Your search keyword '"Glycogen Storage Disease Type IV enzymology"' showing total 37 results

1. Alteration of mitochondrial function in the livers of mice with glycogen branching enzyme deficiency.

Author

Malinska D, Testoni G, Bejtka M, Duran J, Guinovart JJ, and Duszynski J

Subjects

Animals, Electron Transport Complex III genetics, Glycogen Debranching Enzyme System metabolism, Glycogen Storage Disease Type IV genetics, Glycogen Storage Disease Type IV pathology, Mice, Mice, Knockout, Mitochondria, Liver genetics, Mitochondria, Liver pathology, Mitochondrial Proteins genetics, Electron Transport Complex III metabolism, Glycogen Debranching Enzyme System deficiency, Glycogen Storage Disease Type IV enzymology, Mitochondria, Liver enzymology, Mitochondrial Proteins metabolism

Abstract

Glycogen storage disease type IV (GSD IV) is caused by mutations in the glycogen branching enzyme gene (GBE1) that lead to the accumulation of aberrant glycogen in affected tissues, mostly in the liver. To determine whether dysfunctional glycogen metabolism in GSD IV affects other components of cellular bioenergetics, we studied mitochondrial function in heterozygous Gbe1 knockout (Gbe1 +/- ) mice. Mitochondria isolated from the livers of Gbe1 +/- mice showed elevated respiratory complex I activity and increased reactive oxygen species production, particularly by respiratory chain complex III. These observations indicate that GBE1 deficiency leads to broader rearrangements in energy metabolism and that the mechanisms underlying GSD IV pathogenesis may include more than merely mechanical cell damage caused by the presence of glycogen aggregates., Competing Interests: Declaration of competing interest The authors declare no conflict of interests., (Copyright © 2021 Elsevier B.V. and Société Française de Biochimie et Biologie Moléculaire (SFBBM). All rights reserved.)

Published

2021

2. Novel pathogenic variants in GBE1 causing fetal akinesia deformation sequence and severe neuromuscular form of glycogen storage disease type IV.

Author

Radhakrishnan P, Moirangthem A, Nayak SS, Shukla A, Mathew M, and Girisha KM

Subjects

Arthrogryposis pathology, Base Sequence, Female, Fetus pathology, Glycogen Storage Disease Type IV pathology, Humans, Infant, Newborn, Male, Neuromuscular Diseases pathology, Pedigree, Arthrogryposis enzymology, Arthrogryposis genetics, Glycogen Debranching Enzyme System genetics, Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV genetics, Mutation genetics, Neuromuscular Diseases enzymology, Neuromuscular Diseases genetics

Abstract

Glycogen storage disease IV (GSD IV), caused by a defect in GBE1, is a clinically heterogeneous disorder. A classical hepatic form and a neuromuscular form have been described. The severe neuromuscular form presents as a fetal akinesia deformation sequence or a congenital subtype. We ascertained three unrelated families with fetuses/neonates who presented with fetal akinesia deformation sequence to our clinic for genetic counseling. We performed a detailed clinical evaluation, exome sequencing, and histopathology examination of two fetuses and two neonates from three unrelated families presenting with these perinatally lethal neuromuscular forms of GSD IV. Exome sequencing in the affected fetuses/neonates identified four novel pathogenic variants (c.1459G>T, c.144-1G>A, c.1680C>G, and c.1843G>C) in GBE1 (NM_000158). Histopathology examination of tissues from the affected fetuses/neonate was consistent with the diagnosis. Here, we add three more families with the severe perinatally lethal neuromuscular forms of GSD IV to the GBE1 mutation spectrum.

Published

2019

3. Distinctly Elevated Chitotriosidase Activity in a Child with Congenital Andersen Disease (Glycogen Storage Disease Type IV).

Author

Schänzer A, Faas D, Rust S, Podskarbi T, van Kuilenburg AB, Scarpa M, Kunze A, Marquardt T, and Hahn A

Subjects

Biopsy, Carbon-Carbon Ligases deficiency, Carbon-Carbon Ligases genetics, Consanguinity, DNA Mutational Analysis, Female, Genes, Recessive genetics, Germany, Glycogen Storage Disease Type IV genetics, Glycogen Storage Disease Type IV pathology, Humans, Infant, Newborn, Macrophages pathology, Muscle, Skeletal pathology, Myofibrils pathology, Turkey ethnology, Urea Cycle Disorders, Inborn diagnosis, Urea Cycle Disorders, Inborn enzymology, Urea Cycle Disorders, Inborn genetics, Glycogen Storage Disease Type IV diagnosis, Glycogen Storage Disease Type IV enzymology, Hexosaminidases blood

Published

2016

4. A novel GBE1 gene variant in a child with glycogen storage disease type IV.

Author

Said SM, Murphree MI, Mounajjed T, El-Youssef M, and Zhang L

Subjects

Biopsy, Child, Preschool, Exons, Genetic Predisposition to Disease, Glycogen Debranching Enzyme System deficiency, Glycogen Storage Disease Type IV diagnosis, Glycogen Storage Disease Type IV enzymology, Heredity, Heterozygote, Humans, Liver enzymology, Liver ultrastructure, Male, Microscopy, Electron, Molecular Diagnostic Techniques, Pedigree, Phenotype, Genetic Variation, Glycogen Debranching Enzyme System genetics, Glycogen Storage Disease Type IV genetics

Abstract

Glycogen storage disease type IV is an autosomal recessive disorder of carbohydrates caused by deficiency of amylo-1-4-glycanoglycosyltransferase, which leads to accumulation of amylopectin-like polysaccharides in tissues including liver, heart and neuromuscular system. More than 40 different mutations in the glycogen branching enzyme gene (GBE1) have been described. In this study, we report a 2-year-old boy who presented with developmental delay and muscle weakness. He subsequently was diagnosed with glycogen storage disease type IV based on a liver biopsy histology and electron microscopy. Glycogen branching enzyme activity was in the low range. Genetic analysis demonstrated a novel heterozygous variant (c.760A>G; p.Thr254Ala) in exon 6 of the GBE1 gene, which is believed to be pathogenic. This variant was inherited from the patient's mother who was asymptomatic with normal glycogen branching enzyme activity. Whole-exome sequencing failed to reveal additional variations in the GBE1 gene., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016

5. Structural basis of glycogen branching enzyme deficiency and pharmacologic rescue by rational peptide design.

Author

Froese DS, Michaeli A, McCorvie TJ, Krojer T, Sasi M, Melaev E, Goldblum A, Zatsepin M, Lossos A, Álvarez R, Escribá PV, Minassian BA, von Delft F, Kakhlon O, and Yue WW

Subjects

Amino Acid Sequence, Computational Biology, Glycogen Debranching Enzyme System drug effects, Glycogen Debranching Enzyme System metabolism, Glycogen Storage Disease drug therapy, Glycogen Storage Disease genetics, Glycogen Storage Disease Type IV genetics, Humans, Molecular Sequence Data, Nervous System Diseases drug therapy, Nervous System Diseases genetics, Protein Structure, Tertiary, Sequence Alignment, Glycogen Debranching Enzyme System chemistry, Glycogen Debranching Enzyme System genetics, Glycogen Storage Disease enzymology, Glycogen Storage Disease Type IV enzymology, Mutation, Missense, Nervous System Diseases enzymology, Peptides therapeutic use

Abstract

Glycogen branching enzyme 1 (GBE1) plays an essential role in glycogen biosynthesis by generating α-1,6-glucosidic branches from α-1,4-linked glucose chains, to increase solubility of the glycogen polymer. Mutations in the GBE1 gene lead to the heterogeneous early-onset glycogen storage disorder type IV (GSDIV) or the late-onset adult polyglucosan body disease (APBD). To better understand this essential enzyme, we crystallized human GBE1 in the apo form, and in complex with a tetra- or hepta-saccharide. The GBE1 structure reveals a conserved amylase core that houses the active centre for the branching reaction and harbours almost all GSDIV and APBD mutations. A non-catalytic binding cleft, proximal to the site of the common APBD mutation p.Y329S, was found to bind the tetra- and hepta-saccharides and may represent a higher-affinity site employed to anchor the complex glycogen substrate for the branching reaction. Expression of recombinant GBE1-p.Y329S resulted in drastically reduced protein yield and solubility compared with wild type, suggesting this disease allele causes protein misfolding and may be amenable to small molecule stabilization. To explore this, we generated a structural model of GBE1-p.Y329S and designed peptides ab initio to stabilize the mutation. As proof-of-principle, we evaluated treatment of one tetra-peptide, Leu-Thr-Lys-Glu, in APBD patient cells. We demonstrate intracellular transport of this peptide, its binding and stabilization of GBE1-p.Y329S, and 2-fold increased mutant enzymatic activity compared with untreated patient cells. Together, our data provide the rationale and starting point for the screening of small molecule chaperones, which could become novel therapies for this disease., (© The Author 2015. Published by Oxford University Press.)

