Hepatic Suppression of Foxo1 and Foxo3 Causes Hypoglycemia and Hyperlipidemia in Mice

Zhang, Kebin; Li, Ling; Qi, Yajuan; Zhu, Xiaoping; Gan, Boyi; DePinho, Ronald A.; Averitt, Travis; Guo, Shaodong

doi:10.1210/en.2011-1527

Cited by 150 publications

(194 citation statements)

References 58 publications

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“…Previous studies indicate that FOXO1 overexpression in the liver increased hepatic triacylglycerol content, owing to increased triacylglycerol synthesis [40,41], while recent studies suggest that FOXO proteins suppress hepatic lipogenesis and triacylglycerol levels [42,43]. In this study we show that overexpression of FOXQ1 decreases hepatic and serum triacylglycerol contents in db/db and DIO mice.…”

Section: Discussionsupporting

confidence: 49%

The hepatic FOXQ1 transcription factor regulates glucose metabolism in mice

et al. 2016

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Aim/hypothesis Hepatic forkhead box q1 (FOXQ1) expression levels are regulated by nutritional and pathophysiological status. In this study we investigated the role of FOXQ1 in the regulation of hepatic gluconeogenesis. Methods We used multiple mouse and cell models to study the role of FOXQ1 in regulating expression of gluconeogenic genes, and cellular and hepatic glucose production. Results Expression of hepatic FOXQ1 was regulated by fasting in normal mice and was dysregulated in diabetic mice. Overexpression of FOXQ1 in primary hepatocytes inhibited expression of gluconeogenic genes and decreased cellular glucose output. Hepatic FOXQ1 rescue in db/db and high-fat diet-induced obese mice markedly decreased blood glucose level and improved glucose intolerance. In contrast, wildtype C57 mice with hepatic FOXQ1 deficiency displayed increased blood glucose levels and impaired glucose tolerance. Interestingly, studies into molecular mechanisms indicated that FOXQ1 interacts with FOXO1, thereby blocking FOXO1 activity on hepatic gluconeogenesis, preventing it from directly binding to insulin response elements mapped in the promoter region of gluconeogenic genes. Conclusions/interpretation FOXQ1 is a novel factor involved in regulating hepatic gluconeogenesis, and the decreased FOXQ1 expression in liver may contribute to the development of type 2 diabetes.

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Section: Discussionsupporting

confidence: 49%

The hepatic FOXQ1 transcription factor regulates glucose metabolism in mice

et al. 2016

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“…Using a liver-specific deletion strategy, it has been shown that FoxO1, and not FoxO3/4, reduced blood glucose concentration both in normal and diabetic mice (34). Furthermore, the expression of FoxO1 in different tissues caused insulin resistance and glucose intolerance D) and Ad GFP for 24 h prior to incubation with LG or HG glucose for 24 h. A and C, total RNAs were prepared and used to detect catalase mRNA.…”

Section: Discussionmentioning

confidence: 99%

High Glucose Forces a Positive Feedback Loop Connecting Akt Kinase and FoxO1 Transcription Factor to Activate mTORC1 Kinase for Mesangial Cell Hypertrophy and Matrix Protein Expression

Das

Ghosh‐Choudhury

Dey

et al. 2014

Journal of Biological Chemistry

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“…Immunofluorescence staining of untreated liver tissues revealed a primarily nuclear expression pattern of FoxO3 (Fig. 3, A and D), suggesting that FoxO3 functions physiologically in normal liver homeostasis, probably in its ascribed role of lipid metabolism (40,41). Under oxidative stress, however, FoxO3 mainly translocates to the cytoplasm and membranes (Fig.…”

Section: ␤-Catenin-deficient Livers Exhibit Nuclear Retention Of Foxomentioning

confidence: 94%

“…6). Under homeostatic conditions, activation of FoxO3 is required for the control of cellular metabolism, including glycolysis (24) or fatty acid oxidation (40,41). Under oxidative stress, ␤-catenin signaling activates downstream SGK1 in wild-type hepatocytes, which inactivates FoxO3 by phosphorylation, leading to cytoplasmic translocation of FoxO3.…”

Section: ␤-Catenin Signaling Prevents Oxidative Stress-induced Liver mentioning

confidence: 99%

Wnt/β-Catenin Signaling Protects Mouse Liver against Oxidative Stress-induced Apoptosis through the Inhibition of Forkhead Transcription Factor FoxO3

Guo

Lehwald

Jang

et al. 2013

Journal of Biological Chemistry

110

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Background: Wnt/␤-catenin signaling regulates various hepatocellular processes; however, it remains unexplored whether ␤-catenin provides hepatocyte protection against oxidative stress-induced apoptosis. Results: Mice with ␤-catenin-deficient hepatocytes demonstrate significantly increased hepatotoxin-induced liver injury. Conclusion: Hepatic ␤-catenin signaling confers hepatocyte protection against oxidative stress-induced apoptosis. Significance: Our findings have relevance for potential future therapies directed at hepatocyte protection, regeneration, and anti-cancer treatment.

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Hepatic Suppression of Foxo1 and Foxo3 Causes Hypoglycemia and Hyperlipidemia in Mice

Cited by 150 publications

References 58 publications

The hepatic FOXQ1 transcription factor regulates glucose metabolism in mice

The hepatic FOXQ1 transcription factor regulates glucose metabolism in mice

High Glucose Forces a Positive Feedback Loop Connecting Akt Kinase and FoxO1 Transcription Factor to Activate mTORC1 Kinase for Mesangial Cell Hypertrophy and Matrix Protein Expression

Wnt/β-Catenin Signaling Protects Mouse Liver against Oxidative Stress-induced Apoptosis through the Inhibition of Forkhead Transcription Factor FoxO3

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