Your search keyword '"T. Marquardt"' showing total 12 results

1. Treatment of AICA ribosiduria by suppression of de novo purine synthesis.

Author

Park JH, Och U, Braun T, Kriegel MF, Biskup S, Korall H, Uhlig CE, and Marquardt T

Subjects

Humans, Adolescent, Purines

Abstract

AICA ribosiduria is an ultra-rare disorder of de novo purine biosynthesis associated with developmental delay of varying severity, seizures, and varying degrees of visual impairment due to chorioretinal atrophy. Caused by biallelic pathogenic variants in ATIC, accumulation of AICA-riboside is the biochemical hallmark and presumed pathomechanism of the condition. In this study, we report the case of a teenage patient compound-heterozygous for the variants c.1277 A > G (p.K426R) and c.642G > C (p.Q214H) in ATIC, with the latter not previously reported. Excessive secretion of AICA-riboside and succinyladenosine was significantly reduced following the introduction of a purine-enriched diet. By suppressing de novo purine biosynthesis in favour of purine salvage, exogenous purine substitution represents a promising treatment approach for AICA ribosiduria. SYNOPSIS: Suppression of de novo purine biosynthesis by increased exogeneous purine supply leads to decreased accumulation of AICA-riboside and succinyl-adenosine and thus is a promising treatment approach for AICA ribosiduria., Competing Interests: Declaration of competing interest All authors declare no conflict of interest related to this work., (Copyright © 2023. Published by Elsevier Inc.)

Published

2024

2. Application of a glycinated bile acid biomarker for diagnosis and assessment of response to treatment in Niemann-pick disease type C1.

Author

Sidhu R, Kell P, Dietzen DJ, Farhat NY, Do AND, Porter FD, Berry-Kravis E, Reunert J, Marquardt T, Giugliani R, Lourenço CM, Wang RY, Movsesyan N, Plummer E, Schaffer JE, Ory DS, and Jiang X

Subjects

2-Hydroxypropyl-beta-cyclodextrin administration & dosage, Bile Acids and Salts blood, Biomarkers blood, Female, Glycine analogs & derivatives, Glycine isolation & purification, Humans, Male, Niemann-Pick C1 Protein, Niemann-Pick Disease, Type C drug therapy, Niemann-Pick Disease, Type C pathology, Tandem Mass Spectrometry, Vesicular Transport Proteins genetics, Glycine blood, Intracellular Signaling Peptides and Proteins genetics, Niemann-Pick Disease, Type C blood, Niemann-Pick Disease, Type C genetics

Abstract

Niemann-Pick disease type C (NPC) is a neurodegenerative disease in which mutation of NPC1 or NPC2 gene leads to lysosomal accumulation of unesterified cholesterol and sphingolipids. Diagnosis of NPC disease is challenging due to non-specific early symptoms. Biomarker and genetic tests are used as first-line diagnostic tests for NPC. In this study, we developed a plasma test based on N-(3β,5α,6β-trihydroxy-cholan-24-oyl)glycine (TCG) that was markedly increased in the plasma of human NPC1 subjects. The test showed sensitivity of 0.9945 and specificity of 0.9982 to differentiate individuals with NPC1 from NPC1 carriers and controls. Compared to other commonly used biomarkers, cholestane-3β,5α,6β-triol (C-triol) and N-palmitoyl-O-phosphocholine (PPCS, also referred to as lysoSM-509), TCG was equally sensitive for identifying NPC1 but more specific. Unlike C-triol and PPCS, TCG showed excellent stability and no spurious generation of marker in the sample preparation or aging of samples. TCG was also elevated in lysosomal acid lipase deficiency (LALD) and acid sphingomyelinase deficiency (ASMD). Plasma TCG was significantly reduced after intravenous (IV) 2-hydroxypropyl-β-cyclodextrin (HPβCD) treatment. These results demonstrate that plasma TCG was superior to C-triol and PPCS as NPC1 diagnostic biomarker and was able to evaluate the peripheral treatment efficacy of IV HPβCD treatment., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2020

3. Application of N-palmitoyl-O-phosphocholineserine for diagnosis and assessment of response to treatment in Niemann-Pick type C disease.