Published

2015

6. Branching enzyme deficiency: expanding the clinical spectrum.

Author

Paradas C, Akman HO, Ionete C, Lau H, Riskind PN, Jones DE, Smith TW, Hirano M, and Dimauro S

Subjects

Acute Disease, Age of Onset, Disease Progression, Female, Follow-Up Studies, Genetic Carrier Screening, Glycogen Storage Disease Type IV enzymology, Homozygote, Humans, Leukoencephalopathies diagnosis, Leukoencephalopathies genetics, Leukoencephalopathies pathology, Magnetic Resonance Imaging, Male, Middle Aged, Spinocerebellar Ataxias diagnosis, Spinocerebellar Ataxias genetics, Spinocerebellar Ataxias pathology, Glycogen Debranching Enzyme System genetics, Glycogen Storage Disease Type IV genetics, Glycogen Storage Disease Type IV pathology

Abstract

Importance: The neuromuscular presentation of glycogen branching enzyme deficiency includes a severe infantile form and a late-onset variant known as adult polyglucosan body disease. Herein, we describe 2 patients with adult acute onset of fluctuating neurological signs and brain magnetic resonance imaging lesions simulating multiple sclerosis. A better definition of this new clinical entity is needed to facilitate diagnosis., Objectives: To describe the clinical presentation and progression of a new intermediate variant of glycogen branching enzyme deficiency and to discuss genotype-phenotype correlations., Design, Setting, and Participants: Clinical, biochemical, morphological, and molecular study of 2 patients followed up for 6 years and 8 years at academic medical centers. The participants were 2 patients of non-Ashkenazi descent with adult acute onset of neurological signs initially diagnosed as multiple sclerosis., Main Outcomes and Measures: Clinical course, muscle and nerve morphology, longitudinal study of brain magnetic resonance imaging, and glycogen branching enzyme activity and GBE1 molecular analysis., Results: Molecular analysis showed that one patient was homozygous (c.1544G>A) and the other patient was compound heterozygous (c.1544G>A and c.1961-1962delCA) for GBE1 mutations. Residual glycogen branching enzyme activity was 16% and 30% of normal in leukocytes. Both patients manifested acute episodes of transient neurological symptoms, and neurological impairment was mild at age 45 years and 53 years. Brain magnetic resonance imaging revealed nonprogressive white matter lesions and spinocerebellar atrophy similar to typical adult polyglucosan body disease., Conclusions and Relevance: GBE1 mutations can cause an early adult-onset relapsing-remitting form of polyglucosan body disease distinct from adult polyglucosan body disease in several ways, including younger age at onset, history of infantile liver involvement, and subacute and remitting course simulating multiple sclerosis. This should orient neurologists toward the correct diagnosis.

Published

2014

7. Adult polyglucosan body disease: a rare presentation with chronic liver disease and ground-glass hepatocellular inclusions.

Author

Hajdu CH and Lefkowitch JH

Subjects

1,4-alpha-Glucan Branching Enzyme deficiency, Biopsy, Chronic Disease, Diagnosis, Differential, Glycogen Storage Disease Type IV complications, Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV genetics, Glycogen Storage Disease Type IV pathology, Hepatitis enzymology, Hepatitis pathology, Hepatocytes metabolism, Humans, Inclusion Bodies metabolism, Liver Cirrhosis enzymology, Liver Cirrhosis pathology, Liver Function Tests, Male, Middle Aged, Predictive Value of Tests, 1,4-alpha-Glucan Branching Enzyme genetics, Glucans metabolism, Glycogen Storage Disease Type IV diagnosis, Hepatitis genetics, Hepatocytes pathology, Inclusion Bodies pathology, Liver Cirrhosis genetics

Abstract

Liver involvement in genetic and metabolic disorders may result in intrahepatic accumulation of specific precursors or byproducts, which have distinctive features on light microscopy. The "polyglucosan disorders" are diseases in which polyglucosan (abnormal glycogen with decreased branching) is formed and deposited in various tissues because of decreased or absent glycogen branching enzyme activity. These disorders include Lafora disease (myoclonus epilepsy) and type IV glycogen storage disease. Polyglucosan deposits in both conditions result in ground-glass hepatocellular inclusions resembling those seen in chronic hepatitis B virus infection. In the present report, we describe a case of the rare, adulthood form of glycogen branching enzyme deficiency, adult polyglucosan body disease (APBD), in which abnormal serum liver tests prompted a liver biopsy. The pathologic findings of periportal ground-glass hepatocellular inclusions, mild chronic portal inflammation, and periportal fibrosis are not well described in APBD, but resemble the chronic changes that have been reported in Lafora disease. The differential diagnosis of ground-glass hepatocytes and the genetic basis of APBD are discussed., (© 2011 Thieme Medical Publishers, Inc.)

Published

2011

8. Branching enzyme deficiency/glycogenosis storage disease type IV presenting as a severe congenital hypotonia: muscle biopsy and autopsy findings, biochemical and molecular genetic studies.

Author

Taratuto AL, Akman HO, Saccoliti M, Riudavets M, Arakaki N, Mesa L, Sevlever G, Goebel H, and DiMauro S

Subjects

Brain pathology, Fatal Outcome, Female, Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV genetics, Humans, Infant, Infant, Newborn, Infant, Premature, Muscle Hypotonia congenital, Muscle Hypotonia enzymology, Muscle Hypotonia genetics, Muscle, Skeletal enzymology, 1,4-alpha-Glucan Branching Enzyme genetics, Glycogen Storage Disease Type IV pathology, Muscle Hypotonia pathology, Muscle, Skeletal pathology

Abstract

The fatal infantile neuromuscular presentation of branching enzyme deficiency (glycogen storage disease type IV) due to mutations in the gene encoding the glycogen branching enzyme, is a rare but probably underdiagnosed cause of congenital hypotonia. We report an infant girl with severe generalized hypotonia, born at 33 weeks gestation who required ventilatory assistance since birth. She had bilateral ptosis, mild knee and foot contractures and echocardiographic evidence of cardiomyopathy. A muscle biopsy at 1 month of age showed typical polyglucosan storage. The autopsy at 3.5 months of age showed frontal cortex polymicrogyria and polyglucosan bodies in neurons of basal ganglia, thalamus, substantia innominata, brain stem, and myenteric plexus, as well as liver involvement. Glycogen branching enzyme activity in muscle was virtually undetectable. Sequencing of the GBE1 gene revealed a homozygous 28 base pair deletion and a single base insertion at the same site in exon 5. This case confirms previous observations that GBE deficiency ought to be included in the differential diagnosis of congenital hypotonia and that the phenotype correlates with the 'molecular severity' of the mutation., (Copyright © 2010 Elsevier B.V. All rights reserved.)

Published

2010

9. Glycogen storage disease type IV: novel mutations and molecular characterization of a heterogeneous disorder.

Author

Li SC, Chen CM, Goldstein JL, Wu JY, Lemyre E, Burrow TA, Kang PB, Chen YT, and Bali DS

Subjects

Amino Acid Sequence, Base Sequence, DNA Mutational Analysis, Female, Genetic Predisposition to Disease, Genetic Testing methods, Glycogen Debranching Enzyme System metabolism, Glycogen Storage Disease Type IV complications, Glycogen Storage Disease Type IV diagnosis, Glycogen Storage Disease Type IV enzymology, Humans, Infant, Male, Molecular Sequence Data, Pedigree, Phenotype, Prognosis, Severity of Illness Index, Glycogen Debranching Enzyme System genetics, Glycogen Storage Disease Type IV genetics, Mutation, Missense, Sequence Deletion

Abstract

Glycogen storage disease type IV (GSD IV; Andersen disease) is caused by a deficiency of glycogen branching enzyme (GBE), leading to excessive deposition of structurally abnormal, amylopectin-like glycogen in affected tissues. The accumulated glycogen lacks multiple branch points and thus has longer outer branches and poor solubility, causing irreversible tissue and organ damage. Although classic GSD IV presents with early onset of hepatosplenomegaly with progressive liver cirrhosis, GSD IV exhibits extensive clinical heterogeneity with respect to age at onset and variability in pattern and extent of organ and tissue involvement. With the advent of cloning and determination of the genomic structure of the human GBE gene (GBE1), molecular analysis and characterization of underlying disease-causing mutations is now possible. A variety of disease-causing mutations have been identified in the GBE1 gene in GSD IV patients, many of whom presented with diverse clinical phenotypes. Detailed biochemical and genetic analyses of three unrelated patients suspected to have GSD IV are presented here. Two novel missense mutations (p.Met495Thr and p.Pro552Leu) and a novel 1-bp deletion mutation (c.1999delA) were identified. A variety of mutations in GBE1 have been previously reported, including missense and nonsense mutations, nucleotide deletions and insertions, and donor and acceptor splice-site mutations. Mutation analysis is useful in confirming the diagnosis of GSD IV--especially when higher residual GBE enzyme activity levels are seen and enzyme analysis is not definitive--and allows for further determination of potential genotype/phenotype correlations in this disease.

