Abstract
Astragaloside IV (AST) is a major bioactive compound of Radix Astragali with medical and health benefits. Previous studies have found that AST can reduce the body weights of high‐fat diet fed mice. However, the effect of AST on fat metabolism of ageing mice is unclear. In this study, naturally ageing mice were administered intragastrically with AST at 30 mg/kg/day (ageing + AST‐L group) and 90 mg/kg/day (ageing + AST‐H group) for 16–20 months. Adult (4 months old) and ageing mice were given 1% sodium carboxyl methylcellulose as vehicle. Energy metabolism‐related biological parameters of living mice were examined. Moreover, mRNA and protein levels of key enzymes/proteins involved in triglyceride (TG) lipolysis, fatty acid β‐oxidation (FAO), ketone body (KB) production and mitochondrial respiratory chain were also examined after sacrifice. Results demonstrated that treatment with AST significantly reduced body weight, white fat and liver/body weight ratio of ageing mice, significantly reduced serum/hepatic TG levels, respiratory quotient, promoted fatty acid mobilization in white adipose tissue, mitochondrial FAO and KB production and mitochondrial biosynthesis/functions in the liver of ageing mice. AST also up‐regulated the expression of phosphorylated AMP‐activated protein kinase, acetyl‐CoA carboxylase, acetyl‐coenzyme A synthetase, carnitine palmitoyltransferase 1a/1b, enoyl coenzyme A hydratase‐short chain, acyl‐CoA dehydrogenase medium chain and mitochondrial 3‐hydroxy‐3‐methylglutaryl‐CoA synthase‐2 involved in fat metabolism. These results indicated that mitochondrial activity could be the target of AST to treat abnormal fat metabolism during ageing.
Highlights
Ageing is a time-dependent process and controlled by multiple factors, involving the changes in different physiological systems and the complex interactions among genetic, epigenetic, environmental factors and the alterations in the gut microbiome.[1,2] With the body ageing, the physiological functions of most organs are decreased, and the morbidity rate and mortality rate are increased due to different diseases
We examined the effects of Astragaloside IV (AST) on biochemical and physiological parameters related to lipid metabolism pathways and the enzymes/proteins involved in these pathways, including fatty acid biosynthesis and fatty acid β-oxidation, ketone body (KB) production, mitochondrial electron transport chain (ETC) and mitochondrial biosynthesis capacity in hepatocytes and liver of ageing mice
Our results indicate that AST administration stimulated fatty acid β-oxidation (FAO) and KB production by up-regulation of the key enzymes/proteins involved in these two processes and inhibited fatty acid biosynthesis by down-regulating the enzymes/proteins involved in this pathway
Summary
Ageing is a time-dependent process and controlled by multiple factors, involving the changes in different physiological systems and the complex interactions among genetic, epigenetic, environmental factors and the alterations in the gut microbiome.[1,2] With the body ageing, the physiological functions of most organs are decreased, and the morbidity rate and mortality rate are increased due to different diseases. A number of phytochemicals have been known to be beneficial on age-related diseases.[5] For instance, resveratrol, a type of phenol and a phytoalexin naturally produced by plants, can improve the abnormalities of lipid metabolism caused by ageing and reduce ageing-caused weight gain and the increased level of blood TG.[6] Quercetin, an antioxidant found in apples and other types of foods, is effective on delaying metabolic abnormalities caused by ageing.[7] to conduct an in-depth study on the TCM- intervention and its mechanism of abnormal lipid metabolism caused by ageing is of great significance for the prevention and treatment of senile obesity.8–10
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