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1. Neuroblastoma stage 4S: Tumor regression rate and risk factors of progressive disease

Author

Tas, M.L. (Michelle L.), Nagtegaal, M. (Michelle), Kraal, K.C.J.M. (Kathelijne C.J.M.), Tytgat, G.A.M. (Godelieve ), Abeling, N.G.G.M. (Nicolaas), Pluijm, S.M.F. (Saskia), Zwaan, C.M. (Michel), Keizer, B. (Bart) de, Molenaar, J. (Jan), Noesel, M.M. (Max) van, Tas, M.L. (Michelle L.), Nagtegaal, M. (Michelle), Kraal, K.C.J.M. (Kathelijne C.J.M.), Tytgat, G.A.M. (Godelieve ), Abeling, N.G.G.M. (Nicolaas), Pluijm, S.M.F. (Saskia), Zwaan, C.M. (Michel), Keizer, B. (Bart) de, Molenaar, J. (Jan), and Noesel, M.M. (Max) van

Abstract

Background: The clinical course of neuroblastoma stage 4S or MS is characterized by a high rate of spontaneous tumor regression and favorable outcome. However, the clinical course and rate of the regression are poorly understood. Methods: A retrospective cohort study was performed, including all patients with stage 4S neuroblastoma without MYCN amplification, from two Dutch centers between 1972 and 2012. We investigated the clinical characteristics, the biochemical activity reflected in urinary catecholamine excretion, and radiological imaging to describe the kinetics of tumor regression, therapy response and outcome. Results: The cohort of 31 patients reached a 10-year overall survival of 84% ± 7% (median follow-up 16 years; range, 3.3-39). During the regressive phase, liver size normalized in 91% of the patients and catecholamine excretion in 83%, both after a median of two months (liver size: range, 0-131; catecholamines: range, 0-158). The primary tumors completely regressed in 69% after 13 months (range, 6-73), and the liver architecture normalize

Published
2019
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3. Two Greek siblings with sepiapterin reductase deficiency.

Author

Verbeek, M.M., Willemsen, M.A.A.P., Wevers, R.A., Lagerwerf, A.J., Abeling, N.G.G.M., Blau, N., Thony, B., Vargiami, E., Zafeiriou, D.I., Verbeek, M.M., Willemsen, M.A.A.P., Wevers, R.A., Lagerwerf, A.J., Abeling, N.G.G.M., Blau, N., Thony, B., Vargiami, E., and Zafeiriou, D.I.

Abstract

Contains fulltext : 70559.pdf (publisher's version ) (Closed access), BACKGROUND: Sepiapterin reductase (SR) deficiency is a rare inherited disorder of neurotransmitter metabolism; less than 25 cases have been described in the literature so far. METHODS: We describe the clinical history and extensive cerebrospinal fluid (CSF) and urine examination of two Greek siblings with the diagnosis of SR deficiency. The diagnosis was confirmed by enzyme activity measurement in cultured fibroblasts and by mutation analysis. RESULTS: Both patients suffered from a progressive and complex L-dopa responsive movement disorder. Very low concentrations of the neurotransmitter metabolites homovanillic acid (HVA), 5-hydroxyindolacetic acid (5-HIAA) and 3-methoxy-4-hydroxyphenylethyleneglycol (MHPG) were observed in CSF. CSF neopterin and biopterin concentrations were abnormal in one case only, whereas in both cases sepiapterin concentrations were abnormally high and 5-hydroxytryptophan was undetectable. Urine concentrations of HVA, 5-HIAA and vanillyl mandelic acid (VMA) were decreased in both cases. Both patients had no detectable SR enzyme activity in primary dermal fibroblasts, and upon analysis of genomic DNA revealed the same homozygous point mutation introducing a premature stop codon into the reading frame of the SPR gene (mutant allele K251X). CONCLUSIONS: Our cases illustrate that, apart from HVA and 5-HIAA analysis, the specific quantification of sepiapterin in CSF, rather than neopterin and biopterin alone, is crucial to the final diagnosis of SR deficiency. In addition, urinary concentrations of neurotransmitter metabolites may be abnormal in SR deficiency and may provide an initial indication of SR deficiency before CSF analysis is performed. The known, impressive beneficial response of SR deficient patients to treatment with L-dopa, is illustrated again in our cases.