Published

2010

10. Neuropathological study of skeletal muscle, heart, liver, and brain in a neonatal form of glycogen storage disease type IV associated with a new mutation in GBE1 gene.

Author

Lamperti C, Salani S, Lucchiari S, Bordoni A, Ripolone M, Fagiolari G, Fruguglietti ME, Crugnola V, Colombo C, Cappellini A, Prelle A, Bresolin N, Comi GP, and Moggio M

Subjects

Base Sequence, Brain enzymology, Brain pathology, DNA Mutational Analysis, Fatal Outcome, Glycogen Storage Disease Type IV enzymology, Homozygote, Humans, Infant, Newborn, Liver enzymology, Liver pathology, Male, Microscopy, Electron, Transmission, Muscle, Skeletal pathology, Myocardium enzymology, Myocardium pathology, Codon, Nonsense, Glycogen Debranching Enzyme System deficiency, Glycogen Debranching Enzyme System genetics, Glycogen Storage Disease Type IV diagnosis, Glycogen Storage Disease Type IV genetics

Abstract

Glycogen storage disease type IV (GSD IV, or Andersen disease) is an autosomal recessive disorder due to the deficiency of 1,4-alpha-glucan branching enzyme (or glycogen branching enzyme, GBE1), resulting in an accumulation of amylopectin-like polysaccharide in muscle, liver, heart and central and peripheral nervous system. Typically, the presentation is in childhood with liver involvement up to cirrhosis. The neuromuscular form varies in onset (congenital, perinatal, juvenile and adult) and in severity. Congenital cases are rare, and fewer than 20 cases have been described and genetically determined so far. This form is characterized by polyhydramnios, neonatal hypotonia, and neuronal involvement; hepatopathy is uncommon, and the babies usually die between 4 weeks and 4 months of age. We report the case of an infant who presented severe hypotonia, dilatative cardiomyopathy, mild hepatopathy, and brain lateral ventricle haemorrhage, features consistent with the congenital form of GSD IV. He died at one month of life of cardiorespiratory failure. Muscle biopsy and heart and liver autoptic specimens showed many vacuoles filled with PAS-positive diastase-resistant materials. Electron-microscopic analysis showed mainly polyglucosan accumulations in all the tissues examined. Postmortem examination showed the presence of vacuolated neurons containing this abnormal polysaccharide. GBE1 biochemical activity was virtually absent in muscle and fibroblasts, and totally lacking in liver and heart as well as glycogen synthase activity. GBE1 gene sequence analysis revealed a novel homozygous nonsense mutation, p.E152X, in exon 4, correlating with the lack of enzyme activity and with the severe neonatal involvement. Our findings contribute to increasing the spectrum of mutation associated with congenital GSD IV.

Published

2009

11. Multisystem involvement in a patient due to accumulation of amylopectin-like material with diminished branching enzyme activity.

Author

Eminoglu TF, Tumer L, Okur I, Olgunturk R, Hasanoglu A, Gonul II, and Dalgic B

Subjects

1,4-alpha-Glucan Branching Enzyme genetics, Adolescent, Autopsy, Biopsy, Electromyography, Fatal Outcome, Genotype, Glycogen Storage Disease Type IV diagnosis, Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV genetics, Glycogen Storage Disease Type IV pathology, Heart Failure enzymology, Heart Failure etiology, Humans, Inclusion Bodies pathology, Liver pathology, Male, Muscle Weakness enzymology, Muscle Weakness etiology, Muscle, Skeletal pathology, Myocardium pathology, Phenotype, Up-Regulation, 1,4-alpha-Glucan Branching Enzyme deficiency, Amylopectin biosynthesis, Glycogen Storage Disease Type IV complications, Inclusion Bodies enzymology, Liver enzymology, Muscle, Skeletal enzymology, Myocardium enzymology

Abstract

We report a 13-year-old boy with multisystem involvement secondary to accumulation of amylopectin-like material. He was born to consanguineous parents at full term without any complications and his maternal perinatal history was uneventful. His parents were cousins. He had normal growth and development except for his weight. His sister died from an unexplained cardiomyopathy at the age of 8 years. Our patient's initial symptom was severe heart failure. Since he also had a complaint of muscle weakness, electromyography was performed which showed muscle involvement. The diagnosis was suggested by tissue biopsy of skeletal muscle showing intracellular, basophilic, diastase-resistant, periodic acid-Schiff-positive inclusion bodies and was confirmed by the presence of a completed branching enzyme deficiency. Similar intracytoplasmic inclusion-like bodies were also found in liver biopsy, but very few in number compared with the skeletal muscle. The patient died from an intercurrent infection. Postmortem endomyocardial biopsy revealed the same intracytoplasmic inclusions as described above affecting almost all myocardial cells. Ultrastructural examination of liver biopsy was nondiagnostic; however, myocardium showed prominent, large, intracytoplasmic deposits. Glycogen branching enzyme gene sequence was normal, and thus classical branching enzyme deficiency was excluded. Our patient represents the first molecular study performed on a patient in whom there was multiple system involvement secondary to accumulation of amylopectin-like material. We suggest that this is an as yet undefined and different phenotype of glycogen storage disease associated with multisystemic involvement.

Published

2008

12. Congenital type IV glycogenosis: the spectrum of pleomorphic polyglucosan bodies in muscle, nerve, and spinal cord with two novel mutations in the GBE1 gene.

Author

Nolte KW, Janecke AR, Vorgerd M, Weis J, and Schröder JM

Subjects

1,4-alpha-Glucan Branching Enzyme metabolism, Female, Glucans ultrastructure, Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV pathology, Humans, Inclusion Bodies metabolism, Inclusion Bodies ultrastructure, Infant, Infant, Newborn, Male, Microscopy, Electron, Transmission, Muscle, Skeletal metabolism, Muscle, Skeletal ultrastructure, Pregnancy, Spinal Cord metabolism, Spinal Cord ultrastructure, Sural Nerve metabolism, Sural Nerve ultrastructure, 1,4-alpha-Glucan Branching Enzyme genetics, Glucans metabolism, Glycogen Storage Disease Type IV genetics, Mutation

Abstract

A diagnosis of GSD-IV was established in three premature, floppy infants based on characteristic, however unusually pleomorphic polyglucosan bodies at the electron microscopic level, glycogen branching enzyme deficiency in two cases, and the identification of GBE1 mutations in two cases. Pleomorphic polyglucosan bodies in muscle fibers and macrophages, and less severe in Schwann cells and microglial cells were noted. Most of the inclusions were granular and membrane-bound; others had an irregular contour, were more electron dense and were not membrane bound, or homogenous ('hyaline'). A paracrystalline pattern of granules was repeatedly noted showing a periodicity of about 10 nm with an angle of about 60 degrees or 120 degrees at sites of changing linear orientation. Malteser crosses were noted under polarized light in the larger inclusions. Some inclusions were PAS positive and others were not. Severely atrophic muscle fibers without inclusions, but with depletion of myofibrils in the plane of section studied indicated the devastating myopathic nature of the disease. Schwann cells and peripheral axons were less severely affected as was the spinal cord. Two novel protein-truncating mutations (c.1077insT, p.V359fsX16; g.101517_127067del25550insCAGTACTAA, DelExon4-7) were identified in these families. The present findings extend previous studies indicating that truncating GBE1 mutations cause a spectrum of severe diseases ranging from generalized intrauterine hydrops to fatal perinatal hypotonia and fatal cardiomyopathy in the first months of life.

