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• W2166064702 abstract "Hepatic insulin resistance manifested as impaired suppression of glucose production is a key metabolic derangement that contributes to fasting hyperglycemia and increased HbA1c levels in type 2 diabetes (1). Genetic manipulation to overexpress the key enzymes in gluconeogenesis (particularly PEPCK) in preclinical models has shown that a primary defect in this system can result in increased hepatic glucose production (2,3) but, importantly, can lead to defects in insulin resistance in other tissues (muscle/fat) and impairments in insulin secretion (4,5). Despite this, medications that specifically target hepatic glucose overproduction in diabetes are lacking. Currently, the only medication (other than insulin) that targets the liver is the biguanide metformin, and despite being used for more than half a century, the mechanism by which it does this is still not completely understood (6–9). Thus, understanding the mechanism causing hepatic insulin resistance will lead to more effective and targeted therapeutic options.Cyclin D1 is involved in cell cycle regulation and DNA synthesis and has been shown to be upregulated in a variety of tumors (including breast cancer). In addition, a number of articles has shown that cyclin D1 can affect metabolic processes, particularly glycolysis, lipogenesis, and mitochondrial function (10–12). Specifically, the loss of cyclin D1 caused an upregulation of hexokinase II, pyruvate kinase, fatty acid synthase, and acetyl-CoA carboxylase, leading to increased lipogenesis. …" @default.
• W2166064702 created "2016-06-24" @default.
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• W2166064702 date "2014-09-15" @default.
• W2166064702 modified "2023-09-26" @default.
• W2166064702 title "The Proliferative Gene Cyclin D1 and Gluconeogenesis—Could Suppressing Glucose Production Also Promote Cancer?" @default.
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• W2166064702 doi "https://doi.org/10.2337/db14-0857" @default.
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