HYENA detects oncogenes activated by distal enhancers in cancer

Author:

Yu Anqi1,Yesilkanal Ali E1,Thakur Ashish2,Wang Fan1,Yang Yang1,Phillips William1,Wu Xiaoyang13,Muir Alexander13,He Xin2,Spitz Francois2,Yang Lixing123ORCID

Affiliation:

1. Ben May Department for Cancer Research, University of Chicago , Chicago ,  IL , USA

2. Department of Human Genetics, University of Chicago , Chicago ,  IL , USA

3. University of Chicago Comprehensive Cancer Center , Chicago , IL , USA

Abstract

Abstract Somatic structural variations (SVs) in cancer can shuffle DNA content in the genome, relocate regulatory elements, and alter genome organization. Enhancer hijacking occurs when SVs relocate distal enhancers to activate proto-oncogenes. However, most enhancer hijacking studies have only focused on protein-coding genes. Here, we develop a computational algorithm ‘HYENA’ to identify candidate oncogenes (both protein-coding and non-coding) activated by enhancer hijacking based on tumor whole-genome and transcriptome sequencing data. HYENA detects genes whose elevated expression is associated with somatic SVs by using a rank-based regression model. We systematically analyze 1146 tumors across 25 types of adult tumors and identify a total of 108 candidate oncogenes including many non-coding genes. A long non-coding RNA TOB1-AS1 is activated by various types of SVs in 10% of pancreatic cancers through altered 3-dimensional genome structure. We find that high expression of TOB1-AS1 can promote cell invasion and metastasis. Our study highlights the contribution of genetic alterations in non-coding regions to tumorigenesis and tumor progression.

Funder

University of Chicago

Comprehensive Cancer Center

National Institutes of Health

Publisher

Oxford University Press (OUP)

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