Discovery and characterization of bromodomain 2–specific inhibitors of BRDT

Yu, Zhifeng; Ku, Angela F.; Anglin, Justin L.; Sharma, Rajesh; Ucisik, Melek N.; Faver, John C.; Li, Feng; Nyshadham, Pranavanand; Simmons, Nicholas; Sharma, Kiran; Nagarajan, Sureshbabu; Riehle, Kevin; Kaur, Gundeep; Sankaran, Banumathi; Storl-Desmond, Marta; Palmer, Stephen; Young, Damian W.; Kim, Choel; Matzuk, Martin M.

doi:10.1073/pnas.2021102118

Cited by 52 publications

(44 citation statements)

References 31 publications

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“…The BD1 and BD2 domains of each family member show a high level of homology (see the Supporting Information, Figure S2); however, there are some key differences in the binding site residues between these domains, which can be exploited to obtain selectivity . Indeed a number of highly selective compounds that bind preferentially to the four BD1 − or four BD2 − domains of this family have now been reported. It has been shown that the selective inhibition of the BD1 or BD2 domains of the BET proteins results in distinct biological phenotypes; , BD1-selective inhibitors appear to mostly phenocopy pan-BET, especially in oncology, while BD2-selective inhibitors show a more nuanced phenotype appropriate for the treatment of immune-mediated inflammatory diseases …”

Section: Introductionmentioning

confidence: 99%

Discovery of a Highly Selective BET BD2 Inhibitor from a DNA-Encoded Library Technology Screening Hit

et al. 2021

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Second-generation bromodomain and extra terminal (BET) inhibitors, which selectively target one of the two bromodomains in the BET proteins, have begun to emerge in the literature. These inhibitors aim to help determine the roles and functions of each domain and assess whether they can demonstrate an improved safety profile in clinical settings compared to pan-BET inhibitors. Herein, we describe the discovery of a novel BET BD2-selective chemotype using a structure-based drug design from a hit identified by DNA-encoded library technologies, showing a structural differentiation from key previously reported greater than 100-fold BD2-selective chemotypes GSK620, GSK046, and ABBV-744. Following a structure-based hypothesis for the selectivity and optimization of the physicochemical properties of the series, we identified 60 (GSK040), an in vitro ready and in vivo capable BET BD2-inhibitor of unprecedented selectivity (5000-fold) against BET BD1, excellent selectivity against other bromodomains, and good physicochemical properties. This novel chemical probe can be added to the toolbox used in the advancement of epigenetics research.

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Section: Introductionmentioning

confidence: 99%

Discovery of a Highly Selective BET BD2 Inhibitor from a DNA-Encoded Library Technology Screening Hit

et al. 2021

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“…The majority of reported BRD4 inhibitors target BD1 and BD2 indiscriminately. Recently, inhibitors that selectively target BD2 over BD1 revealed an important role of BD2 in the recruitment of BET proteins for gene expression and may provide more effective therapeutic options by avoiding the toxicity associated with inhibition of BD1. − Beyond prototypical BRD4 inhibitors, a series of compounds capable of concurrently inhibiting the KAc site of BRD4 and the adenosine triphosphate (ATP) site of certain kinases have been discovered. , Among these dual BRD4-kinase inhibitors are the diaminopyrimidine Janus kinase 2 (JAK2) inhibitors fedratinib and TG101209, the dihydropteridinone PLK1 inhibitors volasertib and BI2536, , and the benzopyrimidodiazipinones LRRK2-IN-1 and ERK5-IN-1. , While these kinase inhibitors have been studied in the context of BRD4 inhibition, their interaction with other BET bromodomains is unknown. Such information, however, may aid the development of BET inhibitors designed to simultaneously target certain BET bromodomains and kinases differentially, depending on the disease application.…”

Section: Introductionmentioning

confidence: 99%

Differential BET Bromodomain Inhibition by Dihydropteridinone and Pyrimidodiazepinone Kinase Inhibitors

et al. 2021

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BRD4 and other members of the bromodomain and extraterminal (BET) family of proteins are promising epigenetic targets for the development of novel therapeutics. Among the reported BRD4 inhibitors are dihydropteridinones and benzopyrimidodiazepinones originally designed to target the kinases PLK1, ERK5, and LRRK2. While these kinase inhibitors were identified as BRD4 inhibitors, little is known about their binding potential and structural details of interaction with the other BET bromodomains. We comprehensively characterized a series of known and newly identified dual BRD4-kinase inhibitors against all eight individual BET bromodomains. A detailed analysis of 23 novel cocrystal structures of BET-kinase inhibitor complexes in combination with direct binding assays and cell signaling studies revealed significant differences in molecular shape complementarity and inhibitory potential. Collectively, the data offer new insights into the action of kinase inhibitors across BET bromodomains, which may aid the development of drugs to inhibit certain BET proteins and kinases differentially.

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“…The compound RVX-208 was an early BD2-specific compound; however, it exhibited only moderate BD2 potency (>100 nM, IC 50 [the concentration that inhibits response by 50%] = 2 µM in our BRDT-BD2 AlphaScreen assay) and selectivity over BD1 domains (∼10-fold) ( 21 ). More recent efforts from other laboratories and ours have reported the synthesis of pan-BD2 inhibitors with significantly enhanced potency and selectivity [e.g., GSK046 ( 12 ), ABBV-744 ( 22 ), and our CDD-1302 compound ( 23 )].…”

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confidence: 99%

Discovery of potent BET bromodomain 1 stereoselective inhibitors using DNA-encoded chemical library selections

Modukuri

Tan

et al. 2022

Proc. Natl. Acad. Sci. U.S.A.

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Significance BET bromodomain inhibition is therapeutic in multiple diseases; however, pan-BET inhibitors have induced significant myelosuppression and gastrointestinal toxicity, perhaps due to inhibition of both tandem bromodomains (BD) of all BET family members. However, selective inhibition of just the first BD (BD1) phenocopies pan-BET inhibitor activity in preclinical models of cancer, other diseases, and, for BRDT, in the testes for a contraceptive effect. Here, we leveraged our multibillion-molecule collection of DNA-encoded chemical libraries (DECLs) to identify BET BD1-selective inhibitors of specific chirality with high potency, stability, and good cellular activity. Our findings highlight the robustness and efficiency of the DECL platform to identify specific, potent protein binders that have promise as potential anticancer and anti-inflammatory agents and as male contraceptives.

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Discovery and characterization of bromodomain 2–specific inhibitors of BRDT

Cited by 52 publications

References 31 publications

Discovery of a Highly Selective BET BD2 Inhibitor from a DNA-Encoded Library Technology Screening Hit

Discovery of a Highly Selective BET BD2 Inhibitor from a DNA-Encoded Library Technology Screening Hit

Differential BET Bromodomain Inhibition by Dihydropteridinone and Pyrimidodiazepinone Kinase Inhibitors

Discovery of potent BET bromodomain 1 stereoselective inhibitors using DNA-encoded chemical library selections

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