Your search keyword '"Boot, Rolf G."' showing total 12 results

1. Lyso-glycosphingolipids: presence and consequences.

Author

van Eijk M, Ferraz MJ, Boot RG, and Aerts JMFG

Subjects

Acid Ceramidase metabolism, Animals, Humans, Immunity, Lysosomal Storage Diseases immunology, Enzyme Replacement Therapy methods, Genetic Therapy methods, Glycosphingolipids biosynthesis, Lysosomal Storage Diseases drug therapy, Lysosomal Storage Diseases metabolism, Lysosomes metabolism, Molecular Targeted Therapy methods

Abstract

Lyso-glycosphingolipids are generated in excess in glycosphingolipid storage disorders. In the course of these pathologies glycosylated sphingolipid species accumulate within lysosomes due to flaws in the respective lipid degrading machinery. Deacylation of accumulating glycosphingolipids drives the formation of lyso-glycosphingolipids. In lysosomal storage diseases such as Gaucher Disease, Fabry Disease, Krabbe disease, GM1 -and GM2 gangliosidosis, Niemann Pick type C and Metachromatic leukodystrophy massive intra-lysosomal glycosphingolipid accumulation occurs. The lysosomal enzyme acid ceramidase generates the deacylated lyso-glycosphingolipid species. This review discusses how the various lyso-glycosphingolipids are synthesized, how they may contribute to abnormal immunity in glycosphingolipid storing lysosomal diseases and what therapeutic opportunities exist., (© 2020 The Author(s).)

Published

2020

2. Role of β-glucosidase 2 in aberrant glycosphingolipid metabolism: model of glucocerebrosidase deficiency in zebrafish.

Author

Lelieveld LT, Mirzaian M, Kuo CL, Artola M, Ferraz MJ, Peter REA, Akiyama H, Greimel P, van den Berg RJBHN, Overkleeft HS, Boot RG, Meijer AH, and Aerts JMFG

Subjects

Animals, Cells, Cultured, Glucosylceramidase metabolism, Zebrafish, beta-Glucosidase deficiency, Glucosylceramidase deficiency, Glycosphingolipids metabolism, Models, Biological, Zebrafish Proteins deficiency, Zebrafish Proteins metabolism, beta-Glucosidase metabolism

Abstract

β-glucosidases [GBA1 (glucocerebrosidase) and GBA2] are ubiquitous essential enzymes. Lysosomal GBA1 and cytosol-facing GBA2 degrade glucosylceramide (GlcCer); GBA1 deficiency causes Gaucher disease, a lysosomal storage disorder characterized by lysosomal accumulation of GlcCer, which is partly converted to glucosylsphingosine (GlcSph). GBA1 and GBA2 also may transfer glucose from GlcCer to cholesterol, yielding glucosylated cholesterol (GlcChol). Here, we aimed to clarify the role of zebrafish Gba2 in glycosphingolipid metabolism during Gba1 deficiency in zebrafish ( Danio rerio ), which are able to survive total Gba1 deficiency. We developed Gba1 ( gba1 -/- ), Gba2 ( gba2 -/- ), and double ( gba1 -/- :gba2 -/- ) zebrafish knockouts using CRISPR/Cas9 and explored the effects of both genetic and pharmacological interventions on GlcCer metabolism in individual larvae. Activity-based probes and quantification of relevant glycolipid metabolites confirmed enzyme deficiency. GlcSph increased in gba1 -/- larvae (0.09 pmol/fish) but did not increase more in gba1 -/- :gba2 -/- larvae. GlcCer was comparable in gba1 -/- and WT larvae but increased in gba2 -/- and gba1 -/- :gba2 -/- larvae. Independent of Gba1 status, GlcChol was low in all gba2 -/- larvae (0.05 vs. 0.18 pmol/fish in WT). Pharmacologic inactivation of zebrafish Gba1 comparably increased GlcSph. Inhibition of GlcCer synthase (GCS) in Gba1-deficient larvae reduced GlcCer and GlcSph, and concomitant inhibition of GCS and Gba2 with iminosugars also reduced excessive GlcChol. Finally, overexpression of human GBA1 and injection of recombinant GBA1 both decreased GlcSph. We determined that zebrafish larvae offer an attractive model to study glucosidase actions in glycosphingolipid metabolism in vivo, and we identified distinguishing characteristics of zebrafish Gba2 deficiency., (Copyright © 2019 Lelieveld et al.)

