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Brain fatty acid synthase activates PPARα to maintain energy homeostasis
Manu V. Chakravarthy, Yimin Zhu, Miguel López, Li Yin, David F. Wozniak, Trey Coleman, Zhiyuan Hu, Michael Wolfgang, Antonio Vidal-Puig, M. Daniel Lane, Clay F. Semenkovich
Manu V. Chakravarthy, Yimin Zhu, Miguel López, Li Yin, David F. Wozniak, Trey Coleman, Zhiyuan Hu, Michael Wolfgang, Antonio Vidal-Puig, M. Daniel Lane, Clay F. Semenkovich
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Research Article Metabolism

Brain fatty acid synthase activates PPARα to maintain energy homeostasis

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Abstract

Central nervous system control of energy balance affects susceptibility to obesity and diabetes, but how fatty acids, malonyl-CoA, and other metabolites act at this site to alter metabolism is poorly understood. Pharmacological inhibition of fatty acid synthase (FAS), rate limiting for de novo lipogenesis, decreases appetite independently of leptin but also promotes weight loss through activities unrelated to FAS inhibition. Here we report that the conditional genetic inactivation of FAS in pancreatic β cells and hypothalamus produced lean, hypophagic mice with increased physical activity and impaired hypothalamic PPARα signaling. Administration of a PPARα agonist into the hypothalamus increased PPARα target genes and normalized food intake. Inactivation of β cell FAS enzyme activity had no effect on islet function in culture or in vivo. These results suggest a critical role for brain FAS in the regulation of not only feeding, but also physical activity, effects that appear to be mediated through the provision of ligands generated by FAS to PPARα. Thus, 2 diametrically opposed proteins, FAS (induced by feeding) and PPARα (induced by starvation), unexpectedly form an integrative sensory module in the central nervous system to orchestrate energy balance.

Authors

Manu V. Chakravarthy, Yimin Zhu, Miguel López, Li Yin, David F. Wozniak, Trey Coleman, Zhiyuan Hu, Michael Wolfgang, Antonio Vidal-Puig, M. Daniel Lane, Clay F. Semenkovich

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Figure 6

In situ hybridization analysis of hypothalamic orexigenic and anorexigenic neuropeptides.

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In situ hybridization analysis of hypothalamic orexigenic and anorexigen...
(A and B) In situ hybridization showing decreased AgRP and NPY, but increased CART and POMC mRNA expression within the arcuate nucleus of freely fed WT and FASKO mice. No effect of genotype is seen on mRNA levels of MCH and orexin (OX) within the lateral hypothalamus. The rectangles indicate the area analyzed by densitometry to quantify the mRNA abundance in B. Original magnification, ×1.5. All results are mean ± SEM of 8 animals per group from 2 independent experiments. *P < 0.05 compared with WT littermates.

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ISSN: 0021-9738 (print), 1558-8238 (online)

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