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KMID : 0545120210310040540
Journal of Microbiology and Biotechnology
2021 Volume.31 No. 4 p.540 ~ p.549
Non-Polar Myxococcus fulvus KYC4048 Metabolites Exert Anti-Proliferative Effects via Inhibition of Wnt/¥â-Catenin Signaling in MCF-7 Breast Cancer Cells
Park Ju-Ha

Yoo Hee-Jin
Yu Ah-Ran
Kim Hye-Ok
Park Sang-Cheol
Jang Young-Pyo
Lee Cha-Yul
Choe Won-Chae
Kim Sung-Soo
Kang In-Sug
Yoon Kyung-Sik
Abstract
The Wnt/¥â-catenin signaling pathway is involved in breast cancer and Myxococcus fulvus KYC4048 is a myxobacterial strain that can produce a variety of bioactive secondary metabolites. Although a previous study revealed that KYC4048 metabolites exhibit anti-proliferative effects on breast cancer, the biochemical mechanism involved in their effects remains unclear. In the present study, KYC4048 metabolites were separated into polar and non-polar (ethyl acetate and n-hexane) fractions via liquid-liquid extraction. The effects of these polar and non-polar KYC4048 metabolites on the viability of breast cancer cells were then determined by MTT assay. Expression levels of Wnt/¥â-catenin pathway proteins were determined by Western blot analysis. Cell cycle and apoptosis were measured via fluorescence-activated cell sorting (FACS). The results revealed that non-polar KYC4048 metabolites induced cell death of breast cancer cells and decreased expression levels of WNT2B, ¥â-catenin, and Wnt target genes (c-Myc and cyclin D1). Moreover, the n-hexane fraction of non-polar KYC4048 metabolites was found most effective in inducing apoptosis, necrosis, and cell cycle arrest, leading us to conclude that it can induce apoptosis of breast cancer cells through the Wnt/¥â-catenin pathway. These findings provide evidence that the n-hexane fraction of non-polar KYC4048 metabolites can be developed as a potential therapeutic agent for breast cancer via inhibition of the Wnt/¥â-catenin pathway.
KEYWORD
Myxococcus fulvus metabolites, n-hexane fraction, MCF-7, Wnt/¥â-catenin signaling pathway, anti-proliferation
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