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首页> 外文期刊>Biochemical and Biophysical Research Communications >Elevated expression and potential roles of human Sp5, a member of Sp transcription factor family, in human cancers.
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Elevated expression and potential roles of human Sp5, a member of Sp transcription factor family, in human cancers.

机译:Sp转录因子家族成员Sp5在人类癌症中的表达增强和潜在作用。

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摘要

In this report, we describe the expression and function of human Sp5, a member of the Sp family of zinc finger transcription factors. Like other family members, the Sp5 protein contains a Cys2His2 zinc finger DNA binding domain at the C-terminus. Our experiments employing Gal4-Sp5 fusion proteins reveal multiple transcriptional domains, including a N-terminal activity domain, an intrinsic repressive element, and a C-terminal synergistic domain. Elevated expression of Sp5 was noted in several human tumors including hepatocellular carcinoma, gastric cancer, and colon cancer. To study the effects of the Sp5 protein on growth properties of human cancer cells and facilitate the identification of its downstream genes, we combined an inducible gene expression system with microarray analysis to screen for its transcriptional targets. Transfer of Sp5 into MCF-7 cells that expressed no detectable endogenous Sp5 protein elicited significant growth promotion activity. Several of the constitutively deregulated genes have been associated with tumorigenesis (CDC25C, CEACAM6, TMPRSS2, XBP1, MYBL1, ABHD2, and CXCL12) and Wnt/beta-Catenin signaling pathways (BAMBI, SIX1, IGFBP5, AES, and p21WAF1). This information could be utilized for further mechanistic research and for devising optimized therapeutic strategies against human cancers.
机译:在本报告中,我们描述了人Sp5的表达和功能,Sp5是锌指转录因子Sp家族的成员。与其他家族成员一样,Sp5蛋白在C端含有Cys2His2锌指DNA结合结构域。我们使用Gal4-Sp5融合蛋白的实验揭示了多个转录域,包括N端活性域,内在的阻遏元件和C端协同域。在包括肝细胞癌,胃癌和结肠癌在内的几种人类肿瘤中均注意到Sp5的表达升高。为了研究Sp5蛋白对人类癌细胞生长特性的影响并促进其下游基因的鉴定,我们将诱导型基因表达系统与微阵列分析相结合,以筛选其转录靶标。将Sp5转移到未表达可检测的内源Sp5蛋白的MCF-7细胞中会引起明显的生长促进活性。一些组成性失调的基因与肿瘤发生有关(CDC25C,CEACAM6,TMPRSS2,XBP1,MYBL1,ABHD2和CXCL12)和Wnt / beta-Catenin信号通路(BAMBI,SIX1,IGFBP5,AES和p21WAF1)。该信息可用于进一步的机理研究和设计针对人类癌症的优化治疗策略。

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