| Literature DB >> 33468559 |
Xing Lu1, Christophe E Redon2, Wei Tang3, Swetha Parvathaneni1, Bayan Bokhari1,4, Subrata Debnath1, Xiao Ling Li5, Bruna R Muys5, Young Song6, Lorinc S Pongor2, Omar Sheikh7, Andrew R Green7, Srinivasan Madhusudan7, Ashish Lal5, Stefan Ambs3, Javed Khan6, Mirit I Aladjem8, Sudha Sharma9,10.
Abstract
Susceptibility to breast cancer is significantly increased in individuals with germ line mutations in RECQ1 (also known as RECQL or RECQL1), a gene encoding a DNA helicase essential for genome maintenance. We previously reported that RECQ1 expression predicts clinical outcomes for sporadic breast cancer patients stratified by estrogen receptor (ER) status. Here, we utilized an unbiased integrative genomics approach to delineate a cross talk between RECQ1 and ERα, a known master regulatory transcription factor in breast cancer. We found that expression of ESR1, the gene encoding ERα, is directly activated by RECQ1. More than 35% of RECQ1 binding sites were cobound by ERα genome-wide. Mechanistically, RECQ1 cooperates with FOXA1, the pioneer transcription factor for ERα, to enhance chromatin accessibility at the ESR1 regulatory regions in a helicase activity-dependent manner. In clinical ERα-positive breast cancers treated with endocrine therapy, high RECQ1 and high FOXA1 coexpressing tumors were associated with better survival. Collectively, these results identify RECQ1 as a novel cofactor for ERα and uncover a previously unknown mechanism by which RECQ1 regulates disease-driving gene expression in ER-positive breast cancer cells.Entities:
Keywords: DNA helicase; FOXA1; RECQ1; estrogen receptor; transcriptional regulation
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Year: 2021 PMID: 33468559 DOI: 10.1128/MCB.00515-20
Source DB: PubMed Journal: Mol Cell Biol ISSN: 0270-7306 Impact factor: 4.272