Your search keyword '"Mucolipidoses enzymology"' showing total 264 results

1. Structures of the mannose-6-phosphate pathway enzyme, GlcNAc-1-phosphotransferase.

Author

Gorelik A, Illes K, Bui KH, and Nagar B

Subjects

Catalytic Domain, Humans, Lysosomes enzymology, Lysosomal Storage Diseases metabolism, Mannosephosphates metabolism, Mucolipidoses enzymology, Transferases (Other Substituted Phosphate Groups) chemistry, Transferases (Other Substituted Phosphate Groups) genetics

Abstract

The mannose-6-phosphate (M6P) pathway is responsible for the transport of hydrolytic enzymes to lysosomes. N-acetylglucosamine-1-phosphotransferase (GNPT) catalyzes the first step of tagging these hydrolases with M6P, which when recognized by receptors in the Golgi diverts them to lysosomes. Genetic defects in the GNPT subunits, GNPTAB and GNPTG, cause the lysosomal storage diseases mucolipidosis types II and III. To better understand its function, we determined partial three-dimensional structures of the GNPT complex. The catalytic domain contains a deep cavity for binding of uridine diphosphate- N -acetylglucosamine, and the surrounding residues point to a one-step transfer mechanism. An isolated structure of the gamma subunit of GNPT reveals that it can bind to mannose-containing glycans in different configurations, suggesting that it may play a role in directing glycans into the active site. These findings may facilitate the development of therapies for lysosomal storage diseases.

Published

2022

2. Intermittent enzyme replacement therapy with recombinant human β-galactosidase prevents neuraminidase 1 deficiency

Author

Luu AR, Wong C, Agrawal V, Wise N, Handyside B, Lo MJ, Pacheco G, Felix JB, Giaramita A, d'Azzo A, Vincelette J, Bullens S, Bunting S, Christianson TM, Hague CM, LeBowitz JH, and Yogalingam G

Subjects

Animals, CHO Cells, Cricetulus, Humans, Lysosomes genetics, Mice, Mice, Mutant Strains, Neuraminidase genetics, Neuraminidase metabolism, Enzyme Replacement Therapy, Fibroblasts enzymology, Lysosomes enzymology, Mucolipidoses drug therapy, Mucolipidoses enzymology, Mucolipidoses genetics, beta-Galactosidase therapeutic use

Abstract

Mutations in the galactosidase β 1 ( GLB1 ) gene cause lysosomal β-galactosidase (β-Gal) deficiency and clinical onset of the neurodegenerative lysosomal storage disease, GM1 gangliosidosis. β-Gal and neuraminidase 1 (NEU1) form a multienzyme complex in lysosomes along with the molecular chaperone, protective protein cathepsin A (PPCA). NEU1 is deficient in the neurodegenerative lysosomal storage disease sialidosis, and its targeting to and stability in lysosomes strictly depend on PPCA. In contrast, β-Gal only partially depends on PPCA, prompting us to investigate the role that β-Gal plays in the multienzyme complex. Here, we demonstrate that β-Gal negatively regulates NEU1 levels in lysosomes by competitively displacing this labile sialidase from PPCA. Chronic cellular uptake of purified recombinant human β-Gal (rhβ-Gal) or chronic lentiviral-mediated GLB1 overexpression in GM1 gangliosidosis patient fibroblasts coincides with profound secondary NEU1 deficiency. A regimen of intermittent enzyme replacement therapy dosing with rhβ-Gal, followed by enzyme withdrawal, is sufficient to augment β-Gal activity levels in GM1 gangliosidosis patient fibroblasts without promoting NEU1 deficiency. In the absence of β-Gal, NEU1 levels are elevated in the GM1 gangliosidosis mouse brain, which are restored to normal levels following weekly intracerebroventricular dosing with rhβ-Gal. Collectively, our results highlight the need to carefully titrate the dose and dosing frequency of β-Gal augmentation therapy for GM1 gangliosidosis. They further suggest that intermittent intracerebroventricular enzyme replacement therapy dosing with rhβ-Gal is a tunable approach that can safely augment β-Gal levels while maintaining NEU1 at physiological levels in the GM1 gangliosidosis brain., Competing Interests: Conflict of interest—The authors declare that they have no conflicts of interest with the contents of this article., (© 2020 Luu et al.)

Published

2020

3. Mucolipidoses Overview: Past, Present, and Future.

Author

Khan SA and Tomatsu SC

Subjects

Animals, Biological Transport, Active, Disease Models, Animal, Glycosaminoglycans metabolism, Humans, Mannosephosphates metabolism, Mucolipidoses enzymology, Mucolipidoses physiopathology, Mucolipidoses therapy, Enzyme Replacement Therapy methods, Genetic Therapy methods, Hematopoietic Stem Cell Transplantation methods, Lysosomes metabolism, Mucolipidoses diagnosis

Abstract

Mucolipidosis II and III (ML II/III) are caused by a deficiency of uridine-diphosphate N -acetylglucosamine: lysosomal-enzyme- N -acetylglucosamine-1-phosphotransferase (GlcNAc-1-phosphotransferase, EC2.7.8.17), which tags lysosomal enzymes with a mannose 6-phosphate (M6P) marker for transport to the lysosome. The process is performed by a sequential two-step process: first, GlcNAc-1-phosphotransferase catalyzes the transfer of GlcNAc-1-phosphate to the selected mannose residues on lysosomal enzymes in the cis-Golgi network. The second step removes GlcNAc from lysosomal enzymes by N -acetylglucosamine-1-phosphodiester α- N -acetylglucosaminidase (uncovering enzyme) and exposes the mannose 6-phosphate (M6P) residues in the trans-Golgi network, in which the enzymes are targeted to the lysosomes by M6Preceptors. A deficiency of GlcNAc-1-phosphotransferase causes the hypersecretion of lysosomal enzymes out of cells, resulting in a shortage of multiple lysosomal enzymes within lysosomes. Due to a lack of GlcNAc-1-phosphotransferase, the accumulation of cholesterol, phospholipids, glycosaminoglycans (GAGs), and other undegraded substrates occurs in the lysosomes. Clinically, ML II and ML III exhibit quite similar manifestations to mucopolysaccharidoses (MPSs), including specific skeletal deformities known as dysostosis multiplex and gingival hyperplasia. The life expectancy is less than 10 years in the severe type, and there is no definitive treatment for this disease. In this review, we have described the updated diagnosis and therapy on ML II/III.

Published

2020

4. GNPTAB c.2404C > T nonsense mutation in a patient with mucolipidosis III alpha/beta: a case report.

Author

Ho CC, Tsung LL, Liu KT, and Poon WT

Subjects

Child, Preschool, Chondroitinsulfatases genetics, Chondroitinsulfatases metabolism, Gene Expression Regulation, Genes, Recessive, Humans, Iduronate Sulfatase genetics, Iduronate Sulfatase metabolism, Iduronidase genetics, Iduronidase metabolism, Lysosomes enzymology, Lysosomes pathology, Male, Mucolipidoses diagnosis, Mucolipidoses enzymology, Mucolipidoses pathology, N-Acetylgalactosamine-4-Sulfatase genetics, N-Acetylgalactosamine-4-Sulfatase metabolism, Pedigree, Transferases (Other Substituted Phosphate Groups) deficiency, beta-Hexosaminidase alpha Chain genetics, beta-Hexosaminidase alpha Chain metabolism, Codon, Nonsense, Mucolipidoses genetics, Transferases (Other Substituted Phosphate Groups) genetics

Abstract

Background: Mucolipidosis alpha/beta is an inborn error of metabolism characterized by deficiency of GlcNAc-1-phosphotransferase, in which essential alpha/beta subunits are encoded by the GNPTAB gene. The autosomal recessive condition is due to disruptions of hydrolase mannose 6-phosphate marker generation, defective lysosomal targeting and subsequent intracellular accumulation of non-degraded material. Clinical severity depends on residual GlcNAc-1-phosphotransferase activity, which distinguishes between the milder type III disease and the severe, neonatal onset type II disease., Case Presentation: We report the clinical, biochemical and genetic diagnosis of mucolipidosis III alpha/beta in a two-year-old Chinese boy who initially presented with poor weight gain, microcephaly and increased tone. He was confirmed to harbor the common splice site mutation c.2715 + 1G > A and the nonsense variant c.2404C > T (p.Q802*). Clinically, the patient had multiple phenotypic features typical of mucopolysaccharidosis including joint contractures, coarse facial features, kypho-lordosis, pectus carinatum and umbilical hernia. However, the relatively mild developmental delay compared to severe type I and type II mucopolysaccharidosis and the absence of macrocephaly raised the possibility of the less commonly diagnosed mucolipidosis alpha/beta. Critical roles of lysosomal enzyme activity assay, which showed elevated α-iduronidase, iduronate sulfatase, galactose-6-sulphate sulphatase, arylsulfatase B and α-hexosaminidase activities; and genetic study, which confirmed the parental origin of both mutations, were highlighted., Conclusions: The recently reported nonsense variant c.2404C > T in the GNPTAB gene is further recognized and this contributes to the genotype-phenotype spectrum of mucolipidosis alpha/beta.

Published

2018

5. Recycling of Golgi glycosyltransferases requires direct binding to coatomer.

Author

Liu L, Doray B, and Kornfeld S

Subjects

Amino Acid Motifs, COP-Coated Vesicles genetics, Coat Protein Complex I genetics, Coat Protein Complex I metabolism, Glucosyltransferases genetics, Golgi Apparatus genetics, HEK293 Cells, HeLa Cells, Humans, Mucolipidoses enzymology, Mucolipidoses genetics, Mutation, Missense, Protein Domains, COP-Coated Vesicles enzymology, Glucosyltransferases metabolism, Golgi Apparatus enzymology

Abstract

The glycosyltransferases of the mammalian Golgi complex must recycle between the stacked cisternae of that organelle to maintain their proper steady-state localization. This trafficking is mediated by COPI-coated vesicles, but how the glycosyltransferases are incorporated into these transport vesicles is poorly understood. Here we show that the N-terminal cytoplasmic tails (N-tails) of a number of cis Golgi glycosyltransferases which share a ϕ-(K/R)-X-L-X-(K/R) sequence bind directly to the δ- and ζ-subunits of COPI. Mutations of this N-tail motif impair binding to the COPI subunits, leading to mislocalization of the transferases to lysosomes. The physiological importance of these interactions is illustrated by mucolipidosis III patients with missense mutations in the N-tail of GlcNAc-1-phosphotransferase that cause the transferase to be rapidly degraded in lysosomes. These studies establish that direct binding of the N-tails of mammalian cis Golgi glycosyltransferases with COPI subunits is essential for recycling within the Golgi., Competing Interests: The authors declare no conflict of interest.

Published

2018

6. GNPTAB missense mutations cause loss of GlcNAc-1-phosphotransferase activity in mucolipidosis type II through distinct mechanisms.

Author

Ludwig NF, Velho RV, Sperb-Ludwig F, Acosta AX, Ribeiro EM, Kim CA, Gandelman Horovitz DD, Boy R, Rodovalho-Doriqui MJ, Lourenço CM, Santos ES, Braulke T, Pohl S, and Schwartz IVD

Subjects

Adolescent, Adult, Child, Child, Preschool, Female, Genotype, Humans, Infant, Male, Transferases (Other Substituted Phosphate Groups) metabolism, Young Adult, Loss of Function Mutation, Mucolipidoses enzymology, Mucolipidoses genetics, Mutation, Missense, Transferases (Other Substituted Phosphate Groups) genetics

Abstract

Mucolipidoses (ML) II and III alpha/beta are lysosomal storage diseases caused by pathogenic mutations in GNPTAB encoding the α⁄β-subunit precursor of GlcNAc-1-phosphotransferase. To determine genotype-phenotype correlation and functional analysis of mutant GlcNAc-1-phosphotransferase, 13 Brazilian patients clinically and biochemical diagnosed for MLII or III alpha/beta were studied. By sequencing of genomic GNPTAB of the MLII and MLIII alpha/beta patients we identified six novel mutations: p.D76G, p.S385L, p.Q278Kfs*3, p.H588Qfs*27, p.N642Lfs*10 and p.Y1111*. Expression analysis by western blotting and immunofluorescence microscopy revealed that the mutant α⁄β-subunit precursor p.D76G is retained in the endoplasmic reticulum whereas the mutant p.S385L is correctly transported to the cis-Golgi apparatus and proteolytically processed. Both mutations lead to complete loss of GlcNAc-1-phosphotransferase activity, consistent with the severe clinical MLII phenotype of the patients. Our study expands the genotypic spectrum of MLII and provides novel insights into structural requirements to ensure GlcNAc-1-phosphotransferase activity., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

7. Quantitative Proteome Analysis of Mouse Liver Lysosomes Provides Evidence for Mannose 6-phosphate-independent Targeting Mechanisms of Acid Hydrolases in Mucolipidosis II.