Published

2008

13. Unclassified polysaccharidosis of the heart and skeletal muscle in siblings.

Author

Schoser B, Bruno C, Schneider HC, Shin YS, Podskarbi T, Goldfarb L, Müller-Felber W, and Müller-Höcker J

Subjects

Adolescent, Adult, Female, Germany, Glycogen metabolism, Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV genetics, Glycogen Storage Disease Type IV metabolism, Glycogen Storage Disease Type IV pathology, Humans, Male, Muscle, Skeletal enzymology, Muscle, Skeletal pathology, Myocardium enzymology, Myocardium pathology, Pedigree, Siblings, Glycogen Storage Disease Type IV diagnosis, Muscle, Skeletal metabolism, Myocardium metabolism

Abstract

We describe a 15-year-old boy and his 19-year-old sister with progressive dilated cardiomyopathy and mild non-progressive proximal lower limb myopathy, secondary to the accumulation of amylopectin-like fibrillar glycogen, (polyglucosan) bodies, in heart and skeletal muscle. Evidence of idiopathic amylopectinosis or polysaccharidosis was demonstrated in heart and skeletal muscle tissue by histology, electron microscopy, biochemical, and genetic analysis. In both siblings the heart muscle stored PAS-positive, proteinase-k resistant and partly diastase resistant granulo-filamentous material, simulating polyglucosan bodies. Glycogen branching enzyme activity, and phosphofructokinase enzyme activity, measured in skeletal muscle tissue and explanted heart tissue were all within the normal limits, however glycogen content was elevated. Furthermore, GBE1, PRKAG2, desmin, alphabeta-crystallin, ZASP, myotilin, and LAMP-2 gene sequencing revealed no mutation, excluding e.g. glycogen storage disease type 4 and desmin-related myofibrillar cardiomyopathies. In both patients the diagnosis of an idiopathic polysaccharidosis with progressive dilated cardiomyopathy was made, requiring heart transplantation at age 13 and 14, respectively. Both patients belong to an autosomal recessive group of biochemically and genetically unclassified severe vacuolar glycogen storage disease of the heart and skeletal muscle. Up to now unidentified glycogen synthesis or glycogen degradation pathways are supposed to contribute to this idiopathic glycogen storage disease.

Published

2008

14. High frequency of missense mutations in glycogen storage disease type VI.

Author

Beauchamp NJ, Taybert J, Champion MP, Layet V, Heinz-Erian P, Dalton A, Tanner MS, Pronicka E, and Sharrard MJ

Subjects

Amino Acid Sequence, Animals, Blood Glucose metabolism, Child, Preschool, DNA Mutational Analysis, Exons, Female, Genetic Predisposition to Disease, Genotype, Glycogen Phosphorylase, Liver Form chemistry, Glycogen Phosphorylase, Liver Form deficiency, Glycogen Storage Disease Type IV enzymology, Humans, Infant, Introns, Lactic Acid blood, Male, Models, Molecular, Molecular Sequence Data, Pedigree, Phenotype, Protein Conformation, Sequence Alignment, Sequence Homology, Amino Acid, Severity of Illness Index, Glycogen Phosphorylase, Liver Form genetics, Glycogen Storage Disease Type IV genetics, Liver enzymology, Mutation, Missense

Abstract

Deficiency of liver glycogen phosphorylase in glycogen storage disease (GSD) type VI results in a reduced ability to mobilize glucose from glycogen. Six mutations of the PYGL gene, which encodes the liver isoform of the enzyme, have been identified in the literature. We have characterized eight patients from seven families with GSD type VI and identified 11 novel PYGL gene defects. The majority of the mutations were missense, resulting in the substitution of highly conserved residues. These could be grouped into those that were predicted to affect substrate binding (p.V456M, p.E673K, p.S675L, p.S675T), pyridoxal phosphate binding (p.R491C, p.K681T), or activation of glycogen phosphorylase (p.Q13P) or that had an unknown effect (p.N632I and p.D634H). Two mutations were predicted to result in null alleles, p.R399X and [c.1964_1969inv6;c.1969+1_+4delGTAC]. Only 7 of the 23 (30%) reported PYGL alleles carry nonsense, splice site or frameshift mutations compared to 68-80% of affected alleles of the highly homologous muscle glycogen phosphorylase gene, PYGM, that underlie McArdle disease. There was heterogeneity in the clinical symptoms observed in affected individuals. These varied from hepatomegaly and subclinical hypoglycaemia, to severe hepatomegaly with recurrent severe hypoglycaemia and postprandial lactic acidosis. We conclude that deficiency of liver glycogen phosphorylase is predominantly the result of missense mutations affecting enzyme activity. There are no common mutations and the severity of clinical symptoms varies significantly.

Published

2007

15. Neuromuscular forms of glycogen branching enzyme deficiency.

Author

Bruno C, Cassandrini D, Assereto S, Akman HO, Minetti C, and Di Mauro S

Subjects

Amino Acid Substitution, Animals, Chromosomes, Human, Pair 3, Disease Models, Animal, Genotype, Glycogen Storage Disease Type IV genetics, Humans, Mutation, Neuromuscular Diseases genetics, 1,4-alpha-Glucan Branching Enzyme deficiency, Glycogen Storage Disease Type IV enzymology, Neuromuscular Diseases enzymology, Polymorphism, Single Nucleotide

Abstract

Deficiency of glycogen branching enzyme is causative of Glycogen Storage Disease type IV (GSD-IV), a rare autosomal recessive disorder of the glycogen synthesis, characterized by the accumulation of amylopectin-like polysaccharide, also known as polyglucosan, in almost all tissues. Its clinical presentation is variable and involves the liver or the neuromuscular system and different mutations in the GBE1 gene, located on chromosome 3, have been identified in both phenotypes. This review will addresses the neuromuscular clinical variants, focusing on the molecular genetics aspects of this disorder.

Published

2007

16. Allele frequency and likely impact of the glycogen branching enzyme deficiency gene in Quarter Horse and Paint Horse populations.

Author

Wagner ML, Valberg SJ, Ames EG, Bauer MM, Wiseman JA, Penedo MC, Kinde H, Abbitt B, and Mickelson JR

Subjects

1,4-alpha-Glucan Branching Enzyme genetics, Abortion, Veterinary enzymology, Abortion, Veterinary genetics, Abortion, Veterinary pathology, Animals, Animals, Newborn, DNA chemistry, DNA genetics, Female, Genotype, Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV genetics, Glycogen Storage Disease Type IV pathology, Histocytochemistry veterinary, Horse Diseases pathology, Horses, Muscle, Skeletal pathology, Myocardium pathology, Pedigree, Polymerase Chain Reaction veterinary, Pregnancy, Retrospective Studies, 1,4-alpha-Glucan Branching Enzyme deficiency, Alleles, Glycogen Storage Disease Type IV veterinary, Horse Diseases enzymology, Horse Diseases genetics

Abstract

Glycogen Branching Enzyme Deficiency (GBED), a fatal condition recently identified in fetuses and neonatal foals of the Quarter Horse and Paint Horse lineages, is caused by a nonsense mutation in codon 34 of the GBE1 gene, which prevents the synthesis of a functional GBE protein and severely disrupts glycogen metabolism. The aims of this project were to determine the mutant GBE1 allele frequency in random samples from the major relevant horse breeds, as well as the frequency with which GBED is associated with abortion and early neonatal death using the tissue archives from veterinary diagnostic laboratories. The mutant GBE1 allele frequency in registered Quarter Horse, Paint Horse, and Thoroughbred populations was 0.041, 0.036, and 0.000, respectively. Approximately 2.5% of fetal and early neonatal deaths in Quarter Horse-related breeds submitted to 2 different US diagnostic laboratories were homozygous for the mutant GBE1 allele, with the majority of these being abortions. Retrospective histopathology of the homozygotes detected periodic acid Schiff's (PAS)-positive inclusions in the cardiac or skeletal muscle, which is characteristic of GBED, in 8 out of the 9 cases. Pedigree and genotype analyses supported the hypothesis that GBED is inherited as a simple recessive trait from a single founder. The frequency with which GBED is associated with abortion and neonatal mortality in Quarter Horse-related breeds makes the DNA-based test valuable in determining specific diagnoses and designing matings that avoid conception of a GBED foal.

Published

2006

17. Fetal type IV glycogen storage disease: clinical, enzymatic, and genetic data of a pure muscular form with variable and early antenatal manifestations in the same family.

