| Literature DB >> 32424275 |
Mingjun Bi1, Zhao Zhang1, Yi-Zhou Jiang2, Pengya Xue1, Hu Wang1, Zhao Lai1, Xiaoyong Fu3, Carmine De Angelis3, Yue Gong2, Zhen Gao4, Jianhua Ruan1,4, Victor X Jin1, Elisabetta Marangoni5, Elodie Montaudon5, Christopher K Glass6, Wei Li7, Tim Hui-Ming Huang1, Zhi-Ming Shao2, Rachel Schiff3, Lizhen Chen8,9, Zhijie Liu10.
Abstract
Acquired therapy resistance is a major problem for anticancer treatment, yet the underlying molecular mechanisms remain unclear. Using an established breast cancer cellular model, we show that endocrine resistance is associated with enhanced phenotypic plasticity, indicated by a general downregulation of luminal/epithelial differentiation markers and upregulation of basal/mesenchymal invasive markers. Consistently, similar gene expression changes are found in clinical breast tumours and patient-derived xenograft samples that are resistant to endocrine therapies. Mechanistically, the differential interactions between oestrogen receptor α and other oncogenic transcription factors, exemplified by GATA3 and AP1, drive global enhancer gain/loss reprogramming, profoundly altering breast cancer transcriptional programs. Our functional studies in multiple culture and xenograft models reveal a coordinated role of GATA3 and AP1 in re-organizing enhancer landscapes and regulating cancer phenotypes. Collectively, our study suggests that differential high-order assemblies of transcription factors on enhancers trigger genome-wide enhancer reprogramming, resulting in transcriptional transitions that promote tumour phenotypic plasticity and therapy resistance.Entities:
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Year: 2020 PMID: 32424275 PMCID: PMC7737911 DOI: 10.1038/s41556-020-0514-z
Source DB: PubMed Journal: Nat Cell Biol ISSN: 1465-7392 Impact factor: 28.824