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1. Novel PEX3 Gene Mutations Resulting in a Moderate Zellweger Spectrum Disorder

Author

Maxit, C., Denzler, I., Marchione, D., Agosta, G., Koster, J., Wanders, R. J. A., Ferdinandusse, S., Waterham, H. R., Laboratory Genetic Metabolic Diseases, Amsterdam Reproduction & Development (AR&D), Paediatric Metabolic Diseases, and Amsterdam Gastroenterology Endocrinology Metabolism

Abstract

Peroxisome biogenesis disorders (PBDs) may have a variable clinical expression, ranging from severe, lethal to mild phenotypes with progressive evolution. PBDs are autosomal recessive disorders caused by mutations in PEX genes, which encode proteins called peroxins, involved in the assembly of the peroxisome. Patient Description: We herein report a patient who is currently 9 years old and who is compound heterozygous for two novel mutations in the PEX3 gene. Mild biochemical abnormalities of the peroxisomal parameters suggested a Zellweger spectrum defect in the patient. Sequence analysis of the PEX3 gene identified two novel heterozygous, pathogenic mutations. Mutations in PEX3 usually result in a severe, early lethal phenotype. We report a patient compound heterozygous for two novel mutations in the PEX3 gene, who is less affected than previously reported patients with a defect in the PEX3 gene. Our findings indicate that PEX3 defects may cause a disease spectrum similar as previously observed for other PEX gene defects

Published
2017

2. Two Novel Mutations in the SLC25A4 Gene in a Patient with Mitochondrial Myopathy

Author

Körver-Keularts, I. M. L. W., de Visser, M., Bakker, H. D., Wanders, R. J. A., Vansenne, F., Scholte, H. R., Dorland, L., Nicolaes, G. A. F., Spaapen, L. M. J., Smeets, H. J. M., Hendrickx, A. T. M., van den Bosch, B. J. C., Radiotherapie, Biochemie, Klinische Genetica, MUMC+: DA KG Lab Centraal Lab (9), RS: CARIM - R1 - Thrombosis and haemostasis, RS: CARIM - R2 - Cardiac function and failure, Genetica & Celbiologie, RS: FHML MaCSBio, Neurology, Amsterdam Gastroenterology Endocrinology Metabolism, Laboratory Genetic Metabolic Diseases, Other Research, and Human Genetics

Abstract

In a 28-year-old male with a mild mitochondrial myopathy manifesting as exercise intolerance and early signs of cardiomyopathy without muscle weakness or ophthalmoplegia, we identified two novel mutations in the SLC25A4 gene: c.707G>C in exon 3 (p.(R236P)) and c.116_137del in exon 2 (p.(Q39Lfs*14)). Serum lactate levels at rest were elevated (12.7 mM). Both the patient's father and brother were heterozygous carriers of the c.707G>C mutation and were asymptomatic. The second mutation causes a 22 bp deletion leading to a frame shift likely giving rise to a premature stop codon and nonsense-mediated decay (NMD). The segregation of the mutations could not be tested directly as the mother had died before. However, indirect evidence from NMD experiments showed that the two mutations were situated on two different alleles in the patient. This case is unique compared to other previously reported patients with either progressive external ophthalmoplegia (PEO) or clear hypertrophic cardiomyopathy with exercise intolerance and/or muscle weakness carrying recessive mutations leading to a complete absence of the SLC25A4 protein. Most likely in our patient, although severely reduced, SLC25A4 is still partially present and functional.

Published
2015

3. Peroxisomal Diseases

Author

Wanders, R. J. A., Aminoff, Michael, Daroff, Robert, Amsterdam Gastroenterology Endocrinology Metabolism, and Laboratory Genetic Metabolic Diseases

Published
2014

4. Mutations of OCTN2, an Organic Cation/Carnitine Transporter, Lead to Deficient Cellular Carnitine Uptake in Primary Carnitine Deficiency

Author

Tang, N. L., Ganapathy, V., Wu, X., Hui, J., Seth, P., Yuen, P. M., Wanders, R. J., Fok, T. F., Hjelm, N. M., and Other departments

Subjects
Male, medicine.medical_specialty, Genotype, Organic Cation Transport Proteins, Recombinant Fusion Proteins, DNA Mutational Analysis, Molecular Sequence Data, Mutant, Biology, SLC22A5, Cell Line, Carnitine, Internal medicine, Systemic primary carnitine deficiency, Genetics, medicine, Humans, Carnitine palmitoyltransferase II, Missense mutation, Amino Acid Sequence, Solute Carrier Family 22 Member 5, Molecular Biology, Genetics (clinical), Family Health, Organic cation transport proteins, Sequence Homology, Amino Acid, Membrane Proteins, Biological Transport, General Medicine, medicine.disease, Pedigree, Endocrinology, Gene Expression Regulation, Mutation, biology.protein, Female, Carrier Proteins, Primary Carnitine Deficiency, Sequence Alignment, medicine.drug
Abstract