Published
2008

4. Two Greek siblings with sepiapterin reductase deficiency.

Author

Verbeek, M.M., Willemsen, M.A.A.P., Wevers, R.A., Lagerwerf, A.J., Abeling, N.G.G.M., Blau, N., Thony, B., Vargiami, E., Zafeiriou, D.I., Verbeek, M.M., Willemsen, M.A.A.P., Wevers, R.A., Lagerwerf, A.J., Abeling, N.G.G.M., Blau, N., Thony, B., Vargiami, E., and Zafeiriou, D.I.

Abstract

Contains fulltext : 70559.pdf (publisher's version ) (Closed access), BACKGROUND: Sepiapterin reductase (SR) deficiency is a rare inherited disorder of neurotransmitter metabolism; less than 25 cases have been described in the literature so far. METHODS: We describe the clinical history and extensive cerebrospinal fluid (CSF) and urine examination of two Greek siblings with the diagnosis of SR deficiency. The diagnosis was confirmed by enzyme activity measurement in cultured fibroblasts and by mutation analysis. RESULTS: Both patients suffered from a progressive and complex L-dopa responsive movement disorder. Very low concentrations of the neurotransmitter metabolites homovanillic acid (HVA), 5-hydroxyindolacetic acid (5-HIAA) and 3-methoxy-4-hydroxyphenylethyleneglycol (MHPG) were observed in CSF. CSF neopterin and biopterin concentrations were abnormal in one case only, whereas in both cases sepiapterin concentrations were abnormally high and 5-hydroxytryptophan was undetectable. Urine concentrations of HVA, 5-HIAA and vanillyl mandelic acid (VMA) were decreased in both cases. Both patients had no detectable SR enzyme activity in primary dermal fibroblasts, and upon analysis of genomic DNA revealed the same homozygous point mutation introducing a premature stop codon into the reading frame of the SPR gene (mutant allele K251X). CONCLUSIONS: Our cases illustrate that, apart from HVA and 5-HIAA analysis, the specific quantification of sepiapterin in CSF, rather than neopterin and biopterin alone, is crucial to the final diagnosis of SR deficiency. In addition, urinary concentrations of neurotransmitter metabolites may be abnormal in SR deficiency and may provide an initial indication of SR deficiency before CSF analysis is performed. The known, impressive beneficial response of SR deficient patients to treatment with L-dopa, is illustrated again in our cases.

Published
2008

5. Two Greek siblings with sepiapterin reductase deficiency.

Author

Verbeek, M.M., Willemsen, M.A.A.P., Wevers, R.A., Lagerwerf, A.J., Abeling, N.G.G.M., Blau, N., Thony, B., Vargiami, E., Zafeiriou, D.I., Verbeek, M.M., Willemsen, M.A.A.P., Wevers, R.A., Lagerwerf, A.J., Abeling, N.G.G.M., Blau, N., Thony, B., Vargiami, E., and Zafeiriou, D.I.

Abstract

Contains fulltext : 70559.pdf (publisher's version ) (Closed access), BACKGROUND: Sepiapterin reductase (SR) deficiency is a rare inherited disorder of neurotransmitter metabolism; less than 25 cases have been described in the literature so far. METHODS: We describe the clinical history and extensive cerebrospinal fluid (CSF) and urine examination of two Greek siblings with the diagnosis of SR deficiency. The diagnosis was confirmed by enzyme activity measurement in cultured fibroblasts and by mutation analysis. RESULTS: Both patients suffered from a progressive and complex L-dopa responsive movement disorder. Very low concentrations of the neurotransmitter metabolites homovanillic acid (HVA), 5-hydroxyindolacetic acid (5-HIAA) and 3-methoxy-4-hydroxyphenylethyleneglycol (MHPG) were observed in CSF. CSF neopterin and biopterin concentrations were abnormal in one case only, whereas in both cases sepiapterin concentrations were abnormally high and 5-hydroxytryptophan was undetectable. Urine concentrations of HVA, 5-HIAA and vanillyl mandelic acid (VMA) were decreased in both cases. Both patients had no detectable SR enzyme activity in primary dermal fibroblasts, and upon analysis of genomic DNA revealed the same homozygous point mutation introducing a premature stop codon into the reading frame of the SPR gene (mutant allele K251X). CONCLUSIONS: Our cases illustrate that, apart from HVA and 5-HIAA analysis, the specific quantification of sepiapterin in CSF, rather than neopterin and biopterin alone, is crucial to the final diagnosis of SR deficiency. In addition, urinary concentrations of neurotransmitter metabolites may be abnormal in SR deficiency and may provide an initial indication of SR deficiency before CSF analysis is performed. The known, impressive beneficial response of SR deficient patients to treatment with L-dopa, is illustrated again in our cases.

