Department of Radiation Oncology, University of Texas (UT) Southwestern Medical Center, Dallas, Texas, USA.
Department of Radiation Oncology and.
JCI Insight. 2022 Sep 8;7(17):e151851. doi: 10.1172/jci.insight.151851.
Acquired mutations in the ligand-binding domain (LBD) of the gene encoding estrogen receptor α (ESR1) are common mechanisms of endocrine therapy resistance in patients with metastatic ER+ breast cancer. The ESR1 Y537S mutation, in particular, is associated with development of resistance to most endocrine therapies used to treat breast cancer. Employing a high-throughput screen of nearly 1,200 Federal Drug Administration-approved (FDA-approved) drugs, we show that OTX015, a bromodomain and extraterminal domain (BET) inhibitor, is one of the top suppressors of ESR1 mutant cell growth. OTX015 was more efficacious than fulvestrant, a selective ER degrader, in inhibiting ESR1 mutant xenograft growth. When combined with abemaciclib, a CDK4/6 inhibitor, OTX015 induced more potent tumor regression than current standard-of-care treatment of abemaciclib + fulvestrant. OTX015 has preferential activity against Y537S mutant breast cancer cells and blocks their clonal selection in competition studies with WT cells. Thus, BET inhibition has the potential to both prevent and overcome ESR1 mutant-induced endocrine therapy resistance in breast cancer.
在转移性 ER+ 乳腺癌患者中,雌激素受体 α(ESR1)编码基因的配体结合域(LBD)获得性突变是内分泌治疗耐药的常见机制。特别是 ESR1 Y537S 突变与大多数用于治疗乳腺癌的内分泌治疗耐药的发展相关。我们采用近 1200 种美国食品和药物管理局(FDA)批准药物的高通量筛选,显示溴结构域和末端结构域(BET)抑制剂 OTX015 是抑制 ESR1 突变细胞生长的最佳抑制剂之一。与选择性 ER 降解剂氟维司群相比,OTX015 更能抑制 ESR1 突变异种移植物的生长。当与 CDK4/6 抑制剂阿贝西利联合使用时,与当前的标准治疗方案阿贝西利+氟维司群相比,OTX015 诱导更强的肿瘤消退。OTX015 对 Y537S 突变型乳腺癌细胞具有优先活性,并在与 WT 细胞的竞争研究中阻断其克隆选择。因此,BET 抑制有可能预防和克服乳腺癌中 ESR1 突变诱导的内分泌治疗耐药性。
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