Systemic primary carnitine deficiency (CDSP, OMIM 212140) is an autosomal recessive disease characterized by low serum and intracellular concentrations of carnitine. CDSP may present with acute metabolic derangement simulating Reye's syndrome within the first 2 years of life. After 3 years of age, patients with CDSP may present with cardiomyopathy and muscle weakness. A linkage with D5S436 in 5q was reported in a family. A recently cloned homologue of the organic cation transporter, OCTN2, which has sodium-dependent carnitine uptake properties, was also mapped to the same locus. We screened for mutation in OCTN2 in a confirmed CDSP family. One truncating mutation (Trp132Stop) and one missense mutation (Pro478Leu) of OCTN2 were identified together with two silent polymorphisms. Expression of the mutant cDNAs revealed virtually no uptake activity for both mutations. Our data indicate that mutations in OCTN2 are responsible for CDSP. Identification of the underlying gene in this disease will allow rapid detection of carriers and postnatal diagnosis of affected patients.

Published
1999

5. New familial mitochondrial encephalopathy with macrocephaly, cardiomyopathy, and complex I deficiency

Author

Dionisi-Vici, C., Ruitenbeek, W., Fariello, G., Bentlage, H., Wanders, R. J., Schägger, H., Bosman, C., Piantadosi, C., Sabetta, G., Bertini, E., and Other departments

Subjects
Characterization of the respiratory chain proteins in mitochondrial myopathies, Karakterisering van de eiwitten in de ademhalingsketen bij mitochondriële myopathieën, GeneralLiterature_REFERENCE(e.g.,dictionaries,encyclopedias,glossaries)
Abstract

Two siblings presented with a new phenotype consisting of fatal progressive macrocephaly and hypertrophic cardiomyopathy. Onset of symptoms started in both patients at the end of the first month of life with massive brain swelling causing macrocephaly and evolving to extensive brain destruction. Light microscopy of the lesions showed extensive small-vessel proliferation and gliosis. A distinct deficiency of complex I of mitochondrial respiratory chain was established in cultured fibroblasts, skeletal muscle, and heart muscle. Specific lack of complex I protein was demonstrated by two-dimensional gel electrophoresis

Published
1997

6. Screening for dihydropyrimidine dehydrogenase deficiency to prevent severe 5-fluorouracil and capecitabine-associated toxicity

Author

André van Kuilenburg, Ferdinandusse, S., Wanders, R. J. A., Laboratory Genetic Metabolic Diseases, Amsterdam Gastroenterology Endocrinology Metabolism, and Cancer Center Amsterdam

Subjects
DPYD, 5-fluorouracil, Dihydropyrimidine dehydrogenase
Abstract

5-Fluorouracil (5FU) and capecitabine are the cornerstones of all currently applied regimens for the treatment of patients with cancers of the gastrointestinal tract, breast, head and neck. Dihydropyrimidine dehydrogenase (DPD) plays a pivotal role in the metabolism of 5FU and as such, a deficiency of DPD has been recognised as an important risk factor, predisposing patients to develop severe 5FU-associated toxicity. In this manuscript, we discuss a wide range of methods that have been established to assess the genetic and functional status of DPD. Genotyping of DPYD is used to identify DPD deficient patients. However, its suitability for pre-treatment testing is under debate, not least due to conflicting genotype-phenotype relations in mutation carriers and relatively low positive predictive values. In addition to genetic screening, a number of phenotype-based methods have been introduced which appear to be well suited for clinical laboratories and which are an attractive option for monitoring of the DPD status. These phenotype-based screening approaches to detect DPD-deficient patients warrant further clinical validation.

Published
2013

8. Mammalian peroxisomal ABC transporters: from endogenous substrates to pathology and clinical significance

Author

Kemp, S., Theodoulou, F. L., and Wanders, R. J. A.

Subjects
Pharmacology & Pharmacy
Abstract

Peroxisomes are indispensable organelles in higher eukaryotes. They are essential for a number of important metabolic pathways, including fatty acid a- and beta-oxidation, and biosynthesis of etherphospholipids and bile acids. However, the peroxisomal membrane forms an impermeable barrier to these metabolites. Therefore, peroxisomes need specific transporter proteins to transfer these metabolites across their membranes. The mammalian peroxisomal membrane harbours three ATP-binding cassette (ABC) transporters. In recent years, significant progress has been made in unravelling the functions of these ABC transporters. There is ample evidence that they are involved in the transport of very long-chain fatty acids, pristanic acid, di- and trihydroxycholestanoic acid, dicarboxylic acids and tetracosahexaenoic acid (C24:6?3). Surprisingly, only one disease is associated with a deficiency of a peroxisomal ABC transporter. Mutations in the ABCD1 gene encoding the peroxisomal ABC transporter adrenoleukodystrophy protein are the cause for X-linked adrenoleukodystrophy, an inherited metabolic storage disorder. This review describes the current state of knowledge on the mammalian peroxisomal ABC transporters with a particular focus on their function in metabolite transport.

