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  • Interactome Rewiring Following Pharmacological Targeting of BET Bromodomains.

Interactome Rewiring Following Pharmacological Targeting of BET Bromodomains.

Molecular cell (2018-12-18)
Jean-Philippe Lambert, Sarah Picaud, Takao Fujisawa, Huayun Hou, Pavel Savitsky, Liis Uusküla-Reimand, Gagan D Gupta, Hala Abdouni, Zhen-Yuan Lin, Monika Tucholska, James D R Knight, Beatriz Gonzalez-Badillo, Nicole St-Denis, Joseph A Newman, Manuel Stucki, Laurence Pelletier, Nuno Bandeira, Michael D Wilson, Panagis Filippakopoulos, Anne-Claude Gingras
ABSTRACT

Targeting bromodomains (BRDs) of the bromo-and-extra-terminal (BET) family offers opportunities for therapeutic intervention in cancer and other diseases. Here, we profile the interactomes of BRD2, BRD3, BRD4, and BRDT following treatment with the pan-BET BRD inhibitor JQ1, revealing broad rewiring of the interaction landscape, with three distinct classes of behavior for the 603 unique interactors identified. A group of proteins associate in a JQ1-sensitive manner with BET BRDs through canonical and new binding modes, while two classes of extra-terminal (ET)-domain binding motifs mediate acetylation-independent interactions. Last, we identify an unexpected increase in several interactions following JQ1 treatment that define negative functions for BRD3 in the regulation of rRNA synthesis and potentially RNAPII-dependent gene expression that result in decreased cell proliferation. Together, our data highlight the contributions of BET protein modules to their interactomes allowing for a better understanding of pharmacological rewiring in response to JQ1.

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Anti-TCOF1 antibody produced in rabbit, Prestige Antibodies® Powered by Atlas Antibodies, affinity isolated antibody, buffered aqueous glycerol solution