Author

Markmann S, Krambeck S, Hughes CJ, Mirzaian M, Aerts JM, Saftig P, Schweizer M, Vissers JP, Braulke T, and Damme M

Subjects

Animals, Cells, Cultured, Chromatography, Liquid, Disease Models, Animal, Gene Expression Regulation, Liver metabolism, Mass Spectrometry, Mice, Mucolipidoses genetics, Phosphotransferases deficiency, Hydrolases metabolism, Lysosomes metabolism, Mannosephosphates metabolism, Mucolipidoses enzymology, Proteome analysis

Abstract

The efficient receptor-mediated targeting of soluble lysosomal proteins to lysosomes requires the modification with mannose 6-phosphate (M6P) residues. Although the absence of M6P results in misrouting and hypersecretion of lysosomal enzymes in many cells, normal levels of lysosomal enzymes have been reported in liver of patients lacking the M6P-generating phosphotransferase (PT). The identity of lysosomal proteins depending on M6P has not yet been comprehensively analyzed. In this study we purified lysosomes from liver of PT-defective mice and 67 known soluble lysosomal proteins were identified that illustrated quantitative changes using an ion mobility-assisted data-independent label-free LC-MS approach. After validation of various differentially expressed lysosomal components by Western blotting and enzyme activity assays, the data revealed a small number of lysosomal proteins depending on M6P, including neuraminidase 1, cathepsin F, Npc2, and cathepsin L, whereas the majority reach lysosomes by alternative pathways. These data were compared with findings on cultured hepatocytes and liver sinusoid endothelial cells isolated from the liver of wild-type and PT-defective mice. Our findings show that the relative expression, targeting efficiency and lysosomal localization of lysosomal proteins tested in cultured hepatic cells resemble their proportion in isolated liver lysosomes. Hypersecretion of newly synthesized nonphosphorylated lysosomal proteins suggest that secretion-recapture mechanisms contribute to maintain major lysosomal functions in liver., (© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2017

8. Biochemical and molecular characterization of novel mutations in GLB1 and NEU1 in patient cells with lysosomal storage disorders.

Author

Kwak JE, Son MY, Son YS, Son MJ, and Cho YS

Subjects

Amino Acid Sequence, Animals, Fibroblasts metabolism, Humans, Models, Molecular, Molecular Sequence Data, Mutation, Neuraminidase chemistry, Neuraminidase metabolism, Sequence Alignment, beta-Galactosidase chemistry, beta-Galactosidase metabolism, Gangliosidosis, GM1 enzymology, Gangliosidosis, GM1 genetics, Mucolipidoses enzymology, Mucolipidoses genetics, Neuraminidase genetics, beta-Galactosidase genetics

Abstract

Lysosomes are cytoplasmic compartments that contain many acid hydrolases and play critical roles in the metabolism of a wide range of macromolecules. Deficiencies in lysosomal enzyme activities cause genetic diseases, called lysosomal storage disorders (LSDs). Many mutations have been identified in the genes responsible for LSDs, and the identification of mutations is required for the accurate molecular diagnoses. Here, we analyzed cell lines that were derived from two different LSDs, GM1 gangliosidosis and sialidosis. GM1 gangliosidosis is caused by mutations in the GLB1 gene that encodes β-galactosidase. A lack of β-galactosidase activity leads to the massive accumulation of GM1 ganglioside, which results in neurodegenerative pathology. Mutations in the NEU1 gene that encodes lysosomal sialidase cause sialidosis. Insufficient activity of lysosomal sialidase progressively increases the accumulation of sialylated molecules, and various clinical symptoms, including mental retardation, appear. We sequenced the entire coding regions of GLB1 and NEU1 in GM1 gangliosidosis and sialidosis patient cells, respectively. We found the novel mutations p.E186A in GLB1 and p.R347Q in NEU1, as well as many other mutations that have been previously reported. We also demonstrated that patient cells containing the novel mutations showed the molecular phenotypes of the corresponding disease. Further structural analysis suggested that these novel mutation sites are highly conserved and important for enzyme activity., (Copyright © 2015 Elsevier Inc. All rights reserved.)

Published

2015

9. Analysis of mucolipidosis II/III GNPTAB missense mutations identifies domains of UDP-GlcNAc:lysosomal enzyme GlcNAc-1-phosphotransferase involved in catalytic function and lysosomal enzyme recognition.

Author

Qian Y, van Meel E, Flanagan-Steet H, Yox A, Steet R, and Kornfeld S

Subjects

Animals, Humans, Mucolipidoses metabolism, Zebrafish, Lysosomes metabolism, Mucolipidoses enzymology, Mucolipidoses genetics, Mutation, Missense genetics, Transferases (Other Substituted Phosphate Groups) genetics, Transferases (Other Substituted Phosphate Groups) metabolism

Abstract

UDP-GlcNAc:lysosomal enzyme GlcNAc-1-phosphotransferase tags newly synthesized lysosomal enzymes with mannose 6-phosphate recognition markers, which are required for their targeting to the endolysosomal system. GNPTAB encodes the α and β subunits of GlcNAc-1-phosphotransferase, and mutations in this gene cause the lysosomal storage disorders mucolipidosis II and III αβ. Prior investigation of missense mutations in GNPTAB uncovered amino acids in the N-terminal region and within the DMAP domain involved in Golgi retention of GlcNAc-1-phosphotransferase and its ability to specifically recognize lysosomal hydrolases, respectively. Here, we undertook a comprehensive analysis of the remaining missense mutations in GNPTAB reported in mucolipidosis II and III αβ patients using cell- and zebrafish-based approaches. We show that the Stealth domain harbors the catalytic site, as some mutations in these regions greatly impaired the activity of the enzyme without affecting its Golgi localization and proteolytic processing. We also demonstrate a role for the Notch repeat 1 in lysosomal hydrolase recognition, as missense mutations in conserved cysteine residues in this domain do not affect the catalytic activity but impair mannose phosphorylation of certain lysosomal hydrolases. Rescue experiments using mRNA bearing Notch repeat 1 mutations in GNPTAB-deficient zebrafish revealed selective effects on hydrolase recognition that differ from the DMAP mutation. Finally, the mutant R587P, located in the spacer between Notch 2 and DMAP, was partially rescued by overexpression of the γ subunit, suggesting a role for this region in γ subunit binding. These studies provide new insight into the functions of the different domains of the α and β subunits., (© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

10. Mannose 6 phosphorylation of lysosomal enzymes controls B cell functions.

Author

Otomo T, Schweizer M, Kollmann K, Schumacher V, Muschol N, Tolosa E, Mittrücker HW, and Braulke T

Subjects

Animals, Antigen Presentation, Antigens metabolism, B-Lymphocytes immunology, Cell Differentiation, Cell Proliferation, Cells, Cultured, Dendritic Cells enzymology, Dendritic Cells immunology, Humans, Mice, Transgenic, Mucolipidoses enzymology, Mucolipidoses immunology, Phosphorylation, Protein Processing, Post-Translational, T-Lymphocytes immunology, Transferases (Other Substituted Phosphate Groups) genetics, B-Lymphocytes enzymology, Lysosomes enzymology, Mannosephosphates metabolism, Peptide Hydrolases metabolism

Abstract

Antigen processing and presentation and cytotoxic targeting depend on the activities of several lysosomal enzymes that require mannose 6-phosphate (M6P) sorting signals for efficient intracellular transport and localization. In this paper, we show that mice deficient in the formation of M6P residues exhibit significant loss of cathepsin proteases in B cells, leading to lysosomal dysfunction with accumulation of storage material, impaired antigen processing and presentation, and subsequent defects in B cell maturation and antibody production. The targeting of lysosomal and granular enzymes lacking M6P residues is less affected in dendritic cells and T cells and sufficient for maintenance of degradative and lytic functions. M6P deficiency also impairs serum immunoglobulin levels and antibody responses to vaccination in patients. Our data demonstrate the critical role of M6P-dependent transport routes for B cell functions in vivo and humoral immunity in mice and human., (© 2015 Otomo et al.)

Published

2015

11. A novel mouse model of a patient mucolipidosis II mutation recapitulates disease pathology.

Author

Paton L, Bitoun E, Kenyon J, Priestman DA, Oliver PL, Edwards B, Platt FM, and Davies KE

Subjects

2-Hydroxypropyl-beta-cyclodextrin, Animals, Behavior, Animal, Carrier Proteins genetics, Carrier Proteins metabolism, Excipients pharmacology, Glycoproteins genetics, Glycoproteins metabolism, HEK293 Cells, Humans, Mice, Mice, Inbred BALB C, Mice, Mutant Strains, Niemann-Pick Disease, Type C enzymology, Niemann-Pick Disease, Type C genetics, Niemann-Pick Disease, Type C pathology, Vesicular Transport Proteins genetics, Vesicular Transport Proteins metabolism, beta-Cyclodextrins pharmacology, Disease Models, Animal, Homozygote, Mucolipidoses enzymology, Mucolipidoses genetics, Mucolipidoses pathology, Mutation, Purkinje Cells enzymology, Purkinje Cells pathology, Transferases (Other Substituted Phosphate Groups) genetics, Transferases (Other Substituted Phosphate Groups) metabolism

Abstract

Mucolipidosis II (MLII) is a lysosomal storage disorder caused by loss of N-acetylglucosamine-1-phosphotransferase, which tags lysosomal enzymes with a mannose 6-phosphate marker for transport to the lysosome. In MLII, the loss of this marker leads to deficiency of multiple enzymes and non-enzymatic proteins in the lysosome, leading to the storage of multiple substrates. Here we present a novel mouse model of MLII homozygous for a patient mutation in the GNPTAB gene. Whereas the current gene knock-out mouse model of MLII lacks some of the characteristic features of the human disease, our novel mouse model more fully recapitulates the human pathology, showing growth retardation, skeletal and facial abnormalities, increased circulating lysosomal enzymatic activities, intracellular lysosomal storage, and reduced life span. Importantly, MLII behavioral deficits are characterized for the first time, including impaired motor function and psychomotor retardation. Histological analysis of the brain revealed progressive neurodegeneration in the cerebellum with severe Purkinje cell loss as the underlying cause of the ataxic gait. In addition, based on the loss of Npc2 (Niemann-Pick type C 2) protein expression in the brain, the mice were treated with 2-hydroxypropyl-β-cyclodextrin, a drug previously reported to rescue Purkinje cell death in a mouse model of Niemann-Pick type C disease. No improvement in brain pathology was observed. This indicates that cerebellar degeneration is not primarily triggered by loss of Npc2 function. This study emphasizes the value of modeling MLII patient mutations to generate clinically relevant mouse mutants to elucidate the pathogenic molecular pathways of MLII and address their amenability to therapy., (© 2014 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2014

12. Lysosomal multienzyme complex: pros and cons of working together.

Author

Bonten EJ, Annunziata I, and d'Azzo A

Subjects

Animals, Cathepsin A genetics, Disease Models, Animal, Gangliosidosis, GM1 genetics, Gangliosidosis, GM1 pathology, Gene Expression Regulation, Humans, Lysosomal Storage Diseases genetics, Lysosomal Storage Diseases pathology, Lysosomes genetics, Lysosomes pathology, Mice, Mice, Knockout, Mucolipidoses genetics, Mucolipidoses pathology, Multienzyme Complexes genetics, Multienzyme Complexes metabolism, Neuraminidase genetics, Signal Transduction, beta-Galactosidase genetics, Cathepsin A metabolism, Gangliosidosis, GM1 enzymology, Lysosomal Storage Diseases enzymology, Lysosomes enzymology, Mucolipidoses enzymology, Neuraminidase metabolism, beta-Galactosidase metabolism

Abstract

The ubiquitous distribution of lysosomes and their heterogeneous protein composition reflects the versatility of these organelles in maintaining cell homeostasis and their importance in tissue differentiation and remodeling. In lysosomes, the degradation of complex, macromolecular substrates requires the synergistic action of multiple hydrolases that usually work in a stepwise fashion. This catalytic machinery explains the existence of lysosomal enzyme complexes that can be dynamically assembled and disassembled to efficiently and quickly adapt to the pool of substrates to be processed or degraded, adding extra tiers to the regulation of the individual protein components. An example of such a complex is the one composed of three hydrolases that are ubiquitously but differentially expressed: the serine carboxypeptidase, protective protein/cathepsin A (PPCA), the sialidase, neuraminidase-1 (NEU1), and the glycosidase β-galactosidase (β-GAL). Next to this 'core' complex, the existence of sub-complexes, which may contain additional components, and function at the cell surface or extracellularly, suggests as yet unexplored functions of these enzymes. Here we review how studies of basic biological processes in the mouse models of three lysosomal storage disorders, galactosialidosis, sialidosis, and GM1-gangliosidosis, revealed new and unexpected roles for the three respective affected enzymes, Ppca, Neu1, and β-Gal, that go beyond their canonical degradative activities. These findings have broadened our perspective on their functions and may pave the way for the development of new therapies for these lysosomal storage disorders.

