Hinokitiol impedes tumor drug resistance by suppressing protein kinase B/mammalian targets of rapamycin axis

Chemotherapy is a treatment method commonly used for cancer and that patients showing low to no response to the treatment often developed drug resistance via multiple mechanisms. Natural products have been shown to reduce tumor drug resistance. Hinokitiol, a natural tropolone derivative, has potenti...

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Veröffentlicht in:	Journal of Cancer 2022-01, Vol.13 (6), p.1725-1733
Hauptverfasser:	Ni, Ying-Jui, Huang, Zi-Ni, Li, Hsin-Yu, Lee, Chiao-Ching, Tyan, Yu-Chang, Yang, Ming-Hui, Pangilinan, Christian R, Wu, Li-Hsien, Chiang, Yu-Chung, Lee, Che-Hsin
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Sprache:	eng
Schlagworte:	Antibodies Apoptosis Biotechnology Cancer therapies Cell cycle Chemotherapy Cytoplasm Drug dosages Drug resistance Kinases Laboratory animals Leukopenia Phosphorylation Proteins Research Paper Tumors Variance analysis
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container_title	Journal of Cancer
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creator	Ni, Ying-Jui Huang, Zi-Ni Li, Hsin-Yu Lee, Chiao-Ching Tyan, Yu-Chang Yang, Ming-Hui Pangilinan, Christian R Wu, Li-Hsien Chiang, Yu-Chung Lee, Che-Hsin
description	Chemotherapy is a treatment method commonly used for cancer and that patients showing low to no response to the treatment often developed drug resistance via multiple mechanisms. Natural products have been shown to reduce tumor drug resistance. Hinokitiol, a natural tropolone derivative, has potential as an antitumor agent. To improve the efficacy and safety of hinokitiol, a further understanding of hinokitiol interactions with the tumor microenvironment is necessary. The presence of plasma membrane multidrug resistance protein P-glycoprotein (P-gp) is favorable for tumor cells to elicit chemotherapeutic resistance. Here, we showed that hinokitiol dose-dependently decreased P-gp expression and suppressed the P-gp-driven efflux activity based on Rhodamine 123 assay. The protein expression levels of phosph-protein kinase B (P-AKT), phosph-mammalian targets of rapamycin (P-mTOR), and phosph-p70 ribosomal s6 kinase (P-p70s6K) in tumor cells were likewise reduced after hinokitiol treatment. The transfection of cells with active P-AKT rescued hinokitiol-induced downregulation of P-gp, suggesting the involvement of Akt/mTOR/p70s6K signaling in P-gp expression. Our results showed that hinokitiol can chemosensitize cancer cells. These findings indicate that hinokitiol could enhance 5-Fluorouracil therapeutic effects in murine B16F10 and CT26 tumor cells via downregulation of the AKT/mTOR pathway.
doi_str_mv	10.7150/jca.69449
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subjects	Antibodies Apoptosis Biotechnology Cancer therapies Cell cycle Chemotherapy Cytoplasm Drug dosages Drug resistance Kinases Laboratory animals Leukopenia Phosphorylation Proteins Research Paper Tumors Variance analysis
title	Hinokitiol impedes tumor drug resistance by suppressing protein kinase B/mammalian targets of rapamycin axis
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