雌激素受体DNA结合域的破坏及相关分子内通讯的恢复可恢复耐药乳腺癌对他莫昔芬的敏感性。

Disruption of estrogen receptor DNA-binding domain and related intramolecular communication restores tamoxifen sensitivity in resistant breast cancer.

作者信息

Wang Li Hua, Yang Xiao Yi, Zhang Xiaohu, An Ping, Kim Han-Jong, Huang Jiaqiang, Clarke Robert, Osborne C Kent, Inman John K, Appella Ettore, Farrar William L

机构信息

Basic Research Program, SAIC-Frederick, National Cancer Institute-Frederick, Frederick, Maryland 21702, USA.

出版信息

Cancer Cell. 2006 Dec;10(6):487-99. doi: 10.1016/j.ccr.2006.09.015.

DOI:10.1016/j.ccr.2006.09.015

PMID:17157789

Abstract

A serious obstacle to successful treatment of estrogen receptor (ER)-positive human breast cancer is cell resistance to tamoxifen (TAM) therapy. Here we show that the electrophile disulfide benzamide (DIBA), an ER zinc finger inhibitor, blocks ligand-dependent and -independent cell growth of TAM-resistant breast cancer in vitro and in vivo. Such inhibition depends on targeting disruption of the ER DNA-binding domain and its communication with neighboring functional domains, facilitating ERalpha dissociation from its coactivator AIB1 and concomitant association with its corepressor NCoR bound to chromatin. DIBA does not affect phosphorylation of HER2, MAPK, AKT, and AIB1, suggesting that DIBA-modified ERalpha may induce a switch from agonistic to antagonistic effects of TAM on resistant breast cancer cells.

摘要

雌激素受体（ER）阳性的人类乳腺癌成功治疗的一个严重障碍是细胞对他莫昔芬（TAM）治疗产生抗性。我们在此表明，亲电试剂二硫代苯甲酰胺（DIBA）作为一种ER锌指抑制剂，在体外和体内均能阻断TAM抗性乳腺癌的配体依赖性和非依赖性细胞生长。这种抑制作用取决于靶向破坏ER DNA结合结构域及其与相邻功能结构域的通讯，促进ERα与其共激活因子AIB1解离，并同时与结合在染色质上的共抑制因子NCoR结合。DIBA不影响HER2、MAPK、AKT和AIB1的磷酸化，这表明DIBA修饰的ERα可能诱导TAM对耐药乳腺癌细胞的作用从激动效应转变为拮抗效应。

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雌激素受体DNA结合域的破坏及相关分子内通讯的恢复可恢复耐药乳腺癌对他莫昔芬的敏感性。

Disruption of estrogen receptor DNA-binding domain and related intramolecular communication restores tamoxifen sensitivity in resistant breast cancer.

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