Published

2014

13. Mislocalization of phosphotransferase as a cause of mucolipidosis III αβ.

Author

van Meel E, Qian Y, and Kornfeld SA

Subjects

Electrophoresis, Polyacrylamide Gel, HEK293 Cells, HeLa Cells, Humans, Lysosomes metabolism, Microscopy, Fluorescence, Mutation, Missense genetics, Proteolysis, Golgi Apparatus metabolism, Mucolipidoses enzymology, Mucolipidoses etiology, Transferases (Other Substituted Phosphate Groups) genetics, Transferases (Other Substituted Phosphate Groups) metabolism

Abstract

The lysosomal storage disorder mucolipidosis III αβ is caused by mutations in the αβ subunits of UDP-GlcNAc:lysosomal enzyme N-acetylglucosamine-1-phosphotransferase (phosphotransferase). This Golgi-localized enzyme mediates the first step in the synthesis of the mannose 6-phosphate recognition marker on lysosomal acid hydrolases, and loss of function results in impaired lysosomal targeting of these acid hydrolases and decreased lysosomal degradation. Here we show that two patient missense mutations, Lys4Gln and Ser15Tyr, in the N-terminal cytoplasmic tail of the α subunit of phosphotransferase impair retention of the catalytically active enzyme in the Golgi complex. This results in mistargeting of the mutant phosphotransferases to lysosomes, where they are degraded, or to the cell surface and release into the medium. The finding that mislocalization of active phosphotransferase is the basis for mucolipidosis III αβ in a subset of patients shows the importance of single residues in the cytoplasmic tail of a Golgi-resident protein for localization to this compartment.

Published

2014

14. Ultrastructural analysis of neuronal and non-neuronal lysosomal storage in mucolipidosis type II knock-in mice.

Author

Schweizer M, Markmann S, Braulke T, and Kollmann K

Subjects

Animals, Biomarkers metabolism, Cell Survival, Cerebellum enzymology, Disease Models, Animal, Gene Knock-In Techniques, Genetic Predisposition to Disease, Lectins metabolism, Lysosomes enzymology, Mice, Mice, 129 Strain, Mice, Inbred C57BL, Mice, Transgenic, Mucolipidoses enzymology, Mucolipidoses genetics, Mutation, Neurons enzymology, Phenotype, Retina enzymology, Transferases (Other Substituted Phosphate Groups) genetics, Cerebellum ultrastructure, Lysosomes ultrastructure, Mucolipidoses pathology, Neurons ultrastructure, Retina ultrastructure, Transferases (Other Substituted Phosphate Groups) metabolism

Abstract

The GlcNAc-1-phosphotransferase catalyzes the first step in the formation of mannose 6-phosphate (M6P) residues on lysosomal acid hydrolases that is essential for the efficient transport of newly synthesized lysosomal enzymes to lysosomes and the maintenance of lysosomal functions. Mutations in the GlcNAc-1-phosphotransferase cause the lysosomal storage disease mucolipidosis type II (MLII), resulting in mistargeting and hypersecretion of multiple lysosomal hydrolases and subsequent lysosomal accumulation of nondegraded material in several tissues. To describe cell-type specificity, compositional differences, and subcellular distribution of the stored material we performed an in-depth ultrastructural analysis of lysosomal storage in brain and retina of MLII knock-in mice using electron microscopy. Massive vacuoles filled with heterogeneous storage material have been found in the soma, swollen axons, and dendrites of Purkinje, and granular cells in 9-month-old MLII mice. In addition, non-neuronal cells, such as microglial, astroglial, and endothelial cells, exhibit storage material. Fucose-specific lectin histochemistry demonstrated the accumulation of fucose-containing oligosaccharides, indicating that targeting of the lysosomal α-fucosidase is strongly impaired in all cerebellar cell types. The data suggest that the accumulation of storage material might affect neuronal function and survival in a direct cell-autonomous manner, as well as indirectly by disturbed metabolic homeostasis between glial and neuronal cells or by cerebrovascular complications.

Published

2013

15. Two homozygous nonsense mutations of GNPTAB gene in two Chinese families with mucolipidosis II alpha/beta using targeted next-generation sequencing.

Author

Yang Y, Wu J, Liu H, Chen X, Wang Y, Zhao M, and He X

Subjects

China, Female, Humans, Infant, Lysosomes enzymology, Male, Mucolipidoses enzymology, Mucolipidoses pathology, Sequence Analysis, DNA, Transferases (Other Substituted Phosphate Groups) metabolism, Codon, Nonsense, High-Throughput Nucleotide Sequencing, Homozygote, Mucolipidoses genetics, Transferases (Other Substituted Phosphate Groups) genetics

Abstract

Mucolipidosis II alpha/beta (ML II alpha/beta; I-cell disease) is a rare, inherited, metabolic disease and has often been clinically misdiagnosed. ML II alpha/beta results from a deficiency of the enzyme N-acetylglucosamine-1-phosphotransferase (GlcNAc-PT), which causes the lysosomal enzymes to accumulate in plasma. We identified two new Chinese patients with ML II alpha/beta by lysosomal enzyme assay. Using targeted next-generation sequencing genetic analysis, we located two homozygous nonsense mutations in the GNPTAB gene, c.1071G>A (p.W357X) and c.1090C>T (p.R364X). These results were confirmed by Sanger sequencing. To our knowledge, the c.1071G>A mutation has not been previously reported. Our findings add to the number of reported cases of this rare illness and to the GNPTAB pathogenic mutation database. This work also demonstrates the application of lysosomal enzyme assay and targeted next-generation sequencing for the genetic screening analysis and diagnosis of ML II alpha/beta., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

16. The DMAP interaction domain of UDP-GlcNAc:lysosomal enzyme N-acetylglucosamine-1-phosphotransferase is a substrate recognition module.

Author

Qian Y, Flanagan-Steet H, van Meel E, Steet R, and Kornfeld SA

Subjects

Abnormalities, Multiple enzymology, Acetylglucosamine metabolism, Animals, Female, HEK293 Cells, HeLa Cells, Humans, Hydrolases metabolism, Male, Mannosephosphates metabolism, Mice, Mucolipidoses enzymology, Mutagenesis, Site-Directed, Mutation, Missense, Phosphorylation physiology, Protein Structure, Tertiary physiology, Protein Subunits chemistry, Protein Subunits genetics, Protein Subunits metabolism, Ribonucleoproteins, Small Nuclear chemistry, Ribonucleoproteins, Small Nuclear genetics, Ribonucleoproteins, Small Nuclear metabolism, Substrate Specificity, Transferases (Other Substituted Phosphate Groups) chemistry, Transferases (Other Substituted Phosphate Groups) genetics, Zebrafish, Zebrafish Proteins chemistry, Zebrafish Proteins genetics, Abnormalities, Multiple metabolism, Lysosomes enzymology, Mucolipidoses metabolism, Transferases (Other Substituted Phosphate Groups) metabolism, Zebrafish Proteins metabolism

Abstract

UDP-GlcNAc:lysosomal enzyme N-acetylglucosamine-1-phosphotransferase (GlcNAc-1-phosphotransferase) is an α2β2γ2 heterohexamer that mediates the initial step in the formation of the mannose 6-phosphate recognition signal on lysosomal acid hydrolases. We previously reported that the specificity of the reaction is determined by the ability of the α/β subunits to recognize a conformation-dependent protein determinant present on the acid hydrolases. We now present evidence that the DNA methyltransferase-associated protein (DMAP) interaction domain of the α subunit functions in this recognition process. First, GST-DMAP pulled down several acid hydrolases, but not nonlysosomal glycoproteins. Second, recombinant GlcNAc-1-phosphotransferase containing a missense mutation in the DMAP interaction domain (Lys732Asn) identified in a patient with mucolipidosis II exhibited full activity toward the simple sugar α-methyl d-mannoside but impaired phosphorylation of acid hydrolases. Finally, unlike the WT enzyme, expression of the K732N mutant in a zebrafish model of mucolipidosis II failed to correct the phenotypic abnormalities. These results indicate that the DMAP interaction domain of the α subunit functions in the selective recognition of acid hydrolase substrates and provides an explanation for the impaired phosphorylation of acid hydrolases in a patient with mucolipidosis II.

Published

2013

17. Novel mutations in the neuraminidase-1 (NEU1) gene in two patients of sialidosis in India.

Author

Ranganath P, Sharma V, Danda S, Nandineni MR, and Dalal AB

Subjects

Adolescent, Amino Acid Sequence, Base Sequence, Chromatography, Thin Layer, Female, Humans, India, Infant, Molecular Sequence Data, Mutation genetics, Neuraminidase deficiency, Oligosaccharides urine, Sequence Analysis, DNA, Mucolipidoses enzymology, Mucolipidoses pathology, Neuraminidase genetics

Published

2012

18. A role for inherited metabolic deficits in persistent developmental stuttering.

Author

Kang C and Drayna D

Subjects

Animals, Biological Transport, Disease Models, Animal, Humans, Lysosomes pathology, Mice, Mucolipidoses complications, Mucolipidoses genetics, Mutation, Phosphoric Diester Hydrolases metabolism, Stuttering complications, Stuttering enzymology, Transferases (Other Substituted Phosphate Groups) metabolism, Vocalization, Animal, Lysosomes enzymology, Mucolipidoses enzymology, Phosphoric Diester Hydrolases genetics, Stuttering genetics, Transferases (Other Substituted Phosphate Groups) genetics

Abstract

Stuttering is a common but poorly understood speech disorder. Consistent evidence for the involvement of genetic factors in stuttering has motivated studies aimed at identifying causative genetic variants that could shed light on the underlying molecular and cellular deficits in this disorder. Such studies have begun to identify causative genes. The purpose of this review is to summarize the gene discoveries to date, and to cover the subsequent functional studies that are beginning to provide insights into how these gene mutations might cause stuttering. Surprisingly, the first variant genes to be associated with stuttering are those encoding the lysosomal targeting system, GNPTAB, GNPTG, and NAGPA. Although mutations in NAGPA have not been associated with a disorder in humans, mutations in GNPTAB and GNPTG cause mucolipidosis types II and III, which are rare autosomal recessive lysosomal storage disorders, associated with pathology of bone, connective tissue, liver, spleen, and brain. Analysis of mutations in these genes has so far identified predominantly missense mutations in stuttering, in contrast to the truncating and other mutations that result in very low GNPTAB/G enzyme activity and are historically associated with mucolipidosis. Genetic evidence for the role of lysosomal targeting mutations in stuttering has now been buttressed by biochemical studies of the mutant enzymes found in this disorder. While data on the GlcNAc-phosphotransferase encoded by GNPTAB/G remains limited and only suggestive, a study of the enzyme encoded by NAGPA has shown that the mutations found in stuttering reduce the overall cellular activity of this enzyme by about half, and that they result in deficits in intracellular processing and trafficking that lead to a reduced cellular half life. How these deficits result in the presumed speech-specific neuropathology associated with stuttering is not yet known. However these findings have opened several new lines of inquiry, including studies in mice carrying human stuttering mutations, that represent promising approaches to this disorder., (Published by Elsevier Inc.)