Published
2011

11. Recidiverende rabdomyolyse: zoek naar de onderliggende aandoening

Author

Zutt, R., van der Kooi, A. J., Linthorst, G. E., Wanders, R. J. A., Verschuuren, J. J. G. M., de Visser, M., Amsterdam Neuroscience, Neurology, Endocrinology, Amsterdam Gastroenterology Endocrinology Metabolism, and Laboratory Genetic Metabolic Diseases

Abstract

Rhabdomyolysis is a rare potentially dangerous syndrome resulting from the dissolution of skeletal muscle fibres. An isolated attack of rhabdomyolysis can have various causes, such as trauma, hyperpyrexia, infections, electrolyte imbalances, seizures, severe exertion, and drugs or substance abuse or a combination of these. Recurrent episodes and/or a family history of rhabdomyolysis is more likely caused by an underlying genetic defect. Three patients with rhabdomyolysis are described. One patient had an isolated episode due to excessive exercise. The other patients had a medical history or accompanying symptoms that suggested an underlying genetic metabolic myopathy confirmed in both by DNA analysis. An algorithm on when and how to screen for underlying genetic diseases is presented. Diagnosis of these genetic diseases is important for adequate counselling and dietary measures to prevent future episodes

Published
2010

12. Quantitative analysis of N-acetylglutamate and orotic acid by MS-MS

Author

Aires, C., van Cruchten, A., Ruiter, J., Ijlst, L., de Almeida, I. Tavares, Duran, M., Wanders, R. J. A., Silva, M. F. B., and Repositório da Universidade de Lisboa

Subjects
Biochemistry & Molecular Biology
Abstract

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Published
2009

15. BIOSYNTHESIS OF VALPROYLCARNITINE

Author

Aires, C. C. P., van Lenthe, H., Ijlst, L., Ruiter, J., Minkler, P., Hoppel, C. L., de Almeida, I. Tavares, Duran, M., Wanders, R. J. A., Silva, M. F. B., and Repositório da Universidade de Lisboa

Subjects
Genetics & Heredity, Biochemistry & Molecular Biology, Medicine, Research & Experimental
Abstract

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Published
2009

16. ENDOGENOUS POISONS MEDIATING MITOCHONDRIAL DYSFUNCTION

Author

Fátima Ventura, Violante, S., Ruiter, J. P. N., Ijlst, L., Silva, M. J., Houten, S. M., Almeida, I. Tavares, Wanders, R. J. A., and Repositório da Universidade de Lisboa

Subjects
Genetics & Heredity, Biochemistry & Molecular Biology, Medicine, Research & Experimental
Abstract

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Published
2009

18. Inhibition of N-acetyl-glutamate synthase activity in valproate-associated hyperammonemia

Author

Aires, C. C. P., van Cruchten, A., Ruiter, J., Ijlst, L., Tavares, De Almeida, Duran, M., Wanders, R. J. A., Silva, M. F. B., and Repositório da Universidade de Lisboa

Subjects
Genetics & Heredity, Endocrinology & Metabolism
Abstract

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Published
2008

19. Interference of valproic acid on the branched chain amino acid oxidative metabolism

Author

Luis, P. B. M., Ruiter, J. P. N., Ijlst, L., Ofman, R., Diogo, L., Garcia, P., Duran, M., Jerry Vockley, Travares, Almeida, Wanders, R. J. A., Silva, M. F. B., and Repositório da Universidade de Lisboa

Subjects
Genetics & Heredity, Endocrinology & Metabolism
Abstract

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Published
2008

20. Plasmalogens and Polyunsaturated Fatty Acids

Author

Duran, M., Wanders, R. J. A., Blau, Nenad, Duran, Marinus, Gibson, Michael K., AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, and Laboratory Genetic Metabolic Diseases

Published
2008

21. Valproic acid metabolism and its effects on mitochondrial fatty acid oxidation

Author

Silva, M. F. B., Aires, C. C. P., Luis, P. B. M., Ruiter, J. P. N., IJist, L., Duran, M., Wanders, R. J. A., and de Almeida, I. Tavares

Subjects
Genetics & Heredity, Endocrinology & Metabolism
Abstract

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Published
2008

22. Implications for acylcarnitine profiling

Author

Violante, S., Ijlst, L., Tavares, Almeida, Wanders, R. J., Fátima Ventura, and Repositório da Universidade de Lisboa

