Title of article
Enrichment of A Rare Subpopulation of miR-302-Expressing Glioma Cells by Serum Deprivation
Author/Authors
Rafiee، Mahmoud-Reza نويسنده Nanomedicine and Tissue Engineering Center, Shahid Beheshti University of Medical Sciences, Tehran , , Malekzadeh Shafaroudi، Afsaneh نويسنده , , Rohban، Sara نويسنده Department of Molecular Genetics, Faculty of Biological Sciences, Tarbiat Modares University, Tehran, Iran , , Khayatzadeh، Hamid نويسنده Molecular Genetics Department, Faculty of Biological Science, Tarbiat Modares University, Tehran , , Kalhor، Hamid Reza نويسنده Omics Research Center, Golestan University of Medical Sciences, Gorgan , , Mowla، Seyed Javad نويسنده ,
Issue Information
دوفصلنامه با شماره پیاپی 64 سال 2015
Pages
12
From page
494
To page
505
Abstract
Objective: MiR-302-367 is a cluster of polycistronic microRNAs that are exclusively expressed
in embryonic stem (ES) cells. The miR-302-367 promoter is functional during
embryonic development but is turned off in later stages. Motivated by the cancer stem
cell hypothesis, we explored the potential expression of miR-302 in brain tumor cell lines.
Materials and Methods: In the present experimental study, we have tried to expand
our knowledge on the expression pattern and functionality of miR302 cluster by quantifying
its expression in a series of glioma (A-172, 1321N1, U87MG) and medulloblastoma
(DAOY) cell lines. To further assess the functionality of miR-302 in these cell
lines, we cloned its promoter core region upstream of the enhanced green fluorescent
protein (EGFP) or luciferase encoding genes.
Results: Our data demonstrated a very low expression of miR-302 in glioma cell lines,
compared with that of embryonal carcinoma cell line NT2 being used as a positive
control. The expression of miR-302 promoter-EGFP construct in the aforementioned
cell lines demonstrated GFP expression in a rare subpopulation of the cells. Serum
deprivation led to the generation of tumorospheres, enrichment of miR-302 positive
cells and upregulation of a number of pluripotency genes.
Conclusion: Taken together, our data suggest that miR-302 could potentially be used as
a novel putative cancer stem cell marker to identify and target cancer stem cells within
tumor tissues.
Journal title
Cell Journal (Yakhteh)
Serial Year
2015
Journal title
Cell Journal (Yakhteh)
Record number
1871417
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