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Fra-1可诱导上皮样腺癌细胞发生形态学转变,并增强其体外侵袭能力和运动能力。

Fra-1 induces morphological transformation and increases in vitro invasiveness and motility of epithelioid adenocarcinoma cells.

作者信息

Kustikova O, Kramerov D, Grigorian M, Berezin V, Bock E, Lukanidin E, Tulchinsky E

机构信息

Department of Molecular Cancer Biology, Danish Cancer Society, DK-2100 Copenhagen O, Denmark.

出版信息

Mol Cell Biol. 1998 Dec;18(12):7095-105. doi: 10.1128/MCB.18.12.7095.

Abstract

Two cell lines originating from a common ancestral tumor, CSML0 and CSML100, were used as a model to study AP-1 transcription factors at different steps of tumor progression. CSML0 cells have an epithelial morphology; they express epithelial but not mesenchymal markers and are invasive neither in vitro nor in vivo. CSML100 possesses all characteristics of a highly progressive carcinoma. These cells do not form tight contacts, are highly invasive in vitro, and are metastatic in vivo. AP-1 activity was considerably higher in CSML100 cells than in CSML0 cells. There was a common predominant Jun component, namely, JunD, detected in both cell lines. We found that the enhanced level of AP-1 in CSML100 cells was due to high expression of Fra-1 and Fra-2 proteins, which were undetectable in CSML0 nuclear extracts. Analysis of the transcription of different AP-1 members in various cell lines derived from tumors of epithelial origin revealed a correlation of fra-1 expression with mesenchymal characteristics of carcinoma cells. Moreover, we show here for the first time that the expression of exogenous Fra-1 in epithelioid cells results in morphological changes that resemble fibroblastoid conversion. Cells acquire an elongated shape and become more motile and invasive in vitro. Morphological alterations were accompanied by transcriptional activation of certain genes whose expression is often induced at late stages of tumor progression. These data suggest a critical role of the Fra-1 protein in the development of epithelial tumors.

摘要

源自同一祖先肿瘤的两种细胞系CSML0和CSML100被用作模型,以研究肿瘤进展不同阶段的AP-1转录因子。CSML0细胞具有上皮形态;它们表达上皮标志物而非间充质标志物,在体外和体内均无侵袭性。CSML100具有高度进展性癌的所有特征。这些细胞不形成紧密连接,在体外具有高度侵袭性,在体内具有转移性。CSML100细胞中的AP-1活性明显高于CSML0细胞。在两种细胞系中均检测到一种常见的主要Jun成分,即JunD。我们发现CSML100细胞中AP-1水平的升高是由于Fra-1和Fra-2蛋白的高表达,而在CSML0核提取物中未检测到这些蛋白。对源自上皮性肿瘤的各种细胞系中不同AP-1成员转录的分析揭示了fra-1表达与癌细胞间充质特征的相关性。此外,我们首次在此表明,在上皮样细胞中外源Fra-1的表达导致形态变化,类似于成纤维细胞样转化。细胞在体外获得细长形状并变得更具运动性和侵袭性。形态学改变伴随着某些基因的转录激活,这些基因的表达通常在肿瘤进展后期被诱导。这些数据表明Fra-1蛋白在上皮性肿瘤发展中起关键作用。

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