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E1A + cHa-ras转化的大鼠胚胎成纤维细胞的特征是AP-1二聚体具有高且组成显著改变的组成型DNA结合活性。

E1A + cHa-ras transformed rat embryo fibroblast cells are characterized by high and constitutive DNA binding activities of AP-1 dimers with significantly altered composition.

作者信息

Pospelova T V, Medvedev A V, Kukushkin A N, Svetlikova S B, van der Eb A J, Dorsman J C, Pospelov V A

机构信息

Institute of Cytology, Russian Academy of Sciences, St-Petersburg.

出版信息

Gene Expr. 1999;8(1):19-32.

Abstract

Transcription factors of the AP-1/ATF family, including c-Fos, c-Jun, and ATF-2, play an important role in the regulation of cell proliferation and differentiation, and changes in their levels and/or activities may contribute to oncogenesis. We analyzed the alterations of AP-1/ATF transcription factors upon immortalization and transformation in a panel of cell lines derived from rat embryo fibroblast (REF) cells. The tumorigenic E1A + cHa-ras cells are characterized by high and constitutive DNA binding activities of AP-1, in contrast to nontransformed cells and the E1A cells. The expression of c-fos and c-jun genes was affected differently by the oncogenic transformation. By using antibodies to c-Jun and c-Fos proteins in electrophoretic mobility shift assays (EMSA), we showed that E1A + cHa-ras transformants did not contain c-Fos under any condition of cell cultivation and growth factor stimulation, whereas c-Jun was constitutively upregulated. In the absence of c-fos gene expression, c-Fos protein appears to be replaced by proteins of Fos family (Fra-1) and ATF family (ATF-2 and ATFa). To determine the possible mechanisms of c-fos downregulation in E1A + cHa-ras transformants we have obtained populations of geneticin-resistant clones containing integrated reporter construct -711fos-CAT and its mutants in serum-responsive element (SRE) and cAMP-responsive element (CRE). Data obtained show that the mutations within the SRE lead to a manifold activation of fos-CAT expression. This allows to suggest that c-fos downregulation in E1A + cHa-ras transformants is provided by a negative control mediated through the SRE regulatory region. The profound differences in regulation and composition of transcription factors of the AP-1 family probably play a pivotal role in the transformation of REF cells by E1A and cHa-ras oncogenes.

摘要

AP-1/ATF家族的转录因子,包括c-Fos、c-Jun和ATF-2,在细胞增殖和分化的调控中发挥重要作用,其水平和/或活性的变化可能与肿瘤发生有关。我们分析了一组源自大鼠胚胎成纤维细胞(REF)的细胞系在永生化和转化过程中AP-1/ATF转录因子的变化。与未转化细胞和E1A细胞相比,致瘤性E1A + c-Ha-ras细胞的特征是AP-1具有高水平的组成型DNA结合活性。致癌转化对c-fos和c-jun基因的表达有不同影响。通过在电泳迁移率变动分析(EMSA)中使用针对c-Jun和c-Fos蛋白的抗体,我们发现,在任何细胞培养和生长因子刺激条件下,E1A + c-Ha-ras转化体都不含c-Fos,而c-Jun则组成型上调。在没有c-fos基因表达的情况下,c-Fos蛋白似乎被Fos家族(Fra-1)和ATF家族(ATF-2和ATFa)的蛋白所取代。为了确定E1A + c-Ha-ras转化体中c-fos下调的可能机制,我们获得了含有整合报告构建体-711fos-CAT及其在血清反应元件(SRE)和cAMP反应元件(CRE)中的突变体的遗传霉素抗性克隆群体。获得的数据表明,SRE内的突变导致fos-CAT表达的多重激活。这表明E1A + c-Ha-ras转化体中c-fos的下调是由通过SRE调控区域介导的负调控提供的。AP-1家族转录因子在调控和组成上的深刻差异可能在E1A和c-Ha-ras癌基因对REF细胞的转化中起关键作用。

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本文引用的文献

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Transformation by ras modifies AP1 composition and activity.
Oncogene. 1997 Feb 20;14(7):837-47. doi: 10.1038/sj.onc.1200900.

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