Published
2008

6. Genetic analysis of the first 4 patients with beta-ureidopropionase deficiency.

Author

Kuilenburg, A.B.P. van, Meinsma, R., Assman, B., Hoffman, G.F., Voit, T., Ribes, A., Lorente, I., Busch, R., Mayatepek, E., Abeling, N.G.G.M., Wevers, R.A., Rutsch, F., Gennip, A.H. van, Kuilenburg, A.B.P. van, Meinsma, R., Assman, B., Hoffman, G.F., Voit, T., Ribes, A., Lorente, I., Busch, R., Mayatepek, E., Abeling, N.G.G.M., Wevers, R.A., Rutsch, F., and Gennip, A.H. van

Abstract

Item does not contain fulltext, beta-Ureidopropionase is the third enzyme of the pyrimidine degradation pathway and it catalyses the irreversible hydrolysis of N-carbamyl-ss-aminoisobutyric acid or N-carbamyl-ss-alanine to beta-aminoisobutyric acid or ss-alanine, ammonia, and CO2. Analysis of the beta-ureidopropionase gene (UPB1) of the first 4 patients presenting with a complete enzyme deficiency, revealed the presence of 2 splice-site mutations (IVS1-2A>G and IVS8-1G>A) and one missense mutation (A85E). RT-PCR analysis of the complete beta-ureidopropionase cDNA suggested that both splice-site mutations lead to a variety of alternative splice variants, with deletions of a single or several exons. The alanine at position 85 was not conserved in other eukaryotic beta-ureidopropionase protein sequences.

Published
2006

7. Genetic analysis of the first 4 patients with beta-ureidopropionase deficiency.

Author

Kuilenburg, A.B.P. van, Meinsma, R., Assman, B., Hoffman, G.F., Voit, T., Ribes, A., Lorente, I., Busch, R., Mayatepek, E., Abeling, N.G.G.M., Wevers, R.A., Rutsch, F., Gennip, A.H. van, Kuilenburg, A.B.P. van, Meinsma, R., Assman, B., Hoffman, G.F., Voit, T., Ribes, A., Lorente, I., Busch, R., Mayatepek, E., Abeling, N.G.G.M., Wevers, R.A., Rutsch, F., and Gennip, A.H. van

Abstract

Item does not contain fulltext, beta-Ureidopropionase is the third enzyme of the pyrimidine degradation pathway and it catalyses the irreversible hydrolysis of N-carbamyl-ss-aminoisobutyric acid or N-carbamyl-ss-alanine to beta-aminoisobutyric acid or ss-alanine, ammonia, and CO2. Analysis of the beta-ureidopropionase gene (UPB1) of the first 4 patients presenting with a complete enzyme deficiency, revealed the presence of 2 splice-site mutations (IVS1-2A>G and IVS8-1G>A) and one missense mutation (A85E). RT-PCR analysis of the complete beta-ureidopropionase cDNA suggested that both splice-site mutations lead to a variety of alternative splice variants, with deletions of a single or several exons. The alanine at position 85 was not conserved in other eukaryotic beta-ureidopropionase protein sequences.

Published
2006

8. Genetic analysis of the first 4 patients with beta-ureidopropionase deficiency.

Author

Kuilenburg, A.B.P. van, Meinsma, R., Assman, B., Hoffman, G.F., Voit, T., Ribes, A., Lorente, I., Busch, R., Mayatepek, E., Abeling, N.G.G.M., Wevers, R.A., Rutsch, F., Gennip, A.H. van, Kuilenburg, A.B.P. van, Meinsma, R., Assman, B., Hoffman, G.F., Voit, T., Ribes, A., Lorente, I., Busch, R., Mayatepek, E., Abeling, N.G.G.M., Wevers, R.A., Rutsch, F., and Gennip, A.H. van

