AI Article Synopsis
- TxNIP is a potential drug target for type 2 diabetes, linked to high blood sugar effects in pancreatic β cells, but its regulation in liver cells needs more research.
- The study investigates how TxNIP is regulated in liver cells in response to glucose and fasting, focusing on the roles of transcription factors ChREBP and FoxO1.
- Findings show that TxNIP expression in liver cells increases due to both ChREBP and FoxO1, particularly during fasting, indicating its significance in adapting to nutrient scarcity.
Article Abstract
TxNIP (Thioredoxin-interacting protein) is considered as a potential drug target for type 2 diabetes. Although TxNIP expression is correlated with hyperglycemia and glucotoxicity in pancreatic β cells, its regulation in liver cells has been less investigated. In the current study, we aim at providing a better understanding of regulation in hepatocytes in response to physiological stimuli and in the context of hyperglycemia in mice. We focused on regulatory pathways governed by ChREBP (Carbohydrate Responsive Element Binding Protein) and FoxO1 (Forkhead box protein O1), transcription factors that play central roles in mediating the effects of glucose and fasting on gene expression, respectively. Studies using genetically modified mice reveal that hepatic TxNIP is up-regulated by both ChREBP and FoxO1 in liver cells and that its expression strongly correlates with fasting, suggesting a major role for this protein in the physiological adaptation to nutrient restriction.
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Source |
|---|---|
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7966993 | PMC |
| http://dx.doi.org/10.1016/j.isci.2021.102218 | DOI Listing |
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