Published

2012

19. Lysosomal dysfunction causes neurodegeneration in mucolipidosis II 'knock-in' mice.

Author

Kollmann K, Damme M, Markmann S, Morelle W, Schweizer M, Hermans-Borgmeyer I, Röchert AK, Pohl S, Lübke T, Michalski JC, Käkelä R, Walkley SU, and Braulke T

Subjects

Animals, Atrophy, Autophagy, Brain enzymology, Brain pathology, Disease Models, Animal, Lysosomes enzymology, Lysosomes pathology, Mice, Mice, Transgenic, Mucolipidoses enzymology, Mucolipidoses pathology, Nerve Degeneration enzymology, Nerve Degeneration pathology, Vesicular Transport Proteins metabolism, alpha-L-Fucosidase metabolism, alpha-Mannosidase metabolism, beta-N-Acetylhexosaminidases metabolism, Lysosomes genetics, Mucolipidoses genetics, Nerve Degeneration genetics

Abstract

Mucolipidosis II is a neurometabolic lysosomal trafficking disorder of infancy caused by loss of mannose 6-phosphate targeting signals on lysosomal proteins, leading to lysosomal dysfunction and accumulation of non-degraded material. However, the identity of storage material and mechanisms of neurodegeneration in mucolipidosis II are unknown. We have generated 'knock-in' mice with a common mucolipidosis II patient mutation that show growth retardation, progressive brain atrophy, skeletal abnormalities, elevated lysosomal enzyme activities in serum, lysosomal storage in fibroblasts and brain and premature death, closely mimicking the mucolipidosis II disease in humans. The examination of affected mouse brains at different ages by immunohistochemistry, ultrastructural analysis, immunoblotting and mass spectrometric analyses of glycans and anionic lipids revealed that the expression and proteolytic processing of distinct lysosomal proteins such as α-l-fucosidase, β-hexosaminidase, α-mannosidase or Niemann-Pick C2 protein are more significantly impacted by the loss of mannose 6-phosphate residues than enzymes reaching lysosomes independently of this targeting mechanism. As a consequence, fucosylated N-glycans, GM2 and GM3 gangliosides, cholesterol and bis(monoacylglycero)phosphate accumulate progressively in the brain of mucolipidosis II mice. Prominent astrogliosis and the accumulation of organelles and storage material in focally swollen axons were observed in the cerebellum and were accompanied by a loss of Purkinje cells. Moreover, an increased neuronal level of the microtubule-associated protein 1 light chain 3 and the formation of p62-positive neuronal aggregates indicate an impairment of constitutive autophagy in the mucolipidosis II brain. Our findings demonstrate the essential role of mannose 6-phosphate for selected lysosomal proteins to maintain the capability for degradation of sequestered components in lysosomes and autophagolysosomes and prevent neurodegeneration. These lysosomal proteins might be a potential target for a valid therapeutic approach for mucolipidosis II disease.

Published

2012

20. Unusual pulmonary findings in mucolipidosis II.

Author

Ishak M, Zambrano EV, Bazzy-Asaad A, and Esquibies AE

Subjects

Cord Blood Stem Cell Transplantation, Hemosiderosis enzymology, Hemosiderosis pathology, Humans, Infant, Lung Diseases enzymology, Lung Diseases pathology, Male, Mucolipidoses enzymology, Mucolipidoses pathology, Mucolipidoses surgery, Mutation, Pulmonary Fibrosis enzymology, Pulmonary Fibrosis pathology, Transferases (Other Substituted Phosphate Groups) genetics, Hemosiderosis, Pulmonary, Hemosiderosis genetics, Lung Diseases genetics, Mucolipidoses complications, Mucolipidoses genetics, Pulmonary Fibrosis genetics

Abstract

We report undescribed pulmonary findings in a child with mucolipidosis II (ML-II). Children with ML-II bear significant pulmonary morbidity that may include extensive pulmonary fibrosis, persistent hemosiderosis as well as pulmonary airway excrescences as they reach preschool age., (Copyright © 2011 Wiley Periodicals, Inc.)

Published

2012

21. Using next-generation sequencing for the diagnosis of rare disorders: a family with retinitis pigmentosa and skeletal abnormalities.

Author

Schrader KA, Heravi-Moussavi A, Waters PJ, Senz J, Whelan J, Ha G, Eydoux P, Nielsen T, Gallagher B, Oloumi A, Boyd N, Fernandez BA, Young TL, Jones SJ, Hirst M, Shah SP, Marra MA, Green J, and Huntsman DG

Subjects

Adult, Chromosome Mapping methods, Computational Biology methods, DNA Mutational Analysis methods, Female, Gene Deletion, Genetic Linkage, Glycoside Hydrolases blood, Heterozygote, Humans, Male, Mucolipidoses enzymology, Mucolipidoses genetics, Mutation, Osteochondrodysplasias enzymology, Osteochondrodysplasias genetics, Pedigree, Rare Diseases diagnosis, Rare Diseases enzymology, Rare Diseases genetics, Retinitis Pigmentosa enzymology, Retinitis Pigmentosa genetics, Transferases (Other Substituted Phosphate Groups) genetics, Mucolipidoses diagnosis, Osteochondrodysplasias diagnosis, Retinitis Pigmentosa diagnosis

Abstract

Linkage analysis with subsequent candidate gene sequencing is typically used to diagnose novel inherited syndromes. It is now possible to expedite diagnosis through the sequencing of all coding regions of the genome (the exome) or full genomes. We sequenced the exomes of four members of a family presenting with spondylo-epiphyseal dysplasia and retinitis pigmentosa and identified a six-base-pair (6-bp) deletion in GNPTG, the gene implicated in mucolipidosis type IIIγ. The diagnosis was confirmed by biochemical studies and both broadens the mucolipidosis type III phenotype and demonstrates the clinical utility of next-generation sequencing to diagnose rare genetic diseases., (Copyright © 2011 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.)

Published

2011

22. A key enzyme in the biogenesis of lysosomes is a protease that regulates cholesterol metabolism.

Author

Marschner K, Kollmann K, Schweizer M, Braulke T, and Pohl S

Subjects

Animals, CHO Cells, Cell Line, Chondrocytes cytology, Cricetinae, Cricetulus, Enzyme Precursors chemistry, HeLa Cells, Humans, Lipid Metabolism, Lysosomes enzymology, Lysosomes ultrastructure, Mannosephosphates metabolism, Mice, Morphogenesis, Mucolipidoses enzymology, Mucolipidoses genetics, Mucolipidoses metabolism, Mucolipidoses pathology, N-Acetylgalactosamine-4-Sulfatase metabolism, Osteogenesis, Proprotein Convertases genetics, Protein Subunits chemistry, Protein Subunits metabolism, RNA, Small Interfering, Serine Endopeptidases genetics, Transferases (Other Substituted Phosphate Groups) chemistry, Cholesterol metabolism, Enzyme Precursors metabolism, Lysosomes metabolism, Proprotein Convertases metabolism, Serine Endopeptidases metabolism, Transferases (Other Substituted Phosphate Groups) metabolism

Abstract

Mucolipidosis II is a severe lysosomal storage disorder caused by defects in the α and β subunits of the hexameric N-acetylglucosamine-1-phosphotransferase complex essential for the formation of the mannose 6-phosphate targeting signal on lysosomal enzymes. Cleavage of the membrane-bound α/β-subunit precursor by an unknown protease is required for catalytic activity. Here we found that the α/β-subunit precursor is cleaved by the site-1 protease (S1P) that activates sterol regulatory element-binding proteins in response to cholesterol deprivation. S1P-deficient cells failed to activate the α/β-subunit precursor and exhibited a mucolipidosis II-like phenotype. Thus, S1P functions in the biogenesis of lysosomes, and lipid-independent phenotypes of S1P deficiency may be caused by lysosomal dysfunction.

Published

2011

23. Vacuolization of mucolipidosis type II mouse exocrine gland cells represents accumulation of autolysosomes.

Author

Boonen M, van Meel E, Oorschot V, Klumperman J, and Kornfeld S

Subjects

Acid Anhydride Hydrolases metabolism, Animals, Exocrine Glands enzymology, Fibroblasts enzymology, Fibroblasts pathology, Gene Deletion, Humans, Lysosomes enzymology, Mannosephosphates metabolism, Mice, Mice, Knockout, Microscopy, Immunoelectron, Mucolipidoses enzymology, Organ Specificity, Secretory Vesicles enzymology, Secretory Vesicles pathology, Transferases (Other Substituted Phosphate Groups) genetics, Vacuoles enzymology, Exocrine Glands pathology, Lysosomes pathology, Mucolipidoses pathology, Transferases (Other Substituted Phosphate Groups) deficiency, Vacuoles pathology

Abstract

We previously reported that mice deficient in UDP-GlcNAc:lysosomal enzyme GlcNAc-1-phosphotransferase (mucolipidosis type II or Gnptab -/- mice), the enzyme that initiates the addition of the mannose 6-phosphate lysosomal sorting signal on acid hydrolases, exhibited extensive vacuolization of their exocrine gland cells, while the liver, brain, and muscle appeared grossly unaffected. Similar pathological findings were observed in several exocrine glands of patients with mucolipidosis II. To understand the basis for this cell type-specific abnormality, we analyzed these tissues in Gnptab -/- mice using a combined immunoelectron microscopy and biochemical approach. We demonstrate that the vacuoles in the exocrine glands are enlarged autolysosomes containing undigested cytoplasmic material that accumulate secondary to deficient lysosomal function. Surprisingly, the acid hydrolase levels in these tissues ranged from normal to modestly decreased, in contrast to skin fibroblasts, which accumulate enlarged lysosomes and/or autolysosomes also but exhibit very low levels of acid hydrolases. We propose that the lysosomal defect in the exocrine cells is caused by the combination of increased secretion of the acid hydrolases via the constitutive pathway along with their entrapment in secretory granules. Taken together, our results provide new insights into the mechanisms of the tissue-specific abnormalities seen in mucolipidosis type II.

Published

2011

24. The cation channel mucolipin-1 is a bifunctional protein that facilitates membrane remodeling via its serine lipase domain.

Author

LaPlante JM, Falardeau JL, Brown EM, Slaugenhaupt SA, and Vassilev PM

Subjects

Animals, Fibroblasts chemistry, Fibroblasts enzymology, Fibroblasts metabolism, Humans, Lipase genetics, Membrane Fusion Proteins genetics, Membrane Fusion Proteins metabolism, Mucolipidoses enzymology, Mutation, Protein Structure, Tertiary, TRPM Cation Channels genetics, Transient Receptor Potential Channels, Xenopus laevis, Cell Membrane chemistry, Cell Membrane metabolism, Lipase metabolism, TRPM Cation Channels metabolism

Abstract

Phospholipase modulators have been shown to affect the topology of lipid bilayers and the formation of tubulo-vesicular structures, but the specific endogenous phospholipases involved have yet to be identified. Here we show that TRPML1 (MLN1), a Ca(2+)-permeable channel, contributes to membrane remodeling through a serine lipase consensus domain, and thus represents a novel type of bifunctional protein. Remarkably, this serine lipase active site determines the ability of MLN1 to generate tubulo-vesicular extensions in mucolipin-1-expressing oocytes, human fibroblasts and model membrane vesicles. Our demonstration that MLN1 is involved in membrane remodeling and the formation of extensions suggests that it may play a role in the formation of cellular processes linked to the late endosome/lysosome (LE/L) pathway. MLN1 is absent or mutated in patients with mucolipidosis IV (MLIV), a lysosomal disorder with devastating neurological and other consequences. This study provides potential insight into the pathophysiology of MLIV., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

25. A novel single-chain antibody fragment for detection of mannose 6-phosphate-containing proteins: application in mucolipidosis type II patients and mice.