Subjects
Genetics & Heredity, Endocrinology & Metabolism
Abstract

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Published
2008

23. Valproic acid metabolism and its effects on mitochondrial fatty acid oxidation

Author

Silva, M. F. B., Aires, C. C. P., Luis, P. B. M., Ruiter, J. P. N., IJist, L., Duran, M., Wanders, R. J. A., de Almeida, I. Tavares, and Repositório da Universidade de Lisboa

Subjects
Genetics & Heredity, Endocrinology & Metabolism, lipids (amino acids, peptides, and proteins)
Abstract

Valproic acid (VPA; 2-n-propylpentanoic acid) is widely used as a major drug in the treatment of epilepsy and in the control of several types of seizures. Being a simple fatty acid, VPA is a substrate for the fatty acid P-oxidation (FAO) pathway, which takes place primarily in mitochondria. The toxicity of valproate has long been considered to be due primarily to its interference with mitochondrial P-oxidation. The metabolism of the drug, its effects on enzymes of FAO and their cofactors such as CoA and/or carnitine will be reviewed. The cumulative consequences of VPA therapy in inborn errors of metabolism (IEMs) and the importance of recognizing an underlying IEM in cases of VPA-induced steatosis and acute liver toxicity are two different concepts that will be emphasized.

Published
2008

24. Peroxisomes, Refsum's disease and the alpha- and omega-oxidation of phytanic acid

Author

Wanders, R. J. A., Komen, J. C., AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, and Laboratory Genetic Metabolic Diseases

Abstract

In the present paper, we describe the current state of knowledge regarding the enzymology of the phytanic acid alpha-oxidation pathway. The product of phytanic acid alpha-oxidation, i.e. pristanic acid, undergoes three cycles of beta-oxidation in peroxisomes after which the products, including 4,8-dimethylnonanoyl-CoA, propionyl-CoA and acetyl-CoA, are exported from the peroxisome via one of two routes, including (i) the carnitine-dependent route, mediated by CRAT (carnitine acetyltransferase) and CROT (carnitine O-octanoyltransferase), and (ii) the free acid route, mediated by one or more of the peroxisomal ACOTs (acyl-CoA thioesterases). We also describe our recent data on the omega-oxidation of phytanic acid, especially since pharmacological up-regulation of this pathway may form the basis of a new treatment strategy for ARD (adult Refsum's disease). In patients suffering from ARD, phytanic acid accumulates in tissues and body fluids due to a defect in the alpha-oxidation system

Published
2007

25. The human carnitine acylcarnitine translocase (hCACT)

Author

FV, Ventura, Violante, S., Gomes, C., Carvalho, A. L., Romao, M. J., Gaspar, M. M., Cruz, M. E. M., Soveral, G., Wanders, R. J., Leandro, P., de Almeida, Tavares, and Repositório da Universidade de Lisboa

Subjects
Genetics & Heredity, Endocrinology & Metabolism
Abstract

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Published
2007

26. In vivo and in vitro studies on the interaction of valproic acid and metabolites with the leucine oxidative metabolism

Author

Luis, P. M. B., Ruiter, J. P., Ijlst, L., Aires, C. C. P., Diogo, L., Garcia, P., Almeida, I. T., Duran, M., Jerry Vockley, Wanders, R. J. A., Silva, M. F. B., and Repositório da Universidade de Lisboa

Subjects
Genetics & Heredity, Endocrinology & Metabolism
Abstract

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Published
2007

27. Inborn Errors of Metabolism

Author

Duran, M., Abeling, N. G. G. M., van Kuilenburg, A. B. P., Wanders, R. J. A., Waterham, H. R., van Pelt, J., Poland, D.C.W., Amsterdam Gastroenterology Endocrinology Metabolism, Laboratory Genetic Metabolic Diseases, and Cancer Center Amsterdam

Published
2007

29. Omega-oxidation of very long-chain fatty acids in human liver microsomes: Implications for X-linked adrenoleukodystrophy?

Author

Sanders, R. -J, Ofman, R., Duran, M., Stephan Kemp, Wanders, R. J. A., Laboratory Genetic Metabolic Diseases, Amsterdam Gastroenterology Endocrinology Metabolism, Amsterdam Neuroscience, Amsterdam Neuroscience - Cellular & Molecular Mechanisms, and Paediatric Metabolic Diseases

