Targeted transcriptional downregulation of MYC using epigenomic controllers demonstrates antitumor activity in hepatocellular carcinoma models.
William SenapedisKayleigh M GallagherElmer FigueroaJeremiah D FarelliRobert LyngJ Graeme HodgsonCharles W O'DonnellJoseph V NewmanMadison PacaroStephen K SiecinskiJustin ChenThomas G McCauleyPublished in: Nature communications (2024)
Dysregulation of master regulator c-MYC (MYC) plays a central role in hepatocellular carcinoma (HCC) and other cancers but remains an elusive target for therapeutic intervention. MYC expression is epigenetically modulated within naturally occurring DNA loop structures, Insulated Genomic Domains (IGDs). We present a therapeutic approach using an epigenomic controller (EC), a programmable epigenomic mRNA medicine, to precisely modify MYC IGD sub-elements, leading to methylation of MYC regulatory elements and durable downregulation of MYC mRNA transcription. Significant antitumor activity is observed in preclinical models of HCC treated with the MYC-targeted EC, as monotherapy or in combination with tyrosine kinase or immune checkpoint inhibitors. These findings pave the way for clinical development of MYC-targeting epigenomic controllers in HCC patients and provide a framework for programmable epigenomic mRNA therapeutics for cancer and other diseases.
Keyphrases
- transcription factor
- tyrosine kinase
- cell proliferation
- randomized controlled trial
- end stage renal disease
- cancer therapy
- signaling pathway
- binding protein
- epidermal growth factor receptor
- newly diagnosed
- gene expression
- chronic kidney disease
- poor prognosis
- high resolution
- mesenchymal stem cells
- stem cells
- small molecule
- mass spectrometry
- drug delivery
- genome wide
- open label
- study protocol
- long noncoding rna
- circulating tumor cells
- heat shock protein