Author

Müller-Loennies S, Galliciotti G, Kollmann K, Glatzel M, and Braulke T

Subjects

Animals, Child, Preschool, Enzyme-Linked Immunosorbent Assay methods, Gene Knock-In Techniques, Humans, Immunoglobulin Fragments genetics, Male, Mice, Middle Aged, Mucolipidoses enzymology, Single-Chain Antibodies genetics, Transferases (Other Substituted Phosphate Groups) genetics, Transferases (Other Substituted Phosphate Groups) metabolism, Immunoglobulin Fragments metabolism, Mannosephosphates metabolism, Mucolipidoses diagnosis, Proteins chemistry, Single-Chain Antibodies metabolism

Abstract

Newly synthesized soluble lysosomal hydrolases require mannose 6-phosphate (Man6P) residues on their oligosaccharides for their transport to lysosomes. The formation of Man6P residues is catalyzed by the GlcNAc-1-phosphotransferase, which is defective in the lysosomal storage disorders mucolipidosis type II (ML II) and ML III. Both hypersecretion and reduced intracellular level of lysosomal enzymes as well as direct sequencing of GlcNAc-1-phosphotransferase genes are important diagnostic markers for ML II and ML III. A high-affinity Man6P-specific single-chain antibody fragment was generated, allowing the rapid indirect demonstration of defective GlcNAc-1-phosphotransferase. In media and extracts of cultured fibroblasts of healthy controls but not of ML II and ML III patients, several Man6P-containing proteins could be detected by anti-Man6P Western blotting. Immunoprecipitation of Man6P-containing proteins from conditioned media or mouse brain extracts followed by arylsulfatase A and cathepsin D Western blotting confirmed the specificity of the antibody fragment for lysosomal proteins. Application of the antibody fragment in immunohistochemistry of human brain slices from nonaffected patients showed strong neuronal immunoreactivity, which was not observed in cortical sections of an ML II patient. Finally, in brain extracts of a novel GlcNAc-1-phosphotransferase knock-in mouse no Man6P-containing proteins were detectable. Thus, the single-chain antibody fragment against Man6P was demonstrated to allow the specific, rapid, and convenient detection of Man6P-containing proteins and facilitates the diagnosis of ML II and ML III.

Published

2010

26. Thymoquinone from nutraceutical black cumin oil activates Neu4 sialidase in live macrophage, dendritic, and normal and type I sialidosis human fibroblast cells via GPCR Galphai proteins and matrix metalloproteinase-9.

Author

Finlay TM, Jayanth P, Amith SR, Gilmour A, Guzzo C, Gee K, Beyaert R, and Szewczuk MR

Subjects

Animals, Benzoquinones chemistry, Blotting, Western, Cell Line, Cell Survival drug effects, Cells, Cultured, Enzyme Activation drug effects, Flow Cytometry, Humans, Immunohistochemistry, Immunoprecipitation, Mice, Mice, Knockout, Polymerase Chain Reaction, Benzoquinones pharmacology, Fibroblasts enzymology, Macrophages enzymology, Matrix Metalloproteinase 9 metabolism, Mucolipidoses enzymology, Neuraminidase metabolism, Nigella sativa chemistry, Receptors, G-Protein-Coupled metabolism

Abstract

Anti-inflammatory activities of thymoquinone (TQ) have been demonstrated in in vitro and in vivo studies. However, the precise mechanism(s) of TQ in these anti-inflammatory activities is not well understood. Using a newly developed assay to detect sialidase activity in live macrophage cells (Glycoconj J doi: 10.1007/s10719-009-9239-8 ), here we show that TQ has no inhibitory effect on endotoxin lipopolysaccharide (LPS) induced sialidase activity in live BMC-2 macrophage cells. In contrast, the parent black seed oil (BSO) and another constituent of BSO para-cymene (p-CY) completely block LPS induced sialidase activity. All of these compounds had no effect on cell viability. On the other hand, TQ induces a vigorous sialidase activity in live BMC-2 macrophage cells in a dose dependent manner as well in live DC-2.4 dendritic cells, HEK-TLR4/MD2, HEK293, SP1 mammary adenocarcinoma cells, human WT and 1140F01 and WG0544 type I sialidosis fibroblast cells. Tamiflu (oseltamivir phosphate) inhibits TQ-induced sialidase activity in live BMC-2 cells with an IC(50) of 0.0194 microM compared to an IC(50) of 19.1 microM for neuraminidase inhibitor DANA (2-deoxy-2,3-dehydro-N-acetylneuraminic acid). Anti-Neu1, -2 and -3 antibodies have no inhibition of TQ-induced sialidase activity in live BMC-2 and human THP-1 macrophage cells but anti-Neu4 antibodies completely block this activity. There is a vigorous sialidase activity associated with TQ treated live primary bone marrow (BM) macrophage cells derived from WT and hypomorphic cathepsin A mice with a secondary Neu1 deficiency (NeuI KD), but not from Neu4 knockout (Neu4 KO) mice. Pertussis toxin (PTX), a specific inhibitor of Galphai proteins of G-protein coupled receptor (GPCR) and the broad range inhibitors of matrix metalloproteinase (MMP) galardin and piperazine applied to live BMC-2, THP-1 and primary BM macrophage cells completely block TQ-induced sialidase activity. These same inhibitory effects are not observed with the GM1 ganglioside specific cholera toxin subunit B (CTXB) as well as with CTX, tyrosine kinase inhibitor K252a, and the broad range GPCR inhibitor suramin. The specific inhibitor of MMP-9, anti-MMP-9 antibody and anti-Neu4 antibody, but not the specific inhibitor of MMP-3 completely block TQ-induced sialidase activity in live THP-1 cells, which express Neu4 and MMP-9 on the cell surface. Neu4 sialidase activity in cell lysates from TQ-treated live THP-1 cells desialylates natural gangliosides and mucin substrates. RT-PCR and western blot analyses reveal no correlation between mRNA and protein values for Neu3 and Neu4 in human monocytic THP-1 cells, suggesting for the first time a varied post-transcriptional mechanism for these two mammalian sialidases independent of TQ activation. Our findings establish an unprecedented activation of Neu4 sialidase on the cell surface by thymoquinone, which is derived from the nutraceutical black cumin oil. The potentiation of GPCR-signaling by TQ via membrane targeting of Galphai subunit proteins and matrix metalloproteinase-9 activation may be involved in the activation process of Neu4 sialidase on the cell surface.

Published

2010

27. Loss of N-acetylglucosamine-1-phosphotransferase gamma subunit due to intronic mutation in GNPTG causes mucolipidosis type III gamma: Implications for molecular and cellular diagnostics.

Author

Pohl S, Encarnacão M, Castrichini M, Müller-Loennies S, Muschol N, and Braulke T

Subjects

Adolescent, Female, Humans, Male, Mucolipidoses enzymology, Pathology, Molecular, RNA, Messenger genetics, Introns, Mucolipidoses genetics, Mutation, Transferases (Other Substituted Phosphate Groups) genetics

Abstract

Mucolipidosis type III gamma (MLIII, pseudo-Hurler polydystrophy) is a rare autosomal recessive disorder where the activity of the multimeric GlcNAc-1-phosphotransferase is reduced and formation of the mannose 6-phosphate (M6P) recognition marker on lysosomal enzymes is impaired. In this disease, the targeting of lysosomal enzymes is affected resulting in their hypersecretion, and an intracellular deficiency of multiple hydrolases. We report the biochemical and molecular diagnosis of MLIII in three siblings, aged 17, 15, and 14 years, who presented with joint pain and progressive joint stiffness. In addition to missorting of newly synthesized lysosomal protease cathepsin D, there were low levels of M6P-containing proteins in cell extracts and media of cultured fibroblasts of the Patients. Direct sequencing identified a novel homozygous mutation in intron 7, IVS7-10G>A, of the GNPTG gene, which encodes the gamma-subunit of the GlcNAc-1-phosphotransferase. This mutation created a cryptic 3'-splice site resulting in a frameshift and premature translational termination (p.V176GfsX18). The GNPTG mRNA levels were markedly reduced in Patients' fibroblasts indicating that the intronic mutation mediates mRNA decay, which was confirmed by absence of the gamma-subunit protein. These data contribute to an efficient diagnostic strategy to identify Patients with MLIII gamma and characterize their biochemical defect in fibroblasts.

Published

2010

28. Mannose phosphorylation in health and disease.

Author

Kollmann K, Pohl S, Marschner K, Encarnação M, Sakwa I, Tiede S, Poorthuis BJ, Lübke T, Müller-Loennies S, Storch S, and Braulke T

Subjects

Animals, Humans, Mucolipidoses enzymology, Mucolipidoses genetics, Phosphorylation, Transferases (Other Substituted Phosphate Groups) chemistry, Transferases (Other Substituted Phosphate Groups) genetics, Transferases (Other Substituted Phosphate Groups) metabolism, Disease, Health, Mannose metabolism

Abstract

Lysosomal hydrolases catalyze the degradation of a variety of macromolecules including proteins, carbohydrates, nucleic acids and lipids. The biogenesis of lysosomes or lysosome-related organelles requires a continuous substitution of soluble acid hydrolases and lysosomal membrane proteins. The targeting of lysosomal hydrolases depends on mannose 6-phosphate residues (M6P) that are recognized by specific receptors mediating their transport to an endosomal/prelysosomal compartment. The key role in the formation of M6P residues plays the GlcNAc-1-phosphotransferase localized in the Golgi apparatus. Two genes have been identified recently encoding the type III alpha/beta-subunit precursor membrane protein and the soluble gamma-subunit of GlcNAc-1-phosphotransferase. Mutations in these genes result in two severe diseases, mucolipidosis type II (MLII) and III (MLIII), biochemically characterized by the missorting of multiple lysosomal hydrolases due to impaired formation of the M6P recognition marker, and general lysosomal dysfunction. This review gives an update on structural properties, localization and functions of the GlcNAc-1-phosphotransferase subunits and improvements of pre- and postnatal diagnosis of ML patients. Further, the generation of recombinant single-chain antibody fragments against M6P residues and of new mouse models of MLII and MLIII will have considerable impact to provide deeper insight into the cell biology of lysosomal dysfunctions and the pathomechanisms underlying these lysosomal disorders., (Copyright (c) 2009 Elsevier GmbH. All rights reserved.)

Published

2010

29. Molecular analysis of cell lines from patients with mucolipidosis II and mucolipidosis III.

Author

Zarghooni M and Dittakavi SS

Subjects

Blotting, Western, Cell Extracts, Cell Line, DNA Mutational Analysis, Enhancer Elements, Genetic genetics, Exons genetics, Extracellular Space enzymology, Fibroblasts enzymology, Fibroblasts pathology, Hexosaminidases metabolism, Homozygote, Humans, Intracellular Space enzymology, Mucolipidoses enzymology, Mucolipidoses pathology, Mucolipidoses therapy, Mutation genetics, Peptides metabolism, Phenotype, Protein Subunits metabolism, Solubility, Subcellular Fractions enzymology, beta-Galactosidase metabolism, Mucolipidoses genetics

Abstract

Mucolipidosis II and III are autosomal recessive disorders due to mutations in the GNPTAB and GNPTG genes encoding the alphabeta- and gamma-subunits of the GlcNAc-1-phosphotransferase, respectively. This protein has a subunit structure of alpha(2)beta(2)gamma(2) and initiates the first step of tagging lysosomal enzymes with mannose-6-phosphate (M6P). In the present study, we screened four MLII and three MLIII cell lines for mutations in GNPTAB and GNPTG. Nine novel mutations in GNPTAB and two previously reported mutations in GNPTAB and GNPTG were identified. By using anti-peptide antibodies against the alpha- and beta-subunits, we show that mutations in the gamma-subunit affected the assembly and intracellular distribution of the alpha- and beta-subunits. Furthermore, the biochemical phenotypes of MLII and MLIII fibroblasts can be corrected by transfection with wild-type cDNA expression constructs encoding the alpha/beta- and gamma-subunits of GlcNAc-1-phosphotransferase, respectively.

Published

2009

30. Inhibition of autophagosome formation restores mitochondrial function in mucolipidosis II and III skin fibroblasts.

Author

Otomo T, Higaki K, Nanba E, Ozono K, and Sakai N

Subjects

Adaptor Proteins, Signal Transducing metabolism, Autophagy, Cathepsin B metabolism, Cathepsin D metabolism, Fibroblasts enzymology, Humans, Inclusion Bodies metabolism, Lysosomes metabolism, Lysosomes pathology, Mucolipidoses enzymology, Phagosomes pathology, Protein Transport, Sequestosome-1 Protein, Subcellular Fractions enzymology, Ubiquitinated Proteins metabolism, Fibroblasts pathology, Mitochondria metabolism, Mucolipidoses pathology, Mucolipidoses physiopathology, Phagosomes metabolism, Skin pathology

Abstract

Mucolipidosis II and III are progressive lysosomal storage disorders caused by a deficiency of N-acetylglucosamine-1-phosphotransferase, leading to massive accumulation of undigested substrates in lysosomes (inclusion bodies) in skin fibroblast. In this study, we demonstrated accumulation of autolysosomes and increased levels of p62 and ubiquitin proteins in cultured fibroblasts. These autophagic elevations were milder in mucolipidosis III compared with mucolipidosis II. Mitochondrial structure was fragmented and activity was impaired in the affected cells, and 3-methyladenine, an inhibitor of autophagosome formation, restored these. These results show for the first time autophagic and mitochondrial dysfunctions in this disorder.