Abstract

Item does not contain fulltext, beta-Ureidopropionase is the third enzyme of the pyrimidine degradation pathway and it catalyses the irreversible hydrolysis of N-carbamyl-ss-aminoisobutyric acid or N-carbamyl-ss-alanine to beta-aminoisobutyric acid or ss-alanine, ammonia, and CO2. Analysis of the beta-ureidopropionase gene (UPB1) of the first 4 patients presenting with a complete enzyme deficiency, revealed the presence of 2 splice-site mutations (IVS1-2A>G and IVS8-1G>A) and one missense mutation (A85E). RT-PCR analysis of the complete beta-ureidopropionase cDNA suggested that both splice-site mutations lead to a variety of alternative splice variants, with deletions of a single or several exons. The alanine at position 85 was not conserved in other eukaryotic beta-ureidopropionase protein sequences.

Published
2006

9. beta-Ureidopropionase deficiency: an inborn error of pyrimidine degradation associated with neurological abnormalities.

Author

Kuilenburg, A.B.P. van, Meinsma, R., Beke, E., Assmann, B., Ribes, A., Lorente, I., Busch, R., Mayatepek, E., Abeling, N.G.G.M., Cruchten, A.C. van, Stroomer, A.E., Lenthe, H. van, Zoetekouw, L., Kulik, W., Hoffmann, G.F., Voit, T., Wevers, R.A., Rutsch, F., Gennip, A.H. van, Kuilenburg, A.B.P. van, Meinsma, R., Beke, E., Assmann, B., Ribes, A., Lorente, I., Busch, R., Mayatepek, E., Abeling, N.G.G.M., Cruchten, A.C. van, Stroomer, A.E., Lenthe, H. van, Zoetekouw, L., Kulik, W., Hoffmann, G.F., Voit, T., Wevers, R.A., Rutsch, F., and Gennip, A.H. van

Abstract

Contains fulltext : 58877.pdf (publisher's version ) (Closed access), beta-Ureidopropionase deficiency is an inborn error of the pyrimidine degradation pathway, affecting the cleavage of N-carbamyl-beta-alanine and N-carbamyl-beta-aminoisobutyric acid. In this study, we report the elucidation of the genetic basis underlying a beta-ureidopropionase deficiency in four patients presenting with neurological abnormalities and strongly elevated levels of N-carbamyl-beta-alanine and N-carbamyl-beta-aminoisobutyric acid in plasma, cerebrospinal fluid and urine. No beta-ureidopropionase activity could be detected in a liver biopsy obtained from one of the patients, which reflected the complete absence of the beta-ureidopropionase protein. Analysis of the beta-ureidopropionase gene (UPB1) of these patients revealed the presence of two splice-site mutations (IVS1-2A>G and IVS8-1G>A) and one missense mutation (A85E). Heterologous expression of the mutant enzyme in Escherichia coli showed that the A85E mutation resulted in a mutant beta-ureidopropionase enzyme without residual activity. Our results demonstrate that the N-carbamyl-beta-amino aciduria in these patients is due to a deficiency of beta-ureidopropionase, which is caused by mutations in the UPB1 gene. Furthermore, an altered homeostasis of beta-aminoisobutyric acid and/or increased oxidative stress might contribute to some of the clinical abnormalities encountered in patients with a beta-ureidopropionase deficiency. An analysis of the presence of the two splice site mutations and the missense mutation in 95 controls identified one individual who proved to be heterozygous for the IVS8-1G>A mutation. Thus, a beta-ureidopropionase deficiency might not be as rare as is generally considered.

Published
2004

10. beta-Ureidopropionase deficiency: an inborn error of pyrimidine degradation associated with neurological abnormalities.

