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Literature DB >> 31531200

Systematically Mitigating the p38α Activity of Triazole-based BET Inhibitors.

Angela S Carlson¹, Huarui Cui¹, Anand Divakaran¹, Jorden A Johnson¹, Ryan M Brunner¹, William C K Pomerantz¹, Joseph J Topczewski¹.

Abstract

The Bromodomain and Extra Terminal (BET) family of proteins recognize post-translational N-ε-acetylated lysine modifications, regulating transcription as "reader" proteins. Bromodomain inhibitors are interesting targets for the development of potential cancer, inflammation, and heart disease treatments. Several dual kinase-bromodomain inhibitors have been identified by screening kinase inhibitor libraries against BET proteins. Although potentially useful from a polypharmacology standpoint, multitarget binding complicates deciphering molecular mechanisms. This report describes a systematic approach to mitigating kinase activity in a dual kinase-bromodomain inhibitor based on a 1,2,3-triazole-pyrimidine core. By modifying the triazole substituent and altering the pyrimidine core, this structure-activity relationship study enhanced BET activity while reducing the p38α kinase activity >90,000-fold. A BRD4-D1 cocrystal structure indicates that the 1,2,3-triazole is acting as a N-ε-acetylated lysine mimic. A BRD4 sensitive cell line, MM.1S, was used to demonstrate activity in cells, which is further supported by reduced c-Myc expression.

Entities: Chemical Disease Gene

Year: 2019 PMID： 31531200 PMCID： PMC6746085 DOI： 10.1021/acsmedchemlett.9b00227

Source DB: PubMed Journal: ACS Med Chem Lett ISSN： 1948-5875 Impact factor: 4.345

29 in total

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8. Development of a fluorescent-tagged kinase assay system for the detection and characterization of allosteric kinase inhibitors.

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4. Selective N-Terminal BET Bromodomain Inhibitors by Targeting Non-Conserved Residues and Structured Water Displacement*.

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Review 9. Perfluorocarbons in Chemical Biology.

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10. 4-Methyl-1,2,3-Triazoles as N-Acetyl-Lysine Mimics Afford Potent BET Bromodomain Inhibitors with Improved Selectivity.

Authors: Huarui Cui; Angela S Carlson; Mary A Schleiff; Anand Divakaran; Jorden A Johnson; Caroline R Buchholz; Huda Zahid; Nora R Vail; Ke Shi; Hideki Aihara; Daniel A Harki; Grover P Miller; Joseph J Topczewski; William C K Pomerantz
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10 in total