| Literature DB >> 23322301 |
Hideo Watanabe1, Joshua M Francis, Michele S Woo, Banafsheh Etemad, Wenchu Lin, Daniel F Fries, Shouyong Peng, Eric L Snyder, Purushothama Rao Tata, Francesca Izzo, Anna C Schinzel, Jeonghee Cho, Peter S Hammerman, Roel G Verhaak, William C Hahn, Jayaraj Rajagopal, Tyler Jacks, Matthew Meyerson.
Abstract
The NKX2-1 transcription factor, a regulator of normal lung development, is the most significantly amplified gene in human lung adenocarcinoma. To study the transcriptional impact of NKX2-1 amplification, we generated an expression signature associated with NKX2-1 amplification in human lung adenocarcinoma and analyzed DNA-binding sites of NKX2-1 by genome-wide chromatin immunoprecipitation. Integration of these expression and cistromic analyses identified LMO3, itself encoding a transcription regulator, as a candidate direct transcriptional target of NKX2-1. Further cistromic and overexpression analyses indicated that NKX2-1 can cooperate with the forkhead box transcription factor FOXA1 to regulate LMO3 gene expression. RNAi analysis of NKX2-1-amplified cells compared with nonamplified cells demonstrated that LMO3 mediates cell survival downstream from NKX2-1. Our findings provide new insight into the transcriptional regulatory network of NKX2-1 and suggest that LMO3 is a transcriptional signal transducer in NKX2-1-amplified lung adenocarcinomas.Entities:
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Year: 2013 PMID: 23322301 PMCID: PMC3566312 DOI: 10.1101/gad.203208.112
Source DB: PubMed Journal: Genes Dev ISSN: 0890-9369 Impact factor: 11.361