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Egr 转录因子在调节胰岛素生物合成、血糖稳态和胰岛大小方面发挥着关键作用。

Critical role of Egr transcription factors in regulating insulin biosynthesis, blood glucose homeostasis, and islet size.

机构信息

Department of Medical Biochemistry and Molecular Biology, Building 44, University of Saarland Medical Center, d-66421 Homburg, Germany.

出版信息

Endocrinology. 2012 Jul;153(7):3040-53. doi: 10.1210/en.2012-1064. Epub 2012 May 17.

Abstract

Expression of early growth response protein (Egr)-1, a protein of the Egr family of zinc finger transcription factors, is stimulated in glucose-treated pancreatic β-cells and insulinoma cells. The purpose of this study was to elucidate the role of Egr transcription factors in pancreatic β-cells in vivo. To overcome the problem associated with redundancy of functions between Egr proteins, conditional transgenic mice were generated expressing a dominant-negative mutant of Egr-1 in pancreatic β-cells. The Egr-1 mutant interferes with DNA binding of all Egr proteins and thus impairs the biological functions of the entire Egr family. Expression of the Egr-1 mutant reduced expression of TGFβ and basic fibroblast growth factor, known target genes of Egr-1, whereas the expression of Egr-1, Egr-3, Ets-like gene-1 (Elk-1), and specificity protein-3 was not changed in the presence of the Egr-1 mutant. Expression of the homeobox protein pancreas duodenum homeobox-1, a major regulator of insulin biosynthesis, was reduced in islets expressing the Egr-1 mutant. Accordingly, insulin mRNA and protein levels were reduced by 75 or 25%, respectively, whereas expression of glucagon and somatostatin was not altered after expression of the Egr-1 mutant in β-cells. Glucose tolerance tests revealed that transgenic mice expressing the Egr-1 mutant in pancreatic β-cells displayed impaired glucose tolerance. In addition, increased caspase-3/7 activity was detected as a result of transgene expression, leading to a 20% decrease of the size of the islets. These results show that Egr proteins play an important role in controlling insulin biosynthesis, glucose homeostasis, and islet size of pancreatic β-cells in vivo.

摘要

早期生长反应蛋白 (Egr)-1 的表达,Egr 家族锌指转录因子的一种蛋白质,在葡萄糖处理的胰岛 β 细胞和胰岛素瘤细胞中受到刺激。本研究的目的是阐明 Egr 转录因子在体内胰岛 β 细胞中的作用。为了克服 Egr 蛋白功能冗余相关的问题,生成了在胰岛 β 细胞中表达 Egr-1 显性负突变体的条件性转基因小鼠。Egr-1 突变体干扰所有 Egr 蛋白的 DNA 结合,从而损害整个 Egr 家族的生物学功能。Egr-1 突变体的表达降低了 TGFβ 和碱性成纤维细胞生长因子的表达,这是 Egr-1 的已知靶基因,而 Egr-1、Egr-3、Ets 样基因-1(Elk-1)和特异性蛋白-3 的表达在存在 Egr-1 突变体时并未改变。胰岛中表达 Egr-1 突变体时,胰腺十二指肠同源盒-1 基因(homeobox protein pancreas duodenum homeobox-1)的表达减少,该基因是胰岛素生物合成的主要调节因子。因此,胰岛素 mRNA 和蛋白水平分别降低了 75%或 25%,而在 β 细胞中表达 Egr-1 突变体后,胰高血糖素和生长抑素的表达没有改变。葡萄糖耐量试验显示,在胰岛β细胞中表达 Egr-1 突变体的转基因小鼠表现出葡萄糖耐量受损。此外,由于转基因的表达,检测到 caspase-3/7 活性增加,导致胰岛的大小减少了 20%。这些结果表明,Egr 蛋白在体内控制胰岛素生物合成、葡萄糖稳态和胰岛 β 细胞大小方面发挥重要作用。

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