Author

Sidhu R, Kell P, Dietzen DJ, Farhat NY, Do AND, Porter FD, Berry-Kravis E, Vite CH, Reunert J, Marquardt T, Giugliani R, Lourenço CM, Bodamer O, Wang RY, Plummer E, Schaffer JE, Ory DS, and Jiang X

Subjects

Adolescent, Adult, Aged, Animals, Biomarkers blood, Biomarkers cerebrospinal fluid, Cats, Child, Child, Preschool, Chromatography, Liquid, Female, Humans, Infant, Infant, Newborn, Male, Middle Aged, Sensitivity and Specificity, Severity of Illness Index, Tandem Mass Spectrometry, Treatment Outcome, Young Adult, 2-Hydroxypropyl-beta-cyclodextrin therapeutic use, Niemann-Pick Disease, Type C diagnosis, Niemann-Pick Disease, Type C drug therapy, Phosphorylcholine blood, Phosphorylcholine cerebrospinal fluid

Abstract

Niemann-Pick type C (NPC) disease is a rare lysosomal storage disorder caused by mutations in either the NPC1 or the NPC2 gene. A new class of lipids, N-acyl-O-phosphocholineserines were recently identified as NPC biomarkers. The most abundant species in this class of lipid, N-palmitoyl-O-phosphocholineserine (PPCS), was evaluated for diagnosis of NPC disease and treatment efficacy assessment with 2-hydroxypropyl-β-cyclodextrin (HPβCD) in NPC. Liquid chromatography-tandem mass spectrometry (LC-MS/MS) methods were developed and validated to measure PPCS in human plasma and cerebrospinal fluid (CSF). A cutoff of 248 ng/mL in plasma provided a sensitivity of 100.0% and specificity of 96.6% in identifying NPC1 patients from control and NPC1 carrier subjects. PPCS was significantly elevated in CSF from NPC1 patients, and CSF PPCS levels were significantly correlated with NPC neurological disease severity scores. Plasma and CSF PPCS did not change significantly in response to intrathetical (IT) HPβCD treatment. In an intravenous (IV) HPβCD trial, plasma PPCS in all patients was significantly reduced. These results demonstrate that plasma PPCS was able to diagnose NPC1 patients with high sensitivity and specificity, and to evaluate the peripheral treatment efficacy of IV HPβCD treatment., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2020

4. Diagnostic tests for Niemann-Pick disease type C (NP-C): A critical review.

Author

Vanier MT, Gissen P, Bauer P, Coll MJ, Burlina A, Hendriksz CJ, Latour P, Goizet C, Welford RW, Marquardt T, and Kolb SA

Subjects

Age of Onset, Bile Acids and Salts blood, Cholestanes blood, Genetic Testing, Humans, Intracellular Signaling Peptides and Proteins, Niemann-Pick C1 Protein, Niemann-Pick Disease, Type C blood, Niemann-Pick Disease, Type C physiopathology, Phosphorylcholine analogs & derivatives, Phosphorylcholine blood, Sphingosine analogs & derivatives, Sphingosine blood, Vesicular Transport Proteins, Biomarkers blood, Carrier Proteins genetics, Glycoproteins genetics, Membrane Glycoproteins genetics, Niemann-Pick Disease, Type C genetics

Abstract

Niemann-Pick disease type C (NP-C) is a neurovisceral lysosomal cholesterol trafficking and lipid storage disorder caused by mutations in one of the two genes, NPC1 or NPC2. Diagnosis has often been a difficult task, due to the wide range in age of onset of NP-C and clinical presentation of the disease, combined with the complexity of the cell biology (filipin) laboratory testing, even in combination with genetic testing. This has led to substantial delays in diagnosis, largely depending on the access to specialist centres and the level of knowledge about NP-C of the physician in the area. In recent years, advances in mass spectrometry has allowed identification of several sensitive plasma biomarkers elevated in NP-C (e.g. cholestane-3β,5α,6β-triol, lysosphingomyelin isoforms and bile acid metabolites), which, together with the concomitant progress in molecular genetic technology, have greatly impacted the strategy of laboratory testing. Specificity of the biomarkers is currently under investigation and other pathologies are being found to also result in elevations. Molecular genetic testing also has its limitations, notably with unidentified mutations and the classification of new variants. This review is intended to increase awareness on the currently available approaches to laboratory diagnosis of NP-C, to provide an up to date, comprehensive and critical evaluation of the various techniques (cell biology, biochemical biomarkers and molecular genetics), and to briefly discuss ongoing/future developments. The use of current tests in proper combination enables a rapid and correct diagnosis in a large majority of cases. However, even with recent progress, definitive diagnosis remains challenging in some patients, for whom combined genetic/biochemical/cytochemical markers do not provide a clear answer. Expertise and reference laboratories thus remain essential, and further work is still required to fulfill unmet needs., (Copyright © 2016 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2016

