Polycomb deficiency drives a FOXP2-high aggressive state targetable by epigenetic inhibitors.
Fan ChenAria L ByrdJinpeng LiuRobert M FlightTanner J DuCoteKassandra J NaughtonXiulong SongAbigail R GellertAlexsandr LukyanchukDanielle T DixonChristian M GosserDave-Preston EsoeRani D JayswalStuart H OrkinHunter N B MoseleyChi WangChristine Fillmore BrainsonPublished in: Nature communications (2023)
Inhibitors of the Polycomb Repressive Complex 2 (PRC2) histone methyltransferase EZH2 are approved for certain cancers, but realizing their wider utility relies upon understanding PRC2 biology in each cancer system. Using a genetic model to delete Ezh2 in KRAS-driven lung adenocarcinomas, we observed that Ezh2 haplo-insufficient tumors were less lethal and lower grade than Ezh2 fully-insufficient tumors, which were poorly differentiated and metastatic. Using three-dimensional cultures and in vivo experiments, we determined that EZH2-deficient tumors were vulnerable to H3K27 demethylase or BET inhibitors. PRC2 loss/inhibition led to de-repression of FOXP2, a transcription factor that promotes migration and stemness, and FOXP2 could be suppressed by BET inhibition. Poorly differentiated human lung cancers were enriched for an H3K27me3-low state, representing a subtype that may benefit from BET inhibition as a single therapy or combined with additional EZH2 inhibition. These data highlight diverse roles of PRC2 in KRAS-driven lung adenocarcinomas, and demonstrate the utility of three-dimensional cultures for exploring epigenetic drug sensitivities for cancer.
Keyphrases
- long noncoding rna
- long non coding rna
- regulatory t cells
- squamous cell
- dna methylation
- transcription factor
- papillary thyroid
- stem cells
- gene expression
- small cell lung cancer
- squamous cell carcinoma
- wild type
- childhood cancer
- genome wide
- bone marrow
- mesenchymal stem cells
- electronic health record
- adverse drug
- deep learning
- artificial intelligence