Your search keyword '"Orphan Nuclear Receptors metabolism"' showing total 31 results

1. 4β-Hydroxycholesterol is a prolipogenic factor that promotes SREBP1c expression and activity through the liver X receptor.

Author

Moldavski O, Zushin PH, Berdan CA, Van Eijkeren RJ, Jiang X, Qian M, Ory DS, Covey DF, Nomura DK, Stahl A, Weiss EJ, and Zoncu R

Subjects

Animals, Mice, Hepatocytes metabolism, Humans, Signal Transduction, Male, Mice, Inbred C57BL, Liver metabolism, Orphan Nuclear Receptors metabolism, Orphan Nuclear Receptors agonists, Gene Expression Regulation drug effects, Liver X Receptors metabolism, Liver X Receptors agonists, Liver X Receptors genetics, Hydroxycholesterols metabolism, Hydroxycholesterols pharmacology, Sterol Regulatory Element Binding Protein 1 metabolism, Sterol Regulatory Element Binding Protein 1 genetics, Lipogenesis

Abstract

Oxysterols are oxidized derivatives of cholesterol that play regulatory roles in lipid biosynthesis and homeostasis. How oxysterol signaling coordinates different lipid classes such as sterols and triglycerides remains incompletely understood. Here, we show that 4β-hydroxycholesterol (HC) (4β-HC), a liver and serum abundant oxysterol of poorly defined functions, is a potent and selective inducer of the master lipogenic transcription factor, SREBP1c, but not the related steroidogenic transcription factor SREBP2. By correlating tracing of lipid synthesis with lipogenic gene expression profiling, we found that 4β-HC acts as a putative agonist for the liver X receptor (LXR), a sterol sensor and transcriptional regulator previously linked to SREBP1c activation. Unique among the oxysterol agonists of the LXR, 4β-HC induced expression of the lipogenic program downstream of SREBP1c and triggered de novo lipogenesis both in primary hepatocytes and in the mouse liver. In addition, 4β-HC acted in parallel to insulin-PI3K-dependent signaling to stimulate triglyceride synthesis and lipid-droplet accumulation. Thus, 4β-HC is an endogenous regulator of de novo lipogenesis through the LXR-SREBP1c axis., Competing Interests: Conflict of interest R. Z. is cofounder, scientific advisor, and stockholder with Frontier Medicines Corp. All other authors declare that they have no conflicts of interest with the contents of this article., (Copyright © 2021. Published by Elsevier Inc.)

Published

2021

2. 11β-Hydroxysteroid dehydrogenases control access of 7β,27-dihydroxycholesterol to retinoid-related orphan receptor γ.

Author

Beck KR, Inderbinen SG, Kanagaratnam S, Kratschmar DV, Jetten AM, Yamaguchi H, and Odermatt A

Subjects

11-beta-Hydroxysteroid Dehydrogenases genetics, Cell Line, Cell Line, Tumor, Chromatography, High Pressure Liquid, Glucocorticoids metabolism, Humans, Kinetics, Molecular Docking Simulation, Oxysterols metabolism, Tandem Mass Spectrometry, 11-beta-Hydroxysteroid Dehydrogenases metabolism, Orphan Nuclear Receptors metabolism, Receptors, Mineralocorticoid metabolism

Abstract

Oxysterols previously were considered intermediates of bile acid and steroid hormone biosynthetic pathways. However, recent research has emphasized the roles of oxysterols in essential physiologic processes and in various diseases. Despite these discoveries, the metabolic pathways leading to the different oxysterols are still largely unknown and the biosynthetic origin of several oxysterols remains unidentified. Earlier studies demonstrated that the glucocorticoid metabolizing enzymes, 11β-hydroxysteroid dehydrogenase (11β-HSD) types 1 and 2, interconvert 7-ketocholesterol (7kC) and 7β-hydroxycholesterol (7βOHC). We examined the role of 11β-HSDs in the enzymatic control of the intracellular availability of 7β,27-dihydroxycholesterol (7β27OHC), a retinoid-related orphan receptor γ (RORγ) ligand. We used microsomal preparations of cells expressing recombinant 11β-HSD1 and 11β-HSD2 to assess whether 7β27OHC and 7-keto,27-hydroxycholesterol (7k27OHC) are substrates of these enzymes. Binding of 7β27OHC and 7k27OHC to 11β-HSDs was studied by molecular modeling. To our knowledge, the stereospecific oxoreduction of 7k27OHC to 7β27OHC by human 11β-HSD1 and the reverse oxidation reaction of 7β27OHC to 7k27OHC by human 11β-HSD2 were demonstrated for the first time. Apparent enzyme affinities of 11β-HSDs for these novel substrates were equal to or higher than those of the glucocorticoids. This is supported by the fact that 7k27OHC and 7β27OHC are potent inhibitors of the 11β-HSD1-dependent oxoreduction of cortisone and the 11β-HSD2-dependent oxidation of cortisol, respectively. Furthermore, molecular docking calculations explained stereospecific enzyme activities. Finally, using an inducible RORγ reporter system, we showed that 11β-HSD1 and 11β-HSD2 controlled RORγ activity. These findings revealed a novel glucocorticoid-independent prereceptor regulation mechanism by 11β-HSDs that warrants further investigation., (Copyright © 2019 Beck et al. Published by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2019

3. Human monocyte-derived dendritic cells turn into foamy dendritic cells with IL-17A.

Author

Salvatore G, Bernoud-Hubac N, Bissay N, Debard C, Daira P, Meugnier E, Proamer F, Hanau D, Vidal H, Aricò M, Delprat C, and Mahtouk K

Subjects

Atherosclerosis immunology, Atherosclerosis pathology, Cell Differentiation genetics, Cell Proliferation genetics, Dendritic Cells immunology, Foam Cells metabolism, Gene Expression Regulation, Humans, Interleukin-17 genetics, Interleukin-17 immunology, Lipid Droplets immunology, Lipid Droplets metabolism, Lipid Metabolism immunology, Liver X Receptors, Macrophages immunology, Macrophages metabolism, Monocytes immunology, Monocytes metabolism, Orphan Nuclear Receptors biosynthesis, Orphan Nuclear Receptors metabolism, T-Lymphocytes immunology, T-Lymphocytes metabolism, Atherosclerosis metabolism, Dendritic Cells metabolism, Fatty Acids metabolism, Interleukin-17 metabolism

Abstract

Interleukin 17A (IL-17A) is a proinflammatory cytokine involved in the pathogenesis of chronic inflammatory diseases. In the field of immunometabolism, we have studied the impact of IL-17A on the lipid metabolism of human in vitro-generated monocyte-derived dendritic cells (DCs). Microarrays and lipidomic analysis revealed an intense remodeling of lipid metabolism induced by IL-17A in DCs. IL-17A increased 2-12 times the amounts of phospholipids, cholesterol, triglycerides, and cholesteryl esters in DCs. Palmitic (16:0), stearic (18:0), and oleic (18:ln-9c) acid were the main fatty acid chains present in DCs. They were strongly increased in response to IL-17A while their relative proportion remained unchanged. Capture of extracellular lipids was the major mechanism of lipid droplet accumulation, visualized by electron microscopy and Oil Red O staining. Besides this foamy phenotype, IL-17A induced a mixed macrophage-DC phenotype and expression of the nuclear receptor NR1H3/liver X receptor-α, previously identified in the context of atherosclerosis as the master regulator of cholesterol homeostasis in macrophages. These IL-17A-treated DCs were as competent as untreated DCs to stimulate allogeneic naive T-cell proliferation. Following this first characterization of lipid-rich DCs, we propose to call these IL-17A-dependent cells "foamy DCs" and discuss the possible existence of foamy DCs in atherosclerosis, a metabolic and inflammatory disorder involving IL-17A., (Copyright © 2015 by the American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

4. Liver X receptor regulates hepatic nuclear O-GlcNAc signaling and carbohydrate responsive element-binding protein activity.

