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Gadd45a inhibits cell migration and invasion by altering the global RNA expression

机译:Gadd45a通过改变整体RNA表达抑制细胞迁移和侵袭

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Gadd45a, the first well-defined p53 downstream gene, can be induced by multiple DNA-damaging agents, which plays important roles in the control of cell cycle checkpoint, DNA repair process and signaling transduction. Our previous findings suggested that Gadd45a maintains cell-cell adhesion and cell contact inhibition. However, little is known about how Gadd45a participates in the suppression of malignancy in human cancer cells. To examine the functions of Gadd45a in cell invasion and metastasis, we performed the adhesion, wound-healing and transwell assays in Gadd45a+/+ and Gadd45a-/- MEF cell lines. We found the adhesion, migration and invasive abilities were much higher in Gadd45a deficient cells. We furthermore applied high-throughput cDNA microarray analysis and bioinformatics analysis to analyze the mechanisms of Gadd45a gene in invasion and metastasis. Compared with the Gadd45a wild type cells, the Gadd45a deficient cells showed a wide range of transcripts alterations. The altered gene pathways were predicted by the MAS software, which indicated focal adhesion, cell communication, ECM-receptor interaction as the three main pathways. Real-time PCR was employed to validate the differentially expressed genes. Interestingly, we figured out that the deregulations of these genes are caused neither by genomic aberrations nor methylation status. These findings provided a novel insight that Gadd45a may involve in tumor progression by regulating related genes expressions.
机译:Gadd45a是第一个明确定义的p53下游基因,可以被多种DNA破坏剂诱导,它们在控制细胞周期检查点,DNA修复过程和信号转导中起着重要作用。我们以前的发现表明,Gadd45a维持细胞与细胞的粘附和细胞接触抑制。然而,关于Gadd45a如何参与抑制人类癌细胞的恶性肿瘤的了解甚少。为了检查Gadd45a在细胞侵袭和转移中的功能,我们在Gadd45a + / +和Gadd45a-/-MEF细胞系中进行了粘附,伤口愈合和transwell分析。我们发现Gadd45a缺陷细胞的粘附,迁移和侵袭能力更高。我们还应用高通量cDNA微阵列分析和生物信息学分析来分析Gadd45a基因在侵袭和转移中的机制。与Gadd45a野生型细胞相比,Gadd45a缺陷型细胞表现出广泛的转录物变化。 MAS软件预测了改变的基因途径,表明粘着,细胞通讯,ECM-受体相互作用是三个主要途径。实时PCR被用来验证差异表达的基因。有趣的是,我们发现这些基因的失调既不是由基因组畸变也不是由甲基化状态引起的。这些发现提供了新的见解,认为Gadd45a可能通过调节相关基因的表达参与肿瘤的发展。

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