Valproic acid-induced amphiregulin secretion confers resistance to temozolomide treatment in human glioma cells | BMC Cancer | Full Text

Valproic acid-induced amphiregulin secretion confers resistance to temozolomide treatment in human glioma cells | BMC Cancer | Full Text



BMC Cancer

Valproic acid-induced amphiregulin secretion confers resistance to temozolomide treatment in human glioma cells

• Jui-Chieh Chen, 
• I-Neng Lee, 
• Cheng Huang, 
• Yu-Ping Wu, 
• Chiu-Yen Chung, 
• Ming-Hsueh Lee, 
• Martin Hsiu-Chu Lin & 
• Jen-Tsung Yang 

BMC Cancervolume 19, Article number: 756 (2019) | Download Citation

Abstract

Background

Glioblastoma multiforme (GBM) is the most severe type of primary brain tumor with a high mortality rate. Although extensive treatments for GBM, including resection, irradiation, chemotherapy and immunotherapy, have been tried, the prognosis is still poor. Temozolomide (TMZ), an alkylating agent, is a front-line chemotherapeutic drug for the clinical treatment of GBM; however, its effects are very limited because of the chemoresistance. Valproic acid (VPA), an antiepileptic agent with histone deacetylase inhibitor activity, has been shown to have synergistic effects with TMZ against GBM. The mechanism of action of VPA on TMZ combination therapy is still unclear. Accumulating evidence has shown that secreted proteins are responsible for the cross talking among cells in the tumor microenvironment, which may play a critical role in the regulation of drug responses.

Methods

To understand the effect of VPA on secreted proteins in GBM cells, we first used the antibody array to analyze the cell culture supernatant from VPA-treated and untreated GBM cells. The results were further confirmed by lentivirus-mediated knockdown and exogenous recombinant administration.

Results

Our results showed that amphiregulin (AR) was highly secreted in VPA-treated cells. Knockdown of AR can sensitize GBM cells to TMZ. Furthermore, pretreatment of exogenous recombinant AR significantly increased EGFR activation and conferred resistance to TMZ. To further verify the effect of AR on TMZ resistance, cells pre-treated with AR neutralizing antibody markedly increased sensitivity to TMZ. In addition, we also observed that the expression of AR was positively correlated with the resistance of TMZ in different GBM cell lines.

Conclusions

The present study aimed to identify the secreted proteins that contribute to the modulation of drug response. Understanding the full set of secreted proteins present in glial cells might help reveal potential therapeutic opportunities. The results indicated that AR may potentially serve as biomarker and therapeutic approach for chemotherapy regimens in GBM.