| Literature DB >> 32888433 |
Amaia Arruabarrena-Aristorena1, Jesper L V Maag2, Srushti Kittane1, Yanyan Cai3, Wouter R Karthaus1, Erik Ladewig4, Jane Park2, Srinivasaraghavan Kannan5, Lorenzo Ferrando6, Emiliano Cocco1, Sik Y Ho7, Daisylyn S Tan7, Mirna Sallaku1, Fan Wu1, Barbara Acevedo8, Pier Selenica3, Dara S Ross3, Matthew Witkin2, Charles L Sawyers1, Jorge S Reis-Filho3, Chandra S Verma9, Ralf Jauch7, Richard Koche2, José Baselga10, Pedram Razavi11, Eneda Toska12, Maurizio Scaltriti13.
Abstract
Mutations in the pioneer transcription factor FOXA1 are a hallmark of estrogen receptor-positive (ER+) breast cancers. Examining FOXA1 in ∼5,000 breast cancer patients identifies several hotspot mutations in the Wing2 region and a breast cancer-specific mutation SY242CS, located in the third β strand. Using a clinico-genomically curated cohort, together with breast cancer models, we find that FOXA1 mutations associate with a lower response to aromatase inhibitors. Mechanistically, Wing2 mutations display increased chromatin binding at ER loci upon estrogen stimulation, and an enhanced ER-mediated transcription without changes in chromatin accessibility. In contrast, SY242CS shows neomorphic properties that include the ability to open distinct chromatin regions and activate an alternative cistrome and transcriptome. Structural modeling predicts that SY242CS confers a conformational change that mediates stable binding to a non-canonical DNA motif. Taken together, our results provide insights into how FOXA1 mutations perturb its function to dictate cancer progression and therapeutic response.Entities:
Keywords: ESR1 mutations; FOXA1 mutations; breast cancer; chromatin accessibility; endocrine therapy; epigenomics; estrogen receptor; pioneer transcription factor; transcription; transcriptomics
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Year: 2020 PMID: 32888433 PMCID: PMC8311901 DOI: 10.1016/j.ccell.2020.08.003
Source DB: PubMed Journal: Cancer Cell ISSN: 1535-6108 Impact factor: 31.743