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X-ray crystallography study and optimization of novel benzothiophene analogs as potent selective estrogen receptor covalent antagonists (SERCAs) with improved potency and safety profiles

Bioorg Chem. 2023-10; 
Chengfeng Bai, Yang Lv, Shuangshuang Xiong, Shuangjie Wu, Lin Qi, Shengnan Ren, Meiqi Zhu, Haijuan Dong, Hongtao Shen, Zhaoxing Li, Yinxue Zhu, Hui Ye, Haiping Hao, Yibei Xiao, Hua Xiang, Guoshun Luo
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Proteins, Expression, Isolation and Analysis … The codon-optimized genes encoding the ERα-LBD C417S, Y537S (297–554) were synthesized by GenScript and subcloned into BamHI and XhoI sites of a modified pET28a vector, … Get A Quote

摘要

Endocrine therapy (ET) is a well-validated strategy for estrogen receptor α positive (ERα?+?) breast cancer therapy. Despite the clinical success of current standard of care (SoC), endocrine-resistance inevitably emerges and remains a significant medical challenge. Herein, we describe the structural optimization and evaluation of a new series of selective estrogen receptor covalent antagonists (SERCAs) based on benzothiophene scaffold. Among them, compounds 15b and 39d were identified as two highly potent covalent antagonists, which exhibits superior antiproliferation activity than positive controls against MCF-7 cells and shows high selectivity over ERα negative (ERα-) cells. More importantly, their mode... More

關鍵詞

Breast cancer, Covalent antagonist, Estrogen receptor α, SERCAs
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