Discovery of Epigenetic Regulator I-Bet762: Lead Optimization to Afford a Clinical Candidate Inhibitor of the Bet Bromodomains.

Olivier Mirguet,Romain Luc Marie Gosmini,Jérôme Toum,Catherine A. Clement,Mélanie Barnathan,Jean-Marie Brusq,Jacqueline Elizabeth Mordaunt,Richard Martin Grimes,Miriam Crowe,Olivier Pineau,Myriam Ajakane,Alain Claude-Marie Daugan,Phillip Jeffrey,Leanne Cutler,Andrea Haynes,Nicholas Smithers,Chun-wa Chung,Paul Bamborough,Iain Uings,Antonia Lewis,Jason Witherington,Nigel James Parr,Rab K. Prinjha,Edwige Nicodeme

Discovery of Epigenetic Regulator I-Bet762: Lead Optimization to Afford a Clinical Candidate Inhibitor of the Bet Bromodomains.

2013

The bromo and extra C-terminal domain (BET) family of bromodomains are involved in binding epigenetic marks on histone proteins, more specifically acetylated lysine residues. This paper describes the discovery and structure–activity relationships (SAR) of potent benzodiazepine inhibitors that disrupt the function of the BET family of bromodomains (BRD2, BRD3, and BRD4). This work has yielded a potent, selective compound I-BET762 that is now under evaluation in a phase I/II clinical trial for nuclear protein in testis (NUT) midline carcinoma and other cancers.

Keywords:

Acetylation
Nuclear protein
Lysine
Histone
Biochemistry
Bromodomain
BRD4
Biology
Epigenetics
Regulator
Chemistry

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