Structure-Based Design of Highly Selective Inhibitors of the CREB Binding Protein Bromodomain

R. Aldrin Denny,Andrew C. Flick,Jotham Wadsworth Coe,Jonathan Langille,Arindrajit Basak,Shenping Liu,Ingrid A. Stock,Parag Sahasrabudhe,Paul D. Bonin,Duncan A. Hay,Paul E. Brennan,Mathew T. Pletcher,Lyn H. Jones,Eugene Lvovich Piatnitski Chekler

Structure-Based Design of Highly Selective Inhibitors of the CREB Binding Protein Bromodomain

2017

R. Aldrin Denny
Andrew C. Flick
Jotham Wadsworth Coe
Jonathan Langille
Arindrajit Basak
Shenping Liu
Ingrid A. Stock
Parag Sahasrabudhe
Paul D. Bonin
Duncan A. Hay
Paul E. Brennan
Mathew T. Pletcher
Lyn H. Jones
Eugene Lvovich Piatnitski Chekler

Chemical probes are required for preclinical target validation to interrogate novel biological targets and pathways. Selective inhibitors of the CREB binding protein (CREBBP)/EP300 bromodomains are required to facilitate the elucidation of biology associated with these important epigenetic targets. Medicinal chemistry optimization that paid particular attention to physiochemical properties delivered chemical probes with desirable potency, selectivity, and permeability attributes. An important feature of the optimization process was the successful application of rational structure-based drug design to address bromodomain selectivity issues (particularly against the structurally related BRD4 protein).

Keywords:

Potency
Combinatorial chemistry
CREB-binding protein
Biochemistry
Epigenetics
BRD4
Bromodomain
Medicinal chemistry
EP300
Biology
Computational biology
Chemistry
structure based
highly selective

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