Published

2019

3. Lysosomal glycosphingolipid catabolism by acid ceramidase: formation of glycosphingoid bases during deficiency of glycosidases.

Author

Ferraz MJ, Marques AR, Appelman MD, Verhoek M, Strijland A, Mirzaian M, Scheij S, Ouairy CM, Lahav D, Wisse P, Overkleeft HS, Boot RG, and Aerts JM

Subjects

Acid Ceramidase genetics, Acylation, Animals, Disease Models, Animal, Fabry Disease genetics, Female, Gaucher Disease genetics, Glucosylceramidase genetics, Glucosylceramidase metabolism, Glycosphingolipids chemistry, HEK293 Cells, Humans, Lysosomes metabolism, Male, Mice, Mice, Knockout, alpha-Galactosidase genetics, alpha-Galactosidase metabolism, Acid Ceramidase metabolism, Fabry Disease metabolism, Gaucher Disease metabolism, Glycosphingolipids metabolism

Abstract

Glycosphingoid bases are elevated in inherited lysosomal storage disorders with deficient activity of glycosphingolipid catabolizing glycosidases. We investigated the molecular basis of the formation of glucosylsphingosine and globotriaosylsphingosine during deficiency of glucocerebrosidase (Gaucher disease) and α-galactosidase A (Fabry disease). Independent genetic and pharmacological evidence is presented pointing to an active role of acid ceramidase in both processes through deacylation of lysosomal glycosphingolipids. The potential pathophysiological relevance of elevated glycosphingoid bases generated through this alternative metabolism in patients suffering from lysosomal glycosidase defects is discussed., (© 2016 Federation of European Biochemical Societies.)

Published

2016

4. Gaucher disease and Fabry disease: new markers and insights in pathophysiology for two distinct glycosphingolipidoses.

Author

Ferraz MJ, Kallemeijn WW, Mirzaian M, Herrera Moro D, Marques A, Wisse P, Boot RG, Willems LI, Overkleeft HS, and Aerts JM

Subjects

Humans, Biomarkers metabolism, Fabry Disease diagnosis, Fabry Disease physiopathology, Gaucher Disease diagnosis, Gaucher Disease physiopathology, Glycosphingolipids metabolism

Abstract

Gaucher disease (GD) and Fabry disease (FD) are two relatively common inherited glycosphingolipidoses caused by deficiencies in the lysosomal glycosidases glucocerebrosidase and alpha-galactosidase A, respectively. For both diseases enzyme supplementation is presently used as therapy. Cells and tissues of GD and FD patients are uniformly deficient in enzyme activity, but the two diseases markedly differ in cell types showing lysosomal accumulation of the glycosphingolipid substrates glucosylceramide and globotriaosylceramide, respectively. The clinical manifestation of Gaucher disease and Fabry disease is consequently entirely different and the response to enzyme therapy is only impressive in the case of GD patients. This review compares both glycosphingolipid storage disorders with respect to similarities and differences. Presented is an update on insights regarding pathophysiological mechanisms as well as recently available biochemical markers and diagnostic tools for both disorders. Special attention is paid to sphingoid bases of the primary storage lipids in both diseases. The value of elevated glucosylsphingosine in Gaucher disease and globotriaosylsphingosine in Fabry disease for diagnosis and monitoring of disease is discussed as well as the possible contribution of the sphingoid bases to (patho)physiology. This article is part of a Special Issue entitled New Frontiers in Sphingolipid Biology., (Copyright © 2013 Elsevier B.V. All rights reserved.)

