5-Aza-2’-deoxycytidine (5-AzadC) is an anti-cancer drug, currently used in the tumor therapy. However, the underneath mechanisms of the anti-invasiveness effect on human glioma are still unknown. In the present study, we investigated the possibility of whether 5-AzadC can be used to control the invasiveness of human glioma, and the mechanisms by which 5-AzadC regulate cell invasiveness in human glioma cells. We found that malignant human glioma cells constitutively expressed matrix metalloproteinase-2 (MMP-2), and the MMP-2 activities were correlated well with their malignancies. We demonstrated that 5-AzadC suppressed MMP-2 activity in U87MG astrocytoma cells and other primary astrocytoma cell lines. 5-AzadC decreased MMP-2 expression without causing cell death. At the same conditions, we found that 5-AzadC increased glial fibrillary acidic protein (GFAP) expression in U87MG cell suggesting that 5-AzadC induces cell redifferentiation, which was associated with decreased cell invasiveness. Using in vitro invasion assay, we demonstrated that differentiated U87MG cells exhibited lower invasiveness. In addition, we found that 5-AzadC increased TIMP-2 expression, suggesting that 5-AzadC not only reduced MMP-2 expression but also inhibited MMP-2 activation. Taken together, these findings support a safer strategy targeting glioma invasiveness in context of glioma therapy.