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miRNA-7 对 U373-MG 细胞系增殖及厄洛替尼敏感性的影响

MiRNA-7 Replacement Effect on Proliferation and Tarceva-Sensitivity in U373-MG Cell Line.

机构信息

Molecular and Medicine Research Center, Arak University of Medical Sciences, Arak, Iran.

Department of Molecular Medicine and Biotechnology, Arak University of Medical Sciences, Arak, Iran.

出版信息

Asian Pac J Cancer Prev. 2020 Jun 1;21(6):1747-1753. doi: 10.31557/APJCP.2020.21.6.1747.

DOI:10.31557/APJCP.2020.21.6.1747
PMID:32592373
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7568905/
Abstract

BACKGROUND

Deregulation of the EGFR signaling pathway activity has been shown to can be effective in resistance to EGFR-TKIs, such as Tarceva (erlotinib), in glioblastoma cells. In addition, reports have shown that the reduction of miRNA-7 expression levels is associated with an increase in the expression of EGFR. Here, we evaluated the effect of miRNA-7 on EGFR expression and sensitivity of the U373-MG glioblastoma to erlotinib.

METHODS

The effect of miRNA-7 on EGFR expression was examined using RT-qPCR and western blotting. Trypan blue and MTT assays were performed to explore the effect of treatments on cell growth and survival, respectively. The combination index analysis was used to evaluate the interaction between drugs. Apoptosis was measured by ELISA cell death assay.

RESULTS

We showed that miRNA-7 markedly inhibited the expression of EGFR and decreased the growth of glioblastoma cells, relative to blank control and negative control miRNA (p < 0.05). Introduction of miRNA-7 synergistically increased the sensitivity of the U373-MG cells to erlotinib. Results of apoptosis assay demonstrated that miRNA-7 can trigger apoptosis and enhance the erlotinib-mediated apoptosis.

CONCLUSIONS

Our results show that miRNA-7 plays a critical role in the growth, survival and sensitivity of the U373-MG cells to erlotinib by targeting EGFR. Thus, miRNA-7 replacement therapy can become an effective therapeutic procedure in glioblastoma.

摘要

背景

已证实 EGFR 信号通路活性的失调可有效抵抗 EGFR-TKIs(如 Tarceva(厄洛替尼)),从而导致胶质母细胞瘤细胞产生耐药性。此外,有报道表明 miRNA-7 表达水平的降低与 EGFR 表达的增加有关。在这里,我们评估了 miRNA-7 对 EGFR 表达和 U373-MG 胶质母细胞瘤对厄洛替尼敏感性的影响。

方法

使用 RT-qPCR 和 Western blot 检测 miRNA-7 对 EGFR 表达的影响。台盼蓝和 MTT 测定分别用于探索处理对细胞生长和存活的影响。采用组合指数分析评估药物之间的相互作用。通过 ELISA 细胞死亡测定法测量细胞凋亡。

结果

我们表明,与空白对照和阴性对照 miRNA 相比,miRNA-7 明显抑制了 EGFR 的表达并降低了胶质母细胞瘤细胞的生长(p < 0.05)。miRNA-7 的引入协同增强了 U373-MG 细胞对厄洛替尼的敏感性。细胞凋亡测定的结果表明,miRNA-7 可以触发细胞凋亡并增强厄洛替尼介导的细胞凋亡。

结论

我们的结果表明,miRNA-7 通过靶向 EGFR 在 U373-MG 细胞的生长、存活和对厄洛替尼的敏感性中发挥关键作用。因此,miRNA-7 替代疗法可能成为胶质母细胞瘤的有效治疗方法。

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