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Exploring potential target genes of signaling pathways by predicting conserved transcription factor binding sites

机译:通过预测保守的转录因子结合位点来探索信号途径的潜在靶基因

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Many cellular signaling pathways induce gene expression by activating specific transcription factor complexes. Conventional approaches to the prediction of transcription factor binding sites lead to a notoriously high number of false discoveries. To alleviate this problem, we consider only binding sites that are conserved in man-mouse ge-nomic sequence comparisons. We employ two alternative methods for predicting binding sites: exact matches to validated binding site sequences and weight matrix scans. We then ask the question whether there is a characteristic association between a transcription factor or set thereof to a particular group of genes. Our approach is tested on genes, which are induced in dendritic cells in response to the cells' exposure to IPS. We chose this example because the underlying signaling pathways are well understood. We demonstrate the benefit of conserved predicted binding sites in interpreting the LPS experiment. Additionally, we find that both methods for the predictionof conserved binding sites complement one another. Finally, our results suggest a distinct role for SRF in the context of LPS-induced gene expression.
机译:许多细胞信号传导途径通过激活特异性转录因子复合物诱导基因表达。转录因子结合位点预测的常规方法导致了众所周知的大量错误发现。为了缓解这个问题,我们只考虑在人小鼠GE-Nomic序列比较中保守的绑定站点。我们采用两种替代方法来预测结合位点:对验证的绑定站点序列和权重矩阵扫描的精确匹配。然后,我们询问问题是否存在转录因子与特定基因组之间的特征关联。我们的方法是对基因进行测试,响应于细胞暴露于IPS的树突细胞中。我们选择了这个例子,因为潜在的信令途径很好地理解。我们展示了在解释LPS实验中的保守预测的结合位点的益处。另外,我们发现保守的结合位点的预测两种方法都是彼此的补充。最后,我们的结果表明在LPS诱导的基因表达的背景下对SRF具有明显的作用。

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