Abstract
Lung cancer is the leading cause of cancer-related death and lung adenocarcinoma is its most common subtype. Although genetic alterations have been identified as drivers in subsets of lung adenocarcinoma, they do not fully explain tumor development. Epigenetic alterations have been implicated in the pathogenesis of tumors. To identify epigenetic alterations driving lung adenocarcinoma, we used an improved version of the Tracing Enhancer Networks using Epigenetic Traits method (TENET 2.0) in primary normal lung and lung adenocarcinoma cells. We found over 32,000 enhancers that appear differentially activated between normal lung and lung adenocarcinoma. Among the identified transcriptional regulators inactivated in lung adenocarcinoma vs. normal lung, NKX2-1 was linked to a large number of silenced enhancers. Among the activated transcriptional regulators identified, CENPA, FOXM1, and MYBL2 were linked to numerous cancer-specific enhancers. High expression of CENPA, FOXM1, and MYBL2 is particularly observed in a subgroup of lung adenocarcinomas and is associated with poor patient survival. Notably, CENPA, FOXM1, and MYBL2 are also key regulators of cancer-specific enhancers in breast adenocarcinoma of the basal subtype, but they are associated with distinct sets of activated enhancers. We identified individual lung adenocarcinoma enhancers linked to CENPA, FOXM1, or MYBL2 that were associated with poor patient survival. Knockdown experiments of FOXM1 and MYBL2 suggest that these factors regulate genes involved in controlling cell cycle progression and cell division. For example, we found that expression of TK1, a potential target gene of a MYBL2-linked enhancer, is associated with poor patient survival. Identification and characterization of key transcriptional regulators and associated enhancers in lung adenocarcinoma provides important insights into the deregulation of lung adenocarcinoma epigenomes, highlighting novel potential targets for clinical intervention.
Highlights
Lung cancer is the second most commonly diagnosed form of cancer and the leading cause of cancer-related death in both men and women [1]
We identified NKX2-1 as a transcriptional regulator inactivated in lung adenocarcinoma, linked to a large number of enhancers silenced in cancer
Among the activated transcriptional regulators, CENPA, MYBL2, and FOXM1 were linked to numerous cancer-specific enhancers and high expression of these regulators was observed in a subgroup of lung adenocarcinomas showing poor patient survival
Summary
Lung cancer is the second most commonly diagnosed form of cancer and the leading cause of cancer-related death in both men and women [1]. Lung adenocarcinoma (LUAD) arises in the alveolar epithelium of the lung and comprises almost 50% of all lung cancer cases in the United States [2]. Major risk factors for LUAD include tobacco smoking, inherited genetic factors, diet, alcohol consumption, exposure to sources of ionizing radiation and environmental contaminants [3,4]. These risk factors induce molecular and cellular changes in alveolar epithelial cells, leading these purported cells of origin to form LUAD. Approximately a quarter of LUAD cases do not possess any of these genetic alterations [7], suggesting that other molecular changes likely contribute to lung cancer development
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