| Literature DB >> 28835800 |
David S Millan1, Katherine J Kayser-Bricker2, Matthew W Martin1, Adam C Talbot2, Shawn E R Schiller1, Torsten Herbertz1, Grace L Williams1, George P Luke2, Stephen Hubbs2, Monica A Alvarez Morales1, Daniel Cardillo1, Paul Troccolo1, Rachel L Mendes1, Crystal McKinnon1.
Abstract
A protein structure-guided drug design approach was employed to develop small molecule inhibitors of the BET family of bromodomains that were distinct from the known (+)-JQ1 scaffold class. These efforts led to the identification of a series of substituted benzopiperazines with structural features that enable interactions with many of the affinity-driving regions of the bromodomain binding site. Lipophilic efficiency was a guiding principle in improving binding affinity alongside drug-like physicochemical properties that are commensurate with oral bioavailability. Derived from this series was tool compound FT001, which displayed potent biochemical and cellular activity, translating to excellent in vivo activity in a mouse xenograft model (MV-4-11).Entities:
Keywords: BET; BRD4; Bromodomains
Year: 2017 PMID: 28835800 PMCID: PMC5554895 DOI: 10.1021/acsmedchemlett.7b00191
Source DB: PubMed Journal: ACS Med Chem Lett ISSN: 1948-5875 Impact factor: 4.345