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Synergistic inhibitory effects of the oxyresveratrol and dacarbazine combination against melanoma cells

Authors
Lee, Sang GyuLee, Dong GunJoo, Yong HoonChung, Namhyun
Issue Date
9월-2021
Publisher
SPANDIDOS PUBL LTD
Keywords
Notch signaling; S phase arrest; chemical drug; stilbenoid; synergistic effect
Citation
ONCOLOGY LETTERS, v.22, no.3
Indexed
SCIE
SCOPUS
Journal Title
ONCOLOGY LETTERS
Volume
22
Number
3
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/136418
DOI
10.3892/ol.2021.12928
ISSN
1792-1074
Abstract
Various therapies have been developed to target malignant melanoma, which is associated with a high mortality rate worldwide. Although dacarbazine (DTIC) is employed for treating melanoma, it is associated with several side effects. Hence, patients with melanoma are co-treated with additional drugs to mitigate the side effects of DTIC. In the present study, synergistic therapeutic effects of the DTIC/oxyresveratrol (ORT) combination were examined using the human malignant melanoma WM-266-4 cell line. Treatment with ORT and DTIC inhibited the proliferation of WM-266-4 cells. Compared with those in the ORT- and DTIC-treated groups, the proportion of cells arrested at the S phase, as well as apoptotic rates, were increased in the ORT and DTIC co-treatment group. In WM-266-4 cells, synergistic proliferation-inhibitory activities of the ORT/DTIC combination were assessed based on cell viability and migration, antioxidant capacity, cytokine production, cell cycle arrest, apoptotic rate and protein expression through WST-1 assay, wound healing assay, flow cytometry and western blotting. Furthermore, the expression levels of proteins, including NOTCH, involved in the pathogenesis of solid cancers, such as melanoma, were examined. Overall, the ORT/DTIC combination synergistically promoted cell cycle arrest at the S phase and the apoptosis of WM-266-4 cells. Thus, this combination treatment may serve as a novel therapeutic strategy for treating malignant melanoma.
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