Your search keyword '"Zater M"' showing total 13 results

1. Mutation spectrum in the French cohort of galactosemic patients and structural simulation of 27 novel missense variations

Author

Boutron, A, Marabotti, Anna, Facchiano, A, Cheillan, D, Zater, M, Oliveira, C, Costa, C, Labrune, P, Brivet, M, Loisel, N, Morin, G, Barth, M, Altuzarra, C, Mesli, S, Rigalleau, V, Rhead, Mh, de Schrevel, G, Thauvin Robinet, C, Santos, A, Dobbelaere, D, Mention, K, Guffon, N, Cano, A, Feillet, F, Krempf, P, Pitelet, G, Bernard, O, Hermeziu, B, Gonzalez, E, Habes, D, Jacquemin, E, de Baulny, H, Roche, S, Debray, D, de Lonlay, P, Servais, A, Touati, G, Bednarek, N, Garnotel, R, Devaux, Am, Gay, C, Eyer, D, Baruteau, J, Broué, P, Labarthe, F, and Maillot, F.

Subjects

Adult, Galactosemias, Male, Adolescent, Endocrinology, Diabetes and Metabolism, In silico, DNA Mutational Analysis, Biology, medicine.disease_cause, Biochemistry, Cohort Studies, Exon, Endocrinology, Genetics, medicine, Humans, UTP-Hexose-1-Phosphate Uridylyltransferase, Missense mutation, Homology modeling, Child, Molecular Biology, Mutation, Protein Stability, Galactosemia, Infant, Exons, Middle Aged, medicine.disease, Introns, Molecular Docking Simulation, Protein Subunits, Phenotype, Child, Preschool, Female, Allelic heterogeneity, France

Abstract

Background Classic galactosemia refers to galactose-1-phosphate uridyltransferase (GALT) deficiency and is characterized by long-term complications of unknown mechanism and high allelic heterogeneity of GALT gene. Aim To report molecular characterization of GALT variations in 210 French families, to analyze the structural effects of novel missense variations and to assess informativity of structural data in predicting outcome. Methods Sequencing of exons and intron–exon junctions of GALT gene was completed in unsolved cases by analysis of a long range PCR product. Structural consequences of novel missense variations were predicted using a homology model of GALT protein and a semi-automated analysis which integrates simulation of variations, structural analyses and two web servers dedicated to identify mutation-induced change of protein stability. Results Forty four novel variations were identified, among them 27 nucleotide substitutions. In silico modeling of these missense variations showed that 12 variations are predicted to impair subunit interactions and/or active site conformation and that 23 variations modify H-bond or salt-bridge networks. Twenty variations decrease the global stability of the protein. Five variations had apparently no structural effect. Conclusion Our results expand the mutation spectrum in GALT gene and the list of GALT variations analyzed at the structural level, providing new data to assess the pathophysiology of galactosemia.

Published

2012

2. Molecular characterization of 82 patients with pyruvate dehydrogenase complex deficiency. Structural implications of novel amino acid substitutions in E1 protein

Author

Imbard, A., primary, Boutron, A., additional, Vequaud, C., additional, Zater, M., additional, de Lonlay, P., additional, Ogier de Baulny, H., additional, Barnerias, C., additional, Miné, M., additional, Marsac, C., additional, Saudubray, J.-M., additional, and Brivet, M., additional

Published

2011

3. Quantifying Undiscovered Resource Potential

Author

Zater, M., primary

Published

2009

4. Fructose 1,6-bisphosphatase deficiency: clinical, biochemical and genetic features in French patients.

Author

Lebigot E, Brassier A, Zater M, Imanci D, Feillet F, Thérond P, de Lonlay P, and Boutron A

Subjects

Base Sequence, Child, Preschool, Female, France, Fructose-1,6-Diphosphatase Deficiency blood, Gene Deletion, Humans, Infant, Infant, Newborn, Inheritance Patterns, Male, Molecular Sequence Data, Mutation, Missense, RNA Splice Sites genetics, Real-Time Polymerase Chain Reaction, Fructose-1,6-Diphosphatase Deficiency diagnosis, Fructose-1,6-Diphosphatase Deficiency genetics, Fructose-Bisphosphatase genetics