Author

Bindesbøll C, Fan Q, Nørgaard RC, MacPherson L, Ruan HB, Wu J, Pedersen TÅ, Steffensen KR, Yang X, Matthews J, Mandrup S, Nebb HI, and Grønning-Wang LM

Subjects

Acylation drug effects, Animals, Basic Helix-Loop-Helix Leucine Zipper Transcription Factors, Cell Line, Cell Nucleus drug effects, Eating, Fasting, Gene Expression Regulation drug effects, Glucose pharmacology, Humans, Lipogenesis drug effects, Liver drug effects, Liver enzymology, Liver X Receptors, Male, Mice, Nuclear Proteins genetics, Orphan Nuclear Receptors deficiency, Promoter Regions, Genetic genetics, Protein Isoforms genetics, Protein Isoforms metabolism, Protein Transport drug effects, Pyruvate Kinase metabolism, Streptozocin adverse effects, Transcription Factors genetics, Transcriptional Activation drug effects, Triglycerides biosynthesis, Triglycerides blood, Acetylglucosamine metabolism, Cell Nucleus metabolism, Liver cytology, Liver metabolism, Nuclear Proteins metabolism, Orphan Nuclear Receptors metabolism, Signal Transduction drug effects, Transcription Factors metabolism

Abstract

Liver X receptor (LXR)α and LXRβ play key roles in hepatic de novo lipogenesis through their regulation of lipogenic genes, including sterol regulatory element-binding protein (SREBP)-1c and carbohydrate responsive element-binding protein (ChREBP). LXRs activate lipogenic gene transcription in response to feeding, which is believed to be mediated by insulin. We have previously shown that LXRs are targets for glucose-hexosamine-derived O-linked β-N-acetylglucosamine (O-GlcNAc) modification enhancing their ability to regulate SREBP-1c promoter activity in vitro. To elucidate insulin-independent effects of feeding on LXR-mediated lipogenic gene expression in vivo, we subjected control and streptozotocin-treated LXRα/β(+/+) and LXRα/β(-/-) mice to a fasting-refeeding regime. We show that under hyperglycemic and hypoinsulinemic conditions, LXRs maintain their ability to upregulate the expression of glycolytic and lipogenic enzymes, including glucokinase (GK), SREBP-1c, ChREBPα, and the newly identified shorter isoform ChREBPβ. Furthermore, glucose-dependent increases in LXR/retinoid X receptor-regulated luciferase activity driven by the ChREBPα promoter was mediated, at least in part, by O-GlcNAc transferase (OGT) signaling in Huh7 cells. Moreover, we show that LXR and OGT interact and colocalize in the nucleus and that loss of LXRs profoundly reduced nuclear O-GlcNAc signaling and ChREBPα promoter binding activity in vivo. In summary, our study provides evidence that LXRs act as nutrient and glucose metabolic sensors upstream of ChREBP by modulating GK expression, nuclear O-GlcNAc signaling, and ChREBP expression and activity., (Copyright © 2015 by the American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

5. Identification of miR-185 as a regulator of de novo cholesterol biosynthesis and low density lipoprotein uptake.

Author

Yang M, Liu W, Pellicane C, Sahyoun C, Joseph BK, Gallo-Ebert C, Donigan M, Pandya D, Giordano C, Bata A, and Nickels JT Jr

Subjects

3' Untranslated Regions genetics, Animals, Cell Line, Cholesterol blood, Diet, High-Fat adverse effects, Gene Expression Regulation drug effects, Humans, Hydroxymethylglutaryl CoA Reductases metabolism, Insulin pharmacology, Liver X Receptors, Male, Mice, Mice, Inbred C57BL, Orphan Nuclear Receptors metabolism, Protein Transport drug effects, Receptors, LDL metabolism, Sterol Regulatory Element Binding Protein 1 metabolism, Sterol Regulatory Element Binding Protein 2 genetics, Transcription, Genetic drug effects, Cholesterol biosynthesis, Lipoproteins, LDL metabolism, MicroRNAs genetics

Abstract

Dysregulation of cholesterol homeostasis is associated with various metabolic diseases, including atherosclerosis and type 2 diabetes. The sterol response element binding protein (SREBP)-2 transcription factor induces the expression of genes involved in de novo cholesterol biosynthesis and low density lipoprotein (LDL) uptake, thus it plays a crucial role in maintaining cholesterol homeostasis. Here, we found that overexpressing microRNA (miR)-185 in HepG2 cells repressed SREBP-2 expression and protein level. miR-185-directed inhibition caused decreased SREBP-2-dependent gene expression, LDL uptake, and HMG-CoA reductase activity. In addition, we found that miR-185 expression was tightly regulated by SREBP-1c, through its binding to a single sterol response element in the miR-185 promoter. Moreover, we found that miR-185 expression levels were elevated in mice fed a high-fat diet, and this increase correlated with an increase in total cholesterol level and a decrease in SREBP-2 expression and protein. Finally, we found that individuals with high cholesterol had a 5-fold increase in serum miR-185 expression compared with control individuals. Thus, miR-185 controls cholesterol homeostasis through regulating SREBP-2 expression and activity. In turn, SREBP-1c regulates miR-185 expression through a complex cholesterol-responsive feedback loop. Thus, a novel axis regulating cholesterol homeostasis exists that exploits miR-185-dependent regulation of SREBP-2 and requires SREBP-1c for function.

Published

2014

6. LXRα fuels fatty acid-stimulated oxygen consumption in white adipocytes.

Author

Dib L, Bugge A, and Collins S

Subjects

Adipocytes, White cytology, Adipocytes, White drug effects, Animals, Body Weight drug effects, Diet, High-Fat adverse effects, Gene Expression Regulation drug effects, Gene Knockout Techniques, Hydrocarbons, Fluorinated pharmacology, Liver X Receptors, Male, Mice, Mitochondria drug effects, Mitochondria metabolism, Obesity metabolism, Obesity pathology, Orphan Nuclear Receptors deficiency, Orphan Nuclear Receptors genetics, Oxidation-Reduction, Phenotype, Receptors, Adrenergic, beta metabolism, Sulfonamides pharmacology, Adipocytes, White metabolism, Fatty Acids metabolism, Lipolysis drug effects, Orphan Nuclear Receptors metabolism, Oxygen Consumption drug effects

Abstract

Liver X receptors (LXRs) are transcription factors known for their role in hepatic cholesterol and lipid metabolism. Though highly expressed in fat, the role of LXR in this tissue is not well characterized. We generated adipose tissue LXRα knockout (ATaKO) mice and showed that these mice gain more weight and fat mass on a high-fat diet compared with wild-type controls. White adipose tissue (WAT) accretion in ATaKO mice results from both a decrease in WAT lipolytic and oxidative capacities. This was demonstrated by decreased expression of the β2- and β3-adrenergic receptors, reduced level of phosphorylated hormone-sensitive lipase, and lower oxygen consumption rates (OCRs) in WAT of ATaKO mice. Furthermore, LXR activation in vivo and in vitro led to decreased adipocyte size in WAT and increased glycerol release from primary adipocytes, respectively, with a concomitant increase in OCR in both models. Our findings show that absence of LXRα in adipose tissue results in elevated adiposity through a decrease in WAT oxidation, secondary to attenuated FA availability.

Published

2014

7. ABCG1-mediated generation of extracellular cholesterol microdomains.

Author

Freeman SR, Jin X, Anzinger JJ, Xu Q, Purushothaman S, Fessler MB, Addadi L, and Kruth HS

Subjects

ATP Binding Cassette Transporter, Subfamily G, Member 1, Animals, Anticholesteremic Agents pharmacology, Apolipoprotein A-I metabolism, Cells, Cultured, Humans, Hydrocarbons, Fluorinated pharmacology, Lipid Metabolism, Lipoproteins, HDL metabolism, Liver X Receptors, Macrophages metabolism, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Orphan Nuclear Receptors agonists, Orphan Nuclear Receptors metabolism, Probucol pharmacology, Sulfonamides pharmacology, ATP-Binding Cassette Transporters metabolism, Cholesterol metabolism, Membrane Microdomains metabolism

Abstract

Previous studies have demonstrated that the ATP-binding cassette transporters (ABC)A1 and ABCG1 function in many aspects of cholesterol efflux from macrophages. In this current study, we continued our investigation of extracellular cholesterol microdomains that form during enrichment of macrophages with cholesterol. Human monocyte-derived macrophages and mouse bone marrow-derived macrophages, differentiated with macrophage colony-stimulating factor (M-CSF) or granulocyte macrophage colony-stimulation factor (GM-CSF), were incubated with acetylated LDL (AcLDL) to allow for cholesterol enrichment and processing. We utilized an anti-cholesterol microdomain monoclonal antibody to reveal pools of unesterified cholesterol, which were found both in the extracellular matrix and associated with the cell surface, that we show function in reverse cholesterol transport. Coincubation of AcLDL with 50 μg/ml apoA-I eliminated all extracellular and cell surface-associated cholesterol microdomains, while coincubation with the same concentration of HDL only removed extracellular matrix-associated cholesterol microdomains. Only at an HDL concentration of 200 µg/ml did HDL eliminate the cholesterol microdomains that were cell-surface associated. The deposition of cholesterol microdomains was inhibited by probucol, but it was increased by the liver X receptor (LXR) agonist TO901317, which upregulates ABCA1 and ABCG1. Extracellular cholesterol microdomains did not develop when ABCG1-deficient mouse bone marrow-derived macrophages were enriched with cholesterol. Our findings show that generation of extracellular cholesterol microdomains is mediated by ABCG1 and that reverse cholesterol transport occurs not only at the cell surface but also within the extracellular space.

