Selective Inhibition of FOXO1 Activator/Repressor Balance Modulates Hepatic Glucose Handling

Langlet, Fanny; Haeusler, Rebecca A.; Lindén, Daniel; Ericson, Elke; Norris, Tyrrell; Johansson, Anders; Cook, Joshua R.; Aizawa, Kumiko; Wang, Ling; Buettner, Christoph; Accili, Domenico

doi:10.1016/j.cell.2017.09.045

Cited by 155 publications

(124 citation statements)

References 55 publications

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“…The deletion of FOXO1 rescues loss‐of‐AKT‐impaired LR, which is consistent with our finding that FOXO1 has a suppressive role in LR by inhibiting CD36 expression. The transcription repression function of FOXO1 on CD36 might depend on co‐repressors . In summary, the PDK4/AMPK/FOXO1/CD36 axis is critical to resection‐induced LR, and pharmacological inhibition of PDK4 might improve LR efficiency.…”

Section: Discussionmentioning

confidence: 99%

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PDK4‐Deficiency Reprograms Intrahepatic Glucose and Lipid Metabolism to Facilitate Liver Regeneration in Mice

et al. 2020

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Liver regeneration requires intrahepatic and extrahepatic metabolic reprogramming to meet the high hepatic bioenergy demand for liver cell repopulation. This study aims to elucidate how pyruvate dehydrogenase kinase 4 (PDK4), a critical regulator of glucose and lipid metabolism, coordinates metabolic regulation with efficient liver growth. We found that hepatic Pdk4 expression was elevated after two‐thirds partial hepatectomy (PHx). In Pdk4−/− PHx mice, the liver/body weight ratio was more rapidly restored, accompanied by more aggressive hepatic DNA replication; however, Pdk4−/− mice developed more severe hypoglycemia. In Pdk4−/− PHx livers, the pro‐regenerative insulin signaling was potentiated, as demonstrated by early peaking of the phosphorylation of insulin receptor, more remarkable induction of the insulin receptor substrate proteins, IRS1 and IRS2, and more striking activation of Akt. The hepatic up‐regulation of CD36 contributed to the enhanced transient regeneration‐associated steatosis in Pdk4−/− PHx mice. Notably, CD36 overexpression in mice promoted the recovery of liver/body weight ratio and elevated intrahepatic adenosine triphosphate after PHx. CD36 expression was transcriptionally suppressed by FOXO1 (forkhead box protein O1), which was stabilized and translocated to the nucleus following AMPK (adenosine monophosphate–activated protein kinase) activation. PHx remarkably induced AMPK activation, which became incompetent to respond in Pdk4−/− livers. Moreover, we defined that PDK4‐regulated AMPK activation directly depended on intracellular adenosine monophosphate in vitro and in regenerative livers. Conclusion: PDK4 inhibition reprograms glucose and lipid metabolism to promote liver regeneration by enhancing hepatic insulin/Akt signaling and activating an AMPK/FOXO1/CD36 regulatory axis of lipid. These findings may lead to potential therapeutic strategies to prevent hepatic insufficiency and liver failure.

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Section: Discussionmentioning

confidence: 99%

“…The transcription repression function of FOXO1 on CD36 might depend on co-repressors. (45,46) In summary, the PDK4/AMPK/ FOXO1/CD36 axis is critical to resection-induced LR, and pharmacological inhibition of PDK4 might improve LR efficiency.…”

Section: Discussionmentioning

confidence: 99%

PDK4‐Deficiency Reprograms Intrahepatic Glucose and Lipid Metabolism to Facilitate Liver Regeneration in Mice

et al. 2020

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“…Except for its critical regulatory role of insulin signaling in liver (Langlet et al, 2017), FoxO1 maintains β-cell mass (Kitamura et al, 2002;Okamoto et al, 2006), β-cell identity, and proper β-cell function (Kawamori et al, 2006;Talchai, Xuan, Kitamura, DePinho, & Accili, 2012). Impaired FoxO activity causes MODY-like diabetes through the reduced metabolic flexibility of β-cells (Kim-Muller et al, 2014).…”

Section: Discussionmentioning

confidence: 99%

HDAC4 mutations cause diabetes and induce β‐cell FoxO1 nuclear exclusion

Gong

Liang

et al. 2019

Molec Gen & Gen Med

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Background Studying patients with rare Mendelian diabetes has uncovered molecular mechanisms regulating β‐cell pathophysiology. Previous studies have shown that Class IIa histone deacetylases (HDAC4, 5, 7, and 9) modulate mammalian pancreatic endocrine cell function and glucose homeostasis. Methods We performed exome sequencing in one adolescent nonautoimmune diabetic patient and detected one de novo predicted disease‐causing HDAC4 variant (p.His227Arg). We screened our pediatric diabetes cohort with unknown etiology using Sanger sequencing. In mouse pancreatic β‐cell lines (Min6 and SJ cells), we performed insulin secretion assay and quantitative RT‐PCR to measure the β‐cell function transfected with the detected HDAC4 variants and wild type. We carried out immunostaining and Western blot to investigate if the detected HDAC4 variants affect the cellular translocation and acetylation status of Forkhead box protein O1 (FoxO1) in the pancreatic β‐cells. Results We discovered three HDAC4 mutations (p.His227Arg, p.Asp234Asn, and p.Glu374Lys) in unrelated individuals who had nonautoimmune diabetes with various degrees of β‐cell loss. In mouse pancreatic β‐cell lines, we found that these three HDAC4 mutations decrease insulin secretion, down‐regulate β‐cell‐specific transcriptional factors, and cause nuclear exclusion of acetylated FoxO1. Conclusion Mutations in HDAC4 disrupt the deacetylation of FoxO1, subsequently decrease the β‐cell function including insulin secretion, resulting in diabetes.

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“…Adiponectin is an adipose-derived hormone which comprises 0.01% of all plasma proteins. Despite its known protective functions in the body, which include anti-inflammatory, anti-atherosclerotic and anti-fibrotic effects (1), its primary physiological role may be the ability to improve systemic insulin sensitivity. Its role in regulating glucose homeostasis therefore suggests that the observed decrease in serum levels of adiponectin in non-insulin dependent (type 2) diabetes mellitus (NIDDM) is involved in the pathogenesis of insulin resistance and ultimately NIDDM (2,3).…”

Section: Introductionmentioning

confidence: 99%

Dysregulation of the Mitochondrial Proteome Occurs in Mice Lacking Adiponectin Receptor 1

et al. 2019

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Selective Inhibition of FOXO1 Activator/Repressor Balance Modulates Hepatic Glucose Handling

Cited by 155 publications

References 55 publications

PDK4‐Deficiency Reprograms Intrahepatic Glucose and Lipid Metabolism to Facilitate Liver Regeneration in Mice

PDK4‐Deficiency Reprograms Intrahepatic Glucose and Lipid Metabolism to Facilitate Liver Regeneration in Mice

HDAC4 mutations cause diabetes and induce β‐cell FoxO1 nuclear exclusion

Dysregulation of the Mitochondrial Proteome Occurs in Mice Lacking Adiponectin Receptor 1

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