Author

L'herminé-Coulomb A, Beuzen F, Bouvier R, Rolland MO, Froissart R, Menez F, Audibert F, and Labrune P

Subjects

Adult, Female, Fetal Death, Fetal Diseases enzymology, Fetal Diseases genetics, Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV genetics, Humans, Male, Pregnancy, Fetal Diseases physiopathology, Glycogen Storage Disease Type IV physiopathology

Abstract

We report on a family of three consecutive fetuses affected by type IV glycogen storage disease (GSD IV). In all cases, cervical cystic hygroma was observed on the 12-week-ultrasound examination. During the second trimester, fetal hydrops developed in the first pregnancy whereas fetal akinesia appeared in the second pregnancy. The diagnosis was suggested by microscopic examination of fetal tissues showing characteristic inclusions exclusively in striated fibers, then confirmed by enzymatic studies on frozen muscle. Antenatal diagnosis was performed on the third and fourth pregnancies: cervical cystic hygroma and low glycogen branching enzyme (GBE) activity on chorionic villi sample (CVS) were detected in the third pregnancy whereas ultrasound findings were normal and GBE activity within normal range on CVS in the fourth pregnancy. Molecular analysis showed that the mother was heterozygous for a c.1471G > C mutation in exon 12, leading to the replacement of an alanine by a tyrosine at codon 491 (p.A491T); the father was heterozygous for a c.895G > T mutation in exon 7, leading to the creation of a stop codon at position 299 (p.G299X). GSD IV has to be considered in a context of cervical cystic hygroma with normal karyotype, particularly when second trimester hydrops or akinesia develop. Enzymatic analysis of GBE must be performed on CVS or amniotic cells to confirm the diagnosis. Characteristic intracellular inclusions are specific to the disease and should be recognized, even in macerated tissues after fetal death. Genetic analysis of the GBE gene may help to shed some light on the puzzling diversity of GSD IV phenotypes., (Copyright 2005 Wiley-Liss, Inc.)

Published

2005

18. Adult polyglucosan body disease: a case report of a manifesting heterozygote.

Author

Ubogu EE, Hong ST, Akman HO, Dimauro S, Katirji B, Preston DC, and Shapiro BE

Subjects

1,4-alpha-Glucan Branching Enzyme genetics, Aged, Base Sequence, Chromosomes, Human, Pair 3, Diagnosis, Differential, Glycogen Storage Disease Type IV complications, Glycogen Storage Disease Type IV pathology, Heterozygote, Humans, Jews, Magnetic Resonance Imaging, Male, Molecular Sequence Data, Point Mutation, 1,4-alpha-Glucan Branching Enzyme deficiency, Brain pathology, Glucans metabolism, Glycogen Storage Disease Type IV diagnosis, Glycogen Storage Disease Type IV enzymology, Inclusion Bodies

Abstract

A 62-year-old man developed progressive gait instability, bladder dysfunction, proximal weakness, distal sensory loss, and mild cognitive impairment over 6 years. Neurologic examination revealed upper and lower motor neuron dysfunction in the lower extremities, with distal sensory loss. Electrodiagnostic studies, magnetic resonance imaging of the brain, and sural nerve biopsy were consistent with adult polyglucosan body disease. Biochemical and genetic analyses demonstrated reduced glycogen brancher enzyme levels associated with a heterozygous point mutation (Tyr329Ser or Y329S) in the glycogen brancher enzyme gene on chromosome 3. Mutational heterozygosity in the glycogen brancher enzyme gene has not been previously reported as a cause for this rare disease. A review of the clinical presentation, pathogenesis, etiology, and diagnosis of this disease is presented.

Published

2005

19. Amylopectinosis disease isolated to the heart with normal glycogen branching enzyme activity and gene sequence.

Author

Das BB, Narkewicz MR, Sokol RJ, Chen YT, Bali D, Li SC, Matthews MR, Mierau GW, and Ivy DD

Subjects

Amylopectin metabolism, Cardiomyopathies enzymology, Cardiomyopathies genetics, Cardiomyopathies pathology, Electrocardiography, Female, Fibroblasts enzymology, Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV genetics, Glycogen Storage Disease Type IV pathology, Humans, Infant, Ventricular Dysfunction, Left etiology, 1,4-alpha-Glucan Branching Enzyme metabolism, Cardiomyopathies surgery, Glycogen Storage Disease Type IV surgery

Abstract

We report a 17-month-old female patient with a rare cause of cardiomyopathy secondary to accumulation of amylopectin-like material (fibrillar glycogen) isolated to the heart. Evidence of amylopectinosis isolated to cardiac myocytes in this patient was demonstrated by histology and electron microscopy. Glycogen content, glycogen branching enzyme (GBE) activity, as well as phosphofructokinase enzyme activities measured in liver, skeletal muscle, fibroblasts and ex-transplanted heart tissue were all in the normal to lower normal ranges. Normal skeletal muscle and liver tissue histology and GBE activity, normal GBE activity in skin fibroblasts, plus normal GBE gene sequence in this patient exclude the classical branching enzyme deficiency (type IV GSD). We believe that this is an as yet uncharacterized and novel phenotype of GSD associated with cardiomyopathy, in which there is an imbalance in the regulation of glycogen metabolism limited to the heart.

Published

2005

20. Clinical and genetic heterogeneity of branching enzyme deficiency (glycogenosis type IV).

Author

Bruno C, van Diggelen OP, Cassandrini D, Gimpelev M, Giuffrè B, Donati MA, Introvini P, Alegria A, Assereto S, Morandi L, Mora M, Tonoli E, Mascelli S, Traverso M, Pasquini E, Bado M, Vilarinho L, van Noort G, Mosca F, DiMauro S, Zara F, and Minetti C

Subjects

1,4-alpha-Glucan Branching Enzyme chemistry, 1,4-alpha-Glucan Branching Enzyme deficiency, Adult, Age of Onset, Amino Acid Substitution, Cells, Cultured enzymology, Child, Child, Preschool, Consanguinity, DNA genetics, DNA Mutational Analysis, Erythrocytes enzymology, Fatal Outcome, Fibroblasts enzymology, Genotype, Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV epidemiology, Glycogen Storage Disease Type IV pathology, Humans, Hydrogen Bonding, Hydrophobic and Hydrophilic Interactions, Infant, Infant, Newborn, Liver pathology, Models, Molecular, Muscles enzymology, Muscles pathology, Phenotype, Protein Conformation, RNA Splice Sites genetics, Sequence Deletion, 1,4-alpha-Glucan Branching Enzyme genetics, Genetic Heterogeneity, Glycogen Storage Disease Type IV genetics, Mutation

Abstract

Background: Glycogen storage disease type IV (GSD-IV) is a clinically heterogeneous autosomal recessive disorder due to glycogen branching enzyme (GBE) deficiency and resulting in the accumulation of an amylopectin-like polysaccharide. The typical presentation is liver disease of childhood, progressing to lethal cirrhosis. The neuromuscular form of GSD-IV varies in onset (perinatal, congenital, juvenile, or adult) and severity., Objective: To identify the molecular bases of different neuromuscular forms of GSD-IV and to establish possible genotype/phenotype correlations., Methods: Eight patients with GBE deficiency had different neuromuscular presentations: three had fetal akinesia deformation sequence (FADS), three had congenital myopathy, one had juvenile myopathy, and one had combined myopathic and hepatic features. In all patients, the promoter and the entire coding region of the GBE gene at the RNA and genomic level were sequenced., Results: Nine novel mutations were identified, including nonsense, missense, deletion, insertion, and splice-junction mutations. The three cases with FADS were homozygous, whereas all other cases were compound heterozygotes., Conclusions: This study expands the spectrum of mutations in the GBE gene and confirms that the neuromuscular presentation of GSD-IV is clinically and genetically heterogeneous.

Published

2004

21. Mutations in a Sar1 GTPase of COPII vesicles are associated with lipid absorption disorders.

Author

Jones B, Jones EL, Bonney SA, Patel HN, Mensenkamp AR, Eichenbaum-Voline S, Rudling M, Myrdal U, Annesi G, Naik S, Meadows N, Quattrone A, Islam SA, Naoumova RP, Angelin B, Infante R, Levy E, Roy CC, Freemont PS, Scott J, and Shoulders CC

Subjects

COP-Coated Vesicles enzymology, Chylomicrons metabolism, Female, GTP Phosphohydrolases chemistry, Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV genetics, Humans, Intestinal Absorption, Malabsorption Syndromes metabolism, Male, Models, Molecular, Pedigree, Protein Conformation, Spinocerebellar Degenerations enzymology, Spinocerebellar Degenerations genetics, Dietary Fats pharmacokinetics, GTP Phosphohydrolases genetics, Malabsorption Syndromes enzymology, Malabsorption Syndromes genetics, Mutation

Abstract

Dietary fat is an important source of nutrition. Here we identify eight mutations in SARA2 that are associated with three severe disorders of fat malabsorption. The Sar1 family of proteins initiates the intracellular transport of proteins in COPII (coat protein)-coated vesicles. Our data suggest that chylomicrons, which vastly exceed the size of typical COPII vesicles, are selectively recruited by the COPII machinery for transport through the secretory pathways of the cell.