Published

2014

8. Endoplasmic reticulum stress impairs cholesterol efflux and synthesis in hepatic cells.

Author

Röhrl C, Eigner K, Winter K, Korbelius M, Obrowsky S, Kratky D, Kovacs WJ, and Stangl H

Subjects

ATP Binding Cassette Transporter 1 genetics, ATP Binding Cassette Transporter 1 metabolism, Animals, Cholesterol metabolism, Gene Expression, Gene Expression Regulation, Glycosylation, Hep G2 Cells, Humans, Hydroxymethylglutaryl CoA Reductases metabolism, Lipid Metabolism, Liver metabolism, Liver X Receptors, Male, Mice, Mice, Inbred C57BL, Orphan Nuclear Receptors genetics, Orphan Nuclear Receptors metabolism, Protein Processing, Post-Translational, Sterol Regulatory Element Binding Protein 2, Cholesterol biosynthesis, Endoplasmic Reticulum Stress, Hepatocytes metabolism

Abstract

Metabolic disorders such as type 2 diabetes cause hepatic endoplasmic reticulum (ER) stress, which affects neutral lipid metabolism. However, the role of ER stress in cholesterol metabolism is incompletely understood. Here, we show that induction of acute ER stress in human hepatic HepG2 cells reduced ABCA1 expression and caused ABCA1 redistribution to tubular perinuclear compartments. Consequently, cholesterol efflux to apoA-I, a key step in nascent HDL formation, was diminished by 80%. Besides ABCA1, endogenous apoA-I expression was reduced upon ER stress induction, which contributed to reduced cholesterol efflux. Liver X receptor, a key regulator of ABCA1 in peripheral cells, was not involved in this process. Despite reduced cholesterol efflux, cellular cholesterol levels remained unchanged during ER stress. This was due to impaired de novo cholesterol synthesis by reduction of HMG-CoA reductase activity by 70%, although sterol response element-binding protein-2 activity was induced. In mice, ER stress induction led to a marked reduction of hepatic ABCA1 expression. However, HDL cholesterol levels were unaltered, presumably because of scavenger receptor class B, type I downregulation under ER stress. Taken together, our data suggest that ER stress in metabolic disorders reduces HDL biogenesis due to impaired hepatic ABCA1 function.

Published

2014

9. Hormonal modulators of glial ABCA1 and apoE levels.

Author

Fan J, Shimizu Y, Chan J, Wilkinson A, Ito A, Tontonoz P, Dullaghan E, Galea LA, Pfeifer T, and Wellington CL

Subjects

ATP Binding Cassette Transporter 1 genetics, Animals, Apolipoprotein A-I metabolism, Apolipoprotein E3 metabolism, Apolipoproteins E genetics, Astrocytes drug effects, Astrocytes metabolism, Biological Transport drug effects, Cell Line, Cholesterol metabolism, Estrogens pharmacology, Homeostasis drug effects, Humans, Liver X Receptors, Lynestrenol pharmacology, Mice, Orphan Nuclear Receptors metabolism, Progesterone pharmacology, RNA, Messenger genetics, RNA, Messenger metabolism, Receptors, Progesterone metabolism, Sterol Regulatory Element Binding Protein 1 genetics, Up-Regulation drug effects, ATP Binding Cassette Transporter 1 metabolism, Apolipoproteins E metabolism, Hormones pharmacology, Neuroglia drug effects, Neuroglia metabolism

Abstract

Apolipoprotein E (apoE) is the major lipid carrier in the central nervous system. As apoE plays a major role in the pathogenesis of Alzheimer disease (AD) and also mediates repair pathways after several forms of acute brain injury, modulating the expression, secretion, or function of apoE may provide potential therapeutic approaches for several neurological disorders. Here we show that progesterone and a synthetic progestin, lynestrenol, significantly induce apoE secretion from human CCF-STTG1 astrocytoma cells, whereas estrogens and the progesterone metabolite allopregnanolone have negligible effects. Intriguingly, lynestrenol also increases expression of the cholesterol transporter ABCA1 in CCF-STTG1 astrocytoma cells, primary murine glia, and immortalized murine astrocytes that express human apoE3. The progesterone receptor inhibitor RU486 attenuates the effect of progestins on apoE expression in CCF-STTG1 astrocytoma cells but has no effect on ABCA1 expression in all glial cell models tested, suggesting that the progesterone receptor (PR) may participate in apoE but does not affect ABCA1 regulation. These results suggest that selective reproductive steroid hormones have the potential to influence glial lipid homeostasis through liver X receptor-dependent and progesterone receptor-dependent pathways.

Published

2013

10. The LXR-IDOL axis defines a clathrin-, caveolae-, and dynamin-independent endocytic route for LDLR internalization and lysosomal degradation.

Author

Sorrentino V, Nelson JK, Maspero E, Marques ARA, Scheer L, Polo S, and Zelcer N

Subjects

Caveolae metabolism, Cells, Cultured, Clathrin metabolism, Dynamins metabolism, HEK293 Cells, HeLa Cells, Hep G2 Cells, Humans, Liver X Receptors, Endocytosis, Lysosomes metabolism, Orphan Nuclear Receptors metabolism, Receptors, LDL metabolism, Ubiquitin-Protein Ligases metabolism

Abstract

Low density lipoprotein (LDL) cholesterol is taken up into cells via clathrin-mediated endocytosis of the LDL receptor (LDLR). Following dissociation of the LDLR-LDL complex, LDL is directed to lysosomes whereas the LDLR recycles to the plasma membrane. Activation of the sterol-sensing nuclear receptors liver X receptors (LXRs) enhances degradation of the LDLR. This depends on the LXR target gene inducible degrader of the LDLR (IDOL), an E3-ubiquitin ligase that promotes ubiquitylation and lysosomal degradation of the LDLR. How ubiquitylation of the LDLR by IDOL controls its endocytic trafficking is currently unknown. Using genetic- and pharmacological-based approaches coupled to functional assessment of LDL uptake, we show that the LXR-IDOL axis targets a LDLR pool present in lipid rafts. IDOL-dependent internalization of the LDLR is independent of clathrin, caveolin, macroautophagy, and dynamin. Rather, it depends on the endocytic protein epsin. Consistent with LDLR ubiquitylation acting as a sorting signal, degradation of the receptor can be blocked by perturbing the endosomal sorting complex required for transport (ESCRT) or by USP8, a deubiquitylase implicated in sorting ubiquitylated cargo to multivesicular bodies. In summary, we provide evidence for the existence of an LXR-IDOL-mediated internalization pathway for the LDLR that is distinct from that used for lipoprotein uptake.

Published

2013

11. High-fructose diet downregulates long-chain acyl-CoA synthetase 3 expression in liver of hamsters via impairing LXR/RXR signaling pathway.

Author

Dong B, Kan CF, Singh AB, and Liu J

Subjects

Acyl Coenzyme A biosynthesis, Animals, Cricetinae, Fructose administration & dosage, Gene Expression Regulation, Liver metabolism, Liver X Receptors, Retinoid X Receptor beta metabolism, Signal Transduction, Coenzyme A Ligases biosynthesis, Diet, Liver enzymology, Orphan Nuclear Receptors metabolism

Abstract

Long-chain acyl-CoA synthetases (ACSL) play key roles in fatty acid metabolism in liver and other metabolic tissues in an isozyme-specific manner. In this study, we examined the effects of a fructose-enriched diet on expressions of ACSL isoforms in the liver of hamsters. We showed that the fructose diet markedly reduced the mRNA and protein expressions of ACSL3 in hamster liver without significant effects on other ACSLs. The decrease in ACSL3 abundance was accompanied by a reduction in ACSL-catalyzed synthesis of arachidonyl-CoA and oleoyl-CoA in liver homogenates of hamsters fed the fructose diet as opposed to normal diet. We further showed that fructose diet specifically reduced expressions of three key components of the LXR signaling pathway, namely, liver X receptor (LXR)α, LXRβ, and retinoid X receptor (RXR)β. Exogenous expression and activation of LXRα/β increased hamster ACSL3 promoter activities in a LXR-responsive element (LXRE)-dependent fashion. Finally, we showed that treating hamsters with LXR agonist GW3965 increased hepatic ACSL3 expression without affecting other ACSL isoforms. Furthermore, the ligand-induced increases of ACSL3 expression were accompanied with the reduction of hepatic triglyceride levels in GW3965-treated hamster liver. Altogether, our studies demonstrate that fructose diet has a negative impact on LXR signaling pathway in liver tissue and reduction of ACSL3 expression/activity could be a causal factor for fructose-induced hepatic steatosis.

