Epigenome-wide impact of MAT2A sustains the androgen-indifferent state and confers synthetic vulnerability in ERG fusion-positive prostate cancer.
Alessia CacciatoreDheeraj ShindeCarola MusumeciGiada SandriniLuca GuarreraDomenico AlbinoGianluca CivenniElisa StorelliSimone MosoleElisa FedericiAlessio FusinaMarta IozzoAndrea RinaldiMatteo PecoraroRoger GeigerMarco BolisCarlo Vittorio CatapanoGiuseppina M CarbonePublished in: Nature communications (2024)
Castration-resistant prostate cancer (CRPC) is a frequently occurring disease with adverse clinical outcomes and limited therapeutic options. Here, we identify methionine adenosyltransferase 2a (MAT2A) as a critical driver of the androgen-indifferent state in ERG fusion-positive CRPC. MAT2A is upregulated in CRPC and cooperates with ERG in promoting cell plasticity, stemness and tumorigenesis. RNA, ATAC and ChIP-sequencing coupled with histone post-translational modification analysis by mass spectrometry show that MAT2A broadly impacts the transcriptional and epigenetic landscape. MAT2A enhances H3K4me2 at multiple genomic sites, promoting the expression of pro-tumorigenic non-canonical AR target genes. Genetic and pharmacological inhibition of MAT2A reverses the transcriptional and epigenetic remodeling in CRPC models and improves the response to AR and EZH2 inhibitors. These data reveal a role of MAT2A in epigenetic reprogramming and provide a proof of concept for testing MAT2A inhibitors in CRPC patients to improve clinical responses and prevent treatment resistance.
Keyphrases
- dna methylation
- prostate cancer
- gene expression
- genome wide
- single cell
- mass spectrometry
- stem cells
- epithelial mesenchymal transition
- newly diagnosed
- ejection fraction
- climate change
- emergency department
- high throughput
- liquid chromatography
- cell therapy
- mesenchymal stem cells
- high resolution
- oxidative stress
- electronic health record
- prognostic factors
- long non coding rna
- combination therapy
- genome wide analysis