髓系白血病
药理学
癌症
化学
癌症研究
髓样
化疗
癌症治疗
白血病
癌症治疗
毒性
医学
癌细胞
药品
细胞培养
肉瘤
肿瘤细胞
癌细胞系
细胞生长
口服
内科学
机制(生物学)
生物活性
恶性细胞
联合疗法
作者
Yumin Huang,Guizhen Cheng,Xin Tang,Zhiming Chen,Cheng Zhang,Jiankang Hu,Xiaoshan Chen,Di Wu,Zhaoming Chen,Mohan zhao,Jinsong Liu,Tingting Xu,Jinming Ma,Yan Zhang,Bin Lin,H. F. Shen,Yong Xu
标识
DOI:10.1021/acs.jmedchem.5c02858
摘要
BRD9, a unique component of the ncBAF complex, has emerged as a promising therapeutic target in various cancers such as synovial sarcoma (SS) and acute myeloid leukemia (AML). Herein, we report the design, synthesis, and biological evaluation of BRD9 PROTACs based on diverse cereblon-binding ligands. Through structure–activity study, we identified 32 (XYD270) as a highly potent PROTAC demonstrating excellent degradation activity in HS-SY-II cells (DC 50 = 0.082 nM, D max = 96%) and MV4;11 cells (DC 50 = 3.9 nM, D max = 90%). Notably, 32 displayed robust antiproliferative activity in MV4;11 cells (IC 50 = 50 nM) and HS-SY-II cells (IC 50 = 1.65 μM). In an MV4;11 xenograft model, once-daily administration of 32 (10 mg/kg) achieved significant tumor growth inhibition (TGI = 54%). Taken together, our findings establish 32 as a promising BRD9 PROTAC with compelling preclinical efficacy in SS and AML.
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