Published

2003

22. The variable presentations of glycogen storage disease type IV: a review of clinical, enzymatic and molecular studies.

Author

Moses SW and Parvari R

Subjects

1,4-alpha-Glucan Branching Enzyme genetics, Age of Onset, Amino Acid Sequence, Animals, Base Sequence, DNA, Complementary metabolism, Disease Models, Animal, Exons, Female, Glycogen Storage Disease Type IV diagnosis, Glycogen Storage Disease Type IV enzymology, Humans, Male, Molecular Sequence Data, Mutation, Polymorphism, Genetic, Polysaccharides genetics, Pregnancy, Prenatal Diagnosis, Sequence Homology, Amino Acid, Glycogen Storage Disease Type IV genetics, Glycogen Storage Disease Type IV pathology

Abstract

Glycogen storage disease type IV (GSD-IV), also known as Andersen disease or amylopectinosis (MIM 23250), is a rare autosomal recessive disorder caused by a deficiency of glycogen branching enzyme (GBE) leading to the accumulation of amylopectin-like structures in affected tissues. The disease is extremely heterogeneous in terms of tissue involvement, age of onset and clinical manifestations. The human GBE cDNA is approximately 3-kb in length and encodes a 702-amino acid protein. The GBE amino acid sequence shows a high degree of conservation throughout species. The human GBE gene is located on chromosome 3p14 and consists of 16 exons spanning at least 118 kb of chromosomal DNA. Clinically the classic Andersen disease is a rapidly progressive disorder leading to terminal liver failure unless liver transplantation is performed. Several mutations have been reported in the GBE gene in patients with classic phenotype. Mutations in the GBE gene have also been identified in patients with the milder non-progressive hepatic form of the disease. Several other variants of GSD-IV have been reported: a variant with multi-system involvement including skeletal and cardiac muscle, nerve and liver; a juvenile polysaccharidosis with multi-system involvement but normal GBE activity; and the fatal neonatal neuromuscular form associated with a splice site mutation in the GBE gene. Other presentations include cardiomyopathy, arthrogryposis and even hydrops fetalis. Polyglucosan body disease, characterized by widespread upper and lower motor neuron lesions, can present with or without GBE deficiency indicating that different biochemical defects could result in an identical phenotype. It is evident that this disease exists in multiple forms with enzymatic and molecular heterogeneity unparalleled in the other types of glycogen storage diseases.

Published

2002

23. Formation of high molecular weight complexes of mutant Cu, Zn-superoxide dismutase in a mouse model for familial amyotrophic lateral sclerosis.

Author

Johnston JA, Dalton MJ, Gurney ME, and Kopito RR

Subjects

Animals, Cell Line, Enzyme Stability, Female, Genetic Diseases, Inborn, Glycogen Storage Disease Type IV pathology, Humans, Inclusion Bodies metabolism, Male, Mice, Mice, Transgenic, Microtubules metabolism, Molecular Weight, Motor Neurons enzymology, Motor Neurons pathology, Mutagenesis, Superoxide Dismutase genetics, Superoxide Dismutase-1, Glycogen Storage Disease Type IV enzymology, Superoxide Dismutase metabolism

Abstract

Deposition of aggregated protein into neurofilament-rich cytoplasmic inclusion bodies is a common cytopathological feature of neurodegenerative disease. How-or indeed whether-protein aggregation and inclusion body formation cause neurotoxicity are presently unknown. Here, we show that the capacity of superoxide dismutase (SOD) to aggregate into biochemically distinct, high molecular weight, insoluble protein complexes (IPCs) is a gain of function associated with mutations linked to autosomal dominant familial amyotrophic lateral sclerosis. SOD IPCs are detectable in spinal cord extracts from transgenic mice expressing mutant SOD several months before inclusion bodies and motor neuron pathology are apparent. Sequestration of mutant SOD into cytoplasmic inclusion bodies resembling aggresomes requires retrograde transport on microtubules. These data indicate that aggregation and inclusion body formation are mechanistically and temporally distinct processes.

Published

2000

24. Novel missense mutations in the glycogen-branching enzyme gene in adult polyglucosan body disease.

Author

Ziemssen F, Sindern E, Schröder JM, Shin YS, Zange J, Kilimann MW, Malin JP, and Vorgerd M

Subjects

Amino Acid Sequence, Base Sequence, Biopsy, DNA Mutational Analysis, Female, Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV pathology, Humans, Middle Aged, Sural Nerve pathology, 1,4-alpha-Glucan Branching Enzyme genetics, Glycogen Storage Disease Type IV genetics, Mutation, Missense

Abstract

We describe the first non-Ashkenazi patient with adult polyglucosan body disease and decreased glycogen-branching enzyme (GBE) activity in leukocytes. Gene analysis revealed compound heterozygosity for two novel missense mutations Arg515His and Arg524Gln in the GBE gene. Both missense mutations are predicted to impair GBE activity. This is the first identification of GBE mutations underlying adult polyglucosan body disease in a non-Ashkenazi family, and confirms that adult glycogen storage disease type IV can manifest clinically as adult polyglucosan body disease.

Published

2000

25. A novel missense mutation in the glycogen branching enzyme gene in a child with myopathy and hepatopathy.

Author

Bruno C, DiRocco M, Lamba LD, Bado M, Marino C, Tsujino S, Shanske S, Stella G, Minetti C, van Diggelen OP, and DiMauro S

Subjects

Amino Acid Substitution, Arginine, Base Sequence, Cytoplasmic Granules pathology, Cytoplasmic Granules ultrastructure, Glutamine, Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV genetics, Heterozygote, Humans, Infant, Liver ultrastructure, Liver Diseases enzymology, Liver Diseases pathology, Male, Muscle, Skeletal ultrastructure, Muscular Diseases enzymology, Muscular Diseases pathology, 1,4-alpha-Glucan Branching Enzyme genetics, Liver pathology, Liver Diseases genetics, Muscle, Skeletal pathology, Muscular Diseases genetics, Mutation, Missense

Abstract

We have identified a novel missense mutation in the gene for glycogen branching enzyme (GBE 1) in a 16-month-old infant with a combination of hepatic and muscular features, an atypical clinical presentation of glycogenosis type IV (GSD IV). The patient was heterozygous for a G-to-A substitution at codon 524 (R524Q), changing an encoded arginine (CGA) to glutamine (CAA), while the GBE1 gene on the other allele was not expressed. This case broadens the spectrum of mutations in patients with GSD IV and confirms the clinical and molecular heterogeneity of this disease.

Published

1999

26. Early-onset fetal hydrops and muscle degeneration in siblings due to a novel variant of type IV glycogenosis.

Author

Cox PM, Brueton LA, Murphy KW, Worthington VC, Bjelogrlic P, Lazda EJ, Sabire NJ, and Sewry CA

Subjects

1,4-alpha-Glucan Branching Enzyme metabolism, Adult, Age of Onset, Family Health, Fatal Outcome, Female, Genetic Variation, Gestational Age, Glycogen Storage Disease Type IV enzymology, Humans, Hydrops Fetalis genetics, Muscle, Skeletal pathology, Muscle, Skeletal ultrastructure, Muscular Diseases congenital, Muscular Diseases genetics, Pregnancy, Glycogen Storage Disease Type IV genetics, Hydrops Fetalis pathology, Muscular Diseases pathology

Abstract

We report on 3 consecutive sib fetuses, presenting at 13, 12, and 13 weeks of gestation, respectively, with fetal hydrops, limb contractures, and akinesia. Autopsy of the first fetus showed subcutaneous fluid collections and severe degeneration of skeletal muscle. Histologic studies demonstrated massive accumulation of diastase-resistant periodic acid-Schiff-positive material in the skeletal muscle cells and epidermal keratinocytes of all 3 fetuses. Enzyme studies of fibroblasts from the 3rd fetus showed deficient activity of glycogen brancher enzyme, indicating that this is a new, severe form of glycogenosis type IV with onset in the early second trimester., (Copyright 1999 Wiley-Liss, Inc.)

Published

1999

27. Hepatic and neuromuscular forms of glycogen storage disease type IV caused by mutations in the same glycogen-branching enzyme gene.

