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Hesperetin-etoposide combinations induce cytotoxicity in U2OS cells: Implications on therapeutic developments for osteosarcoma

Title
Hesperetin-etoposide combinations induce cytotoxicity in U2OS cells: Implications on therapeutic developments for osteosarcoma
Type
Article in International Scientific Journal
Year
2017
Authors
Coutinho, L
(Author)
Other
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Oliveira, H
(Author)
Other
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Pacheco, AR
(Author)
Other
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Almeida, L
(Author)
Other
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Pimentel, F
(Author)
Other
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Ferreira de Oliveira, JMPF
(Author)
FCUP
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Journal
Title: DNA RepairImported from Authenticus Search for Journal Publications
Vol. 50
Pages: 36-42
ISSN: 1568-7864
Publisher: Elsevier
Other information
Authenticus ID: P-00M-GM6
Abstract (EN): Osteosarcoma chemotherapy has improved survival rates, however, chemoresistance and drug toxicity still limit therapy. Drug combinations may overcome these limitations by allowing fewer chemoresistant cells to survive. The aim of this study was to evaluate the cytotoxic potential of hesperetin to osteosarcoma and to analyze the cell cycle effects of combinations of hesperetin with chemotherapeutic agents. For this, the U2OS human osteosarcoma cell line was exposed to hesperetin or hesperetin combined with etoposide or doxorubicin in defined proportions. Hesperetin was less cytotoxic compared to chemotherapeutic agents, as shown by cell growth, viability and clonogenic assays. Notwithstanding, hesperetin combined with etoposide showed additive effects on the inhibition of cell growth. Furthermore, hesperetin induced G2-phase arrest, associated with decreased gene expression of cyclins B1 and E1 and cyclin-dependent kinases 1 and 2. The combination with higher additive effect resulted in higher percentage of cells in G2-phase, showing that G2-phase arrest is associated with cytotoxicity. Moreover, hesperetin induced cytostatic effects. In conclusion, our results suggest that G2-phase arrest is an important step for hesperetin-induced cytotoxicity in U2OS cells. Hesperetin shows potential cytotoxicity when combined with etoposide, which may have implications on therapeutic developments for osteosarcoma.
Language: English
Type (Professor's evaluation): Scientific
No. of pages: 7
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