Lack of Significant Metabolic Abnormalities in Mice with Liver-Specific Disruption of 11β-Hydroxysteroid Dehydrogenase Type 1

Lavery, Gareth G.; Zielińska, Agnieszka; Gathercole, Laura; Hughes, Beverly; Semjonous, Nina; Guest, Phillip; Saqib, Khalid; Sherlock, Mark; Reynolds, Gary; Morgan, Stuart; Tomlinson, Jeremy W.; Walker, Elizabeth A.; Rabbitt, Elizabeth; Stewart, Paul M.

doi:10.1210/en.2012-1019

Cited by 67 publications

(76 citation statements)

References 56 publications

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“…However, this discrepancy might be attributable to a compensatory production of corticosterone by other tissues and a downregulation of 11b- HSD2 by the liver. In fact, the authors detected around 40% cortisol levels in knockout mice relative to control mice after cortisone challenge 40 . In addition, Dex has been reported to render non-haematological cancer cells more resistant to antitumour drugs [41][42][43][44] .…”

Section: Discussionmentioning

confidence: 96%

“…Therefore, our findings suggest that the downregulation of 11b-HSD1 and upregulation of 11b-HSD2 might generate a profound effect on gluconeogenesis in malignant hepatocytes via regulating GC activities. Recently, Lavery et al 40 found that hepatic PEPCK and G6Pase were expressed in the liver-specific 11b-HSD1 knockout mice, implicating that the loss of 11b-HSD1 does not have a profound effect on gluconeogenesis. However, this discrepancy might be attributable to a compensatory production of corticosterone by other tissues and a downregulation of 11b- HSD2 by the liver.…”

Section: Discussionmentioning

confidence: 99%

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Switch of glycolysis to gluconeogenesis by dexamethasone for treatment of hepatocarcinoma

et al. 2013

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Gluconeogenesis is a fundamental feature of hepatocytes. Whether this gluconeogenic activity is also present in malignant hepatocytes remains unexplored. A better understanding of this biological process may lead to novel therapeutic strategies. Here we show that gluconeogenesis is not present in mouse or human malignant hepatocytes. We find that two critical enzymes 11b-HSD1 and 11b-HSD2 that regulate glucocorticoid activities are expressed inversely in malignant hepatocytes, resulting in the inactivation of endogenous glucocorticoids and the loss of gluconeogenesis. In patients' hepatocarcinoma, the expression of 11b-HSD1 and 11b-HSD2 is closely linked to prognosis and survival. Dexamethasone, an active form of synthesized glucocorticoids, is capable of restoring gluconeogenesis in malignant cells by bypassing the abnormal regulation of 11b-HSD enzymes, leading to therapeutic efficacy against hepatocarcinoma. These findings clarify the molecular basis of malignant hepatocyte loss of gluconeogenesis and suggest new therapeutic strategies.

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Section: Discussionmentioning

confidence: 96%

Section: Discussionmentioning

confidence: 99%

Switch of glycolysis to gluconeogenesis by dexamethasone for treatment of hepatocarcinoma

et al. 2013

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“…All procedures were carried out in accordance with the UK Animals (Scientific Procedures) Act 1986. Six-week-old male global (GKO) (C57BL/6) (31), liver-specific (LKO) (C57BL/6J/129SvJ) (19), and adipose-specific (FKO) C57BL/6J (SI Text) 11β-HSD1 KO mice, with WT controls, had ad libitum access to standard chow and drinking water supplemented with either CORT (100 μg/mL, 0.66% ethanol), 11DHC (100 μg/mL, 0.66% ethanol), or vehicle (0.66% ethanol) for 5 wk. Treatments were replaced twice weekly.…”

Section: Methodsmentioning

confidence: 99%

“…Details with respect to the generation of these transgenic lines are presented in ref. 19, SI Text, and Fig. S6 A-E.…”

mentioning

confidence: 99%

11β-HSD1 is the major regulator of the tissue-specific effects of circulating glucocorticoid excess

Morgan

McCabe

Gathercole

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

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239

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The adverse metabolic effects of prescribed and endogenous glucocorticoid (GC) excess, Cushing syndrome, create a significant health burden. We found that tissue regeneration of GCs by 11β-hydroxysteroid dehydrogenase type 1 (11β-HSD1), rather than circulating delivery, is critical to developing the phenotype of GC excess; 11β-HSD1 KO mice with circulating GC excess are protected from the glucose intolerance, hyperinsulinemia, hepatic steatosis, adiposity, hypertension, myopathy, and dermal atrophy of Cushing syndrome. Whereas liver-specific 11β-HSD1 KO mice developed a full Cushingoid phenotype, adipose-specific 11β-HSD1 KO mice were protected from hepatic steatosis and circulating fatty acid excess. These data challenge our current view of GC action, demonstrating 11β-HSD1, particularly in adipose tissue, is key to the development of the adverse metabolic profile associated with circulating GC excess, offering 11β-HSD1 inhibition as a previously unidentified approach to treat Cushing syndrome.

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“…Genetic knockdown of 11b-HSD1 (69) as well as pharmacological inhibition (70) decreases hepatic steatosis. Interestingly, this may not reflect changes in hepatic GC availability as liver-specific 11b-HSD1 deletion does not impact significantly on metabolic phenotype and this may point to a more crucial role of GC metabolism within adipose tissue (71). The role of the A-ring reductases has been less well explored, although there is some evidence to suggest that deletion of 5aR type 1 increases the risk of development of hepatic steatosis (72).…”

Section: Glucocorticoidsmentioning

confidence: 99%

Mechanisms in endocrinology: Non-alcoholic fatty liver disease in common endocrine disorders

Hazlehurst

Tomlinson

2013

European Journal of Endocrinology

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Non-alcoholic fatty liver disease (NAFLD) is a spectrum of disease spanning from simple benign steatosis to steatohepatitis with fibrosis and scarring that can eventually lead to cirrhosis. Its prevalence is rising rapidly and is developing into the leading indication for liver transplantation worldwide. Abnormalities in endocrine axes have been associated with NALFD, including hypogonadism, hypothyroidism, GH deficiency and hypercortisolaemia. In some instances, correction of the endocrine defects has been shown to have a beneficial impact. While in patients with type 2 diabetes the association with NAFLD is well established and recognised, there is a more limited appreciation of the condition among common endocrine diseases presenting with hormonal excess or deficiency. In this review, we examine the published data that have suggested a mechanistic link between endocrine abnormalities and NAFLD and summarise the clinical data endorsing these observations.

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Lack of Significant Metabolic Abnormalities in Mice with Liver-Specific Disruption of 11β-Hydroxysteroid Dehydrogenase Type 1

Cited by 67 publications

References 56 publications

Switch of glycolysis to gluconeogenesis by dexamethasone for treatment of hepatocarcinoma

Switch of glycolysis to gluconeogenesis by dexamethasone for treatment of hepatocarcinoma

11β-HSD1 is the major regulator of the tissue-specific effects of circulating glucocorticoid excess

Mechanisms in endocrinology: Non-alcoholic fatty liver disease in common endocrine disorders

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