Journal
TUMOR BIOLOGY
Volume 37, Issue 9, Pages 12039-12047Publisher
SAGE PUBLICATIONS LTD
DOI: 10.1007/s13277-016-5072-4
Keywords
TUSC3; Glioblastoma; Akt signaling; Methylation
Categories
Funding
- International S&T Cooperation Program of China [2014DFA31630]
- National Nature Science Foundation of China [81571646, 81471326, 81500924, 81572472, 81501050, 81571108]
- Specialized Research Fund for the Doctoral Program of Higher Education [20132307110029]
- Scientific and Technology Research Fund of the Heilongjiang Education Department [12541469]
- Natural Science Foundation of Heilongjiang Province [H201348, H201434, H2015062]
- Application Technology Research and Development Project of Heilongjiang Province [GA15C108, GA15C103-01]
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Glioblastoma multiform is one of the most common and most aggressive brain tumors in humans. The molecular and cellular mechanisms responsible for the onset and progression of GBM are elusive and controversial. The function of tumor suppressor candidate 3 (TUSC3) has not been previously characterized in GBM. TUSC3 was originally identified as part of an enzyme complex involved in N-glycosylation of proteins, but was recently implicated as a potential tumor suppressor gene in a variety of cancer types. In this study, we demonstrated that the expression levels of TUSC3 were downregulated in both GBM tissues and cells, and also found that overexpression of TUSC3 inhibits GBM cell proliferation and invasion. In addition, the effects of increased levels of methylation on the TUSC3 promoter were responsible for decreased expression of TUSC3 in GBM. Finally, we determined that TUSC3 regulates proliferation and invasion of GBM cells by inhibiting the activity of the Akt signaling pathway.
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