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Clinical Relevance and Therapeutic Significance of MicroRNA‐133a Expression Profiles and Functions in Malignant Osteosarcoma‐Initiating Cells

Authors :
Fujiwara, Tomohiro
Katsuda, Takeshi
Hagiwara, Keitaro
Kosaka, Nobuyoshi
Yoshioka, Yusuke
Takahashi, Ryou‐U
Takeshita, Fumitaka
Kubota, Daisuke
Kondo, Tadashi
Ichikawa, Hitoshi
Yoshida, Akihiko
Kobayashi, Eisuke
Kawai, Akira
Ozaki, Toshifumi
Ochiya, Takahiro
Source :
Stem Cells; April 2014, Vol. 32 Issue: 4 p959-973, 15p
Publication Year :
2014

Abstract

Novel strategies against treatment‐resistant tumor cells remain a challenging but promising therapeutic approach. Despite accumulated evidence suggesting the presence of highly malignant cell populations within tumors, the unsolved issues such as in vivotargeting and clinical relevance remain. Here, we report a preclinical trial based on the identified molecular mechanisms underlying osteosarcoma‐initiating cells and their clinical relevance. We identified key microRNAs (miRNAs) that were deregulated in a highly malignant CD133highpopulation and found that miR‐133a regulated the cell invasion that characterizes a lethal tumor phenotype. Silencing of miR‐133a with locked nucleic acid (LNA) reduced cell invasion of this cell population, and systemic administration of LNA along with chemotherapy suppressed lung metastasis and prolonged the survival of osteosarcoma‐bearing mice. Furthermore, in a clinical study, high expression levels of CD133 and miR‐133a were significantly correlated with poor prognosis, whereas high expression levels of the four miR‐133a target genes were correlated with good prognosis. Overall, silencing of miR‐133a with concurrent chemotherapy would represent a novel strategy that targets multiple regulatory pathways associated with metastasis of the malignant cell population within osteosarcoma. StemCells2014;32:959–973

Details

Language :
English
ISSN :
10665099 and 15494918
Volume :
32
Issue :
4
Database :
Supplemental Index
Journal :
Stem Cells
Publication Type :
Periodical
Accession number :
ejs32404211
Full Text :
https://doi.org/10.1002/stem.1618