Published

2014

5. Glycosphingolipids and insulin resistance.

Author

Aerts JM, Boot RG, van Eijk M, Groener J, Bijl N, Lombardo E, Bietrix FM, Dekker N, Groen AK, Ottenhoff R, van Roomen C, Aten J, Serlie M, Langeveld M, Wennekes T, and Overkleeft HS

Subjects

1-Deoxynojirimycin analogs & derivatives, 1-Deoxynojirimycin therapeutic use, Adamantane analogs & derivatives, Adamantane therapeutic use, Animals, Cardiovascular Diseases metabolism, Ceramides metabolism, Ceramides toxicity, Diabetes Mellitus, Type 2 metabolism, Dioxanes therapeutic use, Disease Models, Animal, Fatty Acids pharmacokinetics, Fatty Liver metabolism, Gaucher Disease drug therapy, Gaucher Disease genetics, Gaucher Disease metabolism, Glucosyltransferases antagonists & inhibitors, Glucosyltransferases physiology, Humans, Metabolic Syndrome metabolism, Mice, Mice, Obese, Non-alcoholic Fatty Liver Disease, Obesity metabolism, Pyrrolidines therapeutic use, Receptor, Insulin chemistry, Receptor, Insulin physiology, Signal Transduction, Glycosphingolipids metabolism, Insulin Resistance physiology

Abstract

Glycosphingolipids are structural membrane components, residing largely in the plasma membrane with their sugar-moieties exposed at the cell's surface. In recent times a crucial role for glycosphingolipids in insulin resistance has been proposed. A chronic state of insulin resistance is a rapidly increasing disease condition in Western and developing countries. It is considered to be the major underlying cause of the metabolic syndrome, a combination of metabolic abnormalities that increases the risk for an individual to develop Type 2 diabetes, obesity, cardiovascular disease, polycystic ovary syndrome and nonalcoholic fatty liver disease. As discussed in this chapter, the evidence for a direct regulatory interaction of glycosphingolipids with insulin signaling is still largely indirect. However, the recent finding in animal models that pharmacological reduction of glycosphingolipid biosynthesis ameliorates insulin resistance and prevents some manifestations of metabolic syndrome, supports the view that somehow glycosphingolipids act as critical regulators, Importantly, since reductions in glycosphingolipid biosynthesis have been found to be well tolerated, such approaches may have a therapeutic potential.

Published

2011

6. Dual-action lipophilic iminosugar improves glycemic control in obese rodents by reduction of visceral glycosphingolipids and buffering of carbohydrate assimilation.

Author

Wennekes T, Meijer AJ, Groen AK, Boot RG, Groener JE, van Eijk M, Ottenhoff R, Bijl N, Ghauharali K, Song H, O'Shea TJ, Liu H, Yew N, Copeland D, van den Berg RJ, van der Marel GA, Overkleeft HS, and Aerts JM

Subjects

Absorption drug effects, Animals, Glycated Hemoglobin drug effects, Imino Sugars chemistry, Imino Sugars therapeutic use, Mice, Mice, Obese, Rats, Rats, Zucker, Structure-Activity Relationship, Viscera metabolism, Blood Glucose drug effects, Carbohydrate Metabolism drug effects, Glycosphingolipids metabolism, Imino Sugars pharmacology, Obesity drug therapy

Abstract

The lipophilic iminosugar N-[5-(adamantan-1-ylmethoxy)pentyl]-1-deoxynojirimycin (2, AMP-DNM) potently controls hyperglycemia in obese rodent models of insulin resistance. The reduction of visceral glycosphingolipids by 2 is thought to underlie its beneficial action. It cannot, however, be excluded that concomitant inhibition of intestinal glycosidases and associated buffering of carbohydrate assimilation add to this. To firmly establish the mode of action of 2, we developed a panel of lipophilic iminosugars varying in configuration at C-4/C-5 and N-substitution of the iminosugar. From these we identified the l-ido derivative of 2, l-ido-AMP-DNM (4), as a selective inhibitor of glycosphingolipid synthesis. Compound 4 lowered visceral glycosphingolipids in ob/ob mice and ZDF rats on a par with 2. In contrast to 2, 4 did not inhibit sucrase activity or sucrose assimilation. Treatment with 4 was significantly less effective in reducing blood glucose and HbA1c. We conclude that the combination of reduction of glycosphingolipids in tissue and buffering of carbohydrate assimilation by 2 produces a superior glucose homeostasis.

Published

2010

7. Modulation of glycosphingolipid metabolism significantly improves hepatic insulin sensitivity and reverses hepatic steatosis in mice.