Published

2013

12. LXR activation by GW3965 alters fat tissue distribution and adipose tissue inflammation in ob/ob female mice.

Author

Archer A, Stolarczyk E, Doria ML, Helguero L, Domingues R, Howard JK, Mode A, Korach-André M, and Gustafsson JÅ

Subjects

Adipogenesis, Animals, Body Fat Distribution, Female, Inflammation metabolism, Inflammation pathology, Lipolysis, Liver X Receptors, Macrophages drug effects, Macrophages metabolism, Mice, Obesity genetics, Obesity pathology, Orphan Nuclear Receptors agonists, Orphan Nuclear Receptors genetics, Adipose Tissue metabolism, Benzoates administration & dosage, Benzylamines administration & dosage, Obesity metabolism, Orphan Nuclear Receptors metabolism

Abstract

To investigate the role of liver X receptor (LXR) in adipose tissue metabolism during obesity, ob/ob mice were treated for 5 weeks with the synthetic LXR agonist GW3965. MRI analysis revealed that pharmacological activation of LXR modified fat distribution by decreasing visceral (VS) fat and inversely increasing subcutaneous (SC) fat storage without affecting whole body fat content. This was concordant with opposite regulation by GW3965 of the lipolytic markers hormone-sensitive lipase (HSL) and adipose triglyceride lipase (ATGL) in the two fat depots; moreover, the expression of genes involved in lipogenesis was significantly induced in SC fat. Lipidomic analysis suggested that changes in lipid composition in response to GW3965 also varied between VS and SC fat. In both depots, the observed alteration in lipid composition indicated an overall change toward less lipotoxic lipids. Flow cytometry analysis showed decreased immune cell infiltration in adipose tissue of ob/ob mice in response to GW3965 treatment, which in VS fat mainly affected the macrophage population and in SC fat the lymphocyte population. In line with this, the expression and secretion of proinflammatory markers was decreased in both fat deposits with GW3965 treatment.

Published

2013

13. On the regulatory role of side-chain hydroxylated oxysterols in the brain. Lessons from CYP27A1 transgenic and Cyp27a1(-/-) mice.

Author

Ali Z, Heverin M, Olin M, Acimovic J, Lövgren-Sandblom A, Shafaati M, Båvner A, Meiner V, Leitersdorf E, and Björkhem I

Subjects

Animals, Brain, Cholestanetriol 26-Monooxygenase genetics, Cholesterol metabolism, Female, Humans, Hydroxymethylglutaryl-CoA Synthase metabolism, Liver X Receptors, Male, Mice, Mice, Knockout, Mice, Transgenic, Orphan Nuclear Receptors metabolism, Cholestanetriol 26-Monooxygenase metabolism, Hydroxycholesterols metabolism

Abstract

The two oxysterols, 27-hydroxycholesterol (27OH) and 24S-hydroxycholesterol (24OH), are both inhibitors of cholesterol synthesis and activators of the liver X receptor (LXR) in vitro. Their role as physiological regulators under in vivo conditions is controversial, however. In the present work, we utilized a previously described mouse model with overexpressed human sterol 27-hydroxylase (CYP27A1). The levels of 27OH were increased about 12-fold in the brain. The brain levels of HMG-CoA reductase mRNA and HMG-CoA synthase mRNA levels were increased. In accordance with increased cholesterol synthesis, most of the cholesterol precursors were also increased. The level of 24OH, the dominating oxysterol in the brain, was decreased by about 25%, most probably due to increased metabolism by CYP27A1. The LXR target genes were unaffected or slightly changed in a direction opposite to that expected for LXR activation. In the brain of Cyp27(-/-) mice, cholesterol synthesis was slightly increased, with increased levels of cholesterol precursors but normal mRNA levels of HMG-CoA reductase and HMG-CoA synthase. The mRNA levels corresponding to LXR target genes were not affected. The results are consistent with the possibility that both 24OH and 27OH are physiological suppressors of cholesterol synthesis in the brain. The results do not support the contention that 27OH is a general activator of LXR target genes in this organ.

Published

2013

14. Quercetin enhances ABCA1 expression and cholesterol efflux through a p38-dependent pathway in macrophages.

Author

Chang YC, Lee TS, and Chiang AN

Subjects

ATP Binding Cassette Transporter 1, ATP-Binding Cassette Transporters genetics, Animals, Binding Sites, Biological Transport drug effects, Cell Line, Enzyme Activation drug effects, Liver X Receptors, MAP Kinase Kinase 3 metabolism, MAP Kinase Kinase 6 metabolism, MAP Kinase Kinase Kinases metabolism, Macrophages metabolism, Mice, Orphan Nuclear Receptors metabolism, Phosphorylation drug effects, Promoter Regions, Genetic drug effects, Sp1 Transcription Factor metabolism, ATP-Binding Cassette Transporters metabolism, Cholesterol metabolism, Gene Expression Regulation drug effects, Macrophages cytology, Quercetin pharmacology, Signal Transduction drug effects, p38 Mitogen-Activated Protein Kinases metabolism

Abstract

ATP-binding cassette transporter A1 (ABCA1) plays a crucial role in exporting cholesterol from macrophages, a function relevant to its involvement in the prevention of atherosclerosis. Quercetin, one of flavonoids, has been described to reduce atherosclerotic lesion formation. This study is aimed to investigate the effect of quercetin on regulation of ABCA1 expression and to explore its underlying mechanisms in macrophages. The results show that quercetin markedly enhanced cholesterol efflux from macrophages in a concentration-dependent manner, which was associated with an increase in ABCA1 mRNA and protein expression. Remarkably, quercetin is able to stimulate the phosphorylation of p38 by up to 234-fold at 6 h via an activation of the transforming growth factor β-activated kinase 1 (TAK1) and mitogen-activated kinase kinase 3/6 (MKK3/6). Inhibition of p38 with a pharmacological inhibitor or small hairpin RNA (shRNA) suppressed the stimulatory effects of quercetin on ABCA1 expression and cholesterol efflux. Moreover, knockdown of p38 reduced quercetin-enhanced ABCA1 promoter activity and the binding of specificity protein 1 (Sp1) and liver X receptor α (LXRα) to the ABCA1 promoter using chromatin immunoprecipitation assays. These findings provide evidence that p38 signaling is essential for the regulation of quercetin-induced ABCA1 expression and cholesterol efflux in macrophages.

Published

2012

15. LXRα is uniquely required for maximal reverse cholesterol transport and atheroprotection in ApoE-deficient mice.

Author

Hong C, Bradley MN, Rong X, Wang X, Wagner A, Grijalva V, Castellani LW, Salazar J, Realegeno S, Boyadjian R, Fogelman AM, Van Lenten BJ, Reddy ST, Lusis AJ, Tangirala RK, and Tontonoz P

Subjects

Animals, Biological Transport, Cell Line, Disease Susceptibility, Gene Expression Regulation, Liver metabolism, Liver X Receptors, Macrophages metabolism, Male, Mice, Mice, Inbred C57BL, Phenotype, Apolipoproteins E deficiency, Atherosclerosis metabolism, Atherosclerosis prevention & control, Cholesterol metabolism, Orphan Nuclear Receptors metabolism

Abstract

The liver X receptor (LXR) signaling pathway is an important modulator of atherosclerosis, but the relative importance of the two LXRs in atheroprotection is incompletely understood. We show here that LXRα, the dominant LXR isotype expressed in liver, plays a particularly important role in whole-body sterol homeostasis. In the context of the ApoE(-/-) background, deletion of LXRα, but not LXRβ, led to prominent increases in atherosclerosis and peripheral cholesterol accumulation. However, combined loss of LXRα and LXRβ on the ApoE(-/-) background led to an even more severe cholesterol accumulation phenotype compared to LXRα(-/-)ApoE(-/-) mice, indicating that LXRβ does contribute to reverse cholesterol transport (RCT) but that this contribution is quantitatively less important than that of LXRα. Unexpectedly, macrophages did not appear to underlie the differential phenotype of LXRα(-/-)ApoE(-/-) and LXRβ(-/-)ApoE(-/-) mice, as in vitro assays revealed no difference in the efficiency of cholesterol efflux from isolated macrophages. By contrast, in vivo assays of RCT using exogenously labeled macrophages revealed a marked defect in fecal sterol efflux in LXRα(-/-)ApoE(-/-) mice. Mechanistically, this defect was linked to a specific requirement for LXRα(-/-) in the expression of hepatic LXR target genes involved in sterol transport and metabolism. These studies reveal a previously unrecognized requirement for hepatic LXRα for optimal reverse cholesterol transport in mice.

Published

2012

16. Chronic caloric restriction attenuates a loss of sulfatide content in PGC-1α-/- mouse cortex: a potential lipidomic role of PGC-1α in neurodegeneration.

