| Literature DB >> 29625054 |
Han Chen1, Chunyan Li2, Xinxin Peng1, Zhicheng Zhou3, John N Weinstein3, Han Liang4.
Abstract
The role of enhancers, a key class of non-coding regulatory DNA elements, in cancer development has increasingly been appreciated. Here, we present the detection and characterization of a large number of expressed enhancers in a genome-wide analysis of 8928 tumor samples across 33 cancer types using TCGA RNA-seq data. Compared with matched normal tissues, global enhancer activation was observed in most cancers. Across cancer types, global enhancer activity was positively associated with aneuploidy, but not mutation load, suggesting a hypothesis centered on "chromatin-state" to explain their interplay. Integrating eQTL, mRNA co-expression, and Hi-C data analysis, we developed a computational method to infer causal enhancer-gene interactions, revealing enhancers of clinically actionable genes. Having identified an enhancer ∼140 kb downstream of PD-L1, a major immunotherapy target, we validated it experimentally. This study provides a systematic view of enhancer activity in diverse tumor contexts and suggests the clinical implications of enhancers.Entities:
Keywords: PD-L1 expression; The Cancer Genome Atlas; aneuploidy; chromatin state; enhancer expression; mutation burden; pan-cancer analysis; prognostic markers
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Year: 2018 PMID: 29625054 PMCID: PMC5890960 DOI: 10.1016/j.cell.2018.03.027
Source DB: PubMed Journal: Cell ISSN: 0092-8674 Impact factor: 41.582