Author

Kuilenburg, A.B.P. van, Meinsma, R., Beke, E., Assmann, B., Ribes, A., Lorente, I., Busch, R., Mayatepek, E., Abeling, N.G.G.M., Cruchten, A.C. van, Stroomer, A.E., Lenthe, H. van, Zoetekouw, L., Kulik, W., Hoffmann, G.F., Voit, T., Wevers, R.A., Rutsch, F., Gennip, A.H. van, Kuilenburg, A.B.P. van, Meinsma, R., Beke, E., Assmann, B., Ribes, A., Lorente, I., Busch, R., Mayatepek, E., Abeling, N.G.G.M., Cruchten, A.C. van, Stroomer, A.E., Lenthe, H. van, Zoetekouw, L., Kulik, W., Hoffmann, G.F., Voit, T., Wevers, R.A., Rutsch, F., and Gennip, A.H. van

Abstract

Contains fulltext : 58877.pdf (publisher's version ) (Closed access), beta-Ureidopropionase deficiency is an inborn error of the pyrimidine degradation pathway, affecting the cleavage of N-carbamyl-beta-alanine and N-carbamyl-beta-aminoisobutyric acid. In this study, we report the elucidation of the genetic basis underlying a beta-ureidopropionase deficiency in four patients presenting with neurological abnormalities and strongly elevated levels of N-carbamyl-beta-alanine and N-carbamyl-beta-aminoisobutyric acid in plasma, cerebrospinal fluid and urine. No beta-ureidopropionase activity could be detected in a liver biopsy obtained from one of the patients, which reflected the complete absence of the beta-ureidopropionase protein. Analysis of the beta-ureidopropionase gene (UPB1) of these patients revealed the presence of two splice-site mutations (IVS1-2A>G and IVS8-1G>A) and one missense mutation (A85E). Heterologous expression of the mutant enzyme in Escherichia coli showed that the A85E mutation resulted in a mutant beta-ureidopropionase enzyme without residual activity. Our results demonstrate that the N-carbamyl-beta-amino aciduria in these patients is due to a deficiency of beta-ureidopropionase, which is caused by mutations in the UPB1 gene. Furthermore, an altered homeostasis of beta-aminoisobutyric acid and/or increased oxidative stress might contribute to some of the clinical abnormalities encountered in patients with a beta-ureidopropionase deficiency. An analysis of the presence of the two splice site mutations and the missense mutation in 95 controls identified one individual who proved to be heterozygous for the IVS8-1G>A mutation. Thus, a beta-ureidopropionase deficiency might not be as rare as is generally considered.

Published
2004

11. beta-Ureidopropionase deficiency: an inborn error of pyrimidine degradation associated with neurological abnormalities.

Author

Kuilenburg, A.B.P. van, Meinsma, R., Beke, E., Assmann, B., Ribes, A., Lorente, I., Busch, R., Mayatepek, E., Abeling, N.G.G.M., Cruchten, A.C. van, Stroomer, A.E., Lenthe, H. van, Zoetekouw, L., Kulik, W., Hoffmann, G.F., Voit, T., Wevers, R.A., Rutsch, F., Gennip, A.H. van, Kuilenburg, A.B.P. van, Meinsma, R., Beke, E., Assmann, B., Ribes, A., Lorente, I., Busch, R., Mayatepek, E., Abeling, N.G.G.M., Cruchten, A.C. van, Stroomer, A.E., Lenthe, H. van, Zoetekouw, L., Kulik, W., Hoffmann, G.F., Voit, T., Wevers, R.A., Rutsch, F., and Gennip, A.H. van

Abstract

Contains fulltext : 58877.pdf (publisher's version ) (Closed access), beta-Ureidopropionase deficiency is an inborn error of the pyrimidine degradation pathway, affecting the cleavage of N-carbamyl-beta-alanine and N-carbamyl-beta-aminoisobutyric acid. In this study, we report the elucidation of the genetic basis underlying a beta-ureidopropionase deficiency in four patients presenting with neurological abnormalities and strongly elevated levels of N-carbamyl-beta-alanine and N-carbamyl-beta-aminoisobutyric acid in plasma, cerebrospinal fluid and urine. No beta-ureidopropionase activity could be detected in a liver biopsy obtained from one of the patients, which reflected the complete absence of the beta-ureidopropionase protein. Analysis of the beta-ureidopropionase gene (UPB1) of these patients revealed the presence of two splice-site mutations (IVS1-2A>G and IVS8-1G>A) and one missense mutation (A85E). Heterologous expression of the mutant enzyme in Escherichia coli showed that the A85E mutation resulted in a mutant beta-ureidopropionase enzyme without residual activity. Our results demonstrate that the N-carbamyl-beta-amino aciduria in these patients is due to a deficiency of beta-ureidopropionase, which is caused by mutations in the UPB1 gene. Furthermore, an altered homeostasis of beta-aminoisobutyric acid and/or increased oxidative stress might contribute to some of the clinical abnormalities encountered in patients with a beta-ureidopropionase deficiency. An analysis of the presence of the two splice site mutations and the missense mutation in 95 controls identified one individual who proved to be heterozygous for the IVS8-1G>A mutation. Thus, a beta-ureidopropionase deficiency might not be as rare as is generally considered.