Author

Bijl N, Sokolović M, Vrins C, Langeveld M, Moerland PD, Ottenhoff R, van Roomen CP, Claessen N, Boot RG, Aten J, Groen AK, Aerts JM, and van Eijk M

Subjects

1-Deoxynojirimycin analogs & derivatives, 1-Deoxynojirimycin pharmacology, 1-Deoxynojirimycin therapeutic use, Adamantane analogs & derivatives, Adamantane pharmacology, Adamantane therapeutic use, Animals, Disease Models, Animal, Fatty Liver drug therapy, Glucose metabolism, Glycosphingolipids antagonists & inhibitors, Homeostasis drug effects, Liver drug effects, Male, Mice, Mice, Inbred C57BL, Mice, Obese, Obesity metabolism, Triglycerides metabolism, Fatty Liver metabolism, Glycosphingolipids metabolism, Insulin metabolism, Insulin Resistance physiology, Liver metabolism

Abstract

Unlabelled: Nonalcoholic fatty liver disease (NAFLD) is associated with obesity, insulin resistance, and type 2 diabetes. The hyperinsulinemia that occurs as a consequence of insulin resistance is thought to be an important contributor to the development of fatty liver. We have shown that the iminosugar N-(5'-adamantane-1'-yl-methoxy)-pentyl-1-deoxynojirimycin (AMP-DNM), an inhibitor of the enzyme glucosylceramide synthase, is a potent enhancer of insulin signaling in rodent models for insulin resistance and type 2 diabetes. The present study was designed to assess the impact of AMP-DNM on insulin levels, liver triglyceride synthesis, and gene expression profile. Treatment of ob/ob mice with AMP-DNM restored insulin signaling in the liver, corrected blood glucose values to levels found in lean mice, and decreased insulin concentration. The expression of sterol regulatory element-binding protein 1c target genes involved in fatty acid synthesis normalized. AMP-DNM treatment significantly reduced liver to body weight ratio and reversed hepatic steatosis, comprising fat as well as inflammatory markers. In addition, AMP-DNM treatment corrected to a large extent the gene expression profile of ob/ob mice livers toward the profile of lean mice., Conclusion: Pharmacological lowering of glycosphingolipids with the iminosugar AMP-DNM is a promising approach to restore insulin signaling and improve glucose homeostasis as well as hepatic steatosis.

Published

2009

8. Reduction of glycosphingolipid biosynthesis stimulates biliary lipid secretion in mice.

Author

Bijl N, van Roomen CP, Triantis V, Sokolovic M, Ottenhoff R, Scheij S, van Eijk M, Boot RG, Aerts JM, and Groen AK

Subjects

1-Deoxynojirimycin analogs & derivatives, 1-Deoxynojirimycin pharmacology, Adamantane analogs & derivatives, Adamantane pharmacology, Animals, Cell Line, Tumor, Cells, Cultured, Cholesterol blood, Cholesterol, HDL metabolism, Gallbladder physiology, Gangliosides physiology, Glycosphingolipids antagonists & inhibitors, Humans, Lipid Metabolism, Lipoproteins, HDL metabolism, Liver Neoplasms, Mice, Mice, Inbred C57BL, RNA, Messenger genetics, Signal Transduction, Triglycerides blood, Bile metabolism, Gallbladder metabolism, Glycosphingolipids biosynthesis