Published

2009

31. Expression and molecular dynamics studies on effect of amino acid substitutions at Arg344 in human cathepsin A on the protein local conformation.

Author

Yoshida T, Kadota Y, Hitaoka S, Kori E, Horikawa Y, Taguchi M, Tsuji D, Hirokawa T, Chuman H, and Itoh K

Subjects

Amino Acid Substitution, Humans, Models, Molecular, Molecular Dynamics Simulation, Mucolipidoses enzymology, Water chemistry, Cathepsin A chemistry, Cathepsin A genetics, Protein Conformation drug effects

Abstract

Human lysosomal protective protein/cathepsin A (CathA) is a multifunctional protein that exhibits not only protective functions as to lysosomal glycosidases, i.e., neuraminidase 1 (NEU1) and beta-galactosidase (GLB), but also its own serine carboxypeptidase activity, and exhibits conserved structural similarity to yeast and wheat homologs (CPY and CPW). Our previous study revealed that the R344 (Arg344) residue in CathA could contribute to the binding and recognition of the serine peptidase inhibitor chymostatin. We examined here the effects of substitution of R344 with other amino acids, including A, D, E, G, I, K, M, N, P, Q, S, and V, denoted as R344X, including the wild-type CathA, on expression of CathA activity and intracellular processing. Among the mutant gene products, the 54-kDa precursor/zymogen with the R344D substitution was not processed to the 32/20-kDa mature form with CathA activity in a fibroblastic cell line derived from a galactosialidosis patient. Molecular dynamics (MD) simulations on the total twelve R344X mutants and the wild-type revealed that only R344D takes on a significantly different conformation of S293-D295 in the excision peptide (M285-R298) compared to the other R344X mutants; the side chains of S293 and D295 in R344D are exposed on the molecular surface, although those in the other twelve R344X mutants are buried inside the protein. The results of the current work strongly suggest that the distinct conformational change of the S293-D295 region in the R344D protein causes the processing defect of the 54-kDa precursor of the R344D mutant gene product in cultured cells.

Published

2009

32. A longitudinal study of Taiwanese sialidosis type 1: an insight into the concept of cherry-red spot myoclonus syndrome.

Author

Lai SC, Chen RS, Wu Chou YH, Chang HC, Kao LY, Huang YZ, Weng YH, Chen JK, Hwu WL, and Lu CS

Subjects

Adolescent, Adult, Ataxia enzymology, Ataxia genetics, Ataxia physiopathology, Child, Disease Progression, Evoked Potentials, Somatosensory, Evoked Potentials, Visual, Female, Humans, Longitudinal Studies, Male, Mucolipidoses enzymology, Myoclonus enzymology, Myoclonus genetics, Myoclonus physiopathology, Neuraminidase metabolism, Neurodegenerative Diseases enzymology, Seizures enzymology, Seizures genetics, Seizures physiopathology, Taiwan, Young Adult, Mucolipidoses genetics, Mucolipidoses physiopathology, Mutation, Missense, Neuraminidase genetics, Neurodegenerative Diseases genetics, Neurodegenerative Diseases physiopathology

Abstract

Background and Purpose: Sialidosis type 1 (ST-1) is a neurodegenerative disorder with limited long-term follow-up report. This study is to document the chronological profile of ST-1., Methods: We perform serial analysis of 17 Taiwanese patients with ST-1 focusing on evolution of clinical features, electrophysiological findings, genetic studies, and neuroimage examinations., Results: All patients had a mutation at 554A-->G in exon 3 of the NEU1 gene causing Ser182Gly substitution. Fifteen patients were homozygous. Two patients were heterozygous with novel mutations, 956C-->T causing Ala319Val in one and 163C-->T causing Gln55stop codon in the other. The neuraminidase activity was markedly decreased in all 11 available patients. Only three patients (17.6%) manifested the macular cherry-red spot. The majority of patients (82.3%) developed full-blown manifestation of myoclonus, ataxia, and seizures within 5 years. Abnormal somatosensory evoked potentials with giant cortical waves were found in all patients. Prolonged P100 peak latency of the visual evoked potentials (VEPs) were found in 16 patients (94.1%) in the early stage even without visual symptoms., Conclusion: ST-1 in Taiwanese population illustrates distinct characteristics of phenotype with infrequent cherry-red spot. We suggest to screen the NEU1 mutations in patients presenting action myoclonus with abnormal VEPs, even without macular cherry-red spots.

Published

2009

33. Molecular analysis of the GNPTAB and GNPTG genes in 13 patients with mucolipidosis type II or type III - identification of eight novel mutations.

Author

Encarnação M, Lacerda L, Costa R, Prata MJ, Coutinho MF, Ribeiro H, Lopes L, Pineda M, Ignatius J, Galvez H, Mustonen A, Vieira P, Lima MR, and Alves S

Subjects

Child, Child, Preschool, Gene Expression Regulation, Enzymologic, Genotype, Humans, Infant, Infant, Newborn, Phenotype, RNA Splicing genetics, RNA, Messenger genetics, RNA, Messenger metabolism, Reverse Transcriptase Polymerase Chain Reaction, Transferases (Other Substituted Phosphate Groups) metabolism, Mucolipidoses enzymology, Mucolipidoses genetics, Mutation genetics, Transferases (Other Substituted Phosphate Groups) genetics

Abstract

Mucolipidosis II (ML II) and mucolipidosis III (ML III) are diseases in which the activity of the uridine diphosphate (UDP)-N-acetylglucosamine:lysosomal enzyme N-acetylglucosamine-1-phosphotransferase (GlcNAc-phosphotransferase) is absent or reduced, respectively. In the absence of mannose phosphorylation, trafficking of lysosomal hydrolases to the lysosome is impaired. In these diseases, mistargeted lysosomal hydrolases are secreted into the blood, resulting in lysosomal deficiency of many hydrolases and a storage-disease phenotype. GlcNAc-phosphotransferase is a multimeric transmembrane enzyme composed of three subunits (alpha, beta and gamma) encoded by two genes -GNPTAB and GNPTG. Defects in GNPTAB result in ML II and III whereas mutations in GNPTG were only found in ML III patients. We have performed a molecular analysis of the GNPTAB and GNPTG genes in 13 mucolipidosis II and III patients (10 Portuguese, one Finnish, one Spanish of Arab origin and one Indian). Mutations were identified by the study of both cDNA and gDNA. The GNPTAB and GNPTG mRNA expressions were determined by quantitative reverse transcriptase polymerase chain reaction (qRT-PCR). The study led to the identification of 11 different mutations. Eight of these mutations are novel, six in the GNPTAB gene [c.121delG (V41FfsX42), c.440delC (A147AfsX5), c.2249_50insA (N750KfsX8), c.242G>T (W81L), c.1208T>C (I403T) and c.1999G>T (p.E667X)] and two in the GNPTG gene [c.610-1G>T and c.639delT (F213LfsX7)]. With regard to the mRNA expression studies, the values obtained by qRT-PCR indicate the possible existence of feedback regulation mechanisms between alpha/beta and the gamma subunits.

Published

2009

34. Identification and molecular characterization of six novel mutations in the UDP-N-acetylglucosamine-1-phosphotransferase gamma subunit (GNPTG) gene in patients with mucolipidosis III gamma.

Author

Persichetti E, Chuzhanova NA, Dardis A, Tappino B, Pohl S, Thomas NS, Rosano C, Balducci C, Paciotti S, Dominissini S, Montalvo AL, Sibilio M, Parini R, Rigoldi M, Di Rocco M, Parenti G, Orlacchio A, Bembi B, Cooper DN, Filocamo M, and Beccari T

Subjects

Adolescent, Adult, Alternative Splicing genetics, Base Sequence, Child, Codon, Nonsense genetics, Female, Fibroblasts enzymology, Fibroblasts pathology, Genotype, Humans, Male, Molecular Sequence Data, Mutation, Missense genetics, RNA Splice Sites genetics, RNA Stability genetics, RNA, Messenger genetics, RNA, Messenger metabolism, Reverse Transcriptase Polymerase Chain Reaction, Sequence Deletion, Mucolipidoses enzymology, Mucolipidoses genetics, Mutation genetics, Protein Subunits genetics, Transferases (Other Substituted Phosphate Groups) genetics

Abstract

Mucolipidosis type III (MLIII) is an autosomal recessive disorder affecting lysosomal hydrolase trafficking. In a study of 10 patients from seven families with a clinical phenotype and enzymatic diagnosis of MLIII, six novel GNPTG gene mutations were identified. These included missense (p.T286M) and nonsense (p.W111X) mutations and a transition in the obligate AG-dinucleotide of the intron 8 acceptor splice site (c.610-2A>G). Three microdeletions were also identified, two of which (c.611delG and c.640_667del28) were located within the coding region whereas one (c.609+28_610-16del) was located entirely within intron 8. RT-PCR analysis of the c.610-2A>G transition demonstrated that the change altered splicing, leading to the production of two distinct aberrantly spliced forms, viz. the skipping of exon 9 (p.G204_K247del) or the retention of introns 8 and 9 (p.G204VfsX28). RT-PCR analysis, performed on a patient homozygous for the intronic deletion (c.609+28_610-16del), failed to detect any GNPTG RNA transcripts. To determine whether c.609+28_610-16del allele-derived transcripts were subject to nonsense-mediated mRNA decay (NMD), patient fibroblasts were incubated with the protein synthesis inhibitor anisomycin. An RT-PCR fragment retaining 43 bp of intron 8 was consistently detected suggesting that the 33-bp genomic deletion had elicited NMD. Quantitative real-time PCR and GNPTG western blot analysis confirmed that the homozygous microdeletion p.G204VfsX17 had elicited NMD resulting in failure to synthesize GNPTG protein. Analysis of the sequences surrounding the microdeletion breakpoints revealed either intrinsic repetitivity of the deleted region or short direct repeats adjacent to the breakpoint junctions. This is consistent with these repeats having mediated the microdeletions via replication slippage and supports the view that the mutational spectrum of the GNPTG gene is strongly influenced by the properties of the local DNA sequence environment.

Published

2009

35. Compensatory expression of human N-acetylglucosaminyl-1-phosphotransferase subunits in mucolipidosis type III gamma.

Author

Pohl S, Tiede S, Castrichini M, Cantz M, Gieselmann V, and Braulke T

Subjects

Animals, COS Cells, Cathepsin D metabolism, Cerebroside-Sulfatase metabolism, Child, Preschool, Chlorocebus aethiops, DNA Mutational Analysis, Humans, Male, Mannosephosphates metabolism, Mucolipidoses genetics, Mutation, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, Mucolipidoses enzymology, Transferases (Other Substituted Phosphate Groups) genetics, Transferases (Other Substituted Phosphate Groups) metabolism

Abstract

The N-Acetylglucosaminyl-1-phosphotransferase plays a key role in the generation of mannose 6-phosphate (M6P) recognition markersessential for efficient transport of lysosomal hydrolases to lysosomes. The phosphotransferase is composed of six subunits (alpha2, beta2, gamma2). The alpha- and beta-subunits are catalytically active and encoded by a single gene, GNPTAB, whereas the gamma-subunit encoded by GNPTG is proposed to recognize conformational structures common to lysosomal enzymes. Defects in GNPTG cause mucolipidosis type III gamma, which is characterized by missorting and cellular loss of lysosomal enzymes leading to lysosomal accumulation of storage material. Using plasmon resonance spectrometry, we showed that recombinant gamma-subunit failed to bind the lysosomal enzyme arylsulfatase A. Additionally, the overexpression of the gamma-subunit in COS7 cells did not result in hypersecretion of newly synthesized lysosomal enzymes expected for competition for binding sites of the endogenous phosphotransferase complex. Analysis of fibroblasts exhibiting a novel mutation in GNPTG (c.619insT, p.K207IfsX7) revealed that the expression of GNPTAB was increased whereas in gamma-subunit overexpressing cells the GNPTAB mRNA was reduced. The data suggest that the gamma-subunit is important for the balance of phosphotransferase subunits rather for general binding of lysosomal enzymes.

Published

2009

36. Mucolipidosis II and III alpha/beta: mutation analysis of 40 Japanese patients showed genotype-phenotype correlation.

