首页> 外文期刊>International journal of molecular medicine >Comprehensive gene expression microarray analysis of Ets-1 blockade in PC3 prostate cancer cells and correlations with prostate cancer tissues: Insights into genes involved in the metastatic cascade
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Comprehensive gene expression microarray analysis of Ets-1 blockade in PC3 prostate cancer cells and correlations with prostate cancer tissues: Insights into genes involved in the metastatic cascade

机译:PC3前列腺癌细胞中Ets-1阻滞及其与前列腺癌组织的相关性的全面基因表达微阵列分析:对参与转移级联反应的基因的见解

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Ets-1 is the prototype of the ETS family of transcription factors and is suggested to play an important role in the malignant progression of prostatic carcinomas. Therefore, in this study we investigated the effect of blocking Ets-1 in PC3 prostate cancer cells on genes involved in the metastatic cascade, and correlated these findings with prostate cancer tissues. Two stable PC3 cell cultures were established by transfection with either an Ets-1 inverse antisense expression vector or a mock control vector. The effect of blocking Ets-1 on genes involved in the metastatic cascade was assessed by a comprehensive gene expression microarray analysis of Ets-1 inverse and mock control cells. Correlating the sets of genes found in the PC3 microarray data with prostate cancer tissues was performed by verifying the genes in a comprehensive gene expression microarray analysis of RNA extracted from laser microdissected normal prostate glands and from carcinoma glands taken from prostate cancer patients. Western blot analysis confirmed the presence of Ets-1 in mock cells and its absence in Ets-1 inverse cells. In the Ets-1 blockade microarray, many differentially expressed genes were found; however, only genes with a greater than 10-fold up- or down-regulation between the Ets-1 blockade and mock control were considered significant. The genes were placed into four groups that play a role in the so-called metastatic cascade based on their known functions in proliferation, apoptosis, migration and angiogenesis. The genes found in the Ets-1 blockade microarray analysis were verified for their presence in the microarray analysis of prostate cancer tissues. Genes found in the microarray analysis of prostate cancer tissues with an >2-fold change and a p-value <0.01 were considered significant. We identified sets of genes that are involved in the metastatic cascade and are known to be implicated in prostate cancer to show changes in the expression patterns due to the Ets-1 blockade in PC3 cells. Correlating these sets of genes with the findings in prostate cancer tissues, we identified 16 genes that are up- or down-regulated in healthy compared to tumor prostate glands. Further investigation revealed that 4 out of the 16 genes have been reported to be regulated by members of the ETS family. These findings provide in?vitro and in?vivo evidence for the importance of Ets-1 in the development and progression of prostate cancer.
机译:Ets-1是ETS转录因子家族的原型,被认为在前列腺癌的恶性进展中起重要作用。因此,在这项研究中,我们研究了在PC3前列腺癌细胞中阻断Ets-1对参与转移级联反应的基因的影响,并将这些发现与前列腺癌组织相关联。通过用Ets-1反义表达载体或模拟对照载体转染,建立了两种稳定的PC3细胞培养物。通过对Ets-1逆向和模拟对照细胞进行全面的基因表达微阵列分析,评估了阻断Ets-1对涉及转移级联的基因的影响。通过在综合基因表达微阵列分析中验证从激光显微切割的正常前列腺和从前列腺癌患者身上提取的RNA中提取的RNA,对PC3微阵列数据中发现的基因组与前列腺癌组织进行关联。蛋白质印迹分析证实了模拟细胞中存在Ets-1,而在Ets-1反向细胞中则不存在。在Ets-1封锁微阵列中,发现了许多差异表达的基因。然而,只有在Ets-1封锁和模拟控制之间具有大于或等于10倍的上调或下调的基因才被认为是重要的。根据基因在增殖,凋亡,迁移和血管生成中的已知功能,将其分为四个在所谓的转移级联中起作用的基因。验证了在Ets-1封锁微阵列分析中发现的基因是否存在于前列腺癌组织的微阵列分析中。在前列腺癌组织的微阵列分析中发现的基因具有> 2倍的变化和p值<0.01的基因被认为是重要的。我们确定了与转移级联有关的基因集,并已知与前列腺癌有关,以显示由于PC3细胞中Ets-1阻滞而导致的表达模式变化。将这些基因组与前列腺癌组织中的发现相关联,我们确定了与肿瘤前列腺相比在健康中上调或下调的16个基因。进一步的调查表明,据报道16种基因中有4种受到ETS家族成员的调控。这些发现为Ets-1在前列腺癌的发生和发展中的重要性提供了体内和体外证据。

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