Published
2004

12. Prolidase deficiency diagnosed by 1H-NMR spectroscopy of urine

Author

Moolenaar, S.H., Engelke, U.F.H., Abeling, N.G.G.M., Mandel, H., Duran, M., Wevers, R.A., Moolenaar, S.H., Engelke, U.F.H., Abeling, N.G.G.M., Mandel, H., Duran, M., and Wevers, R.A.

Abstract

Item does not contain fulltext

Published
2002

13. Prolidase deficiency diagnosed by 1H-NMR spectroscopy of urine

Author

Moolenaar, S.H., Engelke, U.F.H., Abeling, N.G.G.M., Mandel, H., Duran, M., Wevers, R.A., Moolenaar, S.H., Engelke, U.F.H., Abeling, N.G.G.M., Mandel, H., Duran, M., and Wevers, R.A.

Abstract

Item does not contain fulltext

Published
2002

14. Prolidase deficiency diagnosed by 1H-NMR spectroscopy of urine

Author

Moolenaar, S.H., Engelke, U.F.H., Abeling, N.G.G.M., Mandel, H., Duran, M., Wevers, R.A., Moolenaar, S.H., Engelke, U.F.H., Abeling, N.G.G.M., Mandel, H., Duran, M., and Wevers, R.A.

Abstract

Item does not contain fulltext

Published
2002

15. Tyrosine hydroxylase deficiency unresponsive to L-DOPA treatment with unusual clinical and biochemical presentation.

Author

Lonlay, P. de, Nassogne, M.C., Gennip, A.H. van, Cruchten, A.C. van, Bilette de Villemeur, T., Cretz, M., Stoll, C., Launay, J.M., Steenbergen-Spanjers, G.C.H., Heuvel, L.P.W.J. van den, Wevers, R.A., Saudubray, J.M., Abeling, N.G.G.M., Lonlay, P. de, Nassogne, M.C., Gennip, A.H. van, Cruchten, A.C. van, Bilette de Villemeur, T., Cretz, M., Stoll, C., Launay, J.M., Steenbergen-Spanjers, G.C.H., Heuvel, L.P.W.J. van den, Wevers, R.A., Saudubray, J.M., and Abeling, N.G.G.M.

Abstract

Item does not contain fulltext

Published
2000

17. Tyrosine hydroxylase deficiency unresponsive to L-DOPA treatment with unusual clinical and biochemical presentation.

Author

Lonlay, P. de, Nassogne, M.C., Gennip, A.H. van, Cruchten, A.C. van, Bilette de Villemeur, T., Cretz, M., Stoll, C., Launay, J.M., Steenbergen-Spanjers, G.C.H., Heuvel, L.P.W.J. van den, Wevers, R.A., Saudubray, J.M., Abeling, N.G.G.M., Lonlay, P. de, Nassogne, M.C., Gennip, A.H. van, Cruchten, A.C. van, Bilette de Villemeur, T., Cretz, M., Stoll, C., Launay, J.M., Steenbergen-Spanjers, G.C.H., Heuvel, L.P.W.J. van den, Wevers, R.A., Saudubray, J.M., and Abeling, N.G.G.M.

Abstract

Item does not contain fulltext

Published
2000

20. Tyrosine hydroxylase deficiency unresponsive to L-DOPA treatment with unusual clinical and biochemical presentation.

Author

Lonlay, P. de, Nassogne, M.C., Gennip, A.H. van, Cruchten, A.C. van, Bilette de Villemeur, T., Cretz, M., Stoll, C., Launay, J.M., Steenbergen-Spanjers, G.C.H., Heuvel, L.P.W.J. van den, Wevers, R.A., Saudubray, J.M., Abeling, N.G.G.M., Lonlay, P. de, Nassogne, M.C., Gennip, A.H. van, Cruchten, A.C. van, Bilette de Villemeur, T., Cretz, M., Stoll, C., Launay, J.M., Steenbergen-Spanjers, G.C.H., Heuvel, L.P.W.J. van den, Wevers, R.A., Saudubray, J.M., and Abeling, N.G.G.M.

