Genome-wide detection of enhancer-hijacking events from chromatin interaction data in rearranged genomes.
Xiaotao WangJie XuBaozhen ZhangYe HouFan SongHuijue LyuFeng YuePublished in: Nature methods (2021)
Recent efforts have shown that structural variations (SVs) can disrupt three-dimensional genome organization and induce enhancer hijacking, yet no computational tools exist to identify such events from chromatin interaction data. Here, we develop NeoLoopFinder, a computational framework to identify the chromatin interactions induced by SVs, including interchromosomal translocations, large deletions and inversions. Our framework can automatically resolve complex SVs, reconstruct local Hi-C maps surrounding the breakpoints, normalize copy number variation and allele effects and predict chromatin loops induced by SVs. We applied NeoLoopFinder in Hi-C data from 50 cancer cell lines and primary tumors and identified tens of recurrent genes associated with enhancer hijacking. To experimentally validate NeoLoopFinder, we deleted the hijacked enhancers in prostate adenocarcinoma cells using CRISPR-Cas9, which significantly reduced expression of the target oncogene. In summary, NeoLoopFinder enables identification of critical oncogenic regulatory elements that can potentially reveal therapeutic targets.
Keyphrases
- genome wide
- copy number
- transcription factor
- dna methylation
- mitochondrial dna
- binding protein
- crispr cas
- electronic health record
- big data
- gene expression
- prostate cancer
- dna damage
- induced apoptosis
- squamous cell carcinoma
- cell cycle arrest
- poor prognosis
- papillary thyroid
- genome editing
- radiation therapy
- young adults
- endoplasmic reticulum stress
- oxidative stress
- loop mediated isothermal amplification
- locally advanced
- rectal cancer
- single cell
- quality improvement
- long non coding rna
- deep learning