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Genetic profiling of epithelial cells expressing E-cadherin repressors reveals a distinct role for snail, Slug, and E47 Factors in epithelial- mesenchymal transition

机译:表达E-钙粘着蛋白阻遏物的上皮细胞的遗传概况揭示了蜗牛,Slug和E47因子在上皮-间质转化中的独特作用

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摘要

The transcription factors Snail, Slug, and bHLH E47 have been recently described as direct repressors of E-cadherin and inducers of epithelial-mesenchymal transition (EMT) and invasion when overexpressed in epithelial cells. Although a role of those factors in tumor progression and invasion has been proposed, whether the different repressors play distinct or redundant roles in the tumorigenic process has not been established. To further investigate this important issue, we have analyzed the gene expression profiling of Madin-Darby canine kidney (MDCK) epithelial cells expressing the different repressors (MDCK-Snail, MDCK-Slug, and MDCK-E47 cells) versus control MDCK cells by cDNA microarrays. A total of 243 clones (228 genes and 15 expressed sequence tags) were found to be differentially expressed between either of the three MDCK-derived cell lines and control MDCK cells. Twenty two of the candidate genes were validated by Northern blot, Western blot, immunofluorescence, and promoter analyses in cell lines and by immunohistochemistry in xenografted tumors. Gene clustering analysis indicated that about a third of the 243 candidate genes were common to MDCK cells expressing Snail, Slug, or E47 factors, whereas the rest of the genes were regulated in only one or two cell types. Differentially regulated genes include those related to EMT (45 genes), transcriptional regulation (IS genes), cell proliferation and signaling (54 genes), apoptosis (12 genes), and angiogenesis (9 genes). These results indicate that Snail, Slug, and E47 transcription factors induce common and specific genetic programs, supporting a differential role of the factors in tumor progression and invasion. ©2006 American Association for Cancer Research.
机译:转录因子Snail,Slug和bHLH E47最近已被描述为E-钙粘蛋白的直接阻遏物,以及在上皮细胞中过表达时上皮-间质转化和侵袭的诱导剂。尽管已经提出了这些因素在肿瘤进展和侵袭中的作用,但是尚未确定不同的阻遏物在致瘤过程中起不同的作用还是多余的作用。为了进一步研究这个重要问题,我们分析了通过表达不同阻遏物(MDCK-Snail,MDCK-Slug和MDCK-E47细胞)与对照MDCK细胞的Madin-Darby犬肾(MDCK)上皮细胞的基因表达谱芯片。发现总共243个克隆(228个基因和15个表达的序列标签)在三种MDCK来源的细胞系和对照MDCK细胞之一之间差异表达。在细胞系中通过Northern印迹,蛋白质印迹,免疫荧光和启动子分析以及在异种移植肿瘤中的免疫组织化学验证了22个候选基因。基因聚类分析表明,在243个候选基因中,约有三分之一是表达Snail,Slug或E47因子的MDCK细胞共有的,而其余基因仅在一种或两种细胞类型中受到调控。差异调节基因包括与EMT(45个基因),转录调节(IS基因),细胞增殖和信号转导(54个基因),凋亡(12个基因)和血管生成(9个基因)相关的基因。这些结果表明,Snail,Slug和E47转录因子诱导共同的和特定的遗传程序,从而支持这些因子在肿瘤进展和侵袭中的不同作用。 ©2006美国癌症研究协会。

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