Impairment of hepatic Stat-3 activation and reduction of PPARalpha activity in fructose-fed rats

Fructose makes up a significant proportion of energy intake in westernized diets; its increased consumption has paralleled the growing prevalence of obesity and metabolic syndrome over the past two decades. In the current study, we demonstrate that fructose administration (10% wt/vol) in the drinkin...

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Veröffentlicht in:Hepatology (Baltimore, Md.) Md.), 2007-03, Vol.45 (3), p.778-788
Hauptverfasser: Roglans, Núria, Vilà, Laia, Farré, Mireia, Alegret, Marta, Sánchez, Rosa María, Vázquez-Carrera, Manuel, Laguna, Juan Carlos
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container_issue 3
container_start_page 778
container_title Hepatology (Baltimore, Md.)
container_volume 45
creator Roglans, Núria
Vilà, Laia
Farré, Mireia
Alegret, Marta
Sánchez, Rosa María
Vázquez-Carrera, Manuel
Laguna, Juan Carlos
description Fructose makes up a significant proportion of energy intake in westernized diets; its increased consumption has paralleled the growing prevalence of obesity and metabolic syndrome over the past two decades. In the current study, we demonstrate that fructose administration (10% wt/vol) in the drinking water of rats reduces the trans-activating and trans-repressing activity of the hepatic peroxisome proliferator-activated receptor alpha (PPARalpha). As a consequence, fructose decreases hepatic fatty oxidation and increases pro-inflammatory transcription factor nuclear factor kappaB (NF-kappaB) activity. These changes were not observed in glucose-administered rats (10% wt/vol), although both carbohydrates produced similar changes in plasma adiponectin and in the hepatic expression of transcription factors and enzymes involved in fatty acid synthesis. Fructose-fed, but not glucose-fed, rats were hyperleptinemic and exhibited increased tyrosine phosphorylation of the signal transducer and activator of transcription-3 (STAT-3) transcription factor, although they did not present a similar increase in the serine phosphorylation of nuclear STAT3. Thus, an impairment in the hepatic transduction of the leptin signal could be responsible for the observed alterations in PPARalpha activity in fructose-fed rats. Because PPARalpha activity is lower in human than in rodent liver, fructose ingestion in humans should cause even worse effects, which would partly explain the link between increased consumption of fructose and widening epidemics of obesity and metabolic syndrome. Hypertriglyceridemia and hepatic steatosis induced by fructose ingestion result from a reduction in the hepatic catabolism of fatty acids driven by a state of leptin resistance.
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Thus, an impairment in the hepatic transduction of the leptin signal could be responsible for the observed alterations in PPARalpha activity in fructose-fed rats. Because PPARalpha activity is lower in human than in rodent liver, fructose ingestion in humans should cause even worse effects, which would partly explain the link between increased consumption of fructose and widening epidemics of obesity and metabolic syndrome. 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subjects Animals
Diet
Fatty Liver - etiology
Fatty Liver - metabolism
Fructose - metabolism
Gene Expression Regulation
Hypertriglyceridemia - etiology
Hypertriglyceridemia - metabolism
Leptin - genetics
Leptin - metabolism
Liver - metabolism
Male
PPAR alpha - genetics
PPAR alpha - metabolism
Rats
Rats, Sprague-Dawley
Signal Transduction
STAT3 Transcription Factor - genetics
STAT3 Transcription Factor - metabolism
title Impairment of hepatic Stat-3 activation and reduction of PPARalpha activity in fructose-fed rats
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