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Identification of Withaferin A as a Potential Candidate for Anti-Cancer Therapy in Non-Small Cell Lung Cancer

by Lai, Jin-Mei , Tsai, Yu-Chen , Chang, Peter M.-H. , Huang, Tse- Hung , Yang, Yun-Hsuan , Cheng, Tai-Shan , Hsu, Jade H.-M. , Huang, Chi-Ying F. , Kuo, Yu-Lun , Wu, Alexander T.-H. , Chen, Jing-Ming , Chu, Yeh-Shiu , Tran, Thu-Ha

in Apoptosis / Autophagy / Cancer therapies / Cell viability / Chemotherapy / Cisplatin / Cytotoxicity / Drugs / Epidermal growth factor / Epidermal growth factor receptors / Gene expression / Kinases / Lung cancer / Mutation / Non-small cell lung carcinoma / Phagocytosis / Reactive oxygen species / Small cell lung carcinoma / Stat3 protein / Stem cells / TOR protein / Tumorigenesis

2019

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Identification of Withaferin A as a Potential Candidate for Anti-Cancer Therapy in Non-Small Cell Lung Cancer

2019

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Identification of Withaferin A as a Potential Candidate for Anti-Cancer Therapy in Non-Small Cell Lung Cancer

2019

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Journal Article

Identification of Withaferin A as a Potential Candidate for Anti-Cancer Therapy in Non-Small Cell Lung Cancer

Lai, Jin-Mei,

Tsai, Yu-Chen,

Chang, Peter M.-H.,

Huang, Tse- Hung,

Yang, Yun-Hsuan,

Cheng, Tai-Shan,

Hsu, Jade H.-M.,

Huang, Chi-Ying F.,

Kuo, Yu-Lun,

Wu, Alexander T.-H.,

Chen, Jing-Ming,

Chu, Yeh-Shiu,

Tran, Thu-Ha

2019

Overview

Low response rate and recurrence are common issues in lung cancer; thus, identifying a potential compound for these patients is essential. Utilizing an in silico screening method, we identified withaferin A (WA), a cell-permeable steroidal lactone initially extracted from Withania somnifera, as a potential anti–lung cancer and anti–lung cancer stem-like cell (CSC) agent. First, we demonstrated that WA exhibited potent cytotoxicity in several lung cancer cells, as evidenced by low IC50 values. WA concurrently induced autophagy and apoptosis and the activation of reactive oxygen species (ROS), which plays an upstream role in mediating WA-elicited effects. The increase in p62 indicated that WA may modulate the autophagy flux followed by apoptosis. In vivo research also demonstrated the anti-tumor effect of WA treatment. We subsequently demonstrated that WA could inhibit the growth of lung CSCs, decrease side population cells, and inhibit lung cancer spheroid-forming capacity, at least through downregulation of mTOR/STAT3 signaling. Furthermore, the combination of WA and chemotherapeutic drugs, including cisplatin and pemetrexed, exerted synergistic effects on the inhibition of epidermal growth factor receptor (EGFR) wild-type lung cancer cell viability. In addition, WA can further enhance the cytotoxic effect of cisplatin in lung CSCs. Therefore, WA alone or in combination with standard chemotherapy is a potential treatment option for EGFR wild-type lung cancer and may decrease the occurrence of cisplatin resistance by inhibiting lung CSCs.

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