| Literature DB >> 31219186 |
You Mo1, Rui-Hua Fang1, Jiang Wu1, Yuan Si1, Shu-Qing Jia1, Qun Li1, Jing-Zhu Bai1, Xi-Ning She1, Jian-Qin Wang2,3.
Abstract
Melanoma is responsible for the majority of deaths caused by skin cancer. Antitumor activity of microRNA-329 (miR-329) has been seen in several human cancers. In this study, we identify whether miR-329 serves as a candidate regulator in melanoma. Melanoma-related differentially expressed genes were screened with its potential molecular mechanism predicted. Melanoma tissues and pigmented nevus tissues were collected, where the levels of miR-329 and high-mobility group box 2 (HMGB2) were determined. To characterize the regulatory role of miR-329 on HMGB2 and the β-catenin pathway in melanoma cell activities, miR-329 mimics, miR-329 inhibitors, and siRNA-HMGB2 were transfected into melanoma cells. Cell viability, migration, invasion, cell cycle, and apoptosis were assessed. miR-329 was predicted to influence melanoma by targeting HMGB2 via the β-catenin pathway. High level of HMGB2 and low miR-329 expression were observed in melanoma tissues. HMGB2 was targeted and negatively regulated by miR-329. In melanoma cells transfected with miR-329 mimics or siRNA-HMGB2, cell proliferation, migration, and invasion were impeded, yet cell cycle arrest and apoptosis were promoted, corresponding to decreased levels of β-catenin, cyclin D1, and vimentin and increased levels of GSK3β and E-cadherin. Collectively, our results show that miR-329 can suppress the melanoma progression by downregulating HMGB2 via the β-catenin pathway.Entities:
Keywords: apoptosis; high-mobility group box 2; invasion; melanoma; microRNA-329; migration; proliferation; β-catenin pathway
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Year: 2019 PMID: 31219186 DOI: 10.1002/jcp.28920
Source DB: PubMed Journal: J Cell Physiol ISSN: 0021-9541 Impact factor: 6.384