首页> 美国卫生研究院文献>Molecular and Cellular Biology >Functional Conservation of Regulatory Elements in the pdx-1 Gene: PDX-1 and Hepatocyte Nuclear Factor 3β Transcription Factors Mediate β-Cell-Specific Expression
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Functional Conservation of Regulatory Elements in the pdx-1 Gene: PDX-1 and Hepatocyte Nuclear Factor 3β Transcription Factors Mediate β-Cell-Specific Expression

机译:pdx-1基因调节元件的功能保守性:PDX-1和肝细胞核因子3β转录因子介导β细胞特异性表达

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摘要

The PDX-1 transcription factor plays a key role in pancreatic development and in the regulation of the insulin gene in the adult β cell. As its functions appear to be similar in humans and mice, we analyzed the functional conservation of homologous sequences important for the maintenance and the cell-specific regulation of the pdx-1 gene. Apart from the proximal promoter region, three highly homologous (PH1 to PH3) sequences were apparent in the human and mouse 5′ flanking regions of the gene. By transient transfections in β and non-β cells, we show that mainly PH1 and PH2 preferentially confer β-cell-specific activation on a heterologous promoter. DNase I footprinting and binding analyses revealed that both bind to and are transactivated by hepatocyte nuclear factor 3β (HNF-3β). Furthermore, the PH1 enhancer element also binds the PDX-1 transcription factor itself, which acts cooperatively with adjacent HNF-3β to regulate its transcriptional potency. This finding suggests a possible autoregulatory loop as a mechanism for PDX-1 to control its own expression.
机译:PDX-1转录因子在胰腺发育和成年β细胞中胰岛素基因的调控中起关键作用。由于其功能在人类和小鼠中似乎相似,因此我们分析了对pdx-1基因的维持和细胞特异性调控重要的同源序列的功能保守性。除了近端启动子区域外,在该基因的人和小鼠5'侧翼区域中还存在三个高度同源的序列(PH1至PH3)。通过在β和非β细胞中进行瞬时转染,我们显示主要是PH1和PH2优先赋予异源启动子β细胞特异性激活。 DNase I足迹和结合分析表明,两者均与肝细胞核因子3β(HNF-3β)结合并被其激活。此外,PH1增强子元件还结合了PDX-1转录因子本身,该PDX-1转录因子与相邻的HNF-3β协同作用以调节其转录潜能。这一发现表明,可能存在的自动调节循环是PDX-1控制其自身表达的一种机制。

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