Abstract

Fructose-1,6-bisphosphatase (FBPase) deficiency is a very rare autosomal recessive disorder caused by a mutation of the fructose-1,6-bisphosphatase gene(FBP1). Disease is mainly revealed by hypoglycemia and lactic acidosis, both symptoms being characteristic for an enzymatic block in the last steps of the gluconeogenesis. Twelve patients with FBPase deficiency were diagnosed in France in the 2001-2013 period, using a diagnostic system based on a single blood sample which allows simultaneous enzyme activity measurement on mononuclear white blood cells and molecular analysis. Sequencing of exons and intron-exon junctions of FBP1 gene was completed in unsolved cases by a gene dosage assay developed for each exon. For most patients, first metabolic decompensation occurred before two years of age with a similar sequence: the triggering factors were fever, fasting, or decrease of food intake. However, diagnosis was made late at a mean age of 3 years, as mitochondrial defects or glycogen storage diseases were firstly suspected. Enzyme activity in leukocytes was dramatically decreased (<10%). Twelve different mutations were identified in 22 alleles among them seven were novels: one missense mutation c.472C > T, one point deletion c.48del, one point duplication c.865dupA, one deletion-insertion, and two splice mutations (c.427-1del and c.825 + 1G > A). We described the first intragenic deletion in FBP1 (g.97,364,754&#95;97,382,011del) in homozygous state. Our report also confirms that this very rare disease is misdiagnosed, as other energetic defects are firstly suspected.

Published

2015

5. Rapid screening of classic galactosemia patients: a proof-of-concept study using high-throughput FTIR analysis of plasma.

Author

Lacombe C, Untereiner V, Gobinet C, Zater M, Sockalingum GD, and Garnotel R

Subjects

Adult, Child, Child, Preschool, Diabetes Mellitus blood, Feasibility Studies, Female, Humans, Infant, Male, Principal Component Analysis, Support Vector Machine, Galactosemias blood, Galactosemias diagnosis, Spectroscopy, Fourier Transform Infrared

Abstract

Classic galactosemia is an autosomal recessive metabolic disease involving the galactose pathway, caused by the deficiency of galactose-1-phosphate uridyltransferase. Galactose accumulation induces in newborns many symptoms, such as liver disease, cataracts, and sepsis leading to death if untreated. Neonatal screening is developed and applied in many countries using several methods to detect galactose or its derived product accumulation in blood or urine. High-throughput FTIR spectroscopy was investigated as a potential tool in the current screening methods. IR spectra were obtained from blood plasma of healthy, diabetic, and galactosemic patients. The major spectral differences were in the carbohydrate region, which was first analysed in an exploratory manner using principal component analysis (PCA). PCA score plots showed a clear discrimination between diabetic and galactosemic patients and this was more marked as a function of the glucose and galactose increased concentration in these patients' plasma respectively. Then, a support vector machine leave-one-out cross-validation (SVM-LOOCV) classifier was built with the PCA scores as the input and the model was tested on median, mean and all spectra from the three population groups. This classifier was able to discriminate healthy/diabetic, healthy/galactosemic, and diabetic/galactosemic patients with sensitivity and specificity rates ranging from 80% to 94%. The total accuracy rate ranged from 87% to 96%. High-throughput FTIR spectroscopy combined with the SVM-LOOCV classification procedure appears to be a promising tool in the screening of galactosemia patients, with good sensitivity and specificity. Furthermore, this approach presents the advantages of being cost-effective, fast, and straightforward in the screening of galactosemic patients.

Published

2015

6. Mutation spectrum in the French cohort of galactosemic patients and structural simulation of 27 novel missense variations.

Author

Boutron A, Marabotti A, Facchiano A, Cheillan D, Zater M, Oliveira C, Costa C, Labrune P, and Brivet M

Subjects

Adolescent, Adult, Child, Child, Preschool, Cohort Studies, DNA Mutational Analysis, Exons, Female, France epidemiology, Humans, Infant, Introns, Male, Middle Aged, Molecular Docking Simulation, Phenotype, Protein Stability, Protein Subunits deficiency, UTP-Hexose-1-Phosphate Uridylyltransferase deficiency, Galactosemias genetics, Mutation, Protein Subunits genetics, UTP-Hexose-1-Phosphate Uridylyltransferase genetics

