miRâ338â3p mediates gluconeogenesis via targeting of PP4R1 in hepatocytes.
[No authors listed]
摘要
Hyperglycaemia is a characteristic of type 2 diabetes. In hepatocytes, impaired insulin sensitivity leads to increased gluconeogenesis and decreased glycogenesis. MicroRNA (miR)â338â3p is associated with tumour necrosis factor (TNF)âαâinduced suppression of hepatic glycogenesis via regulation of protein phosphatase 4 regulatory subunit 1 (PP4R1). However, the effect of miRâ338â3p on gluconeogenesis in hepatocytes remains unknown. In a previous study, it was demonstrated that miRâ338â3p is downregulated in the livers of mice and in mouse HEPA1â6 hepatocytes following treatment with TNFâα. In the present study, the effect of miRâ338â3p on TNFâαâinduced gluconeogenesis in hepatocytes was investigated. The levels of phosphorylatedâFOXO1/FOXO1, phosphoenolpyruvate carboxykinase (PEPCK), peroxisome proliferatorâactivated receptor γ coactivator (PGCâ1α) and glucoseâ6âphosphatase (G6Pase) were measured by western blotting. The mRNA levels of PEPCK, PGCâ1α and G6Pase were determined by quantitative polymerase chain reaction. Pyruvate tolerance testing was used to determine the gluconeogenesis of mouse livers. The results demonstrated that treatment with TNFâα resulted in increased levels of gluconeogenesis in the livers of mice and decreased miRâ338â3p expression levels in HEPA1â6 cells. Overexpression of miRâ338â3p reversed TNFâαâinduced glucose production via enhancement of phosphorylated forkhead box O1 levels and downregulation of the expression levels of genes associated with gluconeogenesis, including peroxisome proliferatorâactivated receptor γ coactivatorâ1α, phosphoenolpyruvate carboxykinase and glucoseâ6âphosphatase. However, inhibition of miRâ338â3p expression was revealed to enhance gluconeogenesis in the livers of mice and in HEPA1â6 cells. Furthermore, downregulation of PP4R1 was revealed to attenuate the effect on glucose production following treatment with miRâ338â3p inhibitors. In conclusion, the results of the present study revealed that miRâ338â3p may be involved in TNFâαâmediated gluconeogenesis via targeting of PP4R1 in hepatocytes.
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基因功能
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原始数据
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文献解读
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