Abstract

Unlabelled: Recent reports indicate that glycosphingolipids play an important role in regulation of carbohydrate metabolism. We have shown that the iminosugar N-(5'-adamantane-1'-yl-methoxy)-pentyl-1-deoxynojirimycin (AMP-DNM), an inhibitor of the enzyme glucosylceramide synthase, is a potent enhancer of insulin signaling in rodent models for insulin resistance and type 2 diabetes. In this study, we determined whether AMP-DNM also affects lipid homeostasis and, in particular, the reverse cholesterol transport pathway. Treatment of C57BL/6J mice with AMP-DNM for 5 weeks decreased plasma levels of triglycerides and cholesterol by 35%, whereas neutral sterol excretion increased twofold. Secretion of biliary lipid also increased twofold, which resulted in a similar rise in bile flow. This effect was not due to altered expression levels or kinetics of the various export pumps involved in bile formation. However, the bile salt pool size increased and the expression of Cyp7A1 was up-regulated. In vitro experiments using HepG2 hepatoma cell line revealed this to be due to inhibition of fibroblast growth factor-19 (FGF19)-mediated suppression of Cyp7A1 via the FGF receptor., Conclusion: Pharmacological modulation of glycosphingolipid metabolism showed surprising effects on lipid homeostasis in C57BL/6J mice. Upon administration of 100 mg AMP-DNM/kg body weight/day, plasma cholesterol and triglyceride levels decreased, biliary lipid secretion doubled and also the endpoint of reverse cholesterol transport, neutral sterol excretion, doubled.

Published

2009

9. Glycosphingolipids--nature, function, and pharmacological modulation.

Author

Wennekes T, van den Berg RJ, Boot RG, van der Marel GA, Overkleeft HS, and Aerts JM

Subjects

Cell Membrane, Galactosylceramides metabolism, Gaucher Disease therapy, Glucosylceramidase antagonists & inhibitors, Glucosylceramidase metabolism, Glucosyltransferases antagonists & inhibitors, Glucosyltransferases metabolism, Glycosphingolipids biosynthesis, Glycosphingolipids pharmacology, Humans, Sphingolipids biosynthesis, Sphingolipids metabolism, Glycosphingolipids metabolism

Abstract

The discovery of the glycosphingolipids is generally attributed to Johan L. W. Thudichum, who in 1884 published on the chemical composition of the brain. In his studies he isolated several compounds from ethanolic brain extracts which he coined cerebrosides. He subjected one of these, phrenosin (now known as galactosylceramide), to acid hydrolysis, and this produced three distinct components. One he identified as a fatty acid and another proved to be an isomer of D-glucose, which is now known as D-galactose. The third component, with an "alkaloidal nature", presented "many enigmas" to Thudichum, and therefore he named it sphingosine, after the mythological riddle of the Sphinx. Today, sphingolipids and their glycosidated derivatives are the subjects of intense study aimed at elucidating their role in the structural integrity of the cell membrane, their participation in recognition and signaling events, and in particular their involvement in pathological processes that are at the basis of human disease (for example, sphingolipidoses and diabetes type 2). This Review details some of the recent findings on the biosynthesis, function, and degradation of glycosphingolipids in man, with a focus on the glycosphingolipid glucosylceramide. Special attention is paid to the clinical relevance of compounds directed at interfering with the factors responsible for glycosphingolipid metabolism.

Published

2009

10. Substrate reduction therapy of glycosphingolipid storage disorders.

Author

Aerts JM, Hollak CE, Boot RG, Groener JE, and Maas M

Subjects

1-Deoxynojirimycin analogs & derivatives, 1-Deoxynojirimycin pharmacology, 1-Deoxynojirimycin therapeutic use, Anti-Inflammatory Agents pharmacology, Anti-Inflammatory Agents therapeutic use, Biomarkers metabolism, Clinical Trials as Topic, Enzyme Inhibitors pharmacology, Gaucher Disease drug therapy, Gaucher Disease genetics, Gaucher Disease metabolism, Genetic Therapy methods, Glucosylceramidase genetics, Glucosylceramidase metabolism, Glucosylceramidase therapeutic use, Glucosyltransferases antagonists & inhibitors, Glucosyltransferases metabolism, Humans, Lysosomal Storage Diseases drug therapy, Lysosomal Storage Diseases metabolism, Morpholines pharmacology, Morpholines therapeutic use, Practice Guidelines as Topic, Recombinant Proteins therapeutic use, Treatment Outcome, Enzyme Inhibitors therapeutic use, Gaucher Disease therapy, Glycosphingolipids metabolism