5. In vivo monitoring of urea cycle activity with (13)C-acetate as a tracer of ureagenesis.

Author

Opladen T, Lindner M, Das AM, Marquardt T, Khan A, Emre SH, Burton BK, Barshop BA, Böhm T, Meyburg J, Zangerl K, Mayorandan S, Burgard P, Dürr UH, Rosenkranz B, Rennecke J, Derbinski J, Yudkoff M, and Hoffmann GF

Subjects

Administration, Oral, Adolescent, Adult, Carbon Isotopes metabolism, Child, Child, Preschool, Female, Humans, Hyperammonemia diagnosis, Hyperammonemia metabolism, Infant, Infant, Newborn, Male, Middle Aged, Monitoring, Physiologic, Ornithine Carbamoyltransferase Deficiency Disease diagnosis, Radioactive Tracers, Sodium Acetate administration & dosage, Young Adult, Sodium Acetate pharmacokinetics, Urea metabolism, Urea Cycle Disorders, Inborn diagnosis

Abstract

Background: The hepatic urea cycle is the main metabolic pathway for detoxification of ammonia. Inborn errors of urea cycle function present with severe hyperammonemia and a high case fatality rate. Long-term prognosis depends on the residual activity of the defective enzyme. A reliable method to estimate urea cycle activity in-vivo does not exist yet. The aim of this study was to evaluate a practical method to quantify (13)C-urea production as a marker for urea cycle function in healthy subjects, patients with confirmed urea cycle defect (UCD) and asymptomatic carriers of UCD mutations., Methods: (13)C-labeled sodium acetate was applied orally in a single dose to 47 subjects (10 healthy subjects, 28 symptomatic patients, 9 asymptomatic carriers)., Results: The oral (13)C-ureagenesis assay is a safe method. While healthy subjects and asymptomatic carriers did not differ with regards to kinetic variables for urea cycle flux, symptomatic patients had lower (13)C-plasma urea levels. Although the (13)C-ureagenesis assay revealed no significant differences between individual urea cycle enzyme defects, it reflected the heterogeneity between different clinical subgroups, including male neonatal onset ornithine carbamoyltransferase deficiency. Applying the (13)C-urea area under the curve can differentiate between severe from more mildly affected neonates. Late onset patients differ significantly from neonates, carriers and healthy subjects., Conclusion: This study evaluated the oral (13)C-ureagenesis assay as a sensitive in-vivo measure for ureagenesis capacity. The assay has the potential to become a reliable tool to differentiate UCD patient subgroups, follow changes in ureagenesis capacity and could be helpful in monitoring novel therapies of UCD., (Copyright © 2015 Elsevier Inc. All rights reserved.)

Published

2016

6. Expanding the clinical and molecular spectrum of thiamine pyrophosphokinase deficiency: a treatable neurological disorder caused by TPK1 mutations.

Author

Banka S, de Goede C, Yue WW, Morris AA, von Bremen B, Chandler KE, Feichtinger RG, Hart C, Khan N, Lunzer V, Mataković L, Marquardt T, Makowski C, Prokisch H, Debus O, Nosaka K, Sonwalkar H, Zimmermann FA, Sperl W, and Mayr JA

Subjects

Acidosis, Lactic, Amino Acid Sequence, Child, Child, Preschool, Female, Humans, Magnetic Resonance Imaging, Male, Models, Molecular, Nervous System Diseases drug therapy, Nervous System Diseases metabolism, Nervous System Diseases pathology, Phenotype, Protein Conformation, Protein Multimerization, Thiamin Pyrophosphokinase chemistry, Thiamin Pyrophosphokinase metabolism, Thiamine administration & dosage, Thiamine therapeutic use, Thiamine Pyrophosphate metabolism, Mutation, Nervous System Diseases genetics, Thiamin Pyrophosphokinase deficiency, Thiamin Pyrophosphokinase genetics

