雄激素受体
前列腺癌
苯并噻唑
脚手架
雄激素
癌症研究
癌症
终端(电信)
前列腺
化学
医学
内分泌学
内科学
计算机科学
生物化学
激素
生物医学工程
电信
作者
Nane C. Kuznik,Valeria Solozobova,Nicole Jung,Simone Gräßle,Qing Lei,Eric M. Lewandowski,Ravi S. N. Munuganti,Amina Zoubeidi,Yu Chen,Stefan Bräse,Andrew C.B. Cato
标识
DOI:10.1021/acschembio.1c00390
摘要
All current clinically approved androgen deprivation therapies for prostate cancer target the C-terminal ligand-binding domain of the androgen receptor (AR). However, the main transactivation function of the receptor is localized at the AR N-terminal domain (NTD). Targeting the AR NTD directly is a challenge because of its intrinsically disordered structure and the lack of pockets for drugs to bind. Here, we have taken an alternative approach using the cochaperone BAG1L, which interacts with the NTD, to develop a novel AR inhibitor. We describe the identification of 2-(4-fluorophenyl)-5-(trifluoromethyl)-1,3-benzothiazole (A4B17), a small molecule that inhibits BAG1L-AR NTD interaction, attenuates BAG1L-mediated AR NTD activity, downregulates AR target gene expression, and inhibits proliferation of AR-positive prostate cancer cells. This compound represents a prototype of AR antagonists that could be key in the development of future prostate cancer therapeutics.
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