Constructing gene regulatory networks using epigenetic data

被引:17
|
作者
Sonawane, Abhijeet Rajendra [1 ,2 ,3 ]
DeMeo, Dawn L. [1 ,2 ]
Quackenbush, John [1 ,2 ,4 ]
Glass, Kimberly [1 ,2 ,4 ]
机构
[1] Brigham & Womens Hosp, Channing Div Network Med, 75 Francis St, Boston, MA 02115 USA
[2] Harvard Med Sch, Boston, MA 02115 USA
[3] Brigham & Womens Hosp, Div Cardiovasc Med, Ctr Interdisciplinary Cardiovasc Sci, 75 Francis St, Boston, MA 02115 USA
[4] Harvard Chan Sch Publ Hlth, Dept Biostat, Boston, MA 02115 USA
关键词
FACTOR-DNA-BINDING; TRANSCRIPTIONAL REGULATION; OPEN-CHROMATIN; LUNG-CANCER; IN-VIVO; ENHANCERS; CELLS; PROLIFERATION; SPECIFICITY; PROTEINS;
D O I
10.1038/s41540-021-00208-3
中图分类号
Q [生物科学];
学科分类号
07 ; 0710 ; 09 ;
摘要
The biological processes that drive cellular function can be represented by a complex network of interactions between regulators (transcription factors) and their targets (genes). A cell's epigenetic state plays an important role in mediating these interactions, primarily by influencing chromatin accessibility. However, how to effectively use epigenetic data when constructing a gene regulatory network remains an open question. Almost all existing network reconstruction approaches focus on estimating transcription factor to gene connections using transcriptomic data. In contrast, computational approaches for analyzing epigenetic data generally focus on improving transcription factor binding site predictions rather than deducing regulatory network relationships. We bridged this gap by developing SPIDER, a network reconstruction approach that incorporates epigenetic data into a message-passing framework to estimate gene regulatory networks. We validated SPIDER's predictions using ChIP-seq data from ENCODE and found that SPIDER networks are both highly accurate and include cell-line-specific regulatory interactions. Notably, SPIDER can recover ChIP-seq verified transcription factor binding events in the regulatory regions of genes that do not have a corresponding sequence motif. The networks estimated by SPIDER have the potential to identify novel hypotheses that will allow us to better characterize cell-type and phenotype specific regulatory mechanisms.
引用
收藏
页数:13
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