Abstract

Background: Classic galactosemia refers to galactose-1-phosphate uridyltransferase (GALT) deficiency and is characterized by long-term complications of unknown mechanism and high allelic heterogeneity of GALT gene., Aim: To report molecular characterization of GALT variations in 210 French families, to analyze the structural effects of novel missense variations and to assess informativity of structural data in predicting outcome., Methods: Sequencing of exons and intron-exon junctions of GALT gene was completed in unsolved cases by analysis of a long range PCR product. Structural consequences of novel missense variations were predicted using a homology model of GALT protein and a semi-automated analysis which integrates simulation of variations, structural analyses and two web servers dedicated to identify mutation-induced change of protein stability., Results: Forty four novel variations were identified, among them 27 nucleotide substitutions. In silico modeling of these missense variations showed that 12 variations are predicted to impair subunit interactions and/or active site conformation and that 23 variations modify H-bond or salt-bridge networks. Twenty variations decrease the global stability of the protein. Five variations had apparently no structural effect., Conclusion: Our results expand the mutation spectrum in GALT gene and the list of GALT variations analyzed at the structural level, providing new data to assess the pathophysiology of galactosemia., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

7. A Novel Mutation in CPT1A Resulting in Hepatic CPT Deficiency.

Author

Fontaine M, Dessein AF, Douillard C, Dobbelaere D, Brivet M, Boutron A, Zater M, Mention-Mulliez K, Martin-Ponthieu A, Vianey-Saban C, Briand G, Porchet N, and Vamecq J

Abstract

The present work presents a "from gene defect to clinics" pathogenesis study of a patient with a hitherto unreported mutation in the CPT1A gene. In early childhood, the patient developed a life-threatening episode (hypoketotic hypoglycemia, liver cytolysis, and hepatomegaly) evocative of a mitochondrial fatty acid oxidation disorder, and presented deficient fibroblast carnitine palmitoyltransferase 1 (CPT1) activity and homozygosity for the c.1783 C > T nucleotide substitution on exon 15 of CPT1A (p.R595W mutant). While confirming CPT1A deficiency, whole blood de novo acylcarnitine synthesis and the levels of carnitine and its esters formally linked intracellular free-carnitine depletion to intracellular carnitine esterification. Sequence alignment and modeling of wild-type and p.*R595W CPT1A proteins indicated that the Arg595 targeted by the mutated codon is phylogenetically well conversed. It contributes to a hydrogen bond network with neighboring residues Cys304 and Met593 but does not participate in the catalysis and carnitine pocket. Its replacement by tryptophan induces steric hindrance with the side chain of Ile480 located in α-helix 12, affecting protein architecture and function. This hindrance with Ile480 is also originally described with tryptophan 304 in the known mutant p.C304W CPT1A, suggesting that the mechanisms that invalidate CPT1A activity and underlie pathogenesis could be common in both the new (p.R595W) and previously described (p.C304W) mutants.

Published

2012

8. Hereditary fructose intolerance: frequency and spectrum mutations of the aldolase B gene in a large patients cohort from France--identification of eight new mutations.

Author

Davit-Spraul A, Costa C, Zater M, Habes D, Berthelot J, Broué P, Feillet F, Bernard O, Labrune P, and Baussan C

Subjects

Adolescent, Adult, Child, Child, Preschool, Chromosomes, Human, Pair 9, Cohort Studies, DNA Mutational Analysis methods, Female, France, Fructose Intolerance genetics, Fructose-Bisphosphate Aldolase deficiency, Humans, Infant, Infant, Newborn, Male, Fructose Intolerance enzymology, Fructose-Bisphosphate Aldolase genetics, Mutation

Abstract

We investigated the molecular basis of hereditary fructose intolerance (HFI) in 160 patients from 92 families by means of a PCR-based mutation screening strategy, consisting of restriction enzyme digestion and direct sequencing. Sixteen different mutations of the aldolase B (ALDOB) gene were identified in HFI patients. As in previous studies, p.A150P (64%), p.A175D (16%) and p.N335K (5%) were the most common mutated alleles, followed by p.R60X, p.A338V, c.360&#95;363delCAAA (p.N120KfsX30), c.324G>A (p.K108K) and c.625-1G>A. Eight novel mutations were also identified in 10 families with HFI: a one-base deletion (c.146delT (p.V49GfsX27)), a small deletion (c.953del42bp), a small insertion (c.689ins TGCTAA (p.K230MfsX136)), one splice site mutation (c.112+1G>A), one nonsense mutation (c.444G>A (p.W148X)), and three missense mutations (c.170G>C (p.R57P), c.839C>A (p.A280P) and c.932T>C (p.L311P)). Our strategy allows to diagnose 75% of HFI patients using restriction enzymatic analysis and to enlarge the diagnosis to 97% of HFI patients when associated with direct sequencing.

