Insulin-dependent suppression of cholesterol 7alpha-hydroxlase is a possible link between glucose and cholesterol metabolisms.
10.3858/emm.2011.43.10.064
- Author:
Wook Ha PARK
1
;
Youngmi Kim PAK
Author Information
1. Department of Physiology, Department of Neuroscience, College of Medicine, Kyung Hee University, Seoul 130-701, Korea. ykpak@khu.ac.kr
- Publication Type:Original Article ; Research Support, Non-U.S. Gov't
- Keywords:
cholesterol;
cholesterol 7-alpha-hydroxylase;
forkhead transcription factors;
gene expression regulation;
nuclear receptor subfamily 0, group B, member 2
- MeSH:
Animals;
Bile Acids and Salts/metabolism;
Cholesterol/*metabolism;
Cholesterol 7-alpha-Hydroxylase/genetics/*metabolism;
Forkhead Transcription Factors/genetics/*metabolism;
Gene Expression Regulation/drug effects;
Glucose/*metabolism;
Hep G2 Cells;
Humans;
Insulin/pharmacology;
Lipid Metabolism/drug effects;
Liver/*metabolism/pathology;
Mice;
Mice, Inbred C57BL;
Mutagenesis, Site-Directed;
Nerve Tissue Proteins/genetics/*metabolism;
Protein Binding/drug effects/genetics;
Proto-Oncogene Proteins c-akt/metabolism;
Rats;
Receptors, Cytoplasmic and Nuclear/genetics/metabolism;
Sequence Deletion/genetics;
Signal Transduction/drug effects/genetics;
Transcriptional Activation/drug effects/genetics
- From:Experimental & Molecular Medicine
2011;43(10):571-579
- CountryRepublic of Korea
- Language:English
-
Abstract:
Cholesterol 7alpha-hydroxylase (CYP7A1) regulates the balance between cholesterol supply and metabolism by catalyzing the rate-limiting step of bile acid biosynthesis. The transcriptional activity of CYP7A1 is tightly controlled by various nuclear receptors. A forkhead transcription factor O1 (FOXO1) plays a critical role in metabolism, and insulin inactivates FOXO1 through Akt-dependent phosphorylation and nuclear exclusion. We investigated the role of insulin-Akt-FOXO1 signaling pathway in CYP7A1 transcriptional regulation since we found putative insulin-response elements, FOXO1 binding sequences, in both rat and human CYP7A1 promoters. However, ectopic expression of FOXO1 increased the rat CYP7A1-, but mildly reduced human CYP7A1-promoter activities in a dose-dependent manner. Similarly to bile acids, insulin treatment increased small heterodimer partner (SHP) mRNA rapidly and transiently, leading to the suppression of CYP7A1 transcription in both human and rodents. Chromatin immunoprecipitation showed that FOXO1 directly bound to rat CYP1A1 promoter in the absence of insulin. FOXO1 binding to the rat promoter was diminished by insulin treatment as well as by expression of SHP. Our results suggest that the stimulation of insulin- signaling pathway of Akt-FOXO1 and SHP expression may regulate cholesterol/bile acid metabolisms in liver, linking carbohydrate and cholesterol metabolic pathways. A prolonged exposure of insulin in hyperinsulinemic insulin resistance or diabetic status represses CYP7A1 transcription and bile acid biosynthesis through SHP induction and FOXO1 inactivation, leading to impairment of the hepatic cholesterol/bile acid metabolisms.
