Targeting the CoREST complex with dual histone deacetylase and demethylase inhibitors

Author:

Kalin Jay H.,Wu Muzhou,Gomez Andrea V.,Song Yun,Das Jayanta,Hayward Dawn,Adejola Nkosi,Wu Mingxuan,Panova Izabela,Chung Hye Jin,Kim Edward,Roberts Holly J.,Roberts Justin M.ORCID,Prusevich Polina,Jeliazkov Jeliazko R.,Roy Burman Shourya S.,Fairall Louise,Milano Charles,Eroglu Abdulkerim,Proby Charlotte M.,Dinkova-Kostova Albena T.,Hancock Wayne W.,Gray Jeffrey J.ORCID,Bradner James E.ORCID,Valente Sergio,Mai Antonello,Anders Nicole M.,Rudek Michelle A.,Hu Yong,Ryu Byungwoo,Schwabe John W. R.,Mattevi AndreaORCID,Alani Rhoda M.,Cole Philip A.

Abstract

Abstract Here we report corin, a synthetic hybrid agent derived from the class I HDAC inhibitor (entinostat) and an LSD1 inhibitor (tranylcypromine analog). Enzymologic analysis reveals that corin potently targets the CoREST complex and shows more sustained inhibition of CoREST complex HDAC activity compared with entinostat. Cell-based experiments demonstrate that corin exhibits a superior anti-proliferative profile against several melanoma lines and cutaneous squamous cell carcinoma lines compared to its parent monofunctional inhibitors but is less toxic to melanocytes and keratinocytes. CoREST knockdown, gene expression, and ChIP studies suggest that corin’s favorable pharmacologic effects may rely on an intact CoREST complex. Corin was also effective in slowing tumor growth in a melanoma mouse xenograft model. These studies highlight the promise of a new class of two-pronged hybrid agents that may show preferential targeting of particular epigenetic regulatory complexes and offer unique therapeutic opportunities.

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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