Your search keyword '"Koonen, Debby P.Y."' showing total 6 results

1. Soluble CD36−− a marker of the (pathophysiological) role of CD36 in the metabolic syndrome??

Author

Koonen, Debby P.Y., Jensen, Majken K., and Handberg, Aase

Subjects

*PATHOLOGICAL physiology, *METABOLIC syndrome, *TYPE 2 diabetes, *LOW density lipoproteins, *INSULIN resistance, *ATHEROSCLEROSIS, *HUMAN genetic variation, *FATTY degeneration, *INFLAMMATION

Abstract

CD36 is a class B scavenger receptor observed in many cell types and tissues throughout the body. Recent literature has implicated CD36 in the pathogenesis of metabolic dysregulation such as found in obesity, insulin resistance, and atherosclerosis. Genetic variation at the CD36 loci have been associated with obesity and lipid components of the metabolic syndrome, with risk of heart disease and type 2 diabetes. Recently, non-cell bound CD36 was identified in human plasma and was termed soluble CD36 (sCD36). In this review we will describe the functions of CD36 in tissues and address the role of sCD36 in the context of the metabolic syndrome. We will also highlight recent findings from human genetic studies looking at the CD36 locus in relation to metabolic profile in the general population. Finally, we present a model in which insulin resistance, oxLDL, low-grade inflammation and liver steatosis may contribute to elevated levels of sCD36. [ABSTRACT FROM AUTHOR]

Published

2011

2. Enhanced sarcolemmal FAT/CD36 content and triacylglycerol storage in cardiac myocytes from obese zucker rats.

Author

Coort, Susan L. M., Koonen, Debby P.Y., Willems, Jodil, Glatz, Jan F. C., Coumans, Will A., Hasselbaink, Danny M., van der Vusse, Ger J., Chabowski, Adrian, Bonen, Arend, and Luiken, Joost J. F. P.

Subjects

*SARCOLEMMA, *HEART cells, *LABORATORY rats, *FATTY acids, *OBESITY, *INSULIN, *CARDIOMYOPATHIES

Abstract

In obesity, the development of cardiomyopathy is associated with the accumulation of myocardial triacylglycerols (TAGs), possibly stemming from elevation of myocardial long-chain fatty acid (LCFA) uptake. Because LCFA uptake is regulated by insulin and contractions, we examined in cardiac myocytes from lean and obese Zucker rats the effects of insulin and the contraction-mimetic agent oligomycin on the initial rate of LCFA uptake, subcellular distribution of FAT/CD36, and LCFA metabolism. In cardiac myocytes from obese Zucker rats, under basal conditions, FAT/CD36 was relocated to the sarcolemma at the expense of intracellular stores. In addition, the LCFA uptake rate, LCFA esterification rate into TAGs, and the intracellular unesterified LCFA concentration each were significantly increased. All these metabolic processes were normalized by the FAT/CD36 inhibitor sulfo-N-succinimidyloleate, indicating its antidiabetic potential. In cardiac myocytes isolated from lean rats, in vitro administration of insulin induced the translocation of FAT/CD36 to the sarcolemma and stimulated initial rates of LCFA uptake and TAG esterification. In contrast, in myocytes from obese rats, insulin failed to alter the subcellular localization of FAT/CD36 and the rates of LCFA uptake and TAG esterification. In cardiac myocytes from lean and obese animals, oligomycin stimulated the initial rates of LCFA uptake and oxidation, although oligomycin only induced the translocation of FAT/CD36 to the sarcolemma in lean rats. The present results indicate that in cardiac myocytes from obese Zucker rats, a permanent relocation of FAT/CD36 to the sarcolemma is responsible for myocardial TAG accumulation. Furthermore, in vitro these cardiac myocytes, although sensitive to contraction-like stimulation, were completely insensitive to insulin, as the basal conditions in hyperinsulinemic, obese animals resemble the insulin-stimulated condition in lean littermates. [ABSTRACT FROM AUTHOR]

Published

2004

3. Nonalcoholic fatty liver disease: A main driver of insulin resistance or a dangerous liaison?

Author

Gruben, Nanda, Shiri-Sverdlov, Ronit, Koonen, Debby P.Y., and Hofker, Marten H.

