The NCOR-HDAC3 co-repressive complex modulates the leukemogenic potential of the transcription factor ERG.
Eitan KuglerShreyas MadiwaleDarren YongJulie A I ThomsYehudit BirgerDavid Brian SykesJohannes SchmoellerlAneta DrakulValdemar PriebeMuhammad YassinNasma AqaqeAvigail ReinHila FishmanIfat GeronChun-Wei David ChenBrian RaughtQiao LiuHeather OganaElisabeth LiedkeJean-Pierre BourquinJohannes ZuberMichael MilyavskyJohn E PimandaGilbert G PrivéShai IzraeliPublished in: Nature communications (2023)
The ERG (ETS-related gene) transcription factor is linked to various types of cancer, including leukemia. However, the specific ERG domains and co-factors contributing to leukemogenesis are poorly understood. Drug targeting a transcription factor such as ERG is challenging. Our study reveals the critical role of a conserved amino acid, proline, at position 199, located at the 3' end of the PNT (pointed) domain, in ERG's ability to induce leukemia. P199 is necessary for ERG to promote self-renewal, prevent myeloid differentiation in hematopoietic progenitor cells, and initiate leukemia in mouse models. Here we show that P199 facilitates ERG's interaction with the NCoR-HDAC3 co-repressor complex. Inhibiting HDAC3 reduces the growth of ERG-dependent leukemic and prostate cancer cells, indicating that the interaction between ERG and the NCoR-HDAC3 co-repressor complex is crucial for its oncogenic activity. Thus, targeting this interaction may offer a potential therapeutic intervention.
Keyphrases
- transcription factor
- acute myeloid leukemia
- bone marrow
- dna binding
- randomized controlled trial
- histone deacetylase
- mouse model
- emergency department
- genome wide identification
- signaling pathway
- squamous cell carcinoma
- dendritic cells
- dna methylation
- risk assessment
- papillary thyroid
- young adults
- lymph node metastasis
- adverse drug