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microRNA-130a is an oncomir suppressing the expression of CRMP4 in gastric cancer

机译:microRNA-130a是抑制CRMP4在胃癌中表达的疾病

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Gastric cancer is one of the most common causes of death worldwide, although its incidence has steadily declined in recent years. There is strong evidence that aberrantly expressed microRNAs (miRNAs) are involved in gastric cancer tumorigenesis. Furthermore, CRMP4 is closely associated with the occurrence and development of gastric cancer, and our predictions suggest that miR-130a, which can promote gastric cancer tumorigenesis, is a potential CRMP4 regulator. In this study, we investigated the expression of CRMP4 and miR-130a in human gastric cancer cell lines by quantitative reverse transcription polymerase chain reaction (qRT-PCR) and Western blot (WB) examination and direct interactions between miR-130a and CRMP4 by dual-luciferase reporter assay. We also evaluated the biological roles of miR-130a and CRMP4 in gastric cancer cells by flow cytometry, MTT assay, soft agar colony formation assay, and Transwell tests and confirmed CRMP4 function in vivo, using a tumor xenograft model. Our results demonstrated that CRMP4 expression was significantly decreased at both the gene and protein levels, while miR-130a expression was notably increased, in five human gastric cancer cell lines compared with human gastric epithelial cells. Dual-luciferase reporter assays indicated that CRMP4 was the direct target of miR-130a. Moreover, an inverse regulatory relationship between miR-130a and CRMP4 was verified by qRT-PCR and WB, and overexpression of miR-130a in BGC823 cells enhanced apoptosis and cell proliferation, arrested the cell cycle in G0/G1, and facilitated cell colony formation, invasion, migration, and adhesion, while upregulation of CRMP4 had opposite effects. Finally, the growth and weight of transplanted tumors derived from BGC823 cells in which CRMP4 was knocked down were remarkably reduced. These data indicate that miR-130a is an oncomir targeting CRMP4 and could be developed as a potential prognostic factor and a novel therapeutic target in gastric cancer.
机译:胃癌是全球范围内最常见的死亡原因之一,尽管近年来其发病率稳步下降。有强有力的证据表明,异常表达的microRNA(miRNA)与胃癌的肿瘤发生有关。此外,CRMP4与胃癌的发生和发展密切相关,我们的预测表明,可以促进胃癌肿瘤发生的miR-130a是潜在的CRMP4调节剂。在这项研究中,我们通过定量逆转录聚合酶链反应(qRT-PCR)和蛋白质印迹(WB)检查以及miR-130a和CRMP4之间的直接相互作用,研究了CRMP4和miR-130a在人胃癌细胞系中的表达。 -荧光素酶报告基因分析。我们还通过异种移植模型通过流式细胞仪,MTT分析,软琼脂菌落形成分析和Transwell测试评估了miR-130a和CRMP4在胃癌细胞中的生物学作用,并证实了CRMP4在体内的功能。我们的结果表明,与人胃上皮细胞相比,在五个人胃癌细胞系中,CRMP4表达在基因和蛋白质水平上均显着降低,而miR-130a表达则显着提高。双重荧光素酶报告基因检测表明CRMP4是miR-130a的直接靶标。此外,通过qRT-PCR和WB验证了miR-130a和CRMP4之间的反调控关系,miR-130a在BGC823细胞中的过表达增强了细胞凋亡和细胞增殖,阻止了G0 / G1细胞周期,并促进了细胞集落的形成。 ,侵袭,迁移和粘附,而CRMP4的上调则相反。最终,显着降低了其中敲除CRMP4的BGC823细胞衍生的移植瘤的生长和重量。这些数据表明,miR-130a是靶向CRMP4的疾病,可作为胃癌的潜在预后因素和新的治疗靶标开发。

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