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人MUC2粘蛋白基因在胃肠道癌细胞系中受Cdx同源结构域蛋白的转录调控。

Human MUC2 mucin gene is transcriptionally regulated by Cdx homeodomain proteins in gastrointestinal carcinoma cell lines.

作者信息

Mesquita Patrícia, Jonckheere Nicolas, Almeida Raquel, Ducourouble Marie-Paule, Serpa Jacinta, Silva Elisabete, Pigny Pascal, Silva Filipe Santos, Reis Celso, Silberg Debra, Van Seuningen Isabelle, David Leonor

机构信息

Institute of Molecular Pathology and Immunology (IPATIMUP), University of Porto, Rua Dr. Roberto Frias s/n, 4200 Porto, Portugal.

出版信息

J Biol Chem. 2003 Dec 19;278(51):51549-56. doi: 10.1074/jbc.M309019200. Epub 2003 Oct 2.

Abstract

In intestinal metaplasia and 30% of gastric carcinomas, MUC2 intestinal mucin and the intestine-specific transcription factors Cdx-1 and Cdx-2 are aberrantly expressed. The involvement of Cdx-1 and Cdx-2 in the intestinal development and their role in transcription of several intestinal genes support the hypothesis that Cdx-1 and/or Cdx-2 play important roles in the aberrant intestinal differentiation program of intestinal metaplasia and gastric carcinoma. To clarify the mechanisms of transcriptional regulation of the MUC2 mucin gene in gastric cells, pGL3 deletion constructs covering 2.6 kb of the human MUC2 promoter were used in transient transfection assays, enabling us to identify a relevant region for MUC2 transcription in all gastric cell lines. To evaluate the role of Cdx-1 and Cdx-2 in MUC2 transcription we performed co-transfection experiments with expression vectors encoding Cdx-1 and Cdx-2. In two of the four gastric carcinoma cell lines and in all colon carcinoma cell lines we observed transactivation of the MUC2 promoter by Cdx-2. Using gel shift assays we identified two Cdx-2 binding sites at -177/-171 and -191/-187. Only simultaneous mutation of the two sites resulted in inhibition of Cdx-2-mediated transactivation of MUC2 promoter, implying that both Cdx-2 sites are active. Finally, stable expression of Cdx-2 in a gastric cell line initially not expressing Cdx-2, led to induction of MUC2 expression. In conclusion, this work demonstrates that Cdx-2 activates the expression of MUC2 mucin gene in gastric cells, inducing an intestinal transdifferentiation phenotype that parallels what is observed both in intestinal metaplasia and some gastric carcinomas.

摘要

在肠化生以及30%的胃癌中,MUC2肠黏蛋白以及肠道特异性转录因子Cdx-1和Cdx-2表达异常。Cdx-1和Cdx-2参与肠道发育以及它们在多个肠道基因转录中的作用支持了这样一个假说,即Cdx-1和/或Cdx-2在肠化生和胃癌异常的肠道分化程序中发挥重要作用。为了阐明胃细胞中MUC2黏蛋白基因转录调控的机制,在瞬时转染实验中使用了覆盖人类MUC2启动子2.6 kb的pGL3缺失构建体,这使我们能够在所有胃细胞系中鉴定出与MUC2转录相关的区域。为了评估Cdx-1和Cdx-2在MUC2转录中的作用,我们用编码Cdx-1和Cdx-2的表达载体进行了共转染实验。在四个胃癌细胞系中的两个以及所有结肠癌细胞系中,我们观察到Cdx-2对MUC2启动子的反式激活作用。通过凝胶迁移实验,我们在-177/-171和-191/-187处鉴定出两个Cdx-2结合位点。只有这两个位点同时发生突变才会导致Cdx-2介导的MUC2启动子反式激活受到抑制,这意味着这两个Cdx-2位点都是有活性的。最后,在一个最初不表达Cdx-2的胃细胞系中稳定表达Cdx-2,导致了MUC2表达的诱导。总之,这项工作表明Cdx-2在胃细胞中激活MUC2黏蛋白基因的表达,诱导出一种肠道转分化表型,这与在肠化生和一些胃癌中观察到的情况相似。

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