miRâ378aâ3p inhibits cellular proliferation and migration in glioblastoma multiforme by targeting tetraspanin 17.
[No authors listed]
摘要
Glioblastoma multiforme (GBM) is the most common and aggressive brain tumor and patients with this disease tend to have poor clinical outcome. MicroRNAs (miRs) are important regulators of a number of key pathways implicated in tumor pathogenesis. Recently, the expression of miRâ378 was shown to be dysregulated in several different types of cancer, including gastric cancer, colorectal cancer and oral carcinoma. Additional studies have demonstrated that miRâ378 may serve as a potential therapeutic target against human breast cancer. However, the underlying mechanisms and potential targets of miRâ378aâ3p involved in GBM remain unknown. The aim of the present of was to determine the effects of miRâ378aâ3p and its potential targets. Tetraspanin 17 is involved in the neoplastic events in GBM and is a member of the tetraspanin family of proteins. The tetraspanins are involved in the regulation of cell growth, migration and invasion of several different types of cancer cell lines, and may potentially act as an oncogene associated with GBM pathology. The results of the present study showed that high miRâ378aâ3p and low expression levels were associated with improved survival in patients with GBM. Additionally, high levels of Tduanyu1842N17 were linked to the poor prognosis of patients with GBM aged 50â60, larger tumor sizes (â¥5 cm) and an advanced World Health Organization stage. Tduanyu1842N17 was identified and confirmed as a direct target of miRâ378aâ3p using a luciferase reporter assay in human glioma cell lines. Overexpression of miRâ378aâ3p in either of U87MG or MTâ330 cells decreased the expression of promoted apoptosis and decreased proliferation, migration and invasion. Overexpression of Tduanyu1842N17 attenuated the aforementioned effects induced by miRâ378aâ3p overexpression. The present study indicated that miRâ378aâ3p suppresses the progression of GBM by reducing Tduanyu1842N17 expression, and may thus serve as a potential therapeutic target for treating patients with GBM.
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基因功能
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原始数据
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文献解读
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