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01.06.2009 | Original Paper

Arsenic trioxide-induced growth arrest of human hepatocellular carcinoma cells involving FOXO3a expression and localization

verfasst von: Min Fei, Mudan Lu, You Wang, Yueming Zhao, Song He, Shangfeng Gao, Qing Ke, Yonghua Liu, Peng Li, Xiaopeng Cui, Aiguo Shen, Chun Cheng

Erschienen in: Medical Oncology | Ausgabe 2/2009

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Abstract

Human hepatocellular carcinoma (HCC) remains incurable with current therapies, and novel biologically based therapies are urgently needed. Arsenic agents have long been used as anticancer agents in traditional Chinese medicine. In this study, to evaluate the effect of As₂O₃ on HCC cells, we investigate cell growth inhibition, cell cycle arrest, and the molecular mechanism after As₂O₃ treatment in human HCC cells in vitro. We detected the proliferation of HCC cells by the Cell Counting Kit and FACS/Calibur Flow Cytometer and analyzed the expression and localization of FOXO3a by Western blotting Analysis and Cell Fractionation. Furthermore, we study the Akt activation after As₂O₃ treatment and the HCC cells proliferation after combination of As₂O₃ with PI3K inhibitor Wortmannin. As₂O₃ significantly inhibited the proliferation of all the three HCC cell lines (SMMC7721, HepG2, Hep3B) tested in this study in a dose-dependent manner. Western blotting revealed that treatment HCC cells HepG2 with As₂O₃ resulted in the increasing of FOXO3a expression and triggered phosphorylation of FOXO3a at the Thr³² residue decrease. This FOXO3a accumulation correlated well with the As₂O₃-induced reduction of active Akt. Nuclear and cytoplasmic protein extracts isolated from the HCC cell line HepG2 revealed that the amount of nuclear FOXO3a was increased by treatment with As₂O₃, whereas the amount of cytoplasmic FOXO3a was decreased. Both As₂O₃ and PI3K/Akt inhibitor Wortmannin induced cell cycle arrest. However, compared with As₂O₃ alone, PI3K inhibitor Wortmannin combined with As₂O₃ enhanced the antitumor effect of As₂O₃ through induction of apoptosis. These findings suggest that As₂O₃ at a clinically safe concentration may be an effective chemotherapeutic agent, and that As₂O₃ and PI3K/Akt inhibitor Wortmannin may synergize for HCC cells. Taken together, the present study may suggest a specific molecular mechanism by which HCC cell lines are susceptible to the As₂O₃ therapy through FOXO3a expression and localization.

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Titel: Arsenic trioxide-induced growth arrest of human hepatocellular carcinoma cells involving FOXO3a expression and localization
verfasst von: Min Fei
Mudan Lu
You Wang
Yueming Zhao
Song He
Shangfeng Gao
Qing Ke
Yonghua Liu
Peng Li
Xiaopeng Cui
Aiguo Shen
Chun Cheng
Publikationsdatum: 01.06.2009
Verlag: Humana Press Inc
Erschienen in: Medical Oncology / Ausgabe 2/2009
Print ISSN: 1357-0560
Elektronische ISSN: 1559-131X
DOI: https://doi.org/10.1007/s12032-008-9105-8

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Arsenic trioxide-induced growth arrest of human hepatocellular carcinoma cells involving FOXO3a expression and localization

Abstract

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