Author

Otomo T, Muramatsu T, Yorifuji T, Okuyama T, Nakabayashi H, Fukao T, Ohura T, Yoshino M, Tanaka A, Okamoto N, Inui K, Ozono K, and Sakai N

Subjects

Base Sequence, DNA Mutational Analysis, Exons genetics, Gene Duplication, Genotype, Humans, Molecular Sequence Data, Mutation genetics, Phenotype, Polymorphism, Single Nucleotide genetics, Asian People genetics, Mucolipidoses enzymology, Mucolipidoses genetics, Transferases (Other Substituted Phosphate Groups) genetics

Abstract

Mucolipidosis (ML) II alpha/beta and III alpha/beta are autosomal recessive diseases caused by a deficiency of alpha and/or beta subunits of the enzyme N-acetylglucosamine-1-phosphotransferase, which is encoded by the GNPTAB gene. We analyzed the GNPTAB gene in 25 ML II and 15 ML III Japanese patients. In most ML II patients, the clinical conditions 'stand alone', 'walk without support' and 'speak single words' were impaired; however, the frequency of 'heart murmur', 'inguinal hernia' and 'hepatomegaly and/or splenomegaly' did not differ between ML II and III patients. We detected mutations in GNPTAB in 73 of 80 alleles. Fourteen new mutations were c.914_915insA, c.2089_2090insC, c.2427delC, c.2544delA, c.2693delA, c.3310delG, c.3388_3389insC+c.3392C>T, c.3428_3429insA, c.3741_3744delAGAA, p.R334L, p.F374L, p.H956Y, p.N1153S and duplication of exon 2. Previously reported mutations were p.Q104X, p.W894X, p.R1189X and c.2715+1G>A causing skipping of exon 13. Homozygotes or compound heterozygotes of nonsense and frameshift mutations contributed to the severe phenotype. p.F374L, p.N1153S and splicing mutations contributed to the attenuated phenotype, although coupled with nonsense mutation. These results show the effective molecular diagnosis of ML II and III and also provide phenotypic prediction. This is the first and comprehensive report of molecular analysis for ML patients of Japanese origin.

Published

2009

37. Neuraminidase-1, a subunit of the cell surface elastin receptor, desialylates and functionally inactivates adjacent receptors interacting with the mitogenic growth factors PDGF-BB and IGF-2.

Author

Hinek A, Bodnaruk TD, Bunda S, Wang Y, and Liu K

Subjects

Animals, Aorta cytology, Aorta enzymology, Becaplermin, Cell Membrane drug effects, Cell Proliferation drug effects, Cells, Cultured, Child, Preschool, Elastic Tissue drug effects, Elastic Tissue enzymology, Elastin metabolism, Fibroblasts drug effects, Fibroblasts enzymology, Fibroblasts pathology, Humans, Infant, Insulin-Like Growth Factor II pharmacology, Mitogens metabolism, Mitogens pharmacology, Mucolipidoses enzymology, Mucolipidoses pathology, Myocytes, Smooth Muscle cytology, Myocytes, Smooth Muscle drug effects, Myocytes, Smooth Muscle enzymology, Neuraminidase antagonists & inhibitors, Neuraminidase pharmacology, Platelet-Derived Growth Factor pharmacology, Proto-Oncogene Proteins c-sis, Receptor, IGF Type 1 metabolism, Receptors, Platelet-Derived Growth Factor metabolism, Recombinant Proteins pharmacology, Swine, Cell Membrane metabolism, Insulin-Like Growth Factor II metabolism, N-Acetylneuraminic Acid metabolism, Neuraminidase metabolism, Platelet-Derived Growth Factor metabolism, Protein Subunits metabolism, Receptors, Cell Surface metabolism

Abstract

We recently established that the elastin-binding protein, which is identical to the spliced variant of beta-galactosidase, forms a cell surface-targeted complex with two proteins considered "classic lysosomal enzymes": protective protein/cathepsin A and neuraminidase-1 (Neu1). We also found that cell surface-residing Neu1 can desialylate neighboring microfibrillar glycoproteins and facilitate the deposition of insoluble elastin, which contributes to the maintenance of cellular quiescence. Here we provide evidence that cell surface-residing Neu1 contributes to a novel mechanism that limits cellular proliferation by desialylating cell membrane-residing sialoglycoproteins that directly propagate mitogenic signals. We demonstrated that treatment of cultured human aortic smooth muscle cells (SMCs) with either a sialidase inhibitor or an antibody that blocks Neu1 activity induced significant up-regulation in SMC proliferation in response to fetal bovine serum. Conversely, treatment with Clostridium perfringens neuraminidase (which is highly homologous to Neu1) decreased SMC proliferation, even in cultures that did not deposit elastin. Further, we found that pretreatment of aortic SMCs with exogenous neuraminidase abolished their mitogenic responses to recombinant platelet-derived growth factor (PDGF)-BB and insulin-like growth factor (IGF)-2 and that sialidosis fibroblasts (which are exclusively deficient in Neu1) were more responsive to PDGF-BB and IGF-2 compared with normal fibroblasts. Furthermore, we provide direct evidence that neuraminidase caused the desialylation of both PDGF and IGF-1 receptors and diminished the intracellular signals induced by the mitogenic ligands PDGF-BB and IGF-2.

Published

2008

38. Membrane traffic and turnover in TRP-ML1-deficient cells: a revised model for mucolipidosis type IV pathogenesis.

Author

Miedel MT, Rbaibi Y, Guerriero CJ, Colletti G, Weixel KM, Weisz OA, and Kiselyov K

Subjects

Acyltransferases genetics, Endocytosis, HeLa Cells, Humans, Hydrogen-Ion Concentration, Kinetics, Lipids physiology, Lysosomes enzymology, Lysosomes physiology, Models, Biological, Mucolipidoses genetics, RNA, Small Interfering genetics, Transfection, Acyltransferases deficiency, Cell Membrane physiology, Mucolipidoses enzymology

Abstract

The lysosomal storage disorder mucolipidosis type IV (MLIV) is caused by mutations in the transient receptor potential-mucolipin-1 (TRP-ML1) ion channel. The "biogenesis" model for MLIV pathogenesis suggests that TRP-ML1 modulates postendocytic delivery to lysosomes by regulating interactions between late endosomes and lysosomes. This model is based on observed lipid trafficking delays in MLIV patient fibroblasts. Because membrane traffic aberrations may be secondary to lipid buildup in chronically TRP-ML1-deficient cells, we depleted TRP-ML1 in HeLa cells using small interfering RNA and examined the effects on cell morphology and postendocytic traffic. TRP-ML1 knockdown induced gradual accumulation of membranous inclusions and, thus, represents a good model in which to examine the direct effects of acute TRP-ML1 deficiency on membrane traffic. Ratiometric imaging revealed decreased lysosomal pH in TRP-ML1-deficient cells, suggesting a disruption in lysosomal function. Nevertheless, we found no effect of TRP-ML1 knockdown on the kinetics of protein or lipid delivery to lysosomes. In contrast, by comparing degradation kinetics of low density lipoprotein constituents, we confirmed a selective defect in cholesterol but not apolipoprotein B hydrolysis in MLIV fibroblasts. We hypothesize that the effects of TRP-ML1 loss on hydrolytic activity have a cumulative effect on lysosome function, resulting in a lag between TRP-ML1 loss and full manifestation of MLIV.

Published

2008

39. Molecular analysis of the GlcNac-1-phosphotransferase.

Author

Braulke T, Pohl S, and Storch S

Subjects

Animals, Disease Models, Animal, Genetic Predisposition to Disease, Humans, Mucolipidoses genetics, Mutation, Phenotype, Protein Conformation, Structure-Activity Relationship, Substrate Specificity, Transferases (Other Substituted Phosphate Groups) chemistry, Transferases (Other Substituted Phosphate Groups) genetics, Lysosomes enzymology, Mucolipidoses enzymology, Transferases (Other Substituted Phosphate Groups) deficiency

Abstract

Modification of the carbohydrate chains of soluble lysosomal enzymes with mannose 6-phosphate residues is a prerequisite for their mannose 6-phosphate receptor-dependent transport to lysosomes. GlcNac-1-phosphotransferase localized in the Golgi apparatus represents a hexameric alpha(2)beta(2)gamma(2) subunit complex and plays a key role in the formation of the mannose 6-phosphate recognition marker. Defects in the GlcNac-1-phosphotransferase complex cause two diseases, mucolipidosis type II and III, which are characterized by missorting and cellular loss of lysosomal enzymes, and lysosomal accumulation of storage material. The recent identification of two genes, GNPTAB and GNPTG, encoding the three subunits of GlcNac-1-phosphotransferase leads to an improvement of both pre- and postnatal diagnosis of affected individuals, and permits the analysis of structural requirements for efficient formation of mannose 6-phosphate residues on lysosomal enzymes. The alpha/beta subunits precursor matures by proteolytic cleavage and contains the catalytic activity as well as the capability to recognize lysosomal enzymes. The role of the gamma-subunits for activity, stability and oligomerization of the GlcNac-1-phosphotransferase subunits is still unclear.

Published

2008

40. Mucolipidosis II: a single causal mutation in the N-acetylglucosamine-1-phosphotransferase gene (GNPTAB) in a French Canadian founder population.

Author

Plante M, Claveau S, Lepage P, Lavoie EM, Brunet S, Roquis D, Morin C, Vézina H, and Laprise C

Subjects

Canada, Case-Control Studies, Consanguinity, DNA Mutational Analysis, Genealogy and Heraldry, Geography, Humans, Founder Effect, Mucolipidoses enzymology, Mucolipidoses genetics, Mutation genetics, Transferases (Other Substituted Phosphate Groups) genetics, White People genetics

Abstract

Mucolipidosis (ML) II (I-cell disease) is a lysosomal storage disorder caused by a deficiency of UDP-N-acetylglucosamine:lysosomal enzyme N-acetylglucosamine-1-phosphotransferase. MLII is an autosomal recessive disease with a carrier rate estimated at 1/39 in Saguenay-Lac-Saint-Jean (SLSJ) (Quebec, Canada), which is the highest frequency documented worldwide. To identify the causing mutation, we sequenced GNPTAB exons in 27 parents of 16 MLII-deceased children from the SLSJ region as obligatory and potential carriers. We also performed a genealogical reconstruction for each parent to evaluate consanguinity levels and genetic contribution of ancestors. Our goal was to identify which parameters could explain the high MLII frequency observed in the SLSJ population. A single mutation (c.3503_3504delTC) was found in all obligatory carriers. In addition, 11 apparent polymorphisms were identified. The mutation was not detected in genomic DNA of 50 unrelated controls. Genealogical data show six founders (three couples) with a higher probability of having introduced the mutation in the population. The frequency of the mutation was increased as a consequence of this founder effect and of the resulting population structure. We suggest that c.3503_3504delTC is the allele causing MLII in the SLSJ population, and its high carrier rate is most likely explained by a founder effect.

Published

2008

41. Cherry red spot in sialidosis (mucolipidosis type I).

Author

Heroman JW, Rychwalski P, and Barr CC

Subjects

Adolescent, Fibroblasts enzymology, Humans, Male, Mucolipidoses enzymology, Mucolipidoses urine, N-Acetylneuraminic Acid urine, Neuraminidase metabolism, Retinal Diseases enzymology, Retinal Diseases urine, Skin cytology, Macula Lutea pathology, Mucolipidoses diagnosis, Retinal Diseases diagnosis

Published

2008

42. An Alu insertion in compound heterozygosity with a microduplication in GNPTAB gene underlies Mucolipidosis II.

Author

Tappino B, Regis S, Corsolini F, and Filocamo M

Subjects

Base Sequence, Codon, Nonsense genetics, DNA Primers genetics, Exons, Heterozygote, Humans, Infant, Newborn, Male, Molecular Sequence Data, Phenotype, RNA, Messenger genetics, Reverse Transcriptase Polymerase Chain Reaction, Alu Elements, Mucolipidoses enzymology, Mucolipidoses genetics, Transferases (Other Substituted Phosphate Groups) deficiency, Transferases (Other Substituted Phosphate Groups) genetics

Abstract

Mucolipidosis type II (ML II) is a fatal, autosomal recessive, lysosomal storage disorder characterized by severe clinical and radiologic features. ML II results from mutations in alpha and beta subunits, encoded by the GlcNAc-1-phosphotransferase gene (GNPTAB). Most of the 40 different GNPTAB mutations reported so far are insertions and deletions predicting diverse types of aberrant proteins. Alu mobile elements have however never been involved in these events up to now. The Italian ML II patient of our study showed an Alu retrotrasposition in GNPTAB exon 5. The Alu insertion mutation (NM_024312.3:c.555_556insHSU14569) generated a transcript with a skipping of the target exon 5 and a frameshift p.S122fs, causing a premature translation termination codon at position 123. This insertion mutation was found in compound heterozygosity with the frameshift p.S887KfsX33, resulting from a new mono-nucleotide duplication (c.2659dupA) that occurred in GNPTAB exon 13. A possible involvement of cis-splicing elements having an exonic location, such as exon enhancers (ESEs), is discussed as mechanism that led to the production of the aberrant mRNA splicing.

