Selective targeting of IRAK1 attenuates low molecular weight hyaluronic acid-induced stemness and non-canonical STAT3 activation in epithelial ovarian cancer.
David StandingPrasad DandawateSumedha GunewardenaObdulia Covarrubias-ZambranoKatherine F RobyDineo KhabeleAndrea JewellOssama TawfikStefan H BossmannAndrew K GodwinScott J WeirRoy A JensenShrikant AnantPublished in: Cell death & disease (2024)
Advanced epithelial ovarian cancer (EOC) survival rates are dishearteningly low, with ~25% surviving beyond 5 years. Evidence suggests that cancer stem cells contribute to acquired chemoresistance and tumor recurrence. Here, we show that IRAK1 is upregulated in EOC tissues, and enhanced expression correlates with poorer overall survival. Moreover, low molecular weight hyaluronic acid, which is abundant in malignant ascites from patients with advanced EOC, induced IRAK1 phosphorylation leading to STAT3 activation and enhanced spheroid formation. Knockdown of IRAK1 impaired tumor growth in peritoneal disease models, and impaired HA-induced spheroid growth and STAT3 phosphorylation. Finally, we determined that TCS2210, a known inducer of neuronal differentiation in mesenchymal stem cells, is a selective inhibitor of IRAK1. TCS2210 significantly inhibited EOC growth in vitro and in vivo both as monotherapy, and in combination with cisplatin. Collectively, these data demonstrate IRAK1 as a druggable target for EOC.
Keyphrases
- hyaluronic acid
- cancer stem cells
- high glucose
- mesenchymal stem cells
- diabetic rats
- cell proliferation
- drug induced
- poor prognosis
- free survival
- machine learning
- oxidative stress
- clinical trial
- open label
- bone marrow
- umbilical cord
- binding protein
- protein kinase
- deep learning
- brain injury
- artificial intelligence
- long non coding rna
- combination therapy
- signaling pathway
- cerebral ischemia