Subjects

*FATTY liver, *INSULIN resistance, *METABOLIC syndrome, *TYPE 2 diabetes, *FATTY degeneration, *TRIGLYCERIDES, *OBESITY

Abstract

Insulin resistance is one of the key components of the metabolic syndrome and it eventually leads to the development of type 2 diabetes, making it one of the biggest medical problems of modern society. Nonalcoholic fatty liver disease (NAFLD) and nonalcoholic steatohepatitis (NASH) are tightly associated with insulin resistance. While it is fairly clear that insulin resistance causes hepatic steatosis, it is not known if NAFLD causes insulin resistance. Hepatic inflammation and lipid accumulation are believed to be the main drivers of hepatic insulin resistance in NAFLD. Here we give an overview of the evidence linking hepatic lipid accumulation to the development of insulin resistance, including the accumulation of triacylglycerol and lipid metabolites, such as diacylglycerol and ceramides. In particular, we discuss the role of obesity in this relation by reviewing the current evidence in terms of the reported changes in body weight and/or adipose tissue mass. We further discuss whether the activation or inhibition of inflammatory pathways, Kupffer cells and other immune cells influences the development of insulin resistance. We show that, in contrast to what is commonly believed, neither hepatic steatosis nor hepatic inflammation is sufficient to cause insulin resistance. Many studies show that obesity cannot be ignored as an underlying factor in this relationship and NAFLD is therefore less likely to be one of the main drivers of insulin resistance. [ABSTRACT FROM AUTHOR]

Published

2014

4. NF-κB p65 serine 467 phosphorylation sensitizes mice to weight gain and TNFα-or diet-induced inflammation.

Author

Riedlinger, Tabea, Schmitz, M. Lienhard, Dommerholt, Marleen B., Kruit, Janine K., Jonker, Johan W., Huijkman, Nicolette, Dekker, Daphne, Koster, Mirjam, Kloosterhuis, Niels, Koonen, Debby P.Y., Hofker, Marten H., van de Sluis, Bart, Wijshake, Tobias, de Bruin, Alain, Baker, Darren, and van Deursen, Jan

Subjects

*PHOSPHORYLATION, *INFLAMMATION, *LABORATORY mice, *METABOLISM, *GENE expression

Abstract

The NF-κB family of transcription factors is essential for an effective immune response, but also controls cell metabolism, proliferation and apoptosis. Its broad relevance and the high connectivity to diverse signaling pathways require a tight control of NF-κB activity. To investigate the control of NF-κB activity by phosphorylation of the NF-κB p65 subunit, we generated a knock-in mouse model in which serine 467 (the mouse homolog of human p65 serine 468) was replaced with a non-phosphorylatable alanine (S467A). This substitution caused reduced p65 protein synthesis and diminished TNFα-induced expression of a selected group of NF-κB-dependent genes. Intriguingly, high-fat fed S467A mice displayed increased locomotor activity and energy expenditure, which coincided with a reduced body weight gain. Although glucose metabolism or insulin sensitivity was not improved, diet-induced liver inflammation was diminished in S467A mice. Altogether, this study demonstrates that phosphorylation of p65 serine 467 augment NF-κB activity and exacerbates various deleterious effects of overnutrition in mice. [ABSTRACT FROM AUTHOR]

Published

2017

5. Vagus nerve contributes to the development of steatohepatitis and obesity in phosphatidylethanolamine N-methyltransferase deficient mice.

Author

Gao, Xia, van der Veen, Jelske N., Zhu, Linfu, Chaba, Todd, Ordoñez, Marta, Lingrell, Susanne, Koonen, Debby P.Y., Dyck, Jason R.B., Gomez-Muñoz, Antonio, Vance, Dennis E., and Jacobs, René L.

