的信息含量)。这项研究进一步重视了对TF拷贝数的早期研究,该研究表明很大比例的分子未特异性结合到DNA。

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