Author

Bao Y, Kishnani P, Wu JY, and Chen YT

Subjects

1,4-alpha-Glucan Branching Enzyme metabolism, Alleles, Base Sequence, Child, Preschool, DNA Primers chemistry, Female, Gene Expression Regulation, Enzymologic, Glycogen Storage Disease Type IV genetics, Humans, Infant, Molecular Sequence Data, RNA, Messenger genetics, Sequence Deletion, 1,4-alpha-Glucan Branching Enzyme genetics, Glycogen Storage Disease Type IV enzymology, Liver Diseases enzymology, Neuromuscular Diseases enzymology, Point Mutation

Abstract

Glycogen storage disease type IV (GSD-IV) is an autosomal recessive disease resulting from deficient glycogen-branching enzyme (GBE) activity. The classic and most common form is progressive liver cirrhosis and failure leading to either liver transplantation or death by 5 yr of age. However, the liver disease is not always progressive. In addition, a neuromuscular type of the disease has been reported. The molecular basis of GSD-IV is not known, nor is there a known reason for the clinical variability. We studied the GBE gene in patients with various presentations of GSD-IV. Three point mutations in the GBE gene were found in two patients with the classical presentation: R515C, F257L, and R524X. Transient expression experiments showed that these mutations inactivated GBE activity. Two point mutations, L224P and Y329S, were detected in two separate alleles of a patient with the nonprogressive hepatic form. The L224P resulted in complete loss of GBE activity, whereas the Y329S resulted in loss of approximately 50% of GBE activity. The Y329S allele was also detected in another patient with the nonprogressive form of GSD-IV but not in 35 unrelated controls or in patients with the more severe forms of GSD-IV. A 210-bp deletion from nucleotide 873 to 1082 of the GBE cDNA was detected in a patient with the fatal neonatal neuromuscular presentation. This deletion, representing the loss of one full exon, was caused by a 3' acceptor splicing site mutation (ag to aa). The deletion abolished GBE activity. Our studies indicate that the three different forms of GSD-IV were caused by mutations in the same GBE gene. The data also suggest that the significant retention of GBE activity in the Y329S allele may be a reason for the mild disease. Further study of genotype/phenotype correlations may yield useful information in predicting the clinical outcomes.

Published

1996

28. Clinical and laboratory findings in four patients with the non-progressive hepatic form of type IV glycogen storage disease.

Author

McConkie-Rosell A, Wilson C, Piccoli DA, Boyle J, DeClue T, Kishnani P, Shen JJ, Boney A, Brown B, and Chen YT

Subjects

1,4-alpha-Glucan Branching Enzyme metabolism, Adolescent, Adult, Child, Preschool, Failure to Thrive, Female, Fibroblasts enzymology, Glycogen Storage Disease Type IV pathology, Hepatomegaly enzymology, Hepatomegaly pathology, Humans, Liver enzymology, Liver pathology, Male, Skin cytology, Skin enzymology, Splenomegaly enzymology, Splenomegaly pathology, Glycogen Storage Disease Type IV enzymology

Abstract

The classic clinical presentation for type IV glycogen storage disease (branching enzyme deficiency, GSD IV) is hepatosplenomegaly with failure to thrive occurring in the first 18 months of life, followed by progressive liver failure and death by age 5 years. Although there have been two patients without apparent liver progression previously reported, no long-term follow-up clinical data have been available. We present here the clinical spectrum of the non-progressive liver form of GSD IV in four patients, and long-term follow-up of the oldest identified patients (ages 13 and 20 years). None has developed progressive liver cirrhosis, skeletal muscle, cardiac or neurological involvement, and none has been transplanted. Branching enzyme activity was also measured in cultured skin fibroblasts from patients with the classic liver progressive, the early neonatal fatal, and the non-progressive hepatic presentations of GSD IV. The residual branching enzyme activity in the patients without progression was not distinguishable from the other forms and could not be used to predict the clinical course. Our data indicate that GSD IV does not always necessitate hepatic transplantation and that caution should be used when counselling patients regarding the prognosis of GSD IV. Patients should be carefully monitored for evidence of progression before recommending liver transplantation.

Published

1996

29. Concomitant branching enzyme and phosphorylase deficiencies. An unusual glycogenosis with extensive neuronal polyglucosan storage.

Author

Herrick MK, Twiss JL, Vladutiu GD, Glasscock GF, and Horoupian DS

Subjects

Central Nervous System enzymology, Central Nervous System pathology, Female, Glycogen Storage Disease Type IV enzymology, Humans, Inclusion Bodies pathology, Infant, Newborn, Muscles enzymology, Myocardium enzymology, Myocardium pathology, Neurons enzymology, Neurons pathology, Glucans metabolism, Glycogen Storage Disease Type IV pathology, Muscles pathology, Phosphorylases deficiency

Abstract

A baby girl was born hypotonic and was respirator-dependent until death at 43 days of age. A muscle biopsy revealed PAS-positive, diastase-resistant sarcoplasmic inclusions with a vaguely fibrillar structure by electron microscopy. Biochemical studies at autopsy disclosed complete absence of branching enzyme in skeletal muscle and heart, and a deficiency of phosphorylase activity in skeletal muscle with a modest reduction in myocardium. Storage material was present in glia and perikarya of neurons, increasing in amount in the rostrocaudal direction, involving most severely the motor neurons in the brain stem and spinal cord, dorsal root ganglia and myenteric plexi. Inclusions were also present in most organs, especially liver and skeletal muscle. Ultrastructurally, the inclusions ranged from granular aggregates of membrane-bound material concentrated in the region of Golgi apparatus to large filamentous bodies similar to polyglucosan bodies. This baby differs from other patients with infantile glycogenosis IV by the severity and onset of symptoms at birth, involvement of neuronal perikarya and widespread extraneural deposits. The combined deficiencies of branching enzyme and phosphorylase may have accounted for the unique clinical and neuropathological findings.

Published

1994

30. Glycogen storage disease type IV: inherited deficiency of branching enzyme activity in cats.

Author

Fyfe JC, Giger U, Van Winkle TJ, Haskins ME, Steinberg SA, Wang P, and Patterson DF

Subjects

Animals, Cat Diseases enzymology, Cat Diseases pathology, Cats, Female, Genes, Recessive, Glycogen metabolism, Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV genetics, Inclusion Bodies pathology, Male, Muscles pathology, Nervous System pathology, Pedigree, 1,4-alpha-Glucan Branching Enzyme deficiency, Cat Diseases genetics, Glycogen Storage Disease Type IV veterinary

Abstract

Glycogen storage disease type IV due to branching enzyme deficiency was found in an inbred family of Norwegian forest cats, an uncommon breed of domestic cats. Skeletal muscle, heart, and CNS degeneration were clinically apparent and histologically evident in affected cats older than 5 mo of age, but cirrhosis and hepatic failure, hallmarks of the human disorder, were absent. Beginning at or before birth, affected cats accumulated an abnormal glycogen in many tissues that was determined by histochemical, enzymatic, and spectral analysis to be a poorly branched alpha-1,4-D-glucan. Branching enzyme activity was less than 0.1 of normal in liver and muscle of affected cats and partially deficient (0.17-0.75 of normal) in muscle and leukocytes of the parents of affected cats. These data and pedigree analysis indicate that branching enzyme deficiency is a simple autosomal recessive trait in this family. This is the first reported animal model of human glycogen storage disease type IV. A breeding colony derived from a relative of the affected cats has been established.

Published

1992

31. A mild juvenile variant of type IV glycogenosis.

Author

Reusche E, Aksu F, Goebel HH, Shin YS, Yokota T, and Reichmann H

Subjects

Child, Glycogen Storage Disease Type IV enzymology, Histocytochemistry, Humans, Infant, Male, Muscles enzymology, Muscles pathology, Staining and Labeling, Sweat Glands enzymology, Sweat Glands pathology, Glycogen Storage Disease Type IV pathology

Abstract

The mild juvenile form of type IV glycogenosis, confirmed by a profound deficiency of the brancher enzyme in tissue specimens is reported from three Turkish male siblings who, foremost, suffered from chronic progressive myopathy. Muscle fibers contained polyglucosan inclusions of typical fine structure i.e. a mixture of granular and filamentous glycogen. They reacted strongly for myophosphorylase, but were resistant to diastase. These inclusions were ubiquitinated and reacted with antibody KM-279 which previously has been shown to bind to Lafora bodies, corpora amylacea and polyglucosan material in hepatic and cardiac cells of type IV glycogenosis as well as polyglucosan body myopathy without brancher enzyme deficiency. Our findings confirm that although rate, a mild form of type IV glycogenosis is marked by polyglucosan inclusion not only in myofibers, but also in smooth muscle and sweat gland epithelial cells. This further implies that when polyglucosan inclusions are observed within myofibers it is mandatory to examine the muscle tissue for brancher enzyme activity since the brancher enzyme activities in circulating erythrocytes and leucocytes were normal in all three affected siblings and their parents. Therefore, it can be concluded that the patients reported on here represent a variant form of type IV glycogenosis, in which the defect is limited to muscle tissue. This further indicates that there are several different types of type IV glycogenosis with variable clinical manifestations.

