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首页> 外文期刊>Asian Pacific Journal of Cancer Prevention >Microarray Analysis of the Hypoxia-induced Gene Expression Profile in Malignant C6 Glioma Cells
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Microarray Analysis of the Hypoxia-induced Gene Expression Profile in Malignant C6 Glioma Cells

机译:恶性C6胶质瘤细胞缺氧诱导基因表达谱的微阵列分析

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Hypoxia is commonly featured during glioma growth and plays an important role in the processes underlying tumor progression to increasing malignancy. Here we compared the gene expression profiles of rat C6 malignant glioma cells under normoxic and hypoxic conditions by cDNA microarray analysis. Compared to normoxic culture conditions, 180 genes were up-regulated and 67 genes were down-regulated under hypoxia mimicked by treatment. These differentially expressed genes were involved in mutiple biological functions including development and differentiation, immune and stress response, metabolic process, and cellular physiological response. It was found that hypoxia significantly regulated genes involved in regulation of glycolysis and cell differentiation, as well as intracellular signalling pathways related to Notch and focal adhesion, which are closely associated with tumor malignant growth. These results should facilitate investigation of the role of hypoxia in the glioma development and exploration of therapeutic targets for inhibition of glioma growth.
机译:缺氧在胶质瘤生长期间通常在肿瘤进展的过程中发挥重要作用,以增加恶性肿瘤。在这里,我们通过CDNA微阵列分析比较了常氧和缺氧条件下大鼠C6恶性胶质瘤细胞的基因表达谱。与常氧培养条件相比,上调180个基因,并在通过处理模仿的缺氧下下调67个基因。这些差异表达的基因涉及多个生物学功能,包括发育和分化,免疫和应激反应,代谢过程和细胞生理反应。发现缺氧显着调节糖酵解和细胞分化调节的基因,以及与凹口和局部粘附相关的细胞内信号传导途径,其与肿瘤恶性生长密切相关。这些结果应促进缺氧在胶质瘤发展中的作用和抑制胶质瘤生长的治疗靶标的作用。

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