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Article ; Online: Targeting ESR1 mutation–induced transcriptional addiction in breast cancer with BET inhibition

Sm N. Udden / Qian Wang / Sunil Kumar / Venkat S. Malladi / Shwu-Yuan Wu / Shuguang Wei / Bruce A. Posner / Sophie Geboers / Noelle S. Williams / Yulun Liu / Jayesh K. Sharma / Ram S. Mani / Srinivas Malladi / Karla Parra / Mia Hofstad / Ganesh V. Raj / Jose M. Larios / Reshma Jagsi / Max S. Wicha /
Ben Ho Park / Gaorav P. Gupta / Arul M. Chinnaiyan / Cheng-Ming Chiang / Prasanna G. Alluri

JCI Insight, Vol 7, Iss

2022  Volume 17

Abstract: 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 ... ...

Abstract 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.
Keywords Oncology ; Medicine ; R
Subject code 616 ; 610
Language English
Publishing date 2022-09-01T00:00:00Z
Publisher American Society for Clinical investigation
Document type Article ; Online
Database BASE - Bielefeld Academic Search Engine (life sciences selection)

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