Structure-Guided Design of a Domain-Selective Bromodomain and Extra Terminal N-Terminal Bromodomain Chemical Probe

Bradley, Erin; Fusani, Lucia; Chung, Chun-wa; Craggs, Peter D.; Demont, Emmanuel H.; Humphreys, Philip G.; Mitchell, Darren J.; Phillipou, Alex; Rioja, Inmaculada; Shah, Rishi R.; Wellaway, Christopher R.; Prinjha, Rab K.; Palmer, David S.; Kerr, William J.; Reid, Marc; Wall, Ian D.; Cookson, Rosa

doi:10.1021/acs.jmedchem.3c00906

Cited by 6 publications

(1 citation statement)

References 54 publications

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“…Acetylated piperidine ( S )-75 was the most potent compound accessed in the series to date, both from a biochemical and a hWB perspective. Interestingly, ( S )-75 was 100-fold more active at BRD4 BD1 over BRD4 BD2, consistent with what had been observed with the same chiral piperidine substituent on the previously prosecuted benzimidazole series . While the compound had desirable levels of FaSSIF solubility, the passive permeability of 10 nm/s highlighted a risk that oral bioavailability would be limited.…”

Section: Resultsmentioning

confidence: 99%

Structure- and Property-Based Optimization of Efficient Pan-Bromodomain and Extra Terminal Inhibitors to Identify Oral and Intravenous Candidate I-BET787

Hirst,

Bamborough,

Al-Mahdi

et al. 2024

J. Med. Chem.

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Section: Resultsmentioning

confidence: 99%

Structure- and Property-Based Optimization of Efficient Pan-Bromodomain and Extra Terminal Inhibitors to Identify Oral and Intravenous Candidate I-BET787

Hirst,

Bamborough,

Al-Mahdi

et al. 2024

J. Med. Chem.

Self Cite

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Collaborative GSK–University of Strathclyde doctoral research and training programmes: Transforming approaches to industry–academia engagement

Paterson,

Humphreys,

Kelly

et al. 2024

Drug Discovery Today

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Discovery of the First BRD4 Second Bromodomain (BD2)-Selective Inhibitors

Li,

Hu,

Zhu

et al. 2024

J. Med. Chem.

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Pan-BD2 inhibitors have been shown to retain an antileukemia effect and display less dose-limiting toxicities than pan-BET inhibitors. However, it is necessary to consider the potential off-target toxicity associated with the inhibition of four BET BD2 proteins. To date, no BRD4 BD2 domain selective inhibitor has been reported. Based on our previous pan-BD2 inhibitor 12 (XY153), we successfully identified 16o (XY221) as the first BRD4 BD2-selective inhibitor. 16o demonstrated potent binding affinity for BRD4 BD2 (IC 50 = 5.8 nM), along with high pan-BD2 selectivity (667-fold over BRD4 BD1) and BRD4 BD2 domain selectivity (9−32-fold over BRD2/3/T BD2). The BRD4 BD2 selectivity of 16o was further confirmed by the BLI assay, showing 66−144-fold selectivity over other BET BD2 domains. 16o exhibited good liver microsomal stability (T 1/2 > 120 min) and pharmacokinetic properties (F = 13.1%). These data indicate that 16o may serve as a valuable candidate for BRD4 BD2 advancing epigenetic research.

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Structure-Guided Design of a Domain-Selective Bromodomain and Extra Terminal N-Terminal Bromodomain Chemical Probe

Cited by 6 publications

References 54 publications

Structure- and Property-Based Optimization of Efficient Pan-Bromodomain and Extra Terminal Inhibitors to Identify Oral and Intravenous Candidate I-BET787

Structure- and Property-Based Optimization of Efficient Pan-Bromodomain and Extra Terminal Inhibitors to Identify Oral and Intravenous Candidate I-BET787

Collaborative GSK–University of Strathclyde doctoral research and training programmes: Transforming approaches to industry–academia engagement

Discovery of the First BRD4 Second Bromodomain (BD2)-Selective Inhibitors

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