首页> 美国卫生研究院文献>Nucleic Acids Research >Analysis of the Xenopus laevis CCAAT-enhancer binding protein α gene promoter demonstrates species-specific differences in the mechanisms for both auto-activation and regulation by Sp1
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Analysis of the Xenopus laevis CCAAT-enhancer binding protein α gene promoter demonstrates species-specific differences in the mechanisms for both auto-activation and regulation by Sp1

机译:爪蟾的分析 拉维斯CCAAT增强子结合蛋白α基因 启动子显示出机制中物种特异性的差异 用于Sp1的自动激活和调节

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摘要

Transcription factors belonging to the CCAAT-enhancer binding protein (C/EBP) family have been implicated in the regulation of gene expression during differentiation, development and disease. Autoregulation is relatively common in the modulation of C/EBP gene expression and the murine and human C/EBPα genes have been shown to be auto-activated by different mechanisms. In the light of this finding, it is essential that autoregulation of C/EBPα genes from a wider range of different species be investigated in order to gauge the degree of commonality, or otherwise, that may exist. We report here studies that investigate the regulation of the Xenopus laevis C/EBPα gene (xC/EBPα). The –1131/+41 promoter region was capable of directing high levels of expression in both the human hepatoma Hep3B and the Xenopus kidney epithelial A6 cell lines, and was auto-activated by expression vectors specifying for xC/EBPα or xC/EBPβ. Deletion analysis showed that the –321/+41 sequence was sufficient for both the constitutive promoter activity and auto-activation and electrophoretic mobility shift assays identified the interaction of C/EBPs and Sp1 to this region. Although deletion of either the C/EBP or the Sp1 site drastically reduced the xC/EBPα promoter activity, multimers of only the C/EBP site could confer autoregulation to a heterologous SV40 promoter. These results indicate that, in contrast to the human promoter and in common with the murine gene, the xC/EBPα promoter was subject to direct autoregulation. In addition, we demonstrate a novel species-specific action of Sp1 in the regulation of C/EBPα expression, with the factor able to repress the murine promoter but activate the Xenopus gene.
机译:属于CCAAT-增强子结合蛋白(C / EBP)家族的转录因子已经参与了分化,发育和疾病过程中基因表达的调控。自调节在C / EBP基因表达的调节中相对普遍,并且鼠和人C /EBPα基因已经显示出可以通过不同的机制自动激活。根据这一发现,至关重要的是,研究来自多种不同物种的C /EBPα基因的自动调节,以评估可能存在的共通程度。我们在这里报告的研究调查非洲爪蟾C /EBPα基因(xC /EBPα)的调节研究。 –1131 / + 41启动子区域能够指导人肝癌Hep3B和非洲爪蟾肾脏上皮A6细胞系中的高水平表达,并由指定xC /EBPα或xC /EBPβ的表达载体自动激活。缺失分析表明,–321 / + 41序列足以用于组成型启动子活性和 确定了自动激活和电泳迁移率变动分析 C / EBP和Sp1与该区域的相互作用。虽然 彻底删除C / EBP或Sp1站点 减少了xC /EBPα启动子 活性,只有C / EBP位点的多聚体可以赋予 自动调节到异源SV40启动子。这些结果表明 与人类启动子相反,与鼠科动物相同 基因,xC /EBPα启动子 受到直接的自动调节。另外,我们展示 Sp1在C /EBPα表达调控中的新物种特异性作用,该因子能够 抑制鼠启动子,但激活非洲爪蟾基因。

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