4.6 Article

Polydatin, A Glycoside of Resveratrol, Is Better Than Resveratrol in Alleviating Non-alcoholic Fatty Liver Disease in Mice Fed a High-Fructose Diet

Journal

FRONTIERS IN NUTRITION
Volume 9, Issue -, Pages -

Publisher

FRONTIERS MEDIA SA
DOI: 10.3389/fnut.2022.857879

Keywords

polydatin; resveratrol; non-alcoholic fatty liver disease; 5'-aMP-activated protein kinase; gut microbiota; short-chain fatty acids

Funding

  1. Open Fund of State Key Laboratory of Tea Plant Biology and Utilization [SKLTOF20200127, SKLT0F20200108]
  2. Guangdong Modern Agricultural Industrial Technology System Innovation Team Project [2019KJ142, 2020KJ142]
  3. Guangdong Province ordinary universities characteristic innovation project [2020KTSCX060]
  4. Guangdong Pharmaceutical University [S202010573044]

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The study compared the effects of POD and RES in ameliorating energy homeostasis imbalance and found that POD increased the levels of valeric acid and caproic acid in feces by modifying gut microbiota, and was more effective in improving lipid metabolism than RES.
Resveratrol (RES) is considered to be an activator of AMP-activated protein kinase (AMPK) with many reported health benefits. Polydatin (POD) is a natural precursor and glycosylated form of RES. The glycoside structure of POD alters the bioactivity. Overnutrition-stimulated reactive oxygen species (ROS) promote the AMPK suppression and metabolic dysregulation. The present work compared the effects of POD and RES in ameliorating energy homeostasis imbalance in mice fed a high-fructose diet and elucidated the underlying mechanisms of action. Our results showed that POD elevated the fecal levels of valeric acid and caproic acid via modification of gut microbiota, while RES did not significantly influence the levels of fecal short-chain fatty acids (SCFAs). Both POD and RES markedly decreased the oxidative stress and activated the AMPK signaling pathways in the liver. POD and RES exerted a similar effect in alleviating glucose dysmetabolism, but POD was more effective in ameliorating lipid dysmetabolism than RES. Furthermore, valeric acid and caproic acid alone can activate the AMPK and ameliorate hypercholesterolemia, and enhance the effects of POD on improving lipid metabolism in mice. Overall, for the first time, we demonstrated that POD administration elevated the fecal levels of valeric acid and caproic acid by modifying gut microbiota, thus promoting AMPK activation may be the underlying mechanism that POD is superior to RES in alleviating the lipid dysmetabolism. Our results suggest that POD may be an alternative for RES as an AMPK activator.

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