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Attenuation of MUC4 potentiates the anticancer activity of auranofin via regulation of the Her2/Akt/FOXO3 pathway in ovarian cancer cells

Authors
Bae, Jun SangLee, JongsungPark, YoonKookPark, KyungmonKim, Jung RyulCho, Dong HyuJang, Kyu YunPark, See-Hyoung
Issue Date
Oct-2017
Publisher
SPANDIDOS PUBL LTD
Keywords
MUC4; auranofin; Her2; Akt; FOXO3; ovarian; cancer
Citation
ONCOLOGY REPORTS, v.38, no.4, pp.2417 - 2425
Journal Title
ONCOLOGY REPORTS
Volume
38
Number
4
Start Page
2417
End Page
2425
URI
https://scholarworks.bwise.kr/hongik/handle/2020.sw.hongik/5242
DOI
10.3892/or.2017.5853
ISSN
1021-335X
Abstract
Previously, we reported that auranofin induces apoptosis in SKOV3 cells via regulation of the IKK beta/FOXO3 pathway. In the present study, we reveal that the anticancer activity of auranofin in SKOV3 cells could be enhanced by the attenuation of MUC4 through the regulation of the Her2/Akt/FOXO3 pathway. Compared to the control-siRNA, siRNA transfection against MUC4 into SKOV3 cells accelerated the protein degradation of Her2. Under the same conditions, the expression level of phosphorylated Akt was also downregulated leading to an increase of FOXO3 in the nucleus. Notably, auranofin treatment in SKOV3 cells also resulted in the downregulation of the expression levels of both Her2 and phosphorylated Akt. Thus, Her2 was identified as the common molecular target protein by siRNA transfection against MUC4. Western blot analysis of total and nuclear fraction lysates from SKOV3 cells revealed that attenuation of MUC4 combined with auranofin treatment in SKOV3 cells synergistically activated FOXO3 translocation from the cytoplasm to the nucleus through the regulation of the Her2/Akt/FOXO3 pathway. Attenuation of MUC4 by siRNA transfection potentiated the antitumor effect of auranofin which was examined by performing in vitro assays such as WST-1, cell counting, colony formation, TUNEL and Annexin V staining. In addition, western blot analysis of the apoptosis-related proteins such as PARP1, caspase-3, Bim extra large (EL), Bax and Bcl2 revealed that the attenuation of MUC4 by siRNA transfection potentiates the pro-apoptotic activity of auranofin in SKOV3 cells. Collectively, auranofin could regulate the Her2/Akt/FOXO3 signaling pathway in SKOV3 cells and be used as a potential antitumor agent considering the expression of MUC4 in ovarian cancer patients.
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