Author

Kiebish MA, Young DM, Lehman JJ, and Han X

Subjects

Animals, Apolipoproteins E metabolism, Cerebroside-Sulfatase metabolism, Enzymes metabolism, Homeostasis genetics, Liver X Receptors, Membrane Transport Proteins metabolism, Mice, Mice, Mutant Strains, Myelin Proteins metabolism, Myelin and Lymphocyte-Associated Proteolipid Proteins, Neurodegenerative Diseases metabolism, Orphan Nuclear Receptors metabolism, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, Proteolipids metabolism, Retinoid X Receptors metabolism, Sulfotransferases metabolism, Transcription Factors, Caloric Restriction, Cerebral Cortex metabolism, Sulfoglycosphingolipids metabolism, Trans-Activators genetics, Trans-Activators physiology

Abstract

Peroxisome proliferator-activated receptor gamma coactivator-1α (PGC-1α), a key regulator of energy metabolism and lipid homeostasis in multiple highly oxidative tissues, has been implicated in the metabolic derangements of diabetes and obesity. However, relatively less is known regarding its role in neurological functions. Using shotgun lipidomics, we investigated the lipidome of mouse cerebral cortex with generalized deficiency of PGC-1α (PGC-1α(-/-)) versus wild-type (WT) mice under standard diet and chronically calorically restricted conditions. Specific deficiency in sulfatide, a myelin-specific lipid class critically involved in maintaining neurological function, was uncovered in the cortex of PGC-1α(-/-) mice compared with WT mice at all ages examined. Chronic caloric restriction (CR) for 22 months essentially restored the sulfatide reduction in PGC-1α(-/-) mice compared with WT, but sulfatide reduction was not restored in PGC-1α(-/-) with CR for a short term (i.e., 3 months). Mechanistic studies uncovered and differentiated the biochemical mechanisms underpinning the two conditions of altered sulfatide homeostasis. The former is modulated through PGC-1α-MAL pathway, whereas the latter is under the control of LXR/RXR-apoE metabolism pathway. These results suggest a novel mechanistic role of PGC-1α in sulfatide homeostasis, provide new insights into the importance of PGC-1α in neurological functions, and indicate a potential therapeutic approach for treatment of deficient PGC-1α-induced alterations in sulfatide homeostasis.

Published

2012

17. Diabetes-induced myelin abnormalities are associated with an altered lipid pattern: protective effects of LXR activation.

Author

Cermenati G, Abbiati F, Cermenati S, Brioschi E, Volonterio A, Cavaletti G, Saez E, De Fabiani E, Crestani M, Garcia-Segura LM, Melcangi RC, Caruso D, and Mitro N

Subjects

Animals, Cholesterol metabolism, Diabetes Mellitus, Experimental genetics, Gene Expression Regulation, Lipids chemistry, Liver X Receptors, Male, Myelin P0 Protein metabolism, Myelin Sheath chemistry, Phospholipids metabolism, Protein Kinases genetics, Rats, Rats, Sprague-Dawley, Sciatic Nerve pathology, Stearoyl-CoA Desaturase genetics, Sterol Regulatory Element Binding Protein 1 genetics, Sterol Regulatory Element Binding Protein 1 metabolism, Streptozocin, Diabetes Mellitus, Experimental metabolism, Diabetes Mellitus, Experimental physiopathology, Myelin Sheath metabolism, Orphan Nuclear Receptors metabolism

Abstract

Diabetic peripheral neuropathy (DPN) is characterized by myelin abnormalities; however, the molecular mechanisms underlying such deficits remain obscure. To uncover the effects of diabetes on myelin alterations, we have analyzed myelin composition. In a streptozotocin-treated rat model of diabetic neuropathy, analysis of sciatic nerve myelin lipids revealed that diabetes alters myelin's phospholipid, FA, and cholesterol content in a pattern that can modify membrane fluidity. Reduced expression of relevant genes in the FA biosynthetic pathway and decreased levels of the transcriptionally active form of the lipogenic factor sterol-regulatory element binding factor-1c (SREBF-1c) were found in diabetic sciatic nerve. Expression of myelin's major protein, myelin protein zero (P0), was also suppressed by diabetes. In addition, we confirmed that diabetes induces sciatic nerve myelin abnormalities, primarily infoldings that have previously been associated with altered membrane fluidity. In a diabetic setting, synthetic activator of the nuclear receptor liver X receptor (LXR) increased SREBF-1c function and restored myelin lipid species and P0 expression levels to normal. These LXR-modulated improvements were associated with restored myelin structure in sciatic nerve and enhanced performance in functional tests such as thermal nociceptive threshold and nerve conduction velocity. These findings demonstrate an important role for the LXR-SREBF-1c axis in protection from diabetes-induced myelin abnormalities.

Published

2012

18. Constitutive activation of LXR in macrophages regulates metabolic and inflammatory gene expression: identification of ARL7 as a direct target.

Author

Hong C, Walczak R, Dhamko H, Bradley MN, Marathe C, Boyadjian R, Salazar JV, and Tontonoz P

Subjects

Adipose Tissue metabolism, Animals, Cell Line, Cholesterol metabolism, Humans, Inflammation genetics, Ligands, Lipid Metabolism genetics, Liver X Receptors, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, Orphan Nuclear Receptors genetics, Promoter Regions, Genetic genetics, Signal Transduction genetics, ADP-Ribosylation Factors genetics, Gene Expression Regulation, Macrophages metabolism, Orphan Nuclear Receptors metabolism

Abstract

Ligand activation of liver X receptors (LXRs) has been shown to impact both lipid metabolism and inflammation. One complicating factor in studies utilizing synthetic LXR agonists is the potential for pharmacologic and receptor-independent effects. Here, we describe an LXR gain-of-function system that does not depend on the addition of exogenous ligand. We generated transgenic mice expressing a constitutively active VP16-LXRα protein from the aP2 promoter. These mice exhibit increased LXR signaling selectively in adipose and macrophages. Analysis of gene expression in primary macrophages derived from two independent VP16-LXRα transgenic lines confirmed the ability of LXR to drive expression of genes involved in cholesterol efflux and fatty acid synthesis. Moreover, VP16-LXRα expression also suppressed the induction of inflammatory genes by lipopolysaccharide to a comparable degree as synthetic agonist. We further utilized VP16-LXRα-expressing macrophages to identify and validate new targets for LXRs, including the gene encoding ADP-ribosylation factor-like 7 (ARL7). ARL7 has previously been shown to transport cholesterol to the membrane for ABCA1-associated removal and thus may be integral to the LXR-dependent efflux pathway. We show that the ARL7 promoter contains a functional LXRE and can be transactivated by LXRs in a sequence-specific manner, indicating that ARL7 is a direct target of LXR. These findings provide further support for an important role of LXRs in the coordinated regulation of lipid metabolic and inflammatory gene programs in macrophages.

Published

2011

19. Inhibitory effect of LXR activation on cell proliferation and cell cycle progression through lipogenic activity.

Author

Kim KH, Lee GY, Kim JI, Ham M, Won Lee J, and Kim JB

Subjects

Dose-Response Relationship, Drug, Fatty Acids biosynthesis, Fatty Acids metabolism, Humans, Ligands, Liver X Receptors, Tumor Cells, Cultured, Benzoates pharmacology, Benzylamines pharmacology, Cell Cycle drug effects, Cell Proliferation drug effects, Hydrocarbons, Fluorinated pharmacology, Lipogenesis drug effects, Orphan Nuclear Receptors agonists, Orphan Nuclear Receptors metabolism, Sulfonamides pharmacology

Abstract

Liver X receptor (LXR), a sterol-activated nuclear hormone receptor, has been implicated in cholesterol and fatty acid homeostasis via regulation of reverse cholesterol transport and de novo fatty acid synthesis. LXR is also involved in immune responses, including anti-inflammatory action and T cell proliferation. In this study, we demonstrated that activated LXR suppresses cell cycle progression and proliferation in certain cell types. Stimulation of LXR with synthetic ligand T0901317 or GW3965 inhibited cell growth rate and arrested the cell cycle at the G1/S boundary in several cells, such as RWPE1, THP1, SNU16, LNCaP, and HepG2. However, LXR ligands did not exhibit antiproliferative activity in PC3, HEK293, or HeLa cells. Interestingly, activated LXR-mediated cell cycle arrest is closely correlated with the lipogenic gene expression and triacylglyceride accumulation. In accordance with these findings, suppression of FAS via small-interference RNA (siRNA) partially alleviated the antiproliferative effect of LXR activation in RWPE1 cells. Together, these data suggest that LXR activation with its ligands inhibits cell proliferation and induces G1/S arrest through elevated lipogenic activity, thus proposing a novel effect of activated LXR on cell cycle regulation.

