Endocrine resistance and breast cancer plasticity are controlled by CoREST.
Liliana Garcia-MartinezAndrew M AdamsHo Lam ChanYuichiro NakataNatalia WeichStephanie StranskyZhao ZhangMohamed AlshalalfaLeonor SarriaBrandon A MahalSusan B KesmodelToni Celià-TerrassaZhijie LiuSaverio MinucciDaniel BilbaoSimone SidoliRamiro E VerdunLluis MoreyPublished in: Nature structural & molecular biology (2022)
Resistance to cancer treatment remains a major clinical hurdle. Here, we demonstrate that the CoREST complex is a key determinant of endocrine resistance and ER + breast cancer plasticity. In endocrine-sensitive cells, CoREST is recruited to regulatory regions co-bound to ERα and FOXA1 to regulate the estrogen pathway. In contrast, during temporal reprogramming towards a resistant state, CoREST is recruited to AP-1 sites. In reprogrammed cells, CoREST favors chromatin opening, cJUN binding to chromatin, and gene activation by controlling SWI/SNF recruitment independently of the demethylase activity of the CoREST subunit LSD1. Genetic and pharmacological CoREST inhibition reduces tumorigenesis and metastasis of endocrine-sensitive and endocrine-resistant xenograft models. Consistently, CoREST controls a gene signature involved in invasiveness in clinical breast tumors resistant to endocrine therapies. Our studies reveal CoREST functions that are co-opted to drive cellular plasticity and resistance to endocrine therapies and tumorigenesis, thus establishing CoREST as a potential therapeutic target for the treatment of advanced breast cancer.