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Synergistic activation of the insulin gene promoter by the beta-cell enriched transcription factors MafA, Beta2, and Pdx1

机译:富含β细胞的转录因子MafA,Beta2和Pdx1对胰岛素基因启动子的协同激活

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Specific expression of the insulin gene in pancreatic islet beta-cells requires multiple cis-regulatory elements in its promoter. Pdx1, MafA, and Beta2 have been identified as beta-cell enriched transcription factors that bind to these elements. Pdx1 has been shown to bind to A1, A3, A5, and GG2, and Beta2 binds to E1 by forming a heterodimer with the ubiquitous factor E47. MafA was recently identified as a Cl-element binding factor. However, interactions between these factors and the promoter have not been characterized in detail. In this report, we show that these transactivators synergistically stimulate insulin promoter activity. Among multiple binding sites for Pdx1, MafA, and Beta2, at least GG2, Cl, and El elements located in the promoter region between - 150 and - 100 base pairs are necessary for the synergism. We also found that neither MafB nor c-Maf, close relatives of MafA, showed synergistic activation. These results suggest that co-expression and functional synergism of these beta-cell enriched transactivators, MafA, Pdx1, and Beta2, are critical for establishing the beta-cell-specific and efficient expression of the insulin gene. (C) 2005 Elsevier B.V. All rights reserved.
机译:胰岛素基因在胰岛β细胞中的特异性表达在其启动子中需要多个顺式调控元件。 Pdx1,MafA和Beta2已被确定为与这些元素结合的富含β细胞的转录因子。已显示Pdx1与A1,A3,A5和GG2结合,而Beta2通过与泛在因子E47形成异二聚体与E1结合。 MafA最近被确定为Cl元素结合因子。但是,这些因子与启动子之间的相互作用尚未详细描述。在这份报告中,我们显示了这些反式激活剂协同刺激胰岛素启动子的活性。在Pdx1,MafA和Beta2的多个结合位点中,协同作用需要位于启动子区域介于-150和-100个碱基对之间的至少GG2,Cl和E1元素。我们还发现,MafA的近亲MafB和c-Maf均未显示出协同激活作用。这些结果表明,这些富含β细胞的反式激活因子MafA,Pdx1和Beta2的共表达和功能协同作用对于建立β细胞特异性和胰岛素基因的有效表达至关重要。 (C)2005 Elsevier B.V.保留所有权利。

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