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Discovery and optimization of novel N-benzyl-3, 6-dimethylbenzo [d] isoxazol-5-amine derivatives as potent and selective TRIM24 bromodomain inhibitors with …

Bioorganic Chemistry. 2019; 
Qingqing Hu , Chao Wang, Qiuping Xiang, Rui Wanga , Cheng Zhang, Maofeng Zhang, Xiaoqian Xue, Guolong Luo, Xiaomin Liu , Xishan Wu, Yan Zhang, Donghai Wu, Yong Xu
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Gene Synthesis cDNA encoding bromodomain of human TRIM24 (residues Gly896-Glu1014), BRD4 (1) (residues Asn44- Glu168), CREBBP (residues Arg1081-Gly1197), BRD9 (residues Leu14- Gln134) and BAZ2B (residues Ser1858-Ser1972) were synthesized by Genscript Get A Quote

摘要

Tripartite motif-containing protein 24 (TRIM24), recognized as an epigenetic reader for acetylated H3K23 (H3K23ac) via its bromodomain, has been closely involved in tumorigenesis or tumor progression of several cancers. Developing inhibitors of TRIM24 is significant for functional studies and drug discovery. Herein, we report the identification, optimization and evaluation of N-benzyl-3,6-dimethylbenzo[d]isoxazol-5-amines as TRIM24 bromodomain inhibitors starting from an in house library screening. Structure-based optimization leads to two potent and selective compounds 11d and 11h in an Alphascreen assay with IC50values of 1.88 μM and 2.53 μM, respectively. The viability assay demonstrates the gre... More

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