Published

2008

9. Prenatal molecular diagnosis of inherited cholestatic diseases.

Author

Jung C, Driancourt C, Baussan C, Zater M, Hadchouel M, Meunier-Rotival M, Guiochon-Mantel A, and Jacquemin E

Subjects

Alagille Syndrome diagnosis, Alagille Syndrome genetics, Chorionic Villi Sampling, DNA analysis, Female, Genetic Counseling, Humans, Mutation, Pregnancy, Cholestasis, Intrahepatic diagnosis, Cholestasis, Intrahepatic genetics

Abstract

Objectives: Progressive familial intrahepatic cholestasis (PFIC) and to a lesser extent, Alagille syndrome, often lead to end-stage liver disease during childhood. We report our experience of DNA-based prenatal diagnosis of PFIC1-3 and Alagille syndrome., Patients and Methods: Four molecular antenatal diagnoses were performed in 3 PFIC families and 17 in 11 Alagille syndrome families. DNA was isolated from chorionic villus or cultured amniocyte samples from women, without pregnancy complications., Results: All four foetuses with a family history of PFIC1, 2, or 3 were heterozygous for an ATP8B1, ABCB11, or ABCB4 mutation and pregnancies were continued. Three of the infants were healthy after birth, and 1 premature infant, who had an ABCB4 mutation, experienced transient neonatal cholestasis. Among the families with a history of de novo JAG1 mutation, none of the foetuses was mutated, versus 40% of those with a history of familial mutation. Of 4 pregnant women with a JAG1-mutated foetus, 3 cut short their pregnancy and 1 gave birth to a child with overt Alagille syndrome., Conclusions: Molecular antenatal diagnosis of PFIC1-3 and Alagille syndrome is reliable because clinical outcome after birth corresponded to molecular foetal data.

Published

2007

10. A novel SLC25A20 splicing mutation in patients of different ethnic origin with neonatally lethal carnitine-acylcarnitine translocase (CACT) deficiency.

Author

Korman SH, Pitt JJ, Boneh A, Dweikat I, Zater M, Meiner V, Gutman A, and Brivet M

Subjects

Amino Acid Metabolism, Inborn Errors enzymology, Amino Acid Metabolism, Inborn Errors ethnology, DNA, Complementary genetics, Fatal Outcome, Female, Humans, Infant, Newborn, Membrane Transport Proteins analysis, Mutation, RNA Splicing genetics, Sequence Analysis, DNA, Amino Acid Metabolism, Inborn Errors genetics, Genes, Lethal, Membrane Transport Proteins deficiency, Membrane Transport Proteins genetics

Abstract

Carnitine-acylcarnitine translocase (CACT) deficiency is a rare disorder of fatty acid oxidation associated with high mortality. Two female newborns of different ethnic origin (the first Anglo-Celtic and the second Palestinian Arab) both died after sudden collapse on day 2 of life. Both had elevated bloodspot long-chain acylcarnitines consistent with either CACT or carnitine palmitoyltransferase II (CPT2) deficiency; the latter was excluded by demonstrating normal CPT2 activity in fibroblasts. Direct sequencing of all SLC25A20 (CACT) gene exons and exon-intron boundaries revealed that Patient 1 was compound heterozygous for a novel c.609-3c>g (IVS6-3c>g) mutation on the paternal allele and a previously described c.326delG mutation on the maternal allele. Patient 2 was homozygous for the same, novel c.609-3c>g mutation. Previously reported SLC25A20 mutations have been almost exclusively confined to a single family or ethnic group. Analysis of fibroblast cDNA by RT-PCR, agarose gel electrophoresis and sequencing of extracted bands showed that both mutations produce aberrant splicing. c.609-3C>G results in exon 7 skipping leading to a frameshift with premature termination seven amino acids downstream. c.326delG was confirmed to produce skipping of exons 3 or 3 plus 4. CACT activity in both patients' fibroblasts was near-zero. For both families, prenatal diagnosis of an unaffected fetus was performed by mutation analysis on CVS tissue in a subsequent pregnancy. Due to the urgency of prenatal diagnosis in the second family, molecular diagnosis was performed prior to demonstration of CACT enzyme deficiency, illustrating that mutation analysis is a rapid and reliable approach to first-line diagnosis of CACT deficiency.