Published

2010

20. Expression and regulation of GPAT isoforms in cultured human keratinocytes and rodent epidermis.

Author

Lu B, Jiang YJ, Kim P, Moser A, Elias PM, Grunfeld C, and Feingold KR

Subjects

Animals, Cell Differentiation drug effects, Cells, Cultured, Epidermis drug effects, Epidermis growth & development, Female, Gene Expression Regulation, Developmental drug effects, Humans, Isoenzymes genetics, Isoenzymes metabolism, Keratinocytes cytology, Keratinocytes drug effects, Liver X Receptors, Mice, Orphan Nuclear Receptors metabolism, Peroxisome Proliferator-Activated Receptors metabolism, Rats, Thiazolidinediones pharmacology, Transcriptional Activation drug effects, Epidermis metabolism, Gene Expression Regulation, Enzymologic drug effects, Glycerol-3-Phosphate O-Acyltransferase genetics, Glycerol-3-Phosphate O-Acyltransferase metabolism, Keratinocytes metabolism

Abstract

Phospholipids are required for epidermal lamellar body formation. Glycerol 3-phosphate acyltransferases (GPATs) catalyze the initial step in the biosynthesis of glycerolipids. Little is known about the expression and regulation of GPATs in epidermis/keratinocytes. Here, we demonstrate that GPAT 1, 3, and 4 are expressed in epidermis/keratinocytes, whereas GPAT2 is not detected. In mouse epidermis, GPAT 3 and 4 are mainly localized to the upper layers whereas GPAT1 is found in both the upper and lower layers. GPAT1 and 3 mRNA increase during fetal rat epidermal development. No change in GPAT expression was observed in adult mice following acute permeability barrier disruption. Calcium-induced human keratinocyte differentiation increased GPAT3 mRNA whereas both GPAT1 and 4 mRNA levels decreased. In parallel, total GPAT activity increased 2-fold in differentiated keratinocytes attributable to an increase in N-ethylmaleimide (NEM) sensitive GPAT activity localized to microsomes with little change in NEM resistant activity, consistent with an increase in GPAT3. Furthermore, PPARγ or PPARδ activators increased GPAT3 mRNA, microsomal GPAT activity, and glycerol lipid synthesis without affecting the expression of GPAT1 or 4. Finally, both PPARγ and PPARδ activators increased GPAT3 mRNA via increasing its transcription. Thus, multiple isoforms of GPAT are expressed and differentially regulated in epidermis/keratinocytes.

Published

2010

21. Regulation of ABCG1 expression in human keratinocytes and murine epidermis.

Author

Jiang YJ, Lu B, Tarling EJ, Kim P, Man MQ, Crumrine D, Edwards PA, Elias PM, and Feingold KR

Subjects

ATP Binding Cassette Transporter, Subfamily G, Member 1, ATP-Binding Cassette Transporters metabolism, Animals, Cell Differentiation drug effects, Dose-Response Relationship, Drug, Epidermal Cells, Epidermis drug effects, Female, Gene Knockout Techniques, Humans, Hydrocarbons, Fluorinated pharmacology, Keratinocytes cytology, Keratinocytes drug effects, Lipoproteins metabolism, Liver X Receptors, Mice, Orphan Nuclear Receptors metabolism, PPAR delta metabolism, Permeability drug effects, RNA, Messenger genetics, RNA, Messenger metabolism, Sterols pharmacology, Sulfonamides pharmacology, Up-Regulation drug effects, ATP-Binding Cassette Transporters genetics, Epidermis metabolism, Gene Expression Regulation drug effects, Keratinocytes metabolism, Lipoproteins genetics

Abstract

ABCG1, a member of the ATP binding cassette superfamily, facilitates the efflux of cholesterol from cells to HDL. In this study, we demonstrate that ABCG1 is expressed in cultured human keratinocytes and murine epidermis, and induced during keratinocyte differentiation, with increased levels in the outer epidermis. ABCG1 is regulated by liver X receptor (LXR) and peroxisome proliferator-activated receptor-δ (PPAR-δ) activators, cellular sterol levels, and acute barrier disruption. Both LXR and PPAR-δ activators markedly stimulate ABCG1 expression in a dose- and time-dependent fashion. PPAR-γ activators also increase ABCG1 expression, but to a lesser degree. In contrast, activators of PPAR-α, retinoic acid receptor, retinoid X receptor, and vitamin D receptor do not alter ABCG1 expression. In response to increased intracellular sterol levels, ABCG1 expression increases, whereas inhibition of cholesterol biosynthesis decreases ABCG1 expression. In vivo, ABCG1 is stimulated 3-6 h after acute barrier disruption by either tape stripping or acetone treatment, an increase that can be inhibited by occlusion, suggesting a potential role of ABCG1 in permeability barrier homeostasis. Although Abcg1-null mice display normal epidermal permeability barrier function and gross morphology, abnormal lamellar body (LB) contents and secretion leading to impaired lamellar bilayer formation could be demonstrated by electron microscopy, indicating a potential role of ABCG1 in normal LB formation and secretion.

Published

2010

22. Reduced VLDL clearance in Apoe(-/-)Npc1(-/-) mice is associated with increased Pcsk9 and Idol expression and decreased hepatic LDL-receptor levels.

Author

Ishibashi M, Masson D, Westerterp M, Wang N, Sayers S, Li R, Welch CL, and Tall AR

Subjects

Animals, Cells, Cultured, Cholesterol blood, Intracellular Signaling Peptides and Proteins, Lamin Type A metabolism, Liver X Receptors, Macrophages, Peritoneal cytology, Macrophages, Peritoneal metabolism, Mice, Mice, Knockout, Niemann-Pick C1 Protein, Orphan Nuclear Receptors genetics, Orphan Nuclear Receptors metabolism, Proprotein Convertase 9, Proprotein Convertases, Serine Endopeptidases genetics, Sterol Regulatory Element Binding Protein 1 genetics, Sterol Regulatory Element Binding Protein 1 metabolism, Sterol Regulatory Element Binding Protein 2 genetics, Sterol Regulatory Element Binding Protein 2 metabolism, Triglycerides blood, Ubiquitin-Protein Ligases genetics, Apolipoproteins E genetics, Apolipoproteins E metabolism, Cholesterol, VLDL metabolism, Liver physiology, Proteins genetics, Proteins metabolism, Receptors, LDL metabolism, Serine Endopeptidases metabolism, Ubiquitin-Protein Ligases metabolism

Abstract

Niemann-Pick type C1 (NPC1) promotes the transport of LDL receptor (LDL-R)-derived cholesterol from late endosomes/lysosomes to other cellular compartments. NPC1-deficient cells showed impaired regulation of liver_X receptor (LXR) and sterol regulatory element-binding protein (SREBP) target genes. We observed that Apoe(-/-)Npc1(-/-) mice displayed a marked increase in total plasma cholesterol mainly due to increased VLDL, reflecting decreased clearance. Although nuclear SREBP-2 and Ldlr mRNA levels were increased in Apoe(-/-)Npc1(-/-) liver, LDL-R protein levels were decreased in association with marked induction of proprotein convertase subtilisin/kexin type 9 (Pcsk9) and inducible degrader of the LDL-R (Idol), both known to promote proteolytic degradation of LDL-R. While Pcsk9 is known to be an SREBP-2 target, marked upregulation of IDOL in Apoe(-/-)Npc1(-/-) liver was unexpected. However, several other LXR target genes also increased in Apoe(-/-)Npc1(-/-) liver, suggesting increased synthesis of endogenous LXR ligands secondary to activation of sterol biosynthesis. In conclusion, we demonstrate that NPC1 deficiency has a major impact on VLDL metabolism in Apoe(-/-) mice through modulation of hepatic LDL-R protein levels. In contrast to modest induction of hepatic IDOL with synthetic LXR ligands, a striking upregulation of IDOL in Apoe(-/-)Npc1(-/-) mice could indicate a role of endogenous LXR ligands in regulation of hepatic IDOL.

Published

2010

23. Metabolic switching of human myotubes is improved by n-3 fatty acids.

Author

Hessvik NP, Bakke SS, Fredriksson K, Boekschoten MV, Fjørkenstad A, Koster G, Hesselink MK, Kersten S, Kase ET, Rustan AC, and Thoresen GH

Subjects

Biological Transport drug effects, Energy Metabolism drug effects, Fatty Acids, Omega-3 metabolism, Female, Gene Expression Profiling, Glucose metabolism, Humans, Hydrocarbons, Fluorinated pharmacology, Insulin pharmacology, Liver X Receptors, Male, Middle Aged, Muscle Fibers, Skeletal cytology, Oleic Acid metabolism, Orphan Nuclear Receptors agonists, Orphan Nuclear Receptors metabolism, Oxidation-Reduction drug effects, Signal Transduction drug effects, Sulfonamides pharmacology, Fatty Acids, Omega-3 pharmacology, Muscle Fibers, Skeletal drug effects, Muscle Fibers, Skeletal metabolism

Abstract

The aim of the present study was to examine whether pretreatment with different fatty acids, as well as the liver X receptor (LXR) agonist T0901317, could modify metabolic switching of human myotubes. The n-3 FA eicosapentaenoic acid (EPA) increased suppressibility, the ability of glucose to suppress FA oxidation. Substrate-regulated flexibility, the ability to increase FA oxidation when changing from a high glucose, low fatty acid condition ("fed") to a high fatty acid, low glucose ("fasted") condition, was increased by EPA and other n-3 FAs. Adaptability, the capacity to increase FA oxidation with increasing FA availability, was enhanced after pretreatment with EPA, linoleic acid (LA), and palmitic acid (PA). T0901317 counteracted the effect of EPA on suppressibility and adaptability, but it did not affect these parameters alone. EPA per se accumulated less, however, EPA, LA, oleic acid, and T0901317 treatment increased the number of lipid droplets (LD) in myotubes. LD volume and intensity, as well as mitochondrial mass, were independent of FA pretreatment. Microarray analysis showed that EPA regulated more genes than the other FAs and that specific pathways involved in carbohydrate metabolism were induced only by EPA. The present study suggests a favorable effect of n-3 FAs on skeletal muscle metabolic switching and glucose utilization.

