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小鼠肝细胞中S(14)基因表达的葡萄糖调节。一种新型转录因子复合物的参与。

Glucose regulation of mouse S(14) gene expression in hepatocytes. Involvement of a novel transcription factor complex.

作者信息

Koo S H, Towle H C

机构信息

Department of Biochemistry, Molecular Biology and Biophysics, University of Minnesota, Minneapolis, Minnesota 55455, USA.

出版信息

J Biol Chem. 2000 Feb 18;275(7):5200-7. doi: 10.1074/jbc.275.7.5200.

DOI:10.1074/jbc.275.7.5200
PMID:10671567
Abstract

Transcription of genes encoding enzymes required for lipogenesis is induced in hepatocytes in response to elevated glucose metabolism. We have previously mapped the carbohydrate-response elements (ChoREs) of the rat liver-type pyruvate kinase (L-PK) and S(14) genes and found them to share significant sequence similarity. However, progress in unraveling this signaling pathway has been hampered due to the difficulty in identifying the key factor(s) that bind to these ChoREs. To gain further insight into the nature of the carbohydrate-responsive transcription factor, the glucose regulatory sequences from the mouse S(14) gene were examined in primary hepatocytes. Three elements were found to be essential for supporting the glucose response: a thyroid hormone-response element between -1522 and -1494, an accessory factor site between -1421 and -1392, and the ChoRE between -1450 and -1425. Of these, only the accessory factor site was conserved between the rat and mouse S(14) genes. Investigation of the ChoRE sequence indicated that two half E box motifs are critical for the response to glucose. Electrophoretic mobility shift assays revealed a complex formed between the mouse S(14) ChoRE and liver nuclear proteins. This complex was also formed by ChoREs from the rat S(14) and L-PK genes but not by mutants of these sites that are inactive in supporting the glucose response. These results suggest the presence of a novel transcription factor complex that mediates the glucose-regulated transcription of S(14) and L-PK genes.

摘要

响应葡萄糖代谢增加,肝脏细胞中编码脂肪生成所需酶的基因转录被诱导。我们之前已经绘制了大鼠肝型丙酮酸激酶(L-PK)和S(14)基因的碳水化合物反应元件(ChoREs)图谱,发现它们具有显著的序列相似性。然而,由于难以鉴定与这些ChoREs结合的关键因子,在解析这条信号通路方面的进展受到了阻碍。为了进一步深入了解碳水化合物反应转录因子的性质,在原代肝细胞中对小鼠S(14)基因的葡萄糖调节序列进行了研究。发现有三个元件对于支持葡萄糖反应至关重要:位于-1522至-1494之间的甲状腺激素反应元件、位于-1421至-1392之间的辅助因子位点以及位于-1450至-1425之间的ChoRE。其中,只有辅助因子位点在大鼠和小鼠S(14)基因之间是保守的。对ChoRE序列的研究表明,两个半E盒基序对于葡萄糖反应至关重要。电泳迁移率变动分析显示,小鼠S(14) ChoRE与肝核蛋白之间形成了一个复合物。大鼠S(14)和L-PK基因的ChoREs也形成了这种复合物,但这些位点的无活性突变体(在支持葡萄糖反应方面无活性)则不能形成这种复合物。这些结果表明存在一种新型转录因子复合物,它介导S(14)和L-PK基因的葡萄糖调节转录。

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