Subjects

*VAGUS nerve physiology, *FATTY liver, *ANIMAL models in research, *OBESITY, *PHOSPHATIDYLETHANOLAMINES, *METHYLTRANSFERASES, *LABORATORY mice

Abstract

Background & Aims Phosphatidylethanolamine N -methyltransferase (PEMT), a liver enriched enzyme, is responsible for approximately one third of hepatic phosphatidylcholine biosynthesis. When fed a high-fat diet (HFD), Pemt −/− mice are protected from HF-induced obesity; however, they develop steatohepatitis. The vagus nerve relays signals between liver and brain that regulate peripheral adiposity and pancreas function. Here we explore a possible role of the hepatic branch of the vagus nerve in the development of diet induced obesity and steatohepatitis in Pemt −/− mice. Methods 8-week old Pemt −/− and Pemt +/+ mice were subjected to hepatic vagotomy (HV) or capsaicin treatment, which selectively disrupts afferent nerves, and were compared to sham-operated or vehicle-treatment, respectively. After surgery, mice were fed a HFD for 10 weeks. Results HV abolished the protection against the HFD-induced obesity and glucose intolerance in Pemt −/− mice. HV normalized phospholipid content and prevented steatohepatitis in Pemt −/− mice. Moreover, HV increased the hepatic anti-inflammatory cytokine interleukin-10, reduced chemokine monocyte chemotactic protein-1 and the ER stress marker C/EBP homologous protein. Furthermore, HV normalized the expression of mitochondrial electron transport chain proteins and of proteins involved in fatty acid synthesis, acetyl-CoA carboxylase and fatty acid synthase in Pemt −/− mice. However, disruption of the hepatic afferent vagus nerve by capsaicin failed to reverse either the protection against the HFD-induced obesity or the development of HF-induced steatohepatitis in Pemt −/− mice. Conclusions Neuronal signals via the hepatic vagus nerve contribute to the development of steatohepatitis and protection against obesity in HFD fed Pemt −/− mice. [ABSTRACT FROM AUTHOR]

Published

2015

6. Cholesterol-induced hepatic inflammation does not contribute to the development of insulin resistance in male LDL receptor knockout mice.

Author

Funke, Anouk, Schreurs, Marijke, Aparicio-Vergara, Marcela, Sheedfar, Fareeba, Gruben, Nanda, Kloosterhuis, Niels J., Shiri-Sverdlov, Ronit, Groen, Albert K., van de Sluis, Bart, Hofker, Marten H., and Koonen, Debby P.Y.

Subjects

*CHOLESTEROL, *HEPATITIS, *INSULIN resistance, *LOW density lipoproteins, *LABORATORY mice, *KUPFFER cells, *OBESITY

Abstract

Abstract: Objective: It is generally assumed that hepatic inflammation in obesity is linked to the pathogenesis of insulin resistance. Several recent studies have shed doubt on this view, which questions the causality of this association. This study focuses on Kupffer cell-mediated hepatic inflammation as a possible driver of insulin resistance in the absence and presence of obesity. Methods: We used male mice deficient for the low-density lipoprotein receptor (Ldlr −/−) and susceptible to cholesterol-induced hepatic inflammation. Whole body and hepatic insulin resistance was measured in mice fed 4 diets for 2 and 15 weeks, i.e., chow, high-fat (HF), HF-cholesterol (HFC; 0.2% cholesterol) and HF without cholesterol (HFnC). Biochemical parameters in plasma and liver were measured and inflammation was determined using immunohistochemistry and RT-PCR. Results: At 2 weeks, we did not find significant metabolic effects in either diet group, except for the mice fed a HFC diet which showed pronounced hepatic inflammation (p < 0.05) but normal insulin sensitivity. At 15 weeks, a significant increase in insulin levels, HOMA-IR, and hepatic insulin resistance was observed in mice fed a HFC, HFnC, and HF diet compared to chow-fed mice (p < 0.05). Regardless of the level of hepatic inflammation (HFC > HF, HFnC; p < 0.05) insulin resistance in mice fed HFC was no worse compared to mice on a HFnC and HF diet. Conclusion: These data show that cholesterol-induced hepatic inflammation does not contribute to the development of insulin resistance in male Ldlr −/− mice. This study suggests that Kupffer cell-driven hepatic inflammation is a consequence, not a cause, of metabolic dysfunction in obesity. [Copyright &y& Elsevier]

Published

2014