Published

2010

24. Activation of LXR increases acyl-CoA synthetase activity through direct regulation of ACSL3 in human placental trophoblast cells.

Author

Weedon-Fekjaer MS, Dalen KT, Solaas K, Staff AC, Duttaroy AK, and Nebb HI

Subjects

Animals, Base Sequence, Cell Line, Coenzyme A Ligases genetics, Fatty Acids metabolism, Female, Humans, Liver X Receptors, Microarray Analysis, Molecular Sequence Data, Orphan Nuclear Receptors agonists, Orphan Nuclear Receptors genetics, Placenta cytology, Pregnancy, Sequence Alignment, Trophoblasts cytology, Coenzyme A Ligases metabolism, Orphan Nuclear Receptors metabolism, Placenta metabolism, Trophoblasts metabolism

Abstract

Placental fatty acid transport and metabolism are important for proper growth and development of the feto-placental unit. The nuclear receptors, liver X receptors alpha and beta (LXRalpha and LXRbeta), are key regulators of lipid metabolism in many tissues, but little is known about their role in fatty acid transport and metabolism in placenta. The current study investigates the LXR-mediated regulation of long-chain acyl-CoA synthetase 3 (ACSL3) and its functions in human placental trophoblast cells. We demonstrate that activation of LXR increases ACSL3 expression, acyl-CoA synthetase activity, and fatty acid uptake in human tropholast cells. Silencing of ACSL3 in these cells attenuates the LXR-mediated increase in acyl-CoA synthetase activity. Furthermore, we show that ACSL3 is directly regulated by LXR through a conserved LXR responsive element in the ACSL3 promoter. Our results suggest that LXR plays a regulatory role in fatty acid metabolism by direct regulation of ACSL3 in human placental trophoblast cells.

Published

2010

25. Targeted PPAR{gamma} deficiency in alveolar macrophages disrupts surfactant catabolism.

Author

Baker AD, Malur A, Barna BP, Ghosh S, Kavuru MS, Malur AG, and Thomassen MJ

Subjects

ATP Binding Cassette Transporter, Subfamily G, Member 1, ATP-Binding Cassette Transporters metabolism, Animals, Cholesterol metabolism, Gene Knockout Techniques, Lipoproteins metabolism, Lipoproteins, HDL metabolism, Liver X Receptors, Lung metabolism, Mice, Organ Specificity, Orphan Nuclear Receptors metabolism, Macrophages, Alveolar metabolism, PPAR gamma deficiency, PPAR gamma genetics, Surface-Active Agents metabolism

Abstract

Surfactant accumulates in alveolar macrophages of granulocyte-macrophage colony-stimulating factor (GM-CSF) knockout (KO) mice and pulmonary alveolar proteinosis (PAP) patients with a functional loss of GM-CSF resulting from neutralizing anti-GM-CSF antibody. Alveolar macrophages from PAP patients and GM-CSF KO mice are de-ficient in peroxisome proliferator-activated receptor-gamma (PPARgamma) and ATP-binding cassette (ABC) lipid transporter ABCG1. Previous studies have demonstrated that GM-CSF induces PPARgamma. We therefore hypothesized that PPARgamma promotes surfactant catabolism through regulation of ABCG1. To address this hypothesis, macrophage-specific PPARgamma (MacPPARgamma) knockout mice were utilized. MacPPARgamma KO mice develop foamy, lipid-engorged Oil Red O positive alveolar macrophages. Lipid analyses revealed significant increases in the cholesterol and phospholipid contents of MacPPARgamma KO alveolar macrophages and extracellular bronchoalveolar lavage (BAL)-derived fluids. MacPPARgamma KO alveolar macrophages showed decreased expression of ABCG1 and a deficiency in ABCG1-mediated cholesterol efflux to HDL. Lipid metabolism may also be regulated by liver X receptor (LXR)-ABCA1 pathways. Interestingly, ABCA1 and LXRbeta expression were elevated, indicating that this pathway is not sufficient to prevent surfactant accumulation in alveolar macrophages. These results suggest that PPARgamma mediates a critical role in surfactant homeostasis through the regulation of ABCG1.

Published

2010

26. TNF-alpha decreases ABCA1 expression and attenuates HDL cholesterol efflux in the human intestinal cell line Caco-2.

Author

Field FJ, Watt K, and Mathur SN

Subjects

ATP Binding Cassette Transporter 1, Animals, Caco-2 Cells, Humans, Intestinal Mucosa metabolism, Liver X Receptors, NF-kappa B metabolism, Orphan Nuclear Receptors metabolism, Signal Transduction drug effects, ATP-Binding Cassette Transporters genetics, Cholesterol, HDL metabolism, Gene Expression Regulation drug effects, Intestines cytology, Tumor Necrosis Factor-alpha pharmacology

Abstract

HDL cholesterol levels are decreased in Crohn's disease, a tumor necrosis factor-alpha (TNF-alpha)-driven chronic inflammatory condition involving the gastrointestinal tract. ATP-binding cassette transporter A1 (ABCA1), one of several liver X receptor (LXR) target genes, is a cell surface transporter that mediates the rate-controlling step in HDL synthesis. The regulation of ABCA1 and HDL cholesterol efflux by TNF-alpha was investigated in the human intestinal cell line Caco-2. In response to cholesterol micelles or T0901317, an LXR nonsterol agonist, TNF-alpha decreased the basolateral efflux of cholesterol to apolipoprotein A1 (apoA1). TNF-alpha, by attenuating ABCA1 promoter activity, markedly decreased ABCA1 gene expression without attenuating the expression of LXR-alpha, LXR-beta, and most other LXR target genes, such as ABCG1, FAS, ABCG8, scavenger receptor-B1 (SR-B1), and apoC1. TNF-alpha also decreased ABCA1 mass by markedly enhancing the rate of ABCA1 degradation and modestly inhibiting its rate of synthesis. Inhibitors of the nuclear factor-kappaB (NF-kappaB) pathway, which is activated by TNF-alpha, partially reverse the effect of TNF-alpha on ABCA1 protein expression. The results suggest that TNF-alpha, the major cytokine implicated in the inflammation of Crohn's disease, decreases HDL cholesterol levels by attenuating the expression of intestinal ABCA1 and cholesterol efflux to apoA1.

Published

2010

27. Effects of FoxO4 overexpression on cholesterol biosynthesis, triacylglycerol accumulation, and glucose uptake.

Author

Zhu J, Mounzih K, Chehab EF, Mitro N, Saez E, and Chehab FF

Subjects

Biological Transport genetics, Cell Cycle Proteins, Cell Line, Cytochrome P-450 Enzyme Inhibitors, Enzyme Inhibitors pharmacology, Fatty Acids biosynthesis, Fibroblasts drug effects, Fibroblasts metabolism, Forkhead Transcription Factors, Hepatocytes drug effects, Hepatocytes metabolism, Humans, Lanosterol analogs & derivatives, Lanosterol metabolism, Lanosterol pharmacology, Ligands, Liver X Receptors, Orphan Nuclear Receptors chemistry, Orphan Nuclear Receptors metabolism, Protein Structure, Tertiary, Sterol 14-Demethylase, Cholesterol biosynthesis, Gene Expression Regulation, Glucose metabolism, Transcription Factors genetics, Triglycerides metabolism

Abstract

The Forkhead transcription factors FoxO1, FoxO3a, and FoxO4 play a prominent role in regulating cell survival and cell cycle. Whereas FOXO1 was shown to mediate insulin sensitivity and adipocyte differentiation, the role of the transcription factor FoxO4 in metabolism remains ill defined. To uncover the effects of FoxO4, we generated a cellular model of stable FoxO4 overexpression and subjected it to microarray-based gene expression profiling. While pathway analysis revealed a disruption of cholesterol biosynthesis gene expression, biochemical studies revealed an inhibition of cholesterol biosynthesis, which was coupled with decreased mRNA levels of lanosterol 14alpha demethylase (CYP51). FoxO4-mediated repression of CYP51 led to the accumulation of 24,25 dihydrolano-sterol (DHL), which independently and unlike lanosterol inhibited cholesterol biosynthesis. Furthermore, FoxO4-overexpressing cells accumulated lipid droplets and triacylglycerols and had an increase in basal glucose uptake. Recapitulation of these effects was obtained following treatment with CYP51 inhibitors, which also induce DHL buildup. Moreover, DHL but not lanosterol strongly stimulated liver X receptor alpha (LXRalpha) activity, suggesting that DHL and LXRalpha mediate the downstream effects initiated by FoxO4. Together, these studies suggest that FoxO4 acts on CYP51 to regulate the late steps of cholesterol biosynthesis.

