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基于非齐次泊松过程模型的转录因子簇检测。

Detecting clusters of transcription factors based on a nonhomogeneous poisson process model.

机构信息

Department of Statistics, Virginia Tech, 250 Drillfield Drive, Blacksburg, VA, 24061, USA.

Department of Mathematics, Virginia Tech, 225 Stanger Street, Blacksburg, VA, 24061, USA.

出版信息

BMC Bioinformatics. 2022 Dec 9;23(1):535. doi: 10.1186/s12859-022-05090-2.

Abstract

BACKGROUND

Rapidly growing genome-wide ChIP-seq data have provided unprecedented opportunities to explore transcription factor (TF) binding under various cellular conditions. Despite the rich resources, development of analytical methods for studying the interaction among TFs in gene regulation still lags behind.

RESULTS

In order to address cooperative TF binding and detect TF clusters with coordinative functions, we have developed novel computational methods based on clustering the sample paths of nonhomogeneous Poisson processes. Simulation studies demonstrated the capability of these methods to accurately detect TF clusters and uncover the hierarchy of TF interactions. A further application to the multiple-TF ChIP-seq data in mouse embryonic stem cells (ESCs) showed that our methods identified the cluster of core ESC regulators reported in the literature and provided new insights on functional implications of transcrisptional regulatory modules.

CONCLUSIONS

Effective analytical tools are essential for studying protein-DNA relations. Information derived from this research will help us better understand the orchestration of transcription factors in gene regulation processes.

摘要

背景

快速增长的全基因组 ChIP-seq 数据为在各种细胞条件下探索转录因子 (TF) 结合提供了前所未有的机会。尽管资源丰富,但用于研究基因调控中 TF 之间相互作用的分析方法的发展仍然滞后。

结果

为了解决协同 TF 结合并检测具有协调功能的 TF 簇,我们开发了基于聚类非齐次泊松过程样本路径的新计算方法。模拟研究表明,这些方法能够准确检测 TF 簇并揭示 TF 相互作用的层次结构。进一步将这些方法应用于小鼠胚胎干细胞 (ESC) 的多 TF ChIP-seq 数据表明,我们的方法识别了文献中报道的核心 ESC 调节剂簇,并提供了关于转录调控模块功能意义的新见解。

结论

有效的分析工具对于研究蛋白质-DNA 关系至关重要。该研究提供的信息将帮助我们更好地理解转录因子在基因调控过程中的协调作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3218/9738027/894162146eb5/12859_2022_5090_Fig1_HTML.jpg

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