Abstract

X-linked adrenoleukodystrophy (X-ALD) is a severe neurodegenerative disorder biochemically characterized by elevated levels of very long-chain fatty acids (VLCFA). Excess levels of VLCFAs are thought to play an important role in the pathogenesis of X-ALD. Therefore, therapeutic approaches for X-ALD are focused on the reduction or normalization of VLCFAs. In this study, we investigated an alternative oxidation route for VLCFAs, namely omega-oxidation. The results described in this study show that VLCFAs are substrates for the omega-oxidation system in human liver microsomes. Moreover, VLCFAs were not only converted into omega-hydroxy fatty acids, but they were also further oxidized to dicarboxylic acids via cytochrome P450-mediated reactions. High sensitivity toward the specific P450 inhibitor 17-octadecynoic acid suggested that omega-hydroxylation of VLCFAs is catalyzed by P450 enzymes belonging to the CYP4A/F subfamilies. Studies with individually expressed human recombinant P450 enzymes revealed that two P450 enzymes, i.e. CYP4F2 and CYP4F3B, participate in the omega-hydroxylation of VLCFAs. Both enzymes belong to the cytochrome P450 4F subfamily and have a high affinity for VLCFAs. In summary, this study demonstrates that VLCFAs are substrates for the human omega-oxidation system, and for this reason, stimulation of the in vivo VLCFA omega-oxidation pathway may provide an alternative mode of treatment to reduce the levels of VLCFAs in patients with X-ALD

Published
2006

30. Peroxisomal disorders

Author

Poll-The, B. T., Aubourg, P., Wanders, R. J. A., Fernandes, J., Saudubray, J. M., van den Berghe, G., Amsterdam Gastroenterology Endocrinology Metabolism, Amsterdam Neuroscience, Paediatric Neurology, Neurology, and Laboratory Genetic Metabolic Diseases

Published
2006

31. Van gen naar ziekte; primaire hyperoxalurie type I door mutaties in het AGXT-gen

Author

van Woerden, C. S., Groothof, J. W., Wanders, R. J. A., Waterham, H. R., Wijburg, F. R., Amsterdam Gastroenterology Endocrinology Metabolism, Laboratory Genetic Metabolic Diseases, and Paediatric Metabolic Diseases

Abstract

Primary hyperoxaluria type I (PH1) is a congenital defect in glyoxylate metabolism caused by a deficiency in the liver-specific peroxisomal enzyme known as alanine glyoxylate aminotransferase (AGT). The deficiency is due to mutations in the AGXT gene, located on chromosome 2q37.3, and results in the conversion of glyoxylate to oxalate. The crystallisation of oxalate with calcium results in symptoms varying from a solitary kidney stone to end-stage renal disease with systemic oxalosis. The diagnosis is based on increased oxalate and glycolate excretion in the urine, reduced AGT activity in liver tissue, and confirmed mutations in the AGXT gene. Over 50 disease-causing mutations have been identified in PH1, which are associated with a wide range of effects on the AGT enzyme. Homozygous Gly170Arg or Phei52Ile mutations are associated with a reduction in urinary oxalate excretion upon pyridoxine administration and long-term preservation of renal function when treatment is initiated in a timely manner. Homozygous 33insC and Gly82Arg mutations result in a much poorer prognosis. Mutational analysis of the AGXT gene in PH1 patients can be a useful tool for establishing the diagnosis and choosing an appropriate therapeutic strategy

Published
2006

32. VALPROYL-COA IS A POSSIBLE SUBSTRATE FOR CARNITINE PALMITOYL-TRANSFERASE I

Author

Aires, C. C. P., Ruiter, J. P. N., Luis, P. B. M., De Almeida, Tavares, Duran, M., Wanders, R. J. A., Silva, M. F. B., and Repositório da Universidade de Lisboa

Subjects
Genetics & Heredity, Endocrinology & Metabolism
Abstract

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Published
2005

33. Omega-hydroxylation of phytanic acid in rat liver microsomes: implications for Refsum disease

Author

Komen, J. C., Duran, M., Wanders, R. J. A., Laboratory Genetic Metabolic Diseases, and Paediatric Metabolic Diseases

Abstract

The 3-methyl-branched fatty acid phytanic acid is degraded by the peroxisomal alpha-oxidation route because the 3-methyl group blocks beta-oxidation. In adult Refsum disease (ARD), peroxisomal alpha-oxidation is defective, which is caused by mutations in the gene coding for phytanoyl-CoA hydroxylase in the majority of ARD patients. As a consequence, phytanic acid accumulates in tissues and body fluids. This study focuses on an alternative route of phytanic acid degradation, omega-oxidation. The first step in omega-oxidation is hydroxylation at the omega-end of the fatty acid, catalyzed by a member of the cytochrome P450 multienzyme family. To study this first step, the formation of hydroxylated intermediates was studied in rat liver microsomes incubated with phytanic acid and NADPH. Two hydroxylated metabolites of phytanic acid were formed, omega- and (omega-1)-hydroxyphytanic acid (ratio of formation, 5:1). The formation of omega-hydroxyphytanic acid was NADPH dependent and inhibited by imidazole derivatives. These results indicate that phytanic acid undergoes omega-hydroxylation in rat liver microsomes and that an isoform of cytochrome P450 catalyzes the first step of phytanic acid omega-oxidation

Published
2004

38. Peroxisomal disorders

Author

Wanders, R. J. A., Barth, P. G., Poll-The, B. T., Blau, N., Blaskovics, M. E., Duran, M., Gibson, K. M., Paediatric Metabolic Diseases, Laboratory Genetic Metabolic Diseases, Paediatric Neurology, and Neurology

