MicroRNA-184 inhibits cell proliferation and invasion,and specifically targets TNFAIP2 in Glioma

Background: mirna-184 is an oncogene in human hepatocellular carcinoma but acts as a tumor suppressor in tongue squamous cell carcinoma. studies have shown that mir-184 was down-regulated in glioma and tnfα-induced protein 2 (tnfaip2) was closely related to tumorigenesis. this study aimed to determine the functions of mir-184 in glioma and the mechanisms of mirna-184-tnfaip2 mediated glioma progression. methods: real-time reverse-transcription pcr detected expression of mir-184 and tnfaip2. u87 and u251 cells were transfected with mir-184 mimic,inhibitor,or negative control mirna,and their invasion abilities were assayed. cellular proliferation was measured by the cell counting kit-8 assay. mir-184 effects on glioma cell apoptosis and cell cycle were assessed by flow cytometer. biological information software have predicted that mir-184 could target tnfα-induced protein 2 (tnfaip2),which was further validated by western blot and qrt-pcr in glioma cells. in vivo,u87 cells transduced with either lentiviral over-expressed mir-184 or control lentivirus were injected into nude mice subcutaneously and intracranial respectively. results: expression of mir-184 was significantly lower in glioma tissues and cell-lines compared to normal brain tissues. protein and mrna expression of tnfaip2 were inversely correlated with mir-184 in glioma. in vitro,proliferation and invasion abilities were also decreased in u87 and u251 cells after transfection with mir-184 mimic. in vivo,the xenografted tumor size in the mir-184 overexpressing group were smaller than the mir-nc group. concordantly,u87 and u251 cells transfected with mir-184 mimic had a higher apoptosis rate,triggering an accumulation of cells at the g0/g1 phase and decreased cells in s-phase. conclusions: mir-184 could regulate tnfaip2 expression and affected its translation in glioma. mir-184 could also inhibit glioma progression and might serve as a novel therapeutic target in glioma. © 2015 cheng et al.; licensee biomed central.