| Literature DB >> 32356386 |
Mohammad Askandar Iqbal1, Shilpi Chattopadhyay2, Farid Ahmad Siddiqui1,3, Asad Ur Rehman1,4, Shumaila Siddiqui1, Gopinath Prakasam5,6, Asifa Khan1,7, Sarwat Sultana2, Rameshwar Nk Bamezai5.
Abstract
Triple-negative breast cancer (TNBC) is an aggressive form of breast cancer with limited treatment modalities and poor prognosis. Metabolic reprogramming in cancer is considered a hallmark of therapeutic relevance. Here, we report disruption of metabolic reprogramming in TNBC cells by silibinin via modulation of EGFR-MYC-TXNIP signaling. Metabolic assays combined with LC-MS-based metabolomics revealed inhibition of glycolysis and other key biosynthetic pathways by silibinin, to induce metabolic catastrophe in TNBC cells. Silibinin-induced metabolic suppression resulted in decreased cell biomass, proliferation, and stem cell properties. Mechanistically, we identify EGFR-MYC-TXNIP as an important regulator of TNBC metabolism and mediator of inhibitory effects of silibinin. Highlighting the clinical relevance of our observations, the analysis of METABRIC dataset revealed deregulation of EGFR-MYC-TXNIP axis in TNBC and association of EGFRhigh -MYChigh -TXNIPlow signature with aggressive glycolytic metabolism and poor disease-specific and metastasis-free survival. Importantly, combination treatment of silibinin or 2-deoxyglucose (glycolysis inhibitor) with paclitaxel synergistically inhibited proliferation of TNBC cells. Together, our results highlight the importance of EGFR-MYC-TXNIP axis in regulating TNBC metabolism, demonstrate the anti-TNBC activity of silibinin, and argue in favor of targeting metabolic vulnerabilities of TNBC, at least in combination with mainstay chemotherapeutic drugs, to effectively treat TNBC patients.Entities:
Keywords: EGFR; MYC; TXNIP; cancer metabolism; silibinin; triple-negative breast cancer
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Year: 2020 PMID: 32356386 DOI: 10.1111/febs.15353
Source DB: PubMed Journal: FEBS J ISSN: 1742-464X Impact factor: 5.542