Published
2003

41. Clinical features of galactokinase deficiency: a review of the literature

Author

Bosch, A. M., Bakker, H. D., van Gennip, A. H., van Kempen, J. V., Wanders, R. J. A., Wijburg, F. A., Paediatric Metabolic Diseases, and Laboratory Genetic Metabolic Diseases

Abstract

Galactokinase deficiency (McKusick 230200) is a rare autosomal recessive inborn error of galactose metabolism. Cataract and, rarely, pseudotumor cerebri caused by galactitol accumulation seem to be the only consistently reported abnormalities in this disorder. We performed a literature search to obtain information on the clinical spectrum of galactokinase deficiency. A total of 25 publications were traced describing 55 galactokinase-deficient patients. Cataract was reported in most patients. Clinical abnormalities other than cataract were reported in 15 (35%) out of 43 cases on which information was available. However, all symptoms were reported infrequently and a causal relationship with the galactokinase deficiency is unlikely. As cataract and pseudotumor cerebri appear to be the sole complications of galactokinase deficiency, the outcome for patients with galactokinase deficiency is much better than for patients with classical galactosaemia (McKusick 230400), a more common autosomal recessive disorder of galactose metabolism caused by galactose-1-phosphate uridyltransferase (GALT; EC 2.7.7.12) deficiency. Long-term follow-up of patients with this disorder has shown that, in spite of a severely galactose-restricted diet, most patients develop abnormalities such as a disturbed mental and/or motor development, dyspraxia and hypergonadotropic hypogonadism. Endogenous production of galactose has been considered an important aetiological factor. Although damage may well occur in utero, available evidence suggests that damage will continue after birth. Inhibition of galactokinase may then be a promising approach for controlling damage in GALT-deficient patients

Published
2002

42. Biochemical markers predicting survival in peroxisome biogenesis disorders

Author

Gootjes, J., Mooijer, P. A. W., Dekker, C., Barth, P. G., Poll-The, B. T., Waterham, H. R., Wanders, R. J. A., Paediatric Neurology, Paediatric Metabolic Diseases, Neurology, and Laboratory Genetic Metabolic Diseases

Subjects
lipids (amino acids, peptides, and proteins)
Abstract

OBJECTIVE: To identify prognostic markers reflecting the extent of peroxisome dysfunction in primary skin fibroblasts from patients with peroxisome biogenesis disorders (PBD). BACKGROUND: PBD are a genetically heterogeneous group of disorders due to defects in at least 11 distinct genes. Zellweger syndrome is the prototype of this group of disorders, with neonatal adrenoleukodystrophy and infantile Refsum disease as milder variants. Common to these three disorders are liver disease, variable neurodevelopmental delay, retinopathy, and perceptive deafness. Because genotype-phenotype studies are complicated by the genetic heterogeneity among patients with PBD, the authors evaluated a series of biochemical markers as a measure of peroxisome dysfunction in skin fibroblasts. METHODS: Multiple peroxisomal functions including de novo plasmalogen synthesis, dihydroxyacetonephosphate acyltransferase (DHAPAT) activity, C26:0/C22:0 ratio, C26:0 and pristanic acid beta-oxidation, and phytanic acid alpha-oxidation were analyzed in fibroblasts from a series of patients with defined clinical phenotypes. RESULTS: A poor correlation with age at death was found for de novo plasmalogen synthesis, C26:0/C22:0 ratio, and phytanic acid alpha-oxidation. A fairly good correlation was found for pristanic acid beta-oxidation, but the best correlation was found for DHAPAT activity and C26:0 beta-oxidation. A mathematic combination of DHAPAT activity and C26:0 beta-oxidation showed an even better correlation. CONCLUSIONS: DHAPAT activity and C26:0 beta-oxidation are the best markers in predicting life expectancy of patients with PBD. Combination of both markers gives an even better prediction. These results contribute to the management of patients with PBD

Published
2002

43. Identification of the peroxisomal beta-oxidation enzymes involved in the biosynthesis of docosahexaenoic acid

Author

Ferdinandusse, S., Denis, S., Mooijer, P. A., Zhang, Z., Reddy, J. K., Spector, A. A., Wanders, R. J., and Other departments

