Structure-Based Optimization of Naphthyridones into Potent ATAD2 Bromodomain Inhibitors

Paul Bamborough,Chun-wa Chung,Rebecca C. Furze,Paola Grandi,Anne-Marie Michon,Robert J. Sheppard,Heather Anne Barnett,Hawa Diallo,David P Dixon,Clement Douault,Emma Jones,Bhumika Karamshi,Darren Jason Mitchell,Rab K. Prinjha,Christina Rau,Robert J. Watson,Thilo Werner,Emmanuel Hubert Demont

Structure-Based Optimization of Naphthyridones into Potent ATAD2 Bromodomain Inhibitors

2015

Paul Bamborough
Chun-wa Chung
Rebecca C. Furze
Paola Grandi
Anne-Marie Michon
Robert J. Sheppard
Heather Anne Barnett
Hawa Diallo
David P Dixon
Clement Douault
Emma Jones
Bhumika Karamshi
Darren Jason Mitchell
Rab K. Prinjha
Christina Rau
Robert J. Watson
Thilo Werner
Emmanuel Hubert Demont

ATAD2 is a bromodomain-containing protein whose overexpression is linked to poor outcomes in a number of different cancer types. To date, no potent and selective inhibitors of the bromodomain have been reported. This article describes the structure-based optimization of a series of naphthyridones from micromolar leads with no selectivity over the BET bromodomains to inhibitors with sub-100 nM ATAD2 potency and 100-fold BET selectivity.

Keywords:

Chemistry
Biochemistry
Hydrolase
Bromodomain
Potency
Stereochemistry
Selectivity
structure based

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