Discovery of Potent BET Bromodomain 1 Stereoselective Inhibitors Using DNA-Encoded Chemical Library Selections

Authors

Ram K Modukuri
Zhifeng Yu
Zhi Tan
Hai Minh Ta
Melek Nihan Ucisik
Zhuang Jin
Justin L Anglin
Kiran L Sharma
Pranavanand Nyshadham
Feng Li
Kevin Riehle
John C Faver
Kevin Duong
Sureshbabu Nagarajan
Nicholas Simmons
Stephen S Palmer
Mingxing Teng
Damian W Young
Joanna S Yi
Choel Kim
Martin M Matzuk

Language

English

Publication Date

5-31-2022

Journal

Proceedings of the National Academy of Sciences of the United States of America

DOI

10.1073/pnas.2122506119

PMID

35622893

PMCID

PMC9295786

PubMedCentral® Posted Date

5-27-2022

PubMedCentral® Full Text Version

Post-print

Abstract

BRDT, BRD2, BRD3, and BRD4 comprise the bromodomain and extraterminal (BET) subfamily which contain two similar tandem bromodomains (BD1 and BD2). Selective BD1 inhibition phenocopies effects of tandem BET BD inhibition both in cancer models and, as we and others have reported of BRDT, in the testes. To find novel BET BD1 binders, we screened >4.5 billion molecules from our DNA-encoded chemical libraries with BRDT-BD1 or BRDT-BD2 proteins in parallel. A compound series enriched only by BRDT-BD1 was resynthesized off-DNA, uncovering a potent chiral compound, CDD-724, with >2,000-fold selectivity for inhibiting BRDT-BD1 over BRDT-BD2. CDD-724 stereoisomers exhibited remarkable differences in inhibiting BRDT-BD1, with the R-enantiomer (CDD-787) being 50-fold more potent than the S-enantiomer (CDD-786). From structure–activity relationship studies, we produced CDD-956, which maintained picomolar BET BD1 binding potency and high selectivity over BET BD2 proteins and had improved stability in human liver microsomes over CDD-787. BROMOscan profiling confirmed the excellent pan-BET BD1 affinity and selectivity of CDD-787 and CDD-956 on BD1 versus BD2 and all other BD-containing proteins. A cocrystal structure of BRDT-BD1 bound with CDD-956 was determined at 1.82 Å and revealed BRDT-BD1–specific contacts with the αZ and αC helices that explain the high affinity and selectivity for BET BD1 versus BD2. CDD-787 and CDD-956 maintain cellular BD1-selectivity in NanoBRET assays and show potent antileukemic activity in acute myeloid leukemia cell lines. These BET BD1-specific and highly potent compounds are structurally unique and provide insight into the importance of chirality to achieve BET specificity.

Keywords

Anti-Inflammatory Agents, Non-Steroidal, Antineoplastic Agents, Contraceptive Agents, Male, DNA, Drug Discovery, Humans, Male, Nuclear Proteins, Protein Domains, Small Molecule Libraries, Structure-Activity Relationship, BET bromodomains, BRDT, DNA-encoded chemistry technology, small-molecule inhibitors

Published Open-Access

yes

Recommended Citation

Modukuri, Ram K; Yu, Zhifeng; Tan, Zhi; et al., "Discovery of Potent BET Bromodomain 1 Stereoselective Inhibitors Using DNA-Encoded Chemical Library Selections" (2022). Duncan NRI Faculty and Staff Publications. 192.
https://digitalcommons.library.tmc.edu/duncar_nri_pub/192