Subjects
lipids (amino acids, peptides, and proteins)
Abstract

DHA (C22:6n-3) is an important PUFA implicated in a number of (patho)physiological processes. For a long time, the exact mechanism of DHA formation has remained unclear, but now it is known that it involves the production of tetracosahexaenoic acid (C24:6n-3) from dietary linolenic acid (C18:3n-3) via a series of elongation and desaturation reactions, followed by beta-oxidation of C24:6n-3 to C22:6n-3. Although DHA is deficient in patients lacking peroxisomes, the intracellular site of retroconversion of C24:6n-3 has remained controversial. By making use of fibroblasts from patients with defined mitochondrial and peroxisomal fatty acid oxidation defects, we show in this article that peroxisomes, and not mitochondria, are involved in DHA formation by catalyzing the beta-oxidation of C24:6n-3 to C22:6n-3. Additional studies of fibroblasts from patients with X-linked adrenoleukodystrophy, straight-chain acyl-CoA oxidase (SCOX) deficiency, d-bifunctional protein (DBP) deficiency, and rhizomelic chondrodysplasia punctata type 1, and of fibroblasts from l-bifunctional protein and sterol carrier protein X (SCPx) knockout mice, show that the main enzymes involved in beta-oxidation of C24:6n-3 to C22:6n-3 are SCOX, DBP, and both 3-ketoacyl-CoA thiolase and SCPx. These findings are of importance for the treatment of patients with a defect in peroxisomal beta-oxidation

Published
2001

44. Carnitine palmityl transferase I deficiency

Author

Al-Aqeel, A. I., Rashed, M. S., Ruiter, J. P., Al-Husseini, H. F., Al-Amoudi, M. S., Wanders, R. J., and Other departments

Abstract

Carnitine palmityl transferase I is the key enzyme in the carnitine dependent transport of long chain fatty acids across the mitochondrial inner membrane and its deficiency results in a decrease rate of fatty acids beta-oxidation with decreased energy production. We reported a family of 3 affected siblings who are the product of a first degree cousin marriage. The first 2 presented with typical Reye-like syndrome with unconsciousness, hepatomegaly, hypoglycemia, hyperammonemia and very high liver enzymes. Liver biopsy showed steatosis. On screening of the complete family, the 3rd sibling was found to have hepatomegaly. The 3 siblings showed an acyl carnitine profile with very high free carnitine with almost absent long chain acyl carnitines, suggestive of carnitine palmityl transferase I deficiency. This was confirmed by enzyme analyses in fibroblast cultures. These patients were effectively treated with a diet high in carbohydrate, low in long chain fatty acids with medium chain triglycerides. In conclusion, carnitine palmityl transferase I deficiency is an important cause of Reye-like syndrome, which may be treated easily with very good results if detected early in life

Published
2001

45. Peroxisomal fatty acid alpha- and beta-oxidation in humans: enzymology, peroxisomal metabolite transporters and peroxisomal diseases

Author

Wanders, R. J., Vreken, P., Ferdinandusse, S., Jansen, G. A., Waterham, H. R., van Roermund, C. W., van Grunsven, E. G., and Other departments

Abstract

Peroxisomes are subcellular organelles with an indispensable role in cellular metabolism. The importance of peroxisomes for humans is stressed by the existence of a group of genetic diseases in humans in which there is an impairment in one or more peroxisomal functions. Most of these functions have to do with lipid metabolism including the alpha- and beta-oxidation of fatty acids. Here we describe the current state of knowledge about peroxisomal fatty acid alpha- and beta-oxidation with particular emphasis on the following: (1) the substrates beta-oxidized in peroxisomes; (2) the enzymology of the alpha- and beta-oxidation systems; (3) the permeability properties of the peroxisomal membrane and the role of the different transporters therein; (4) the interaction with other subcellular compartments, including the mitochondria, which are the ultimate site of NADH re-oxidation and full degradation of acetyl-CoA to CO(2) and water; and (5) the different disorders of peroxisomal alpha- and beta-oxidation

Published
2001

46. Organization of the mevalonate kinase (MVK) gene and identification of novel mutations causing mevalonic aciduria and hyperimmunoglobulinaemia D and periodic fever syndrome (vol 9, pg 253, 2001)

Author

Houten, S. M., Koster, J., Romeijn, G. J., Frenkel, J., Di Rocco, M., Caruso, U., Landrieu, P., Kelley, R. I., Kuis, W., Poll-The, B. T., Gibson, K. M., Wanders, R. J. A., Waterham, H. R., Other departments, AGEM - Inborn errors of metabolism, and Laboratory Genetic Metabolic Diseases

Published
2001

47. Plasma analysis of di- and trihydroxycholestanoic acid diastereoisomers in peroxisomal alpha-methylacyl-CoA racemase deficiency

Author

Ferdinandusse, S., Overmars, H., Denis, S., Waterham, H. R., Wanders, R. J., Vreken, P., and Other departments

