Discovery of a new chemical series of BRD4(1) inhibitors using protein-ligand docking and structure-guided design

Bryan C Duffy; Shuang Liu; Gregory S Martin; Ruifang Wang; Ming Min Hsia; He Zhao; Cheng Guo; Michael Ellis; John F Quinn; Olesya A Kharenko; Karen Norek; Emily M Gesner; Peter R Young; Kevin G McLure; Gregory S Wagner; Damodharan Lakshminarasimhan; Andre White; Robert K Suto; Henrik C Hansen; Douglas B Kitchen

doi:10.1016/j.bmcl.2015.04.107

Discovery of a new chemical series of BRD4(1) inhibitors using protein-ligand docking and structure-guided design

Bioorg Med Chem Lett. 2015 Jul 15;25(14):2818-23. doi: 10.1016/j.bmcl.2015.04.107. Epub 2015 May 11.

Authors

Bryan C Duffy¹, Shuang Liu¹, Gregory S Martin¹, Ruifang Wang¹, Ming Min Hsia¹, He Zhao¹, Cheng Guo¹, Michael Ellis¹, John F Quinn², Olesya A Kharenko³, Karen Norek³, Emily M Gesner³, Peter R Young³, Kevin G McLure³, Gregory S Wagner³, Damodharan Lakshminarasimhan⁴, Andre White⁴, Robert K Suto⁴, Henrik C Hansen³, Douglas B Kitchen⁵

Affiliations

¹ Albany Molecular Research (AMRI), 26 Corporate Circle, PO Box 15098, Albany, NY 12212-5098, USA.
² JFQuinn Consulting, 113 Jay St., Albany, NY 12210, USA.
³ Zenith Epigenetics Corp., Suite 300, 4820 Richard Road SW, Calgary, Alberta T3E 6L1, Canada.
⁴ Xtal BioStructures, Inc., 12 Michigan Dr., Natick, MA 01760, USA.
⁵ Albany Molecular Research (AMRI), 26 Corporate Circle, PO Box 15098, Albany, NY 12212-5098, USA. Electronic address: douglas.kitchen@amriglobal.com.

PMID: 26022843
DOI: 10.1016/j.bmcl.2015.04.107

Abstract

Bromodomains are key transcriptional regulators that are thought to be druggable epigenetic targets for cancer, inflammation, diabetes and cardiovascular therapeutics. Of particular importance is the first of two bromodomains in bromodomain containing 4 protein (BRD4(1)). Protein-ligand docking in BRD4(1) was used to purchase a small, focused screening set of compounds possessing a large variety of core structures. Within this set, a small number of weak hits each contained a dihydroquinoxalinone ring system. We purchased other analogs with this ring system and further validated the new hit series and obtained improvement in binding inhibition. Limited exploration by new analog synthesis showed that the binding inhibition in a FRET assay could be improved to the low μM level making this new core a potential hit-to-lead series. Additionally, the predicted geometries of the initial hit and an improved analog were confirmed by X-ray co-crystallography with BRD4(1).

Keywords: BRD4(1); Bromodomain inhibitors; Hit triage; Protein-ligand docking; Virtual screening.

MeSH terms

Binding Sites
Cell Cycle Proteins
Crystallography, X-Ray
Drug Design*
Drug Evaluation, Preclinical
Humans
Ligands*
Molecular Docking Simulation
Nuclear Proteins / antagonists & inhibitors*
Nuclear Proteins / metabolism
Protein Binding
Protein Structure, Tertiary
Quinoxalines / chemistry
Quinoxalines / metabolism
Structure-Activity Relationship
Transcription Factors / antagonists & inhibitors*
Transcription Factors / metabolism

Substances

BRD4 protein, human
Cell Cycle Proteins
Ligands
Nuclear Proteins
Quinoxalines
Transcription Factors