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Sterol Regulatory Element-binding Protein-1 Is Regulated by Glucose at the Transcriptional Level

Authors :
Ken Ohashi
Nobuhiro Yamada
Tomohiro Yoshikawa
Stéphane Perrey
Yoshiaki Tamura
Ryozo Nagai
Alyssa H. Hasty
Naoya Yahagi
Hiroaki Okazaki
Takanari Gotoda
Michiyo Amemiya-Kudo
Hitoshi Shimano
Kenji Harada
Jun-ichi Osuga
Yoko Iizuka
Shun Ishibashi
Futoshi Shionoiri
Source :
Scopus-Elsevier
Publication Year :
2000
Publisher :
Elsevier BV, 2000.

Abstract

In vivo studies suggest that sterol regulatory element-binding protein (SREBP)-1 plays a key role in the up-regulation of lipogenic genes in the livers of animals that have consumed excess amounts of carbohydrates. In light of this, we sought to use an established mouse hepatocyte cell line, H2-35, to further define the mechanism by which glucose regulates nuclear SREBP-1 levels. First, we show that these cells transcribe high levels of SREBP-1c that are increased 4-fold upon differentiation from a prehepatocyte to a hepatocyte phenotype, making them an ideal cell culture model for the study of SREBP-1c induction. Second, we demonstrate that the presence of precursor and mature forms of SREBP-1 protein are positively regulated by medium glucose concentrations ranging from 5.5 to 25 mm and are also regulated by insulin, with the amount of insulin in the fetal bovine serum being sufficient for maximal stimulation of SREBP-1 expression. Third, we show that the increase in SREBP-1 protein is due to an increase in SREBP-1 mRNA. Reporter gene analysis of the SREBP-1c promoter demonstrated a glucose-dependent induction of transcription. In contrast, expression of a fixed amount of the precursor form of SREBP-1c protein showed that glucose does not influence its cleavage. Fourth, we demonstrate that the glucose induction of SREBP could not be reproduced by fructose, xylose, or galactose nor by glucose analogs 2-deoxy glucose and 3-O-methyl glucopyranose. These data provide strong evidence for the induction of SREBP-1c mRNA by glucose leading to increased mature protein in the nucleus, thus providing a potential mechanism for the up-regulation of lipogenic genes by glucosein vivo.

Details

ISSN :
00219258
Volume :
275
Database :
OpenAIRE
Journal :
Journal of Biological Chemistry
Accession number :
edsair.doi.dedup.....e3266ec648d9ead660fbb8c9854b44ee
Full Text :
https://doi.org/10.1074/jbc.m003335200