Abstract

Thiamine pyrophosphokinase (TPK) produces thiamine pyrophosphate, a cofactor for a number of enzymes, including pyruvate dehydrogenase and 2-ketoglutarate dehydrogenase. Episodic encephalopathy type thiamine metabolism dysfunction (OMIM 614458) due to TPK1 mutations is a recently described rare disorder. The mechanism of the disease, its phenotype and treatment are not entirely clear. We present two patients with novel homozygous TPK1 mutations (Patient 1 with p.Ser160Leu and Patient 2 with p.Asp222His). Unlike the previously described phenotype, Patient 2 presented with a Leigh syndrome like non-episodic early-onset global developmental delay, thus extending the phenotypic spectrum of the disorder. We, therefore, propose that TPK deficiency may be a better name for the condition. The two cases help to further refine the neuroradiological features of TPK deficiency and show that MRI changes can be either fleeting or progressive and can affect either white or gray matter. We also show that in some cases lactic acidosis can be absent and 2-ketoglutaric aciduria may be the only biochemical marker. Furthermore, we have established the assays for TPK enzyme activity measurement and thiamine pyrophosphate quantification in frozen muscle and blood. These tests will help to diagnose or confirm the diagnosis of TPK deficiency in a clinical setting. Early thiamine supplementation prevented encephalopathic episodes and improved developmental progression of Patient 1, emphasizing the importance of early diagnosis and treatment of TPK deficiency. We present evidence suggesting that thiamine supplementation may rescue TPK enzyme activity. Lastly, in silico protein structural analysis shows that the p.Ser160Leu mutation is predicted to interfere with TPK dimerization, which may be a novel mechanism for the disease., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2014

7. Neurocognitive functioning in adults with phenylketonuria: results of a long term study.

Author

Weglage J, Fromm J, van Teeffelen-Heithoff A, Möller HE, Koletzko B, Marquardt T, Rutsch F, and Feldmann R

Subjects

Adolescent, Adult, Age Factors, Case-Control Studies, Child, Female, Humans, Intelligence, Intelligence Tests, Magnetic Resonance Imaging, Male, Neuropsychological Tests, Phenylketonurias diet therapy, Young Adult, Brain physiopathology, Cognition, Phenylalanine blood, Phenylketonurias psychology

Abstract

Objectives: A controlled long-term study was performed to assess the neurological and neuropsychological performance in adult patients with early-treated phenylketonuria (PKU)., Methods: We investigated 57 patients with early-treated classical PKU aged 19 to 41 years (mean age 31 years) and 46 matched healthy controls, matched for age and socioeconomic status. Patients and controls were assessed for their intelligence quotient (IQ), and attention and information-processing abilities. Magnetic resonance imaging (MRI) of the brain was performed in all patients. Neuropsychological assessments and MRI were repeated at a five-year-follow-up., Results: In the five-year interval IQ, information processing and attention of patients and controls remained constant. At both assessment times the IQ scores were significantly lower in patients compared to controls. Older adult patients (>32 years) showed poorer information processing and attention at both assessment times compared to young adult patients (<32 years) and controls. IQ, information processing and attention showed no correlation to imaging results but were significantly correlated to blood phenylalanine (Phe) levels in patients' childhood and adolescence, and Phe levels had been higher in the adolescent years of older adult patients., Conclusions: Cognitive performance in adult patients with early-treated PKU does not seem to be subject to deterioration observable in a five-year interval. Neuropsychological assessment in adults with PKU revealed neurocognitive impairment particularly in older adult patients. This seems to refer to an early relaxation of diet that was recommended when the older patients were adolescents. Results indicate a benefit of dietary control during adolescence in PKU., (© 2013.)

Published

2013

8. Congenital disorder of glycosylation type Ij (CDG-Ij, DPAGT1-CDG): extending the clinical and molecular spectrum of a rare disease.

Author

Würde AE, Reunert J, Rust S, Hertzberg C, Haverkämper S, Nürnberg G, Nürnberg P, Lehle L, Rossi R, and Marquardt T

Subjects

Adult, Amino Acid Sequence, Cells, Cultured, Chromatography, High Pressure Liquid, Electrophoresis, Polyacrylamide Gel, Female, Fibroblasts cytology, Fibroblasts enzymology, Glycosylation, Homozygote, Humans, Immunoprecipitation, Infant, Newborn, Lipopolysaccharides metabolism, Molecular Sequence Data, Sequence Homology, Amino Acid, Skin cytology, Skin enzymology, Congenital Disorders of Glycosylation enzymology, Congenital Disorders of Glycosylation genetics, Mutation genetics, Rare Diseases enzymology, Rare Diseases genetics, Transferases (Other Substituted Phosphate Groups) genetics