Abstract

Item does not contain fulltext

Published
2000

23. Genotype and phenotype in patients with dihydropyrimidine dehydrogenase deficiency

Author

Kuilenburg, A.B.P. van, Vreken, P., Abeling, N.G.G.M., Bakker, H., Meinsma, R., Lenthe, G.H. van, Abreu, R.A. de, Smeitink, J.A.M., Kayserili, H., Apak, M.Y., Christensen, E., Holopainen, I., Pulkki, K., Riva, D., Botteon, G., Holme, E., Tulinius, M., Kleijer, W.J., Beemer, F.A., Duran, M., Niezen-Koning, K.E., Smit, G.P., Jakobs, C., Smit, L.M.E., Moog, U., Spaapen, L.J., Gennip, A.H. van, Kuilenburg, A.B.P. van, Vreken, P., Abeling, N.G.G.M., Bakker, H., Meinsma, R., Lenthe, G.H. van, Abreu, R.A. de, Smeitink, J.A.M., Kayserili, H., Apak, M.Y., Christensen, E., Holopainen, I., Pulkki, K., Riva, D., Botteon, G., Holme, E., Tulinius, M., Kleijer, W.J., Beemer, F.A., Duran, M., Niezen-Koning, K.E., Smit, G.P., Jakobs, C., Smit, L.M.E., Moog, U., Spaapen, L.J., and Gennip, A.H. van

Abstract

Item does not contain fulltext

Published
1999

25. Genotype and phenotype in patients with dihydropyrimidine dehydrogenase deficiency

Author

Kuilenburg, A.B.P. van, Vreken, P., Abeling, N.G.G.M., Bakker, H., Meinsma, R., Lenthe, G.H. van, Abreu, R.A. de, Smeitink, J.A.M., Kayserili, H., Apak, M.Y., Christensen, E., Holopainen, I., Pulkki, K., Riva, D., Botteon, G., Holme, E., Tulinius, M., Kleijer, W.J., Beemer, F.A., Duran, M., Niezen-Koning, K.E., Smit, G.P., Jakobs, C., Smit, L.M.E., Moog, U., Spaapen, L.J., Gennip, A.H. van, Kuilenburg, A.B.P. van, Vreken, P., Abeling, N.G.G.M., Bakker, H., Meinsma, R., Lenthe, G.H. van, Abreu, R.A. de, Smeitink, J.A.M., Kayserili, H., Apak, M.Y., Christensen, E., Holopainen, I., Pulkki, K., Riva, D., Botteon, G., Holme, E., Tulinius, M., Kleijer, W.J., Beemer, F.A., Duran, M., Niezen-Koning, K.E., Smit, G.P., Jakobs, C., Smit, L.M.E., Moog, U., Spaapen, L.J., and Gennip, A.H. van

Abstract

Item does not contain fulltext

Published
1999

27. Genotype and phenotype in patients with dihydropyrimidine dehydrogenase deficiency

Author

Kuilenburg, A.B.P. van, Vreken, P., Abeling, N.G.G.M., Bakker, H., Meinsma, R., Lenthe, G.H. van, Abreu, R.A. de, Smeitink, J.A.M., Kayserili, H., Apak, M.Y., Christensen, E., Holopainen, I., Pulkki, K., Riva, D., Botteon, G., Holme, E., Tulinius, M., Kleijer, W.J., Beemer, F.A., Duran, M., Niezen-Koning, K.E., Smit, G.P., Jakobs, C., Smit, L.M.E., Moog, U., Spaapen, L.J., Gennip, A.H. van, Kuilenburg, A.B.P. van, Vreken, P., Abeling, N.G.G.M., Bakker, H., Meinsma, R., Lenthe, G.H. van, Abreu, R.A. de, Smeitink, J.A.M., Kayserili, H., Apak, M.Y., Christensen, E., Holopainen, I., Pulkki, K., Riva, D., Botteon, G., Holme, E., Tulinius, M., Kleijer, W.J., Beemer, F.A., Duran, M., Niezen-Koning, K.E., Smit, G.P., Jakobs, C., Smit, L.M.E., Moog, U., Spaapen, L.J., and Gennip, A.H. van