Abstract

In the last 15 years enormous progress has been made regarding therapy of type I Gaucher disease, a severely disabling disorder characterized by intralysosomal storage of glucosylceramide in tissue macrophages. Effective enzyme replacement therapy of type I Gaucher disease, based on chronic intravenous administration of mannose-terminated recombinant human glucocerebrosidase, has been available since 1990 and has been applied in several thousand patients without serious adverse effects. An alternative therapeutic approach, so-called substrate reduction therapy, is based on partial reduction of the synthesis of glucosylceramide and hence of subsequent metabolites. Oral administration of an inhibitor of glucosylceramide synthesis (N-butyldeoxynojirimycin, registered in Europe since 2002 as miglustat (Zavesca)), is effective in reversing clinical symptoms in type I Gaucher patients with mild to moderate disease manifestations. The growing long-term experience with substrate reduction therapy indicates that this treatment is also without major adverse effects. Substrate reduction therapy, in conjunction with enzyme replacement therapy, may play an important role in the future clinical management of patients suffering from type I Gaucher disease. Clinical trials are under way that should reveal the value of substrate reduction for maintenance therapy of type I Gaucher disease and for treatment of neuronopathic variants of Gaucher disease, Niemann-Pick disease type C, late-onset Tay-Sachs disease and Sandhoff disease.

Published

2006

11. Development of an acid ceramidase activity-based probe.

Author

Ouairy, Cécile M. J., Ferraz, Maria J., Boot, Rolf G., Baggelaar, Marc P., van der Stelt, Mario, Appelman, Monique, van der Marel, Gijsbert A., Florea, Bogdan I., Aerts, Johannes M. F. G., and Overkleeft, Herman S.

Subjects

ACID ceramidase, GLYCOSPHINGOLIPIDS, MOLECULAR probes, METABOLISM, HYDROLYSIS, FREE fatty acids, FARBER disease

Abstract

Acid ceramidase is responsible for the ultimate step in the catabolism of (glyco)sphingolipids by hydrolysis of ceramide into sphingosine and free fatty acid. Deficiency in acid ceramidase is the molecular basis of Farber disease. Here we report the synthesis and characterization of an activity-based acid ceramidase probe. [ABSTRACT FROM AUTHOR]

Published

2015

12. Phenotype diversity in type 1 Gaucher disease: discovering the genetic basis of Gaucher disease/hematologic malignancy phenotype by individual genome analysis.

Author

Lo, Sarah M., Choi, Murim, Jun Liu, Jain, Dhanpat, Boot, Rolf G., Kallemeijn, Wouter W., Aerts, Johannes M. R G., Pashankar, Farzana, Kupfer, Gary M., Mane, Shrikant, Lifton, Richard P., and Mistry, Pramod K.

Subjects

*PHENOTYPES, *GAUCHER'S disease, *HEMATOLOGIC malignancies, *MACROPHAGES, *GLYCOSPHINGOLIPIDS, *LIPIDOSES, *GENETIC mutation, *GENETICS

Abstract

Gaucher disease (GD), an inherited macrophage glycosphingolipidosis, manifests with an extraordinary variety of phe-notypes that show imperfect correlation with mutations in the GBA gene. In addition to the classic manifestations, patients suffer from increased susceptibility to hematologic and nonhematologic malignancies. The mechanism(s) underlying malignancy in GD is not known, but is postulated to be secondary to macrophage dysfunction and immune dysregu-lation arising from lysosomal accumulation of glucocerebroside. However, there is weak correlation between GD/cancer phenotype and the systemic burden of glucocerebroside-laden macrophages. Therefore, we hypothesized that genetic modif ier(s) may underlie the GD/cancer phenotype. In the present study, the genetic basis of GD/T-cell acute lymphoblastic lymphoma in 2 affected siblings was deciphered through genomic analysis. GBA gene sequencing revealed homozygosity for a novel mutation, D137N. Whole-exome capture and massively parallel sequencing combined with homozygosity mapping identified a homozygous novel mutation in the MSH6 gene that leads to constitutional mismatch repair deficiency syndrome and increased cancer risk. Enzyme studies demonstrated that the D137N mutation in GBA is a pathogenic mutation, and immunohistochemistry confirmed the absence of the MSH6 protein. Therefore, precise phenotype annotation followed by individual genome analysis has the potential to identify genetic modifiers of GD, facilitate personalized management, and provide novel insights into disease pathophysiology [ABSTRACT FROM AUTHOR]

Published

2012