Abstract

We identified a new peroxisomal disorder caused by a deficiency of the enzyme alpha-methylacyl-coenzyme A (CoA) racemase. Patients with this disorder show elevated plasma levels of pristanic acid and the bile acid intermediates di- and trihydroxycholestanoic acid (DHCA and THCA), which are all substrates for the peroxisomal beta-oxidation system. alpha-Methylacyl-CoA racemase plays an important role in the beta-oxidation of branched-chain fatty acids and fatty acid derivatives because it catalyzes the conversion of several (2R)-methyl-branched-chain fatty acyl-CoAs to their (2S)-isomers. Only stereoisomers with the 2-methyl group in the (S)-configuration can be degraded via beta-oxidation. In this study we used liquid chromatography/tandem mass spectrometry (LC-MS/MS) to analyze the bile acid intermediates that accumulate in plasma from patients with a deficiency of alpha-methylacyl-CoA racemase and, for comparison, in plasma from patients with Zellweger syndrome and patients with cholestatic liver disease.We found that racemase-deficient patients accumulate exclusively the (R)-isomer of free and taurine-conjugated DHCA and THCA, whereas in plasma of patients with Zellweger syndrome and patients with cholestatic liver disease both isomers were present. On the basis of these results we describe an easy and reliable method for the diagnosis of alpha-methylacyl-CoA racemase-deficient patients by plasma analysis. Our results also show that alpha-methylacyl-CoA racemase plays a unique role in bile acid formation. - Ferdinandusse, S., H. Overmars, S. Denis, H. R. Waterham, R. J. A. Wanders, and P. Vreken. Plasma analysis of di- and trihydroxycholestanoic acid diastereoisomers in peroxisomal alpha-methylacyl-CoA racemase deficiency. J. Lipid Res. 2001. 42: 137;-141

Published
2001

48. Targeted fluorescent probes in peroxisome function

Author

Dansen, T. B., Pap, E. H. W., Wanders, R. J., Wirtz, K. W., and Other departments

Abstract

Fluorescent peptides form a new generation of analytical tools for visualizing intracellular processes and molecular interactions at the level of single cells. The peptide-based reporters combine the sensitivity of fluorescence detection with the information specificity of amino acid sequences. Recently we have succeeded in targeting a fluorescent heptapeptide (acetyl-CKGGAKL) carrying a peroxisomal targeting signal (PTS1) to peroxisomes in intact cells. The fluorophores conjugated to the PTS1-peptide were fluorescein, BODIPY and the pH-sensitive SNAFL-2. When added to cells, these fluorescent peptides were internalized at 37 degrees C and typically visible in the cell after 15 min or less. Cells lacking an active peroxisomal protein import system, as in the case of Zellweger syndrome, were stained diffusely throughout the cell. Uptake of the peptide probes was not inhibited at 4 degrees C or when the cells were depleted of ATP. Under these conditions translocation to peroxisomes was blocked. This indicates that the uptake by cells is diffusion-driven and not an active process. Using the SNAFL-2-PTS1 peptide, we established by ratio-imaging that peroxisomes of human fibroblasts have an internal pH of 8.2. The concurrent pH gradient over the peroxisomal membrane was dissipated when an ionophore (CCCP) was added. In fibroblasts of chondrodysplasia punctata patients with defects in the peroxisomal import of proteins carrying a PTS2 sequence, import of the PTS1-peptide probe into peroxisomes appeared normal, but these peroxisomes have a pH of 6.8 equal to that of the cytosol. Coupling different fluorophores to the PTS1-peptide offers the possibility of determining in time and space as to how peroxisomes function in living cells

Published
2001

50. Subcellular localization and physiological role of alpha-methylacyl-CoA racemase

Author

Ferdinandusse, S., Denis, S., IJlst, L., Dacremont, G., Waterham, H. R., Wanders, R. J., and Other departments

Abstract

alpha-Methylacyl-CoA racemase plays an important role in the beta-oxidation of branched-chain fatty acids and fatty acid derivatives because it catalyzes the conversion of several (2R)-methyl-branched-chain fatty acyl-CoAs to their (S)-stereoisomers. Only stereoisomers with the 2-methyl group in the (S)-configuration can be degraded via beta-oxidation. Patients with a deficiency of alpha-methylacyl-CoA racemase accumulate in their plasma pristanic acid and the bile acid intermediates di- and trihydroxycholestanoic acid, which are all substrates of the peroxisomal beta-oxidation system. Subcellular fractionation experiments, however, revealed that both in humans and rats alpha-methylacyl-CoA racemase is bimodally distributed to both the peroxisome and the mitochondrion. Our findings show that the peroxisomal and mitochondrial enzymes are produced from the same gene and that, as a consequence, the bimodal distribution pattern must be the result of differential targeting of the same gene product. In addition, we investigated the physiological role of the enzyme in the mitochondrion. Both in vitro studies with purified heterologously expressed protein and in vivo studies in fibroblasts of patients with an alpha-methylacyl-CoA racemase deficiency revealed that the mitochondrial enzyme plays a crucial role in the mitochondrial beta-oxidation of the breakdown products of pristanic acid byconverting (2R,6)-dimethylheptanoyl-CoA to its (S)-stereoisomer

Published
2000

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