Published

2008

43. Low and high affinity receptors mediate cellular uptake of heparanase.

Author

Ben-Zaken O, Shafat I, Gingis-Velitski S, Bangio H, Kelson IK, Alergand T, Amor Y, Maya RB, Vlodavsky I, and Ilan N

Subjects

Animals, Cell Line, Tumor, Cricetinae, Extracellular Matrix enzymology, Extracellular Matrix metabolism, Fibroblasts enzymology, Glucuronidase isolation & purification, Humans, Mucolipidoses enzymology, Mucolipidoses metabolism, Recombinant Proteins, Fibroblasts metabolism, Glucuronidase metabolism, Heparitin Sulfate metabolism, Mannosephosphates metabolism, Receptors, Cell Surface metabolism

Abstract

Heparanase is an endoglycosidase which cleaves heparan sulfate and hence participates in degradation and remodeling of the extracellular matrix. Importantly, heparanase activity correlated with the metastatic potential of tumor-derived cells, attributed to enhanced cell dissemination as a consequence of heparan sulfate cleavage and remodeling of the extracellular matrix barrier. Heparanase has been characterized as a glycoprotein, yet glycan biochemical analysis was not performed to date. Here, we applied the Qproteometrade mark GlycoArray kit to perform glycan analysis of heparanase, and compared the kit results with the more commonly used biochemical analyses. We employed fibroblasts isolated from patients with I-cell disease (mucolipidosis II), fibroblasts deficient of low density lipoprotein receptor-related protein and fibroblasts lacking mannose 6-phosphate receptor, to explore the role of mannose 6-phosphate in heparanase uptake. Iodinated heparanase has been utilized to calculate binding affinity. We provide evidence for hierarchy of binding to cellular receptors as a function of heparanase concentration. We report the existence of a high affinity, low abundant (i.e., low density lipoprotein receptor-related protein, mannose 6-phosphate receptor), as well as a low affinity, high abundant (i.e., heparan sulfate proteoglycan) receptors that mediate heparanase binding, and suggest that these receptors co-operate to establish high affinity binding sites for heparanase, thus maintaining extracellular retention of the enzyme tightly regulated.

Published

2008

44. Mice lacking alpha/beta subunits of GlcNAc-1-phosphotransferase exhibit growth retardation, retinal degeneration, and secretory cell lesions.

Author

Gelfman CM, Vogel P, Issa TM, Turner CA, Lee WS, Kornfeld S, and Rice DS

Subjects

Animals, Cathepsin D metabolism, Disease Models, Animal, Electroretinography, Genotype, Glycoside Hydrolases blood, Growth Disorders blood, Growth Disorders physiopathology, In Situ Hybridization, In Situ Nick-End Labeling, Mice, Mice, Inbred C57BL, Mice, Knockout, Mucolipidoses blood, Mucolipidoses physiopathology, Photography, Retina physiopathology, Retinal Degeneration blood, Retinal Degeneration physiopathology, Reverse Transcriptase Polymerase Chain Reaction, Exocrine Glands pathology, Growth Disorders enzymology, Mucolipidoses enzymology, Retinal Degeneration enzymology, Transferases (Other Substituted Phosphate Groups) physiology

Abstract

Purpose: Mucolipidosis II and III (ML II; ML III) are lysosomal storage diseases characterized by a deficiency in GlcNAc-1-phosphotransferase. Patients with ML III have retinal disease, but in cases of the more clinically severe ML II, human ophthalmic studies are limited. In this study, retinal function and overall disease were assessed in mice lacking GNPTAB, the gene mutated in patients with ML II., Methods: Mice deficient in GNPTAB were generated from Omnibank, a sequence-tagged gene-trap library of >270,000 mouse embryonic stem cell clones as part of a large-scale effort to knock out, phenotypically screen, and thereby validate pharmaceutically tractable genes for drug development. Routine diagnostics, expression analysis, histopathology, and ERG analyses were performed on mice lacking GNPTAB. In addition, measurements of serum lysosomal enzymes were performed., Results: Severe retinal degeneration was observed in mice deficient in GNPTAB. Heterozygous mice were phenotypically normal and in situ hybridization showed expression across the neural retina. Compared to wild-type mice, the GNPTAB homozygous mice were smaller, had elevated levels of serum lysosomal enzymes, exhibited cartilage defects, and had cytoplasmic alterations in secretory cells of several exocrine glands., Conclusions: Mice deficient in GNPTAB exhibited severe retinal degeneration. Additional features observed in patients with ML II, a lysosomal storage disease, are also present in these mice. Understanding underlying mechanisms of this gene in the eye will increase its therapeutic potential for the treatment of retinal diseases.

Published

2007

45. Abnormal expressions of the subunits of the UDP-N-acetylglucosamine: lysosomal enzyme, N-acetylglucosamine-1-phosphotransferase, result in the formation of cytoplasmic vacuoles resembling those of the I-cells.

Author

Ho CY, Tang NL, Yeung AK, Lau AK, Hui J, and Lo AW

Subjects

Cell Culture Techniques, Cell Line, Humans, Mucolipidoses enzymology, Transferases (Other Substituted Phosphate Groups) genetics, Vacuoles, Gene Expression Regulation, Enzymologic physiology, Lysosomes enzymology, Transferases (Other Substituted Phosphate Groups) metabolism

Abstract

Defects in the multimeric enzyme, UDP-N-acetylglucosamine:lysosomal enzyme N-acetylglucosamine-1-phosphotransferase (GNPT), result in the diseases of mucolipidosis (ML). This enzyme generates the mannose 6-phosphate residues on newly synthesized lysosomal enzymes for the efficient receptor-mediated transport to lysosomes. The enzyme contains alpha/beta and gamma subunits. Mutations in the alpha/beta subunit result in the classical ML II and IIIA, while defects in the gamma subunit results in the clinically milder ML IIIC. I-cells, a distinct histological feature characterized by the presence of abnormal cytoplasmic vacuoles, are detected in many cell types, most noticeably, in ML II patients. In this study, we investigated the interactions of the alpha/beta and gamma subunits in the pathogenesis of I-cells. We noted low and deranged alpha/beta subunit expressions in human mucolipidosis cell lines. Unexpectedly, high gamma subunit expressions were also observed. In normal mouse fibroblasts, when alpha/beta subunit was suppressed, abnormal cytoplasmic vacuoles were induced, and up-regulation of the gamma subunit was also observed. On the other hand, suppressing the gamma subunit resulted in biphasic responses of the alpha/beta subunit, while abnormal cytoplasmic vacuoles were not formed, regardless of the expression levels of the alpha/beta subunit. Our data suggest reciprocal feedback mechanisms between alpha/beta and the gamma subunits. A fine balance of the expressions of these subunits may play an important role in the formation of I-cells in this group of lysosomal storage disorders.

Published

2007

46. Short femurs detected at 25 and 31 weeks of gestation diagnosed as Leroy I-cell disease in the postnatal period: a report of two cases.

Author

Yuksel A, Kayserili H, and Gungor F

Subjects

Adult, Consanguinity, Diagnosis, Differential, Female, Femur diagnostic imaging, Genes, Recessive, Gestational Age, Hexosaminidases blood, Humans, Infant, Newborn, Male, Mucolipidoses diagnostic imaging, Mucolipidoses enzymology, Mucolipidoses genetics, Pregnancy, Ultrasonography, Prenatal, alpha-Mannosidase blood, beta-N-Acetylhexosaminidases blood, Femur abnormalities, Mucolipidoses diagnosis

Abstract

Leroy I-cell disease is a rare autosomal recessive lysosomal storage disorder characterized by marked psychomotor and growth retardation, skeletal anomalies, and typical facial features. There is a biochemical defect in uridine diphospho-N-acetylglucosamine-1-phosphotransferase, which is the enzyme responsible for addition of a mannose phosphate residue for lysosomal trafficking. Prenatal diagnosis is possible by analysis of enzyme activity in chorionic villi or cultured amniocytes, but this is offered to families only known to be at increased risk. We describe two cases that had bilateral shortness of the femurs at 25 and 31 weeks of gestation in the ultrasound scan and were diagnosed as Leroy I-cell disease by plasma enzyme analysis in the postnatal period. There was also bowing of the femurs in one case. None of the two families had a history of Leroy I-cell disease. The parents of one case were second-degree cousins. In view of these two cases that are presented, we propose that Leroy I-cell disease should be included in the differential diagnosis of short femurs even when there is no evident family history., ((c) 2007 S. Karger AG, Basel.)

Published

2007

47. Mucolipidosis II (I-cell disease) and mucolipidosis IIIA (classical pseudo-hurler polydystrophy) are caused by mutations in the GlcNAc-phosphotransferase alpha / beta -subunits precursor gene.

Author

Kudo M, Brem MS, and Canfield WM

Subjects

Adolescent, Adult, Alternative Splicing genetics, Amino Acid Sequence, Child, Child, Preschool, Exons genetics, Female, Fibroblasts enzymology, Humans, Infant, Infant, Newborn, Male, Middle Aged, Molecular Sequence Data, Mucolipidoses enzymology, Mutation, Pedigree, Transferases (Other Substituted Phosphate Groups) metabolism, Gene Frequency, Mucolipidoses genetics, Transferases (Other Substituted Phosphate Groups) genetics

Abstract

Mucolipidosis II (MLII; I-cell disease) and mucolipidosis IIIA (MLIIIA; classical pseudo-Hurler polydystrophy) are diseases in which the activity of the uridine diphosphate (UDP)-N-acetylglucosamine:lysosomal enzyme N-acetylglucosamine-1-phosphotransferase (GlcNAc-phosphotransferase) is absent or reduced, respectively. In the absence of mannose phosphorylation, trafficking of lysosomal hydrolases to the lysosome is impaired. In these diseases, mistargeted lysosomal hydrolases are secreted into the blood, resulting in lysosomal deficiency of many hydrolases and a storage-disease phenotype. To determine whether these diseases are caused by mutations in the GlcNAc-phosphotransferase alpha / beta -subunits precursor gene (GNPTAB), we sequenced GNPTAB exons and flanking intronic sequences and measured GlcNAc-phosphotransferase activity in patient fibroblasts. We identified 15 different mutations in GNPTAB from 18 pedigrees with MLII or MLIIIA and demonstrated that these two diseases are allelic. Mutations in both alleles were identified in each case, which demonstrated that GNPTAB mutations are the cause of both diseases. Some pedigrees had identical mutations. One frameshift mutation (truncation at amino acid 1171) predominated and was found in both MLII and MLIIIA. This mutation was found in combination with severe mutations (i.e., mutations preventing the generation of active enzyme) in MLII and with mild mutations (i.e., mutations allowing the generation of active enzyme) in MLIIIA. Some cases of MLII and MLIIIA were the result of mutations that cause aberrant splicing. Substitutions were inside the invariant splice-site sequence in MLII and were outside it in MLIIIA. When the mutations were analyzed along with GlcNAc-phosphotransferase activity, it was possible to confidently distinguish these two clinically related but distinct diseases. We propose criteria for distinguishing these two disorders by a combination of mutation detection and GlcNAc-phosphotransferase activity determination.

Published

2006

48. Serum hyaluronidase aberrations in metabolic and morphogenetic disorders.

Author

Fiszer-Szafarz B, Czartoryska B, and Tylki-Szymanska A

Subjects

Acetylglucosaminidase blood, Acetylglucosaminidase genetics, Achondroplasia enzymology, Adolescent, Child, Child, Preschool, Dysostoses enzymology, Female, Glucuronidase blood, Glucuronidase genetics, Humans, Hyaluronoglucosaminidase deficiency, Hypophosphatemia, Familial enzymology, Male, Mucolipidoses enzymology, Bone Diseases, Metabolic enzymology, Hyaluronoglucosaