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tmp基因编码一种膜蛋白,是具有致瘤活性的c-Myc靶点。

The tmp gene, encoding a membrane protein, is a c-Myc target with a tumorigenic activity.

作者信息

Ben-Porath I, Yanuka O, Benvenisty N

机构信息

Department of Genetics, Institute for Life Sciences, The Hebrew University of Jerusalem, Jerusalem 91904, Israel.

出版信息

Mol Cell Biol. 1999 May;19(5):3529-39. doi: 10.1128/MCB.19.5.3529.

Abstract

The c-Myc oncoprotein induces cell proliferation and transformation through its activity as a transcription factor. Uncovering the genes regulated by c-Myc is an essential step for understanding these processes. We recently isolated the tumor-associated membrane protein gene, Tmp, from a c-myc-induced mouse brain tumor. Here we show that Tmp is specifically highly expressed in mammary tumors and T-cell lymphomas which develop in c-myc transgenic mice, suggesting that Tmp expression is a general characteristic of c-Myc-induced tumors. In addition, Tmp expression is induced upon serum stimulation of fibroblasts as shown in a time course closely correlated with c-myc expression. We have isolated the Tmp promoter region and identified a putative c-Myc binding element, CACGTG, located in the first intron of the gene. We show here that constructs containing the Tmp regulatory region fused to a reporter gene are activated by c-Myc through this CACGTG element and that the c-Myc-Max protein complex can bind to this element. Moreover, an inducible form of c-Myc, the MycER fusion protein, can activate the endogenous Tmp gene. We also show that Tmp-overexpressing fibroblasts induce rapidly growing tumors when injected into nude mice, suggesting that Tmp may possess a tumorigenic activity. Thus, TMP, a member of a novel family of membrane glycoproteins with a suggested role in cellular contact, is a c-Myc target and is possibly involved in c-Myc-induced transformation.

摘要

c-Myc癌蛋白通过作为转录因子的活性诱导细胞增殖和转化。揭示受c-Myc调控的基因是理解这些过程的关键步骤。我们最近从c-myc诱导的小鼠脑肿瘤中分离出肿瘤相关膜蛋白基因Tmp。在此我们表明,Tmp在c-myc转基因小鼠发生的乳腺肿瘤和T细胞淋巴瘤中特异性高表达,提示Tmp表达是c-Myc诱导肿瘤的一个普遍特征。此外,如在与c-myc表达密切相关的时间进程中所示,血清刺激成纤维细胞可诱导Tmp表达。我们分离出了Tmp启动子区域,并鉴定出一个假定的c-Myc结合元件CACGTG,位于该基因的第一个内含子中。我们在此表明,含有与报告基因融合的Tmp调控区域的构建体可被c-Myc通过该CACGTG元件激活,且c-Myc-Max蛋白复合物可结合至该元件。此外,一种可诱导形式的c-Myc,即MycER融合蛋白,可激活内源性Tmp基因。我们还表明,过表达Tmp的成纤维细胞注射到裸鼠中时可诱导快速生长的肿瘤,提示Tmp可能具有致瘤活性。因此,TMP是一个新型膜糖蛋白家族的成员,在细胞接触中可能起作用,它是c-Myc的一个靶标,可能参与c-Myc诱导的转化。

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