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Let-7 underlies metformin-induced inhibition of hepatic glucose production

Di Xie, Fan Chen, Yuanyuan Zhang, Bei Shi, Jiahui Song, Kiran Chaudhari, Shao‐Hua Yang, Gary J. Zhang, Xiaoli Sun, Hugh S. Taylor, Da Li, Yingqun Huang

2022Proceedings of the National Academy of Sciences22 citationsDOIOpen Access PDF

Abstract

SignificanceA clear mechanistic understanding of metformin's antidiabetic effects is lacking. This is because suprapharmacological concentrations of metformin have been used in most studies. Using mouse models and human primary hepatocytes, we show that metformin, at clinically relevant doses, suppresses hepatic glucose production by activating a conserved regulatory pathway encompassing let-7, TET3, and a fetal isoform of hepatocyte nuclear factor 4 alpha (HNF4α). We demonstrate that metformin no longer has potent antidiabetic actions in a liver-specific let-7 loss-of-function mouse model and that hepatic delivery of let-7 ameliorates hyperglycemia and improves glucose homeostasis. Our results thus reveal an important role of the hepatic let-7/TET3/HNF4α axis in mediating the therapeutic effects of metformin and suggest that targeting this axis may be a potential therapeutic for diabetes.

Topics & Concepts

MetforminGlucose homeostasisHepatocyte nuclear factorsDiabetes mellitusEndocrinologyInternal medicineHepatocyteGene isoformMedicinePharmacologyChemistryBiologyInsulin resistanceTranscription factorIn vitroGeneBiochemistryPancreatic function and diabetesMetabolism, Diabetes, and CancerDiabetes Treatment and Management
Let-7 underlies metformin-induced inhibition of hepatic glucose production | Litcius