Oxidative stress and altered lipid homeostasis in the programming of offspring fatty liver by maternal obesity
AJP Regulatory Integrative and Comparative Physiology
Published online on April 30, 2014
Abstract
Changes in the maternal nutritional environment during fetal development can influence offspring metabolic risk in later life. Animal models have demonstrated that offspring of diet-induced obese dams develop metabolic complications, including non-alcoholic fatty liver disease. In this study we investigated the mechanisms in young offspring that lead to the development of NAFLD. Female offspring of C57BL/6J dams fed either a control or obesogenic diet were studied at 8 weeks of age. We investigated the roles of oxidative stress and lipid metabolism in contributing to offspring fatty liver. There were no differences in body weight or adiposity at 8 weeks of age; however offspring of obese dams were hyperinsulinemic. Oxidative damage markers were significantly increased in their livers, with reduced levels of the antioxidant enzyme glutathione peroxidase-1. Mitochondrial complex I and II activities were elevated, while levels of mitochondrial cytochrome c were significantly reduced and glutamate dehydrogenase was significantly increased, suggesting mitochondrial dysfunction. Offspring of obese dams also had significantly greater hepatic lipid content, associated with increased levels of PPAR and reduced triglyceride lipase. Liver glycogen and protein content were concomitantly reduced in offspring of obese dams. In conclusion, offspring of diet-induced obese dams have disrupted liver metabolism and develop NAFLD prior to any differences in body weight or body composition. Oxidative stress may play a mechanistic role in the progression of fatty liver in these offspring.