Published

1992

32. Hereditary branching enzyme dysfunction in adult polyglucosan body disease: a possible metabolic cause in two patients.

Author

Lossos A, Barash V, Soffer D, Argov Z, Gomori M, Ben-Nariah Z, Abramsky O, and Steiner I

Subjects

Brain pathology, Consanguinity, Female, Genes, Recessive, Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV genetics, Humans, Jews, Magnetic Resonance Imaging, Male, Middle Aged, Nervous System Diseases ethnology, Nervous System Diseases genetics, Nervous System Diseases pathology, Pedigree, Sural Nerve pathology, 1,4-alpha-Glucan Branching Enzyme deficiency, Glycogen metabolism, Nervous System Diseases enzymology, Neutrophils enzymology

Abstract

We describe 2 unrelated patients with adult polyglucosan body disease (APBD) diagnosed by sural nerve biopsy. Both patients were offspring of consanguineous marriages. They presented clinically with late onset pyramidal tetraparesis, micturition difficulties, peripheral neuropathy, and mild cognitive impairment. Magnetic resonance imaging of the brain revealed extensive white matter abnormalities in both. In search of a possible metabolic defect, we evaluated glycogen metabolism in these patients and their clinically unaffected children. Branching enzyme activity in the patients' polymorphonuclear leukocytes was about 15% of control values, whereas their children displayed values of 50 to 60%, suggesting a possible autosomal recessive mode of transmission. This is the first report of an inherited metabolic defect in patients with adult polyglucosan body disease. We suggest that branching enzyme dysfunction may be implicated in the pathogenesis of some patients with adult polyglucosan body disease.

Published

1991

33. Type IV glycogen-storage disease. Light-microscopic, electron-microscopic, and enzymatic study.

Author

Bannayan GA, Dean WJ, and Howell RR

Subjects

Female, Humans, Infant, Liver enzymology, Liver ultrastructure, Liver Glycogen metabolism, Skin enzymology, 1,4-alpha-Glucan Branching Enzyme deficiency, Glucosyltransferases deficiency, Glycogen Storage Disease, Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV pathology

Abstract

The case of a 14-month-old Latin American girl with the diagnosis of Type IV glycogen-storage disease is reported. The diagnosis was reached on the basis of the typical clinical manifestations, the light- and electron-microscopic findings, and the demonstration of absence of the branching enzyme alpha-1,4-glucan:alpha-1,4-glucan 6-glucosyl transferase in the liver and in the cultured skin fibroblasts.

Published

1976

34. A new variant of type IV glycogenosis: deficiency of branching enzyme activity without apparent progressive liver disease.

Author

Greene HL, Brown BI, McClenathan DT, Agostini RM Jr, and Taylor SR

Subjects

1,4-alpha-Glucan Branching Enzyme metabolism, Biopsy, Cells, Cultured, Child, Preschool, Fibroblasts enzymology, Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV pathology, Glycogen Storage Disease Type IV physiopathology, Humans, Liver physiopathology, Liver ultrastructure, Male, Muscles enzymology, Muscles pathology, Muscles physiopathology, Muscles ultrastructure, Skin enzymology, Glycogen Storage Disease classification, Glycogen Storage Disease Type IV classification, Liver pathology

Abstract

Type IV glycogenosis is due to branching enzyme deficiency and is usually manifested clinically by progressive liver disease with cirrhosis and hepatic failure between the second and fourth years of life. We describe a 5-year-old boy who, following an acute febrile illness at 2 years of age, was first noted to have hepatomegaly with mildly elevated serum transaminase levels. Liver biopsy revealed hepatic fibrosis with periodic-acid Schiff-positive, diastase-resistant inclusions in hepatocytes and fibrillar inclusions characteristic of amylopectin by electron microscopy. Enzymatic assay revealed deficient hepatic branching enzyme activity with normal activity of glucose-6-phosphatase, debranching enzyme and phosphorylase activities. During the succeeding 3 years, he grew and developed normally with apparent resolution of any clinical evidence of liver disease and only intermittent elevation in serum transaminase levels associated with fever and prolonged fasting. Repeat liver biopsy at 4 years of age showed persistence of scattered hepatocellular periodic-acid Schiff-positive, diastase-resistant inclusions, but no progression of hepatic fibrosis in spite of persistent deficiency of hepatic branching enzyme activity. Skeletal muscle and skin fibroblasts from the patient also showed deficient enzyme activity. Skin fibroblasts from both parents exhibited half the normal control activity, suggesting a heterozygote state. This is the first documented patient with deficiency of branching enzyme but without evidence of progressive hepatic disease. This patient, coupled with reports of other patients with late onset hepatic or muscle disease with branching enzyme deficiency, suggests that the defect resulting in Type IV glycogen storage disease is more heterogenous and possibly more common than previously suspected.

Published

1988

35. Branching enzyme activity of cultured amniocytes and chorionic villi: prenatal testing for type IV glycogen storage disease.

Author

Brown BI and Brown DH

Subjects

Female, Fetal Diseases diagnosis, Glycogen Storage Disease Type IV enzymology, Heterozygote, Humans, Pregnancy, 1,4-alpha-Glucan Branching Enzyme deficiency, Amnion enzymology, Chorionic Villi enzymology, Glucosyltransferases deficiency, Glycogen Storage Disease diagnosis, Glycogen Storage Disease Type IV diagnosis, Prenatal Diagnosis

Abstract

Although type IV glycogen storage disease (Andersen disease; McKusick 23250) is considered to be a rare, autosomally recessive disorder, of the more than 600 patients with glycogenosis identified in our laboratory by enzymatic assays, 6% have been shown to be deficient in the glycogen branching enzyme. Most of the 38 patients with type IV glycogen storage disease who are known to us have succumbed at a very early age, with the exception of one male teenager, an apparently healthy 7-year-old male, and several 5-year-old patients. Fourteen pregnancies at risk for branching enzyme deficiency have been monitored using cultured amniotic fluid cells, and four additional pregnancies have been screened using cultured chorionic villi. Essentially no branching enzyme activity was detectable in eight samples (amniocytes); activities within the control range were found in five samples (three amniocyte and two chorionic villi samples); and five samples appeared to have been derived from carriers. In two of the cases lacking branching enzyme activity, in which the pregnancies were terminated and fibroblasts were successfully cultured from the aborted fetuses, no branching enzyme activity was found. Another fetus, which was predicted by antenatal assay to be affected, was carried to term. Skin fibroblasts from this baby were deficient in branching enzyme. Pregnancies at risk for glycogen storage disease due to the deficiency of branching enzyme can be successfully monitored using either cultured chorionic villi or amniocytes.

Published

1989

36. [Early diagnosis of glycogenosis type VI and the detection of heterozygotes].

Author

Saint-Rome G, Roy CC, Lescop J, Brochu P, and Znokiewicz MH

Subjects

Glycogen Storage Disease Type IV enzymology, Glycogen Storage Disease Type IV genetics, Glycogen Storage Disease Type IV pathology, Heterozygote, Humans, Infant, Rectum pathology, Glycogen Storage Disease diagnosis, Glycogen Storage Disease Type IV diagnosis

Published

1976

37. Studies of the residual glycogen branching enzyme activity present in human skin fibroblasts from patients with type IV glycogen storage disease.

Author

Brown DH and Brown BI

Subjects

Cells, Cultured, Cross Reactions, Fibroblasts enzymology, Glycogen Synthase analysis, Humans, Liver enzymology, Uridine Diphosphate Glucose metabolism, 1,4-alpha-Glucan Branching Enzyme analysis, Glucosyltransferases analysis, Glycogen Storage Disease enzymology, Glycogen Storage Disease Type IV enzymology, Skin enzymology

Abstract

Human skin fibroblasts from patients with Type IV glycogen storage disease, in which there is a demonstrable deficiency of glycogen branching enzyme, were shown to be able to synthesize [14C]glycogen containing [14C]glucose at branch points when sonicates containing endogenous glycogen synthase a were incubated with UDP[14C]glucose. The branch point content of the glycogen synthesized by the Type IV cells was essentially the same as that formed by normal cells, but the total synthetic capacity of the Type IV cells was lower. A new assay for the branching enzyme using glycogen synthase as the indicator enzyme has been developed. Using this assay it has been shown that the residual branching enzyme of affected children and of their heterozygote parents is less easily inhibited by an IgG antibody raised in rabbits against the normal human liver enzyme than is the branching enzyme of normal fibroblasts.

Published

1983