Transcription factor ZNF703 activates linc-UBC1 to stimulate the progression of glioma
J. Wang, L.-S. Zhu, Y. Luo, C.-H. Wang, Y.-Y. Wei, L.-M. Zhou Department of Neurosurgery, The First Affiliated Hospital of Jinzhou Medical University, Jinzhou, China. 43205350@qq.com
OBJECTIVE: To investigate the role of the transcription factor Zinc finger 703 (ZNF703) in influencing the progression of glioma by regulating linc-UBC1 level.
MATERIALS AND METHODS: Linc-UBC1 level in glioma with different staging and tumor sizes was determined. The potential influences of linc-UBC1 on viability, cell cycle progression, and invasiveness of glioma cells were evaluated. Through RNA binding protein immunoprecipitation (RIP) assay and Dual-Luciferase reporter gene assay, the interaction between ZNF703 and linc-UBC1 was assessed. The rescue experiments were conducted to identify the role of ZNF703 in regulating cellular performances of glioma by interacting with linc-UBC1.
RESULTS: Linc-UBC1 was highly expressed in glioma. Its level was higher in glioma with larger tumor size or advanced staging. The knockdown of linc-UBC1 reduced viability, arrested cell cycle in the G0/G1 phase, and attenuated invasiveness of U87 and LN229 cells. The presence of the binding sites was observed in the promoter regions of ZNF703 and linc-UBC1. The overexpression of ZNF703 could alleviate the inhibited proliferative and invasive potentials in U87 and LN229 cells with the linc-UBC1 knockdown.
CONCLUSIONS: The transcription factor ZNF703 promotes the proliferative and invasive potentials in glioma cells by regulating the transcriptional activity of linc-UBC1.
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To cite this article
J. Wang, L.-S. Zhu, Y. Luo, C.-H. Wang, Y.-Y. Wei, L.-M. Zhou
Transcription factor ZNF703 activates linc-UBC1 to stimulate the progression of glioma
Eur Rev Med Pharmacol Sci
Year: 2020
Vol. 24 - N. 6
Pages: 3183-3189
DOI: 10.26355/eurrev_202003_20685