Abstract

Congenital disorders of glycosylation (CDG) are caused by enzymatic defects of the formation or processing of lipid-linked oligosaccharides and glycoproteins. Since the majority of proteins is glycosylated, a defect in a singular CDG enzyme leads to a multisytemic disease with secondary malfunction of thousands of proteins. CDG-Ij (DPAGT1-CDG) is caused by a defect of the human DPAGT1 (UDP-GlcNAc: Dolichol Phosphate N-Acetylglucosamine-1-Phosphotransferase), catalyzing the first step of N-linked glycosylation. So far the clinical phenotype of only one CDG-Ij patient has been described. The patient showed severe muscular hypotonia, intractable seizures, developmental delay, mental retardation, microcephaly and exotropia. Molecular studies of this patient revealed the heterozygous mutation c.660A>G (Y170C; paternal) in combination with an uncharacterized splicing defect (maternal). Two further mutations, c.890A>T (I297F) and c.162-8G>A as a splicing defect were detected when analyzing DPAGT1 in two affected siblings of a second family. We report two new patients with the novel homozygous mutation, c.341C>G (A114 G), causing a severe clinical phenotype, characterized by hyperexcitability, intractable seizures, bilateral cataracts, progressive microcephaly and muscular hypotonia. Both our patients died within their first year of life. With the discovery of this novel mutation and a detailed clinical description we extend the clinical features of CDG-Ij in order to improve early detection of this disease., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

9. Life with too much polyprenol: polyprenol reductase deficiency.

Author

Gründahl JE, Guan Z, Rust S, Reunert J, Müller B, Du Chesne I, Zerres K, Rudnik-Schöneborn S, Ortiz-Brüchle N, Häusler MG, Siedlecka J, Swiezewska E, Raetz CR, and Marquardt T

Subjects

Cells, Cultured, Chromatography, High Pressure Liquid, Congenital Disorders of Glycosylation diagnosis, Dolichols metabolism, Electrophoresis, Polyacrylamide Gel, Female, Fibroblasts, Genetic Complementation Test, Glycosylation, Homozygote, Humans, Immunoprecipitation, Infant, Newborn, Isoelectric Focusing, Male, Pedigree, 3-Oxo-5-alpha-Steroid 4-Dehydrogenase genetics, Congenital Disorders of Glycosylation enzymology, Congenital Disorders of Glycosylation genetics, Membrane Proteins genetics, Mutation genetics, Pentanols metabolism

Abstract

Congenital disorders of glycosylation (CDG) are caused by a dysfunction of glycosylation, an essential step in the manufacturing process of glycoproteins. This paper focuses on a 6-year-old patient with a new type of CDG-I caused by a defect of the steroid 5α reductase type 3 gene (SRD5A3). The clinical features were psychomotor retardation, pathological nystagmus, slight muscular hypotonia and microcephaly. SRD5A3 was recently identified encoding the polyprenol reductase, an enzyme catalyzing the final step of the biosynthesis of dolichol, which is required for the assembly of the glycans needed for N-glycosylation. Although an early homozygous stop-codon (c.57G>A [W19X]) with no functional protein was found in the patient, about 70% of transferrin (Tf) was correctly glycosylated. Quantification of dolichol and unreduced polyprenol in the patient's fibroblasts demonstrated a high polyprenol/dolichol ratio with normal amounts of dolichol, indicating that high polyprenol levels might compete with dolichol for the initiation of N-glycan assembly but without supporting normal glycosylation and that there must be an alternative pathway for dolichol biosynthesis., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2012

10. Miglustat in patients with Niemann-Pick disease Type C (NP-C): a multicenter observational retrospective cohort study.

Author

Pineda M, Wraith JE, Mengel E, Sedel F, Hwu WL, Rohrbach M, Bembi B, Walterfang M, Korenke GC, Marquardt T, Luzy C, Giorgino R, and Patterson MC

Subjects

1-Deoxynojirimycin administration & dosage, 1-Deoxynojirimycin therapeutic use, Adolescent, Child, Cohort Studies, Enzyme Inhibitors administration & dosage, Female, Humans, Male, Niemann-Pick Disease, Type C pathology, Retrospective Studies, Treatment Outcome, 1-Deoxynojirimycin analogs & derivatives, Enzyme Inhibitors therapeutic use, Niemann-Pick Disease, Type C drug therapy

