FXR-deficiency confers increased susceptibility to torpor |
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Authors: | Cariou Bertrand Bouchaert Emmanuel Abdelkarim Mouaadh Dumont Julie Caron Sandrine Fruchart Jean-Charles Burcelin Rémy Kuipers Folkert Staels Bart |
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Affiliation: | Institut Pasteur de Lille, Département d'Athérosclérose, Lille F-59019, France. |
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Abstract: | ![]() The role of the nuclear receptor FXR in adaptive thermogenesis was investigated using FXR-deficient mice. Despite elevated serum bile acid concentrations and increased mRNA expression profiles of thermogenic genes in brown adipose tissue, FXR-deficiency did not alter energy expenditure under basal conditions. However, FXR-deficiency accelerated the fasting-induced entry into torpor in a leptin-dependent manner. FXR-deficient mice were also extremely cold-intolerant. These altered responses may be linked to a more rapid decrease in plasma concentrations of metabolic fuels (glucose, triglycerides) thus impairing uncoupling protein 1-driven thermogenesis. These results identify FXR as a modulator of energy homeostasis. |
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Keywords: | Thermogenesis Fasting Cold-exposure Nuclear receptor |
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