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Clock Gene Expression in the Liver and Adipose Tissues of Non-Obese Type 2 Diabetic Goto-Kakizaki Rats
30
Citations
21
References
2009
Year
Metabolic DisorderInsulin SignalingClock Gene ExpressionOxidative StressObesityMetabolic SyndromeWistar RatsMetabolismMetabolic StateNon-obese Type 2Health SciencesLiver PhysiologyMolecular Clock ImpairmentEndocrinologyGene ExpressionDiabetic Goto-kakizaki RatsDevelopmental BiologyPhysiologyDiabetesMetabolic RegulationSystems BiologyMedicine
Recent studies have revealed a close relationship between the pathophysiology of metabolic syndrome, which is characterized by obesity and hyperglycemia, and the functioning of internal molecular clocks. In this study, we show that the rhythmic mRNA expression of clock genes (Clock, Bmal1, Cry1, and Dbp) is not attenuated in the liver and visceral adipose tissues of Goto-Kakizaki rats, a model of nonobese, type 2 diabetes, as compared to control Wistar rats. Our results suggest that molecular clock impairment in peripheral tissues of obese diabetic animals may be either caused by obesity-related factor(s), but not hyperglycemia, or be a cause, but not a consequence, of hyperglycemia.
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