Published

2010

28. Non-redundant roles for LXRalpha and LXRbeta in atherosclerosis susceptibility in low density lipoprotein receptor knockout mice.

Author

Bischoff ED, Daige CL, Petrowski M, Dedman H, Pattison J, Juliano J, Li AC, and Schulman IG

Subjects

Animals, Bone Marrow Cells metabolism, Disease Susceptibility metabolism, Gene Expression Regulation, Liver X Receptors, Macrophages metabolism, Male, Mice, Mice, Knockout, Orphan Nuclear Receptors agonists, Orphan Nuclear Receptors deficiency, Orphan Nuclear Receptors genetics, Atherosclerosis metabolism, Gene Knockout Techniques, Orphan Nuclear Receptors metabolism, Receptors, LDL deficiency, Receptors, LDL genetics

Abstract

The liver X receptors LXRalpha and LXRbeta play critical roles in maintaining lipid homeostasis by functioning as transcription factors that regulate genetic networks controlling the transport, catabolism, and excretion of cholesterol. The studies described in this report examine the individual anti-atherogenic activity of LXRalpha and LXRbeta and determine the ability of each subtype to mediate the biological response to LXR agonists. Utilizing individual knockouts of LXRalpha and LXRbeta in the Ldlr(-/-) background, we demonstrate that LXRalpha has a dominant role in limiting atherosclerosis in vivo. Functional studies in macrophages indicate that LXRalpha is required for a robust response to LXR ligands, whereas LXRbeta functions more strongly as a repressor. Furthermore, selective knockout of LXRalpha in hematopoietic cells and rescue experiments indicate that the anti-atherogenic activity of this LXR subtype is not restricted to macrophages. These studies indicate that LXRalpha plays a selective role in limiting atherosclerosis in response to hyperlipidemia.

Published

2010

29. LXR ligand lowers LDL cholesterol in primates, is lipid neutral in hamster, and reduces atherosclerosis in mouse.

Author

Quinet EM, Basso MD, Halpern AR, Yates DW, Steffan RJ, Clerin V, Resmini C, Keith JC, Berrodin TJ, Feingold I, Zhong W, Hartman HB, Evans MJ, Gardell SJ, DiBlasio-Smith E, Mounts WM, LaVallie ER, Wrobel J, Nambi P, and Vlasuk GP

Subjects

Animals, Atherosclerosis metabolism, Caco-2 Cells, Cricetinae, Disease Models, Animal, Humans, Indazoles blood, Indazoles chemistry, Ligands, Liver enzymology, Liver metabolism, Liver X Receptors, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Orphan Nuclear Receptors metabolism, Atherosclerosis drug therapy, Cholesterol, LDL drug effects, Cholesterol, LDL metabolism, Indazoles pharmacology, Lipid Metabolism drug effects, Macaca fascicularis metabolism, Orphan Nuclear Receptors agonists

Abstract

Liver X receptors (LXRs) are ligand-activated transcription factors that coordinate regulation of gene expression involved in several cellular functions but most notably cholesterol homeostasis encompassing cholesterol transport, catabolism, and absorption. WAY-252623 (LXR-623) is a highly selective and orally bioavailable synthetic modulator of LXR, which demonstrated efficacy for reducing lesion progression in the murine LDLR(-/-) atherosclerosis model with no associated increase in hepatic lipogenesis either in this model or Syrian hamsters. In nonhuman primates with normal lipid levels, WAY-252623 significantly reduced total (50-55%) and LDL-cholesterol (LDLc) (70-77%) in a time- and dose-dependent manner as well as increased expression of the target genes ABCA1/G1 in peripheral blood cells. Statistically significant decreases in LDLc were noted as early as day 7, reached a maximum by day 28, and exceeded reductions observed for simvastatin alone (20 mg/kg). Transient increases in circulating triglycerides and liver enzymes reverted to baseline levels over the course of the study. Complementary microarray analysis of duodenum and liver gene expression revealed differential activation of LXR target genes and suggested no direct activation of hepatic lipogenesis. WAY-252623 displays a unique and favorable pharmacological profile suggesting synthetic LXR ligands with these characteristics may be suitable for evaluation in patients with atherosclerotic dyslipidemia.

Published

2009

30. LXR and ABCA1 control cholesterol homeostasis in the proximal mouse epididymis in a cell-specific manner.

Author

Ouvrier A, Cadet R, Vernet P, Laillet B, Chardigny JM, Lobaccaro JM, Drevet JR, and Saez F

Subjects

ATP Binding Cassette Transporter 1, Animals, Apoptosis, Biological Transport, Cholesterol biosynthesis, Cholesterol chemistry, Cholesterol Esters metabolism, Epididymis physiopathology, Epithelial Cells pathology, Fatty Acids metabolism, Fertility, Liver X Receptors, Male, Mice, Organ Specificity, Sperm Maturation, ATP-Binding Cassette Transporters metabolism, Cholesterol metabolism, Epididymis metabolism, Epididymis pathology, Homeostasis, Orphan Nuclear Receptors metabolism

Abstract

Mammalian spermatozoa undergo important plasma membrane maturation steps during epididymal transit. Among these, changes in lipids and cholesterol are of particular interest as they are necessary for fertilization. However, molecular mechanisms regulating these transformations inside the epididymis are still poorly understood. Liver X receptors (LXRs), the nuclear receptors for oxysterols, are of major importance in intracellular cholesterol homeostasis, and LXR(-/-)-deficient male mice have already been shown to have reduced fertility at an age of 5 months and complete sterility for 9-month-old animals. This sterility phenotype is associated with testes and caput epididymides epithelial defects. The research presented here was aimed at investigating how LXRs act in the male caput epididymidis by analyzing key actors in cholesterol homeostasis. We show that accumulation of cholesteryl esters in LXR(-/-) male mice is associated with a specific loss of ABCA1 and an increase in apoptosis of apical cells of the proximal caput epididymidis. ATP-binding cassette G1 (ABCG1) and scavenger receptor B1 (SR-B1), two other cholesterol transporters, show little if any modifications. Our study also revealed that SR-B1 appears to have a peculiar expression pattern along the epididymal duct. These results should help in understanding the functional roles of LXR in cholesterol trafficking processes in caput epididymidis.

Published

2009

31. Reduced insulin-mediated inhibition of VLDL secretion upon pharmacological activation of the liver X receptor in mice.

Author

Grefhorst A and Parks EJ

Subjects

Animals, Blood Glucose metabolism, Gene Expression, Glucose Clamp Technique, Hydrocarbons, Fluorinated metabolism, Hyperinsulinism metabolism, Liver metabolism, Liver physiology, Liver X Receptors, Male, Mice, Mice, Inbred C57BL, Particle Size, Sterol Regulatory Element Binding Protein 1 metabolism, Sulfonamides metabolism, Lipoproteins, VLDL metabolism, Orphan Nuclear Receptors metabolism, Triglycerides metabolism

Abstract

The nuclear liver X receptor (LXR) regulates multiple aspects of cholesterol, triacylglycerol (TG), and carbohydrate metabolism. Activation of LXR induces the expression of genes encoding enzymes involved in de novo lipogenesis (DNL) resulting in hepatic steatosis in mice. Pharmacological LXR activation has also been reported to improve insulin sensitivity and glucose homeostasis in diabetic rodents. The effects of pharmacological LXR ligands on insulin's action on hepatic lipid metabolism are not known. We evaluated secretion of VLDL during a hyperinsulinemic euglycemic clamp in mice treated with the LXR-ligand T0901317. In untreated mice, hyperinsulinemia reduced the availability of plasma NEFA for VLDL-TG synthesis, increased the contribution of DNL to VLDL-TG, reduced VLDL particle size, and suppressed overall VLDL-TG production rate by approximately 50%. Upon T0901317 treatment, hyperinsulinemia failed to reduce VLDL particle size or suppress VLDL-TG production rate, but the contribution of DNL to VLDL-TG was increased. In conclusion, the effects of LXR activation by T0901317 on lipid metabolism can override the normal control of insulin to suppress VLDL particle secretion.

Published

2009