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miR-548c-5p inhibits proliferation and migration and promotes apoptosis in CD90+ HepG2 cells Cover

miR-548c-5p inhibits proliferation and migration and promotes apoptosis in CD90+ HepG2 cells

Open Access
|Apr 2012

Abstract

Background. Since the introduction of the theory of tumour stem cells (TSCs), the liver cancer stem cell (LCSC)-like cells have become one of the focuses in the research on liver cancer.

Materials and methods. In this study, CD90+ cells were applied as the possible LCSC-like cells, and the miRNA and gene expression were analyzed in the CD90+ HepG2 cells. The pilot study showed miR-548c-5p exerted potential effect on the CD90+ HepG2 cells and was thereafter applied for the further study. CD90+ HepG2 cells were assigned to miR-548c-5p mimic transfection group and control group. MTT assay was performed to detect the proliferation of CD90+ HepG2 cells. The migration and invasion abilities were examined by wound healing assay and transwell migration assay, respectively. A detection of apoptosis was performed by fluorescence microscopy.

Results. Our results showed that caspase-3 and bcl-2 were down-regulated while caspase-8 was up-regulated in the CD90+ HepG2 cells. Moreover, the miR-548c-5p transfection could down-regulate the expression of β-catenin, Tg737, bcl-2, bcl-XL, and caspase-3, inhibit the proliferation, migration and invasion and promote the apoptosis of the CD90+ HepG2 cells.

Conclusions. Our findings indicate the imbalance between apoptosis and anti-apoptosis in the LCSC-like cells, which influence the biological features of LCSC-like cells. miRNA plays a regulatory role in the LCSC-like cells among which miR-548c-5p might be a suppressor.

DOI: https://doi.org/10.2478/v10019-012-0025-z | Journal eISSN: 1581-3207 | Journal ISSN: 1318-2099
Language: English
Page range: 233 - 241
Published on: Apr 11, 2012
In partnership with: Paradigm Publishing Services
Publication frequency: 4 issues per year

© 2012 Lin Fang, Hai-Bing Zhang, Hua Li, Yong Fu, Guang-Shun Yang, published by Association of Radiology and Oncology
This work is licensed under the Creative Commons License.

Volume 46 (2012): Issue 3 (September 2012)