Hypoxia-induced TGF-β–RBFOX2–ESRP1 axis regulates human MENA alternative splicing and promotes EMT in breast cancer
Author(s) -
Neha Ahuja,
Cheemala Ashok,
Subhashis Natua,
Deepak Pant,
Anna Cherian,
Madhura R. Pandkar,
Pooja Yadav,
Vishnu Narayanan S.S.,
Jharna Mishra,
Atul Samaiya,
Sanjeev Shukla
Publication year - 2020
Publication title -
nar cancer
Language(s) - English
Resource type - Journals
ISSN - 2632-8674
DOI - 10.1093/narcan/zcaa021
Subject(s) - epithelial–mesenchymal transition , alternative splicing , cancer research , hypoxia (environmental) , rna splicing , downregulation and upregulation , signal transduction , biology , slug , transforming growth factor , microbiology and biotechnology , metastasis , psychological repression , exon , chemistry , cancer , gene , gene expression , rna , genetics , organic chemistry , oxygen
Hypoxic microenvironment heralds epithelial–mesenchymal transition (EMT), invasion and metastasis in solid tumors. Deregulation of alternative splicing (AS) of several cancer-associated genes has been instrumental in hypoxia-induced EMT. Our study in breast cancer unveils a previously unreported mechanism underlying hypoxia-mediated AS of hMENA , a crucial cytoskeleton remodeler during EMT. We report that the hypoxia-driven depletion of splicing regulator ESRP1 leads to skipping of hMENA exon 11a producing a pro-metastatic isoform, hMENAΔ11a . The transcriptional repression of ESRP1 is mediated by SLUG, which gets stimulated via hypoxia-driven TGF-β signaling. Interestingly, RBFOX2, an otherwise RNA-binding protein, is also found to transcriptionally repress ESRP1 while interacting with SLUG. Similar to SLUG , RBFOX2 gets upregulated under hypoxia via TGF-β signaling. Notably, we found that the exosomal delivery of TGF-β contributes to the elevation of TGF-β signaling under hypoxia. Moreover, our results show that in addition to hMENA, hypoxia-induced TGF-β signaling contributes to global changes in AS of genes associated with EMT. Overall, our findings reveal a new paradigm of hypoxia-driven AS regulation of hMENA and insinuate important implications in therapeutics targeting EMT.
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