Transcription factor 4 is a key mediator of oncogenesis in neuroblastoma by promoting MYC activity.
Nour A AljoudaDewan ShresthaChelsea DeVauxRachelle R OlsenSatyanarayana AlleboinaMegan WalkerYong ChengKevin W FreemanPublished in: Molecular oncology (2024)
Super-enhancer-associated transcription factor networks define cell identity in neuroblastoma (NB). Dysregulation of these transcription factors contributes to the initiation and maintenance of NB by enforcing early developmental identity states. We report that the class I basic helix-loop-helix (bHLH) transcription factor 4 (TCF4; also known as E2-2) is a critical NB dependency gene that significantly contributes to these identity states through heterodimerization with cell-identity-specific bHLH transcription factors. Knockdown of TCF4 significantly induces apoptosis in vitro and inhibits tumorigenicity in vivo. We used genome-wide expression profiling, TCF4 chromatin immunoprecipitation sequencing (ChIP-seq) and TCF4 immunoprecipitation-mass spectrometry to determine the role of TCF4 in NB cells. Our results, along with recent findings in NB for the transcription factors T-box transcription factor TBX2, heart- and neural crest derivatives-expressed protein 2 (HAND2) and twist-related protein 1 (TWIST1), propose a role for TCF4 in regulating forkhead box protein M1 (FOXM1)/transcription factor E2F-driven gene regulatory networks that control cell cycle progression in cooperation with N-myc proto-oncogene protein (MYCN), TBX2, and the TCF4 dimerization partners HAND2 and TWIST1. Collectively, we showed that TCF4 promotes cell proliferation through direct transcriptional regulation of the c-MYC/MYCN oncogenic program that drives high-risk NB. Mechanistically, our data suggest the novel finding that TCF4 acts to support MYC activity by recruiting multiple factors known to regulate MYC function to sites of colocalization between critical NB transcription factors, TCF4 and MYC oncoproteins. Many of the TCF4-recruited factors are druggable, giving insight into potential therapies for high-risk NB. This study identifies a new function for class I bHLH transcription factors (e.g., TCF3, TCF4, and TCF12) that are important in cancer and development.
Keyphrases
- transcription factor
- dna binding
- genome wide
- genome wide identification
- cell cycle
- cell proliferation
- mass spectrometry
- single cell
- heart failure
- stem cells
- machine learning
- epithelial mesenchymal transition
- dna methylation
- cell death
- ms ms
- oxidative stress
- dna damage
- big data
- high throughput
- cell therapy
- young adults
- cell cycle arrest
- atrial fibrillation
- artificial intelligence
- human immunodeficiency virus
- lymph node metastasis