Recently, glucokinase activators (GKAs) have emerged as a breakthrough in treating type 2 diabetes. Marketed drugs such as dorzagliatin have proven effective in lowering blood glucose levels. However, GKAs may disrupt lipid metabolism, leading to fat accumulation in the liver. Consequently, more research is required to establish the safety of GKAs in type 2 diabetes patients who also have non-alcoholic fatty liver disease. Additionally, the link between hepatic glucokinase activation and the endoplasmic reticulum stress response remains ambiguous. Further studies are needed to clarify this relationship.
In a study published in the KeAi journal Liver Research, a research team in China found that GKAs improved glucose tolerance and insulin sensitivity. However, under high-fat diet feeding, GKAs also induced hepatic lipid accumulation by increasing lipogenic gene expression, which subsequently activated the hepatic PERK-UPR signaling pathway.
“We established a mouse model with high-fat diet-induced obesity to study the impact of GKA treatment on glucose and lipid metabolism in obese mice. We then evaluated the effect of GKA treatment on glucose metabolism in mice with diet-induced obesity using glucose and insulin tolerance tests,” explained Nan Cai, lead author of the authors.
The team’s findings indicated that GKA enhanced glucose tolerance by improving both islet β cell function and insulin signaling. Additionally, GKA exacerbated hepatic lipid accumulation in mice fed on high-fat diet, while not in mice fed with chow diet, as demonstrated by hematoxylin and eosin staining, Oil Red O staining, and transmission electron microscopy. This accumulation induced hepatic pathological changes.
Overall, the study illustrated that while glucokinase activation improves glucose tolerance in mice with diet-induced obesity, it also induces hepatic lipid accumulation that activates the PERK-UPR pathway. The findings provide a theoretical basis and reference for the application of GKAs in personalized treatment of chronic diseases such as type 2 diabetes and non-alcoholic fatty liver disease.
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References
DOI
10.1016/j.livres.2023.05.003
Original Source URL
https://doi.org/10.1016/j.livres.2023.05.003
Funding information
This research was funded by Natural Science Foundation of Guangdong Province (2018B030311012), Natural Science Foundation of China (82070811, 81770826), Sci-Tech Research Development Program of Guangzhou City (202201020497), National Key R&D Program of China (2017YFA0105803), and Key Area R&D Program of Guangdong Province (2019B020227003).
Journal
Liver Research