Abstract

Miglustat has been shown to stabilize disease progression in children, juveniles and adults with Niemann-Pick disease type C (NP-C), a rare genetic disorder characterized by progressive neurological deterioration. We report findings from a retrospective observational cohort study assessing the effects of miglustat on neurological disease progression in patients treated in the clinical practice setting. Data from all NP-C patients prescribed miglustat at 25 expert centers were evaluated using a disease disability scale. The scale analyzed four key parameters of neurological disease progression in NP-C (ambulation, manipulation, language, swallowing). Mean individual parameter scores and a composite score were calculated at baseline (time of diagnosis) and up to 4 follow-up visits. Overall, 66 patients were included (mean [SD] age at diagnosis, 9.7 [7.6] years, and at treatment start, 12.8 [9.5] years). The median (range) miglustat exposure was 1.46 (0.05-4.51) years. Mean annual progression was +0.11 score units/year from diagnosis to treatment start, indicating disease progression prior to therapy, and decreasing to -0.01 score units/year from treatment start to last clinic visit, indicating stabilization. Stabilization of neurological disease on miglustat was observed in all age groups, but the magnitude of the effect was greater in patients diagnosed in late childhood and in juveniles and adults. Stabilization of neurological disease was also observed in a subset of 19 patients with extended pre-treatment information. Overall, these data support previous clinical trial findings indicating clinically relevant beneficial effects of miglustat on neurological disease progression in patients with NP-C.

Published

2009

11. Novel ALG8 mutations expand the clinical spectrum of congenital disorder of glycosylation type Ih.

Author

Stölting T, Omran H, Erlekotte A, Denecke J, Reunert J, and Marquardt T

Subjects

Carbohydrate Metabolism, Inborn Errors pathology, Glycosylation, Humans, Phenotype, Siblings, Carbohydrate Metabolism, Inborn Errors genetics, Glucosyltransferases genetics, Mutation

Abstract

Congenital disorders of glycosylation (CDG) are an expanding group of inherited disorders caused by defects in the N- or O-Glycosylation of proteins and lipids. Several CDG subtypes have been described so far, including CDG type Ih which is caused by a deficiency of the dolichyl-P-Glc:Glc(1)Man(9)GlcNAc(2)-PP-dolichyl alpha1,3-glucosyltransferase (hALG8). The defect leads to an accumulation of Dol-PP-GlcNAc(2)Man(9) and Dol-PP-GlcNAc(2)Man(9)Glc(1) in the endoplasmic reticulum of patients' fibroblasts that can be detected by analyzing the lipid-linked oligosaccharyl intermediates. Five patients with CDG-Ih have been described so far. The clinical presentation of four of these patients was severe with death in early infancy. In this report, we describe two mildly affected siblings with CDG-Ih caused by two novel mutations. While one mutation (c.1434delC) causes a frame shift resulting in a premature termination codon (p.485X), the point mutation of the other allele (c.845C>T, p.A282V) causes an amino acid replacement in a highly conserved region of the hALG8 gene. The two siblings show similar symptoms, including pseudo-gynecomastia, epicanthus, muscular hypotonia, mental retardation and ataxia, expanding the genetic and clinical spectrum of CDG-Ih.

Published

2009

12. Analysis of multiple mutations in the hALG6 gene in a patient with congenital disorder of glycosylation Ic.

Author

Westphal V, Schottstädt C, Marquardt T, and Freeze HH

Subjects

Alleles, Child, Congenital Disorders of Glycosylation enzymology, DNA Mutational Analysis, DNA Primers chemistry, Exons genetics, Fibroblasts enzymology, Glycosylation, Humans, Male, Polymorphism, Genetic, RNA, Messenger analysis, Reverse Transcriptase Polymerase Chain Reaction, Saccharomyces cerevisiae genetics, Congenital Disorders of Glycosylation genetics, Glucosyltransferases genetics, Membrane Proteins, Mutation

Abstract

Congenital disorder of glycosylation Ic is caused by mutations in the hALG6 gene that encodes an alpha-1,3 glucosyltransferase. This enzyme is required for the addition of the first glucose residue to the lipid-linked oligosaccharide precursor for N-linked glycosylation. Here we describe the biochemical and molecular analysis of a patient with three mutations in the hALG6 gene. The maternal allele has an intronic G --> A mutation resulting in skipping of exon3 (IVS3 + 5G > A). This produces a nonfunctional enzyme as shown by its inability to restore normal glycosylation in a Saccharomyces cerevisiae strain lacking a functional ALG6. The paternal allele has two mutations. One is a deletion of three bases (895-897delATA) leading to an in-frame deletion of isoleucine 299 (delI299) located in a transmembrane domain. The second mutation on the same allele 911T > C causes a F304S change. When expressed in the ALG6 deficient yeast strain, this allele restores glycosylation but the mRNA is unstable or inefficiently transcribed, contributing to the impaired glycosylation in the patient., (Copyright 2000 Academic Press.)

Published

2000