Abstract

Item does not contain fulltext

Published
1999

39. Specific genetic deficiencies of the A and B isoenzymes of monoamine oxidase are characterized by distinct neurochemical and clinical phenotypes

Author

Lenders, J.W.M., Eisenhofer, G., Abeling, N.G.G.M., Berger, W., Murphy, D.L., Konings, H., Bleeker-Wagemakers, P.L.M., Kopin, I.J., Karoum, F., Gennip, A.H. van, Brunner, H.G., Lenders, J.W.M., Eisenhofer, G., Abeling, N.G.G.M., Berger, W., Murphy, D.L., Konings, H., Bleeker-Wagemakers, P.L.M., Kopin, I.J., Karoum, F., Gennip, A.H. van, and Brunner, H.G.

Abstract

Contains fulltext : 23002___.PDF (publisher's version ) (Open Access)

Published
1996

40. Specific genetic deficiencies of the A and B isoenzymes of monoamine oxidase are characterized by distinct neurochemical and clinical phenotypes

Author

Lenders, J.W.M., Eisenhofer, G., Abeling, N.G.G.M., Berger, W., Murphy, D.L., Konings, H., Bleeker-Wagemakers, P.L.M., Kopin, I.J., Karoum, F., Gennip, A.H. van, Brunner, H.G., Lenders, J.W.M., Eisenhofer, G., Abeling, N.G.G.M., Berger, W., Murphy, D.L., Konings, H., Bleeker-Wagemakers, P.L.M., Kopin, I.J., Karoum, F., Gennip, A.H. van, and Brunner, H.G.

Abstract

Item does not contain fulltext

Published
1996

43. Specific genetic deficiencies of the A and B isoenzymes of monoamine oxidase are characterized by distinct neurochemical and clinical phenotypes

Author

Lenders, J.W.M., Eisenhofer, G., Abeling, N.G.G.M., Berger, W., Murphy, D.L., Konings, H., Bleeker-Wagemakers, P.L.M., Kopin, I.J., Karoum, F., Gennip, A.H. van, Brunner, H.G., Lenders, J.W.M., Eisenhofer, G., Abeling, N.G.G.M., Berger, W., Murphy, D.L., Konings, H., Bleeker-Wagemakers, P.L.M., Kopin, I.J., Karoum, F., Gennip, A.H. van, and Brunner, H.G.

Abstract

Contains fulltext : 23002___.PDF (publisher's version ) (Open Access)

Published
1996

45. Specific genetic deficiencies of the A and B isoenzymes of monoamine oxidase are characterized by distinct neurochemical and clinical phenotypes

Author

Lenders, J.W.M., Eisenhofer, G., Abeling, N.G.G.M., Berger, W., Murphy, D.L., Konings, H., Bleeker-Wagemakers, P.L.M., Kopin, I.J., Karoum, F., Gennip, A.H. van, Brunner, H.G., Lenders, J.W.M., Eisenhofer, G., Abeling, N.G.G.M., Berger, W., Murphy, D.L., Konings, H., Bleeker-Wagemakers, P.L.M., Kopin, I.J., Karoum, F., Gennip, A.H. van, and Brunner, H.G.

Abstract

Contains fulltext : 23002___.PDF (publisher's version ) (Open Access)

Published
1996

47. 1H-NMR spectroscopie in lichaamsvloeistoffen en leucocyten

Author

Wevers, R.A., Engelke, U.F.H., Abeling, N.G.G.M., Abreu, R.A. de, Berg, G.B. van de, Heerschap, A., Wevers, R.A., Engelke, U.F.H., Abeling, N.G.G.M., Abreu, R.A. de, Berg, G.B. van de, and Heerschap, A.

Abstract

Item does not contain fulltext

Published
1995

50. 1H-NMR Spectroscopie in lichaamsvloeistoffen en leucocyten

Author

Wevers, R.A., Engelke, U.F.H., Abeling, N.G.G.M., Abreu, R.A. de, Berg, G.B. van de, Heerschap, A., Wevers, R.A., Engelke, U.F.H., Abeling, N.G.G.M., Abreu, R.A. de, Berg, G.B. van de, and Heerschap, A.

Abstract

Item does not contain fulltext

Published
1995

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