| Literature DB >> 30511964 |
Bing Song1, Su-Hong Park1, Jonathan C Zhao1, Ka-Wing Fong1, Shangze Li1, Yongik Lee1, Yeqing A Yang1, Subhasree Sridhar1, Xiaodong Lu1, Sarki A Abdulkadir2, Robert L Vessella3, Colm Morrissey3, Timothy M Kuzel1, William Catalona2, Ximing Yang2, Jindan Yu1,2,4.
Abstract
Prostate cancer (PC) progressed to castration resistance (CRPC) is a fatal disease. CRPC tumors develop resistance to new-generation antiandrogen enzalutamide through lineage plasticity, characterized by epithelial-mesenchymal transition (EMT) and a basal-like phenotype. FOXA1 is a transcription factor essential for epithelial lineage differentiation. Here, we demonstrate that FOXA1 loss leads to remarkable upregulation of transforming growth factor beta 3 (TGFB3), which encodes a ligand of the TGF-β pathway. Mechanistically, this is due to genomic occupancy of FOXA1 on an upstream enhancer of the TGFB3 gene to directly inhibit its transcription. Functionally, FOXA1 downregulation induces TGF-β signaling, EMT, and cell motility, which is effectively blocked by the TGF-β receptor I inhibitor galunisertib (LY2157299). Tissue microarray analysis confirmed reduced levels of FOXA1 protein and a concordant increase in TGF-β signaling, indicated by SMAD2 phosphorylation, in CRPC as compared with primary tumors. Importantly, combinatorial LY2157299 treatment sensitized PC cells to enzalutamide, leading to synergistic effects in inhibiting cell invasion in vitro and xenograft CRPC tumor growth and metastasis in vivo. Therefore, our study establishes FOXA1 as an important regulator of lineage plasticity mediated in part by TGF-β signaling, and supports a novel therapeutic strategy to control lineage switching and potentially extend clinical response to antiandrogen therapies.Entities:
Keywords: Genetics; Oncology; Prostate cancer
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Year: 2018 PMID: 30511964 PMCID: PMC6355239 DOI: 10.1172/JCI122367
Source DB: PubMed Journal: J Clin Invest ISSN: 0021-9738 Impact factor: 14.808