Published

2006

11. Urinary cystatin C as a specific marker of tubular dysfunction.

Author

Conti M, Moutereau S, Zater M, Lallali K, Durrbach A, Manivet P, Eschwège P, and Loric S

Subjects

Aged, Automation, Biological Assay, Cystatin C, Disease Progression, Female, Humans, Kidney Diseases diagnosis, Kidney Diseases urine, Kidney Function Tests, Kidney Tubules pathology, Male, Middle Aged, Renal Insufficiency diagnosis, Reproducibility of Results, Sensitivity and Specificity, Biomarkers urine, Cystatins urine, Cysteine Proteinase Inhibitors urine, Kidney Tubules metabolism, Renal Insufficiency urine

Abstract

Background: Cystatin C (CST3), a strong inhibitor of cysteine proteinases, is freely filtered by the kidney glomerulus and is reabsorbed by the tubules, where it is almost totally catabolized, with the remainder then eliminated in urine. In tubular diseases, it seems sensible to postulate that CST3 degradation would be reduced and consequently an increase in its urinary elimination would be observed., Methods: We report here the development of an automatic quantitative assay to measure CST3 concentrations in urine using a Behring N-Latex Cystatin C kit on a BNII laser nephelometer. We tested its clinical relevance on several kidney disease patients., Results: This assay is sensitive (limit of detection 0.008 mg/L) and precise (within- and between-day CVs < 4%). Reference values for freshly collected urine samples range from 0.03 to 0.18 mg/L. Mean urine CST3 concentrations obtained from 52 patients with kidney tubular disease (4.31 +/- 3.85 mg/L) were significantly higher than those for 60 controls (0.096 +/- 0.044 mg/L; p < 0.0001) and 47 glomerular disease patients (0.106 +/- 0.133 mg/L; p < 0.0001)., Conclusion: Increased urinary CST3 concentrations allow the accurate detection of tubular dysfunction among pure and mixed nephropathies. Because of its ability to be processed on automated clinical chemistry analyzers, this assay could easily be used as an adjunct to the standard panel used to screen kidney pathologies, even in emergency situations.

Published

2006

12. First characterization of a large deletion of the PDHA 1 gene.

Author

Brivet M, Moutard ML, Zater M, Venet L, Chenel C, Mine M, and Legrand A

Subjects

Base Sequence, Child, Preschool, DNA genetics, DNA Mutational Analysis, Female, Humans, Introns, Polymerase Chain Reaction, Polynesia, Repetitive Sequences, Nucleic Acid, Restriction Mapping, Sequence Deletion, Pyruvate Dehydrogenase (Lipoamide) genetics, Pyruvate Dehydrogenase Complex Deficiency Disease enzymology, Pyruvate Dehydrogenase Complex Deficiency Disease genetics

Abstract

Pyruvate dehydrogenase complex (PDC) deficiency is one of the major recognized causes of congenital lactic acidosis. The most common form is due to PDHA 1 gene (Xp22.12) defects. Here, we report the case of a Polynesian girl presenting with delayed neurological development, cortical atrophy, and posterior corpus callosum agenesis. Elevated lactate and pyruvate levels in blood and cerebrospinal fluid suggested PDC deficiency. However, PDC activity was within the normal range in lymphocytes and the direct sequencing of the 11 exons and intron-exon junctions of the PDHA 1 gene did not show any changes. Long-range PCR amplification of the whole gene (16 kb) from blood DNA revealed a heterozygous deletion of approximately 4.2kb. Fine mapping of the deletion breakpoint was achieved using purified long-range PCR products for restriction enzyme analysis and direct sequencing. The deletion removed a 4,227 bp region covering part of intron 5 to part of intron 9 [g.10,145&#95;14,371 del 4,227]. The deletion breakpoint contained a short direct repeat (GTAG), which may be derived either from the upstream or the downstream homologous sequence. The presence of a GAG triplet and inverted repeats in the vicinity of the deletion suggest replication slippage at a polymerase alpha arrest site. This is the first time that a large intragenic deletion of the PDHA 1 gene has been characterized.

Published

2005

13. Absence of circadian variations in urine cystatin C allows its use on urinary samples.

Author

Conti M, Zater M, Lallali K, Durrbach A, Moutereau S, Manivet P, Eschwège P, and Loric S

Subjects

Cystatin C, Humans, Reference Values, Circadian Rhythm, Cystatins urine

Published

2005