溴尿嘧啶
BET抑制剂
选择性
化学
基因
生物化学
表观遗传学
催化作用
作者
S. Picaud,Christopher Wells,I. Felletar,Deborah H. Brotherton,Sarah Martin,P. Savitsky,Beatriz Díez-Dacal,Martin Philpott,C. Bountra,Hannah Lingard,O. Fedorov,Susanne Müller,Paul E. Brennan,Stefan Knapp,P. Filippakopoulos
标识
DOI:10.1073/pnas.1310658110
摘要
Bromodomains have emerged as attractive candidates for the development of inhibitors targeting gene transcription. Inhibitors of the bromo and extraterminal (BET) family recently showed promising activity in diverse disease models. However, the pleiotropic nature of BET proteins regulating tissue-specific transcription has raised safety concerns and suggested that attempts should be made for domain-specific targeting. Here, we report that RVX-208, a compound currently in phase II clinical trials, is a BET bromodomain inhibitor specific for second bromodomains (BD2s). Cocrystal structures revealed binding modes of RVX-208 and its synthetic precursor, and fluorescent recovery after photobleaching demonstrated that RVX-208 displaces BET proteins from chromatin. However, gene-expression data showed that BD2 inhibition only modestly affects BET-dependent gene transcription. Our data demonstrate the feasibility of specific targeting within the BET family resulting in different transcriptional outcomes and highlight the importance of BD1 in transcriptional regulation.
科研通智能强力驱动
Strongly Powered by AbleSci AI