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Thioridazine Enhances P62-Mediated Autophagy and Apoptosis Through Wnt/β-Catenin Signaling Pathway in Glioma Cells

by Chu, Cheng-Wei , Lin, Chen-Yen , Su, Chun-Li , Cheng, Tai-Shan , Huang, Chi-Ying F. , Cheng, Jiin-Tsuey , Ko, Huey-Jiun , Loh, Joon-Khim , Chou, Chia-Hua , Cheng, Hui-Wen , Lai, Yun-Ling , Chiou, Shean-Jaw , Liang, Yu-Hsin , Wang, Chihuei , Hong, Yi-Ren

in Adapter proteins / Apoptosis / Autophagy / Brain cancer / Cancer therapies / Cell cycle / Cell growth / Chemotherapy / Cytotoxicity / Drug dosages / Flow cytometry / Glioma / Kinases / Psychotropic drugs / Stem cells

2019

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Thioridazine Enhances P62-Mediated Autophagy and Apoptosis Through Wnt/β-Catenin Signaling Pathway in Glioma Cells

2019

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Thioridazine Enhances P62-Mediated Autophagy and Apoptosis Through Wnt/β-Catenin Signaling Pathway in Glioma Cells

2019

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Journal Article

Thioridazine Enhances P62-Mediated Autophagy and Apoptosis Through Wnt/β-Catenin Signaling Pathway in Glioma Cells

Chu, Cheng-Wei,

Lin, Chen-Yen,

Su, Chun-Li,

Cheng, Tai-Shan,

Huang, Chi-Ying F.,

Cheng, Jiin-Tsuey,

Ko, Huey-Jiun,

Loh, Joon-Khim,

Chou, Chia-Hua,

Cheng, Hui-Wen,

Lai, Yun-Ling,

Chiou, Shean-Jaw,

Liang, Yu-Hsin,

Wang, Chihuei,

Hong, Yi-Ren

2019

Overview

Thioridazine (THD) is a common phenothiazine antipsychotic drug reported to suppress growth in several types of cancer cells. We previously showed that THD acts as an antiglioblastoma and anticancer stem-like cell agent. However, the signaling pathway underlying autophagy and apoptosis induction remains unclear. THD treatment significantly induced autophagy with upregulated AMPK activity and engendered cell death with increased sub-G1 in glioblastoma multiform (GBM) cell lines. Notably, through whole gene expression screening with THD treatment, frizzled (Fzd) proteins, a family of G-protein-coupled receptors, were found, suggesting the participation of Wnt/β-catenin signaling. After THD treatment, Fzd-1 and GSK3β-S9 phosphorylation (inactivated form) was reduced to promote β-catenin degradation, which attenuated P62 inhibition. The autophagy marker LC3-II markedly increased when P62 was released from β-catenin inhibition. Additionally, the P62-dependent caspase-8 activation that induced P53-independent apoptosis was confirmed by inhibiting T-cell factor/β-catenin and autophagy flux. Moreover, treatment with THD combined with temozolomide (TMZ) engendered increased LC3-II expression and caspase-3 activity, indicating promising drug synergism. In conclusion, THD induces autophagy in GBM cells by not only upregulating AMPK activity, but also enhancing P62-mediated autophagy and apoptosis through Wnt/β-catenin signaling. Therefore, THD is a potential alternative therapeutic agent for drug repositioning in GBM.

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