化学
雷洛昔芬
亚甲蓝
结合
降级(电信)
乳腺肿瘤
合理设计
亚甲基
组合化学
乳腺癌
药理学
立体化学
有机化学
内科学
三苯氧胺
纳米技术
癌症
电信
催化作用
材料科学
数学分析
医学
光催化
计算机科学
数学
作者
Yu Zhang,Qiying Yu,Ziwei Wang,Luolong Qing,Xiaokui Mo,Bing Liu,Yoke Chin Chai,Bingqiong Yu,Yongxi Dong,Weidong Pan,Silong Zhang,Huan He
标识
DOI:10.1021/acs.jmedchem.5c00490
摘要
Small molecules capable of degrading estrogen receptor α (ERα) are of significant interest in breast cancer treatment. Herein, we rationally designed a series of ERα degraders (MR1–MR3) by conjugating methylene blue, a bifunctional photosensitizer, with the raloxifene pharmacophore. The lead compound MR3 exhibited high affinity to ERα, and it can induce a complete depletion of ERα in MCF7 breast cancer cells after 660 nm irradiation (0.4 W/cm2) for 1 min. Owing to the ERα degradation merit, MR3 displayed a 45-fold boosted anticancer activity (IC50 = 0.55 μM) after irradiation. In the breast cancer xenograft mouse model, MR3 induced an obvious tumor regression (tumor growth inhibition = 118%), which was superior to that of the FDA-approved ERα degrader Faslodex. These important features make MR3 extremely intriguing for breast cancer treatment.
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