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Satiety induced by bile acids is mediated via vagal afferent pathways
Xiaoyin Wu, Ji-Yao Li, Allen Lee, Yuan-Xu Lu, Shi-Yi Zhou, Chung Owyang
Xiaoyin Wu, Ji-Yao Li, Allen Lee, Yuan-Xu Lu, Shi-Yi Zhou, Chung Owyang
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Research Article Gastroenterology

Satiety induced by bile acids is mediated via vagal afferent pathways

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Abstract

The aim of this study was to elucidate the role and the pathways used by bile acid receptor TGR5 in transmitting satiety signals. We showed TGR5 colocalized with cholecystokinin type A (CCK-A) receptors in a subpopulation of rat nodose ganglia (NG) neurons. Intra-arterial injection of deoxycholic acid (DCA) dose-dependently increased firing rate in NG while a subthreshold dose of DCA and CCK-8 increased firing rates synergistically. TGR5-specific agonist oleanolic acid induced NG neuronal firing in a dose-dependent manner. However, the same units did not respond to GW4064, a nuclear receptor–specific agonist. Quantity of DCA-activated neurons in the hypothalamus was determined by c-Fos expression. Combining DCA and CCK-8 caused a 4-fold increase in c-Fos activation. In the arcuate nucleus, c-Fos–positive neurons coexpressed cocaine and amphetamine regulated transcript and proopiomelanocortin. DCA-induced c-Fos expression was eliminated following truncal vagotomy or silencing of TGR5 in the NG. Feeding studies showed intravenous injection of 1 μg/kg of DCA reduced food intake by 12% ± 3%, 24% ± 5%, and 32% ± 6% in the first 3 hours, respectively. Silencing of TGR5 or CCK-A receptor in the NG enhanced spontaneous feeding by 18% ± 2% and 13.5% ± 2.4%, respectively. When both TGR5 and CCK-A receptor were silenced, spontaneous feeding was enhanced by 37% ± 4% in the first 3 hours, suggesting that bile acid may have a physiological role in regulating satiety. Working in concert with CCK, bile acid synergistically enhanced satiety signals to reduce spontaneous feeding.

Authors

Xiaoyin Wu, Ji-Yao Li, Allen Lee, Yuan-Xu Lu, Shi-Yi Zhou, Chung Owyang

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Figure 7

Proopiomelanocortin/CART neurons in ARC and CRF neurons in the PVN are activated by DCA.

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Proopiomelanocortin/CART neurons in ARC and CRF neurons in the PVN are a...
Double immunofluorescence staining of neurons in the hypothalamic ARC showing (A) c-Fos, (B) proopiomelanocortin (POMC), and (C) merged imaged of c-Fos and POMC staining 1 hour after DCA (1 μg/kg) intravenous injection. Double immunofluorescence staining of neurons in the ARC showing (D) c-Fos, (E) CART, and (F) merged image of c-Fos and CART staining after DCA injection. Double immunofluorescence staining of neurons in the PVN showing (G) c-Fos, (H) CRF, and (I) merged image of c-Fos and CRF staining. Arrows show colocalization of c-Fos with neurons. Insets show that c-Fos is located in the nucleus and neuropeptides in the cytosol of neurons. Three sections per rat were stained and 5 rats were used (n = 5).

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