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CCAT: Combinatorial Code Analysis Tool for transcriptional regulation

机译:CCAT:用于转录调控的组合代码分析工具

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Combinatorial interplay among transcription factors (TFs) is an important mechanism by which transcriptional regulatory specificity is achieved. However, despite the increasing number of TFs for which either binding specificities or genome-wide occupancy data are known, knowledge about cooperativity between TFs remains limited. To address this, we developed a computational framework for predicting genome-wide co-binding between TFs (CCAT, Combinatorial Code Analysis Tool), and applied it to Drosophila melanogaster to uncover cooperativity among TFs during embryo development. Using publicly available TF binding specificity data and DNasel chromatin accessibility data, we first predicted genome-wide binding sites for 324 TFs across five stages of D. melanogaster embryo development. We then applied CCAT in each of these developmental stages, and identified from 19 to 58 pairs of TFs in each stage whose predicted binding sites are significantly co-localized. We found that nearby binding sites for pairs of TFs predicted to cooperate were enriched in regions bound in relevant ChIP experiments, and were more evolutionarily conserved than other pairs. Further, we found that TFs tend to be co-localized with other TFs in a dynamic manner across developmental stages. All generated data as well as source code for our front-to-end pipeline are available at http://cat.princeton.edu.
机译:转录因子(TFs)之间的组合相互作用是实现转录调控特异性的重要机制。但是,尽管已知结合特异性或全基因组占用数据的TF数量不断增加,但是关于TF之间协同作用的知识仍然有限。为了解决这个问题,我们开发了一个计算框架来预测TF之间的全基因组协同结合(CCAT,组合代码分析工具),并将其应用于果蝇(Drosophila melanogaster),以发现胚胎发育过程中TF之间的协同作用。使用公开可用的TF结合特异性数据和DNasel染色质可及性数据,我们首先预测了D. melanogaster胚胎发育五个阶段中324个TF的全基因组结合位点。然后,我们在这些发育阶段的每个阶段应用CCAT,并在每个阶段鉴定出19至58对TF,这些TF的预测结合位点明显共定位。我们发现,预计相关合作的TF对的附近结合位点在相关ChIP实验中结合的区域中富集,并且在进化上比其他对保守。此外,我们发现TF倾向于以跨开发阶段的动态方式与其他TF共定位。可从http://cat.princeton.edu获得所有生成的数据以及我们的前端管道的源代码。

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