BET degrader exhibits lower antiproliferative activity than its inhibitor via EGR1 recruiting septins to promote E2F1-3 transcription in triple-negative breast cancer

溴尿嘧啶 BRD4 BET抑制剂 E2F1 癌症研究 转录因子 生物 三阴性乳腺癌 细胞周期 细胞生长 细胞生物学 分子生物学 表观遗传学 细胞 癌症 生物化学 乳腺癌 遗传学 基因
作者
Nan Liu,Shuai Wang,Munan Li,Nan Zhao,Deyu Wang,Rui Zhang,Mingxin Yu,Luoyi Zhao,Siwei Zhang,Fangbin Han,Ying Zhao,Quan Liu
出处
期刊:Pharmacological Research [Elsevier BV]
卷期号:208: 107377-107377 被引量:5
标识
DOI:10.1016/j.phrs.2024.107377
摘要

The bromodomain and extraterminal domain (BET) family proteins serve as primary readers of acetylated lysine residues and play crucial roles in cell proliferation and differentiation. Dysregulation of BET proteins has been implicated in tumorigenesis, making them important therapeutic targets. BET-bromodomain (BD) inhibitors and BET-targeting degraders have been developed to inhibit BET proteins. In this study, we found that the BET inhibitor MS645 exhibited superior antiproliferative activity than BET degraders including ARV771, AT1, MZ1 and dBET1 in triple-negative breast cancer (TNBC) cells. Treatment with MS645 led to the dissociation of BETs, MED1 and RNA polymerase II from the E2F1-3 promoter, resulting in the suppression of E2F1-3 transcription and subsequent inhibition of cell growth in TNBC. In contrast, while ARV771 displaced BET proteins from chromatin, it did not significantly alter E2F1-3 expression. Mechanistically, ARV771 induced BRD4 depletion at protein level, which markedly increased EGR1 expression. This elevation of EGR1 subsequently recruited septin 2 and septin 9 to E2F1-3 promoters, enhancing E2F1-3 transcription and promoting cell proliferation rate in vitro and in vivo. Our findings provide valuable insights into differential mechanisms of BET inhibition and highlight potential of developing BET-targeting molecules as therapeutic strategies for TNBC.
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