皮肤癌中C/EBPα表达降低与致癌性Ras相关，且癌细胞中C/EBPα的重新表达会抑制增殖。

Diminished expression of C/EBPalpha in skin carcinomas is linked to oncogenic Ras and reexpression of C/EBPalpha in carcinoma cells inhibits proliferation.

作者信息

Shim Minsub, Powers Kristina L, Ewing Sarah J, Zhu Songyun, Smart Robert C

机构信息

Cell Signaling and Cancer Group, Department of Environmental and Molecular Toxicology, North Carolina State University, Raleigh, NC 27695-7633, USA.

出版信息

Cancer Res. 2005 Feb 1;65(3):861-7.

PMID:15705884

Abstract

The basic leucine zipper transcription factor, CCAAT/enhancer binding protein alpha (C/EBPalpha) is involved in mitotic growth arrest and has been implicated as a human tumor suppressor in acute myeloid leukemia. We have previously shown that C/EBPalpha is abundantly expressed in mouse epidermal keratinocytes. In the current study, the expression of C/EBPalpha was evaluated in seven mouse skin squamous cell carcinoma (SCC) cell lines that contain oncogenic Ha-Ras. C/EBPalpha mRNA and protein levels were greatly diminished in all seven SCC cell lines compared with normal primary keratinocytes, whereas C/EBPbeta levels were not dramatically changed. Reexpression of C/EBPalpha in these SCC cell lines resulted in the inhibition in SCC cell proliferation. To determine whether the decrease in C/EBPalpha expression observed in the SCC cell lines also occurred in the carcinoma itself, immunohistochemical staining for C/EBPalpha in mouse skin SCCs was conducted. All 14 SCCs evaluated displayed negligible C/EBPalpha protein expression and normal C/EBPbeta levels compared with the epidermis and all 14 carcinomas contained mutant Ras. To determine whether oncogenic Ras is involved in the down-regulation of C/EBPalpha, BALB/MK2 keratinocytes were infected with a retrovirus containing Ras12V, and C/EBPalpha protein, mRNA and DNA binding levels were determined. Keratinocytes infected with the retrovirus containing oncogenic Ras12V displayed greatly diminished C/EBPalpha protein, mRNA and DNA binding levels. In addition, BALB/MK2 cells containing endogenous mutant Ras displayed diminished C/EBPalpha expression and the ectopic expression of a dominant-negative RasN17 partially restored C/EBPalpha levels in these cells. These results indicate that oncogenic Ras negatively regulates C/EBPalpha expression and the loss of C/EBPalpha expression may contribute to the development of skin SCCs.

摘要

碱性亮氨酸拉链转录因子CCAAT/增强子结合蛋白α（C/EBPα）参与有丝分裂生长停滞，并被认为是急性髓系白血病中的一种人类肿瘤抑制因子。我们之前已经表明C/EBPα在小鼠表皮角质形成细胞中大量表达。在当前研究中，我们评估了七种含有致癌性Ha-Ras的小鼠皮肤鳞状细胞癌（SCC）细胞系中C/EBPα的表达情况。与正常原代角质形成细胞相比，所有七种SCC细胞系中C/EBPα的mRNA和蛋白水平均大幅降低，而C/EBPβ水平没有显著变化。在这些SCC细胞系中重新表达C/EBPα导致SCC细胞增殖受到抑制。为了确定在SCC细胞系中观察到的C/EBPα表达降低是否也发生在癌组织本身，我们对小鼠皮肤SCC进行了C/EBPα的免疫组织化学染色。与表皮相比，所有评估的14个SCC均显示C/EBPα蛋白表达可忽略不计且C/EBPβ水平正常，并且所有14个癌组织均含有突变型Ras。为了确定致癌性Ras是否参与C/EBPα的下调，我们用含有Ras12V的逆转录病毒感染BALB/MK2角质形成细胞，并测定C/EBPα蛋白、mRNA和DNA结合水平。用含有致癌性Ras12V的逆转录病毒感染的角质形成细胞显示C/EBPα蛋白、mRNA和DNA结合水平大幅降低。此外，含有内源性突变型Ras的BALB/MK2细胞显示C/EBPα表达降低，并且显性负性RasN17的异位表达部分恢复了这些细胞中的C/EBPα水平。这些结果表明致癌性Ras负向调节C/EBPα表达，并且C/EBPα表达的丧失可能有助于皮肤SCC的发生发展。