期刊
DIABETES
卷 60, 期 5, 页码 1399-1413出版社
AMER DIABETES ASSOC
DOI: 10.2337/db10-0452
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资金
- Agence Nationale de la Recherche (ANR) GENOPAT
- Fondation pour la Recherche Medicale (FRM Labelisation Equipe
- Association de Langue Francaise pour L'Etude du Diabete et des Maladies Metaboliques (ALFEDIAM)
- FRM
- ANR DIABO-GLYC
OBJECTIVE Carbohydrate-responsive element-binding protein (ChREBP) is a key transcription factor that mediates the effects of glucose on glycolytic and lipogenic genes in the liver. We have previously reported that liver-specific inhibition of ChREBP prevents hepatic steatosis in ob/ob mice by specifically decreasing lipogenic rates in vivo. To better understand the regulation of ChREBP activity in the liver, we investigated the implication of O-linked p-N-acetylglucosamine (O-G1eNAc or O-G1cNAcylation), an important glucose-dependent posttranslational modification playing multiple roles in transcription, protein stabilization, nuclear localization, and signal transduction. RESEARCH DESIGN AND METHODS-O-G1cNAcylation is highly dynamic through the action of two enzymes: the O-G1eNAc transferase (OGT), which transfers the monosaccharide to serine/threonine residues on a target protein, and the O-G1cNAcase (OGA), which hydrolyses the sugar. To modulate ChREBP G in vitro and in vivo, the OGT and OGA enzymes were overexpressed or inhibited via adenoviral approaches in mouse hepatocytes and in the liver of C57BL/6J or obese db/db mice. RESULTS Our study shows that ChREBP interacts with OGT and is subjected to O-G1cNAcylation in liver cells. O-GleNAcylation stabilizes the ChREBP protein and increases its transcriptional activity toward its target glycolytic (L-PK) and lipogenic genes (ACC, FAS, and SCD1) when combined with an active glucose flux in vivo. Indeed, OGT overexpression significantly increased ChREBP G in liver nuclear extracts from fed C57BL/6J mice, leading in turn to enhanced lipogenic gene expression and to excessive hepatic triglyceride deposition. In the livers of hyperglycemic obese db/db mice, ChREBP G levels were elevated compared with controls. Interestingly, reducing ChREBP G levels via OGA overexpression decreased lipogenic protein content (ACC, FAS), prevented hepatic steatosis, and improved the lipidic profile of OGA-treated db/db mice. CONCLUSIONS Taken together, our results reveal that O-GlcNAcylation represents an important novel regulation of ChREBP activity in the liver under both physiological and pathophysiological conditions. Diabetes 60:1399-1413, 2011
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