Downregulation of the urokinase-type plasminogen activator receptor through inhibition of translation by antisense oligonucleotide suppresses invasion of human glioblastoma cells

被引:0
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作者
Pamarthi M. Mohan
Sajani S. Lakka
Sanjeeva Mohanam
Yoshiaki Kin
Raymond Sawaya
Anthanassios P. Kyritsis
Garth L. Nicolson
Jasti S. Rao
机构
[1] Department of Neurosurgery,Department of Neuro
[2] The University of Texas M.D. Anderson Cancer Center,Oncology
[3] The Institute for Molecular Medicine,undefined
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关键词
urokinase receptor; antisense; recombinant adenovirus; gliomas; invasion;
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摘要
We previously showed that downregulation of the urokinase-type plasminogen activator receptor (uPAR) in the SNB19 human glioblastoma cell line by the stable transfection of a plasmid expressing a 300 bp antisense sequence to the 5′ end of the uPAR gene produced a decrease in the amount of target mRNA. In a more recent study, we found that adenovirus-mediated transduction (Ad-uPAR) of the same uPAR antisense gene construct in SNB19 cells also downregulated uPAR protein levels. We report here that Ad-uPAR-transfected SNB19 cells produced the same amounts of target uPAR mRNA but significantly less protein by in vitro translation and by in situ [35S] labeling compared to Ad-CMV vector-transfected and mock-transfected cells. This antisense construct also inhibited glioblastoma cell invasion confirming previous results. We conclude that downregulation of uPAR by this antisense gene construct results from inhibition of protein translation.
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页码:617 / 621
页数:4
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