Pharmacologic inhibition of BAF chromatin remodeling complexes as a therapeutic approach to transcription factor-dependent cancers

Author:

Centore Richard C.1,Soares Luis M. M.1,Topal Salih1,Vaswani Rishi G.1,Ichikawa Kana1,Li Zhifang1,Fan Hong1,Setser Jeremy W.1,Lahr David L.1,Zawadzke Laura E.1,Chen Xueying1,Barnash Kimberly D.1,Muwanguzi Jordana1,Anthony Neville1,Sandoval Gabriel J.1,Feldman Katharine1,Elliott GiNell1,Adam Ammar1,Huang David1,Davenport Yunji1,Schiller Shawn1,Wilson Kevin J.1,Voigt Johannes1,Xu Lan1,Hentemann Martin1,Millan David S.1,Chan Ho Man1,Decicco Carl P.1,Kruger Ryan G.1,Bellon Steven F.1

Affiliation:

1. Foghorn Therapeutics, 500 Technology Square

Abstract

The BRG/Brahma-associated factors (BAF or mSWI/SNF) family of chromatin remodeling complexes are critical regulators of gene expression and are major determinants of cancer and other diseases. Two paralog ATPases, SMARCA4 and SMARCA2 (BRG1 and BRM, respectively), provide the enzymatic activity required for chromatin remodeling. Here, we discover and characterize a novel series of compounds that potently and selectively inhibit SMARCA4/SMARCA2. Mutational and biochemical studies demonstrate that these inhibitors act through a unique mode of inhibition, distinct from reported SMARCA4/SMARCA2 inhibitors. Across a range of cancer cell lines, SMARCA4/SMARCA2 inhibition resulted in lineage-specific changes in chromatin accessibility at binding sites for key transcription factors (TFs). In uveal melanoma (UM), BAF inhibition resulted in loss of enhancer occupancy of SOX10 and MITF, two essential TFs, leading to down-regulation of the melanocytic gene expression program. In a mouse xenograft model of UM, SMARCA4/SMARCA2 inhibition was well tolerated and resulted in dose-dependent tumor regression correlating with pharmacodynamic modulation of BAF-target gene expression. These data provide the foundation for first-in-human studies of BAF ATPase inhibition as a novel therapeutic to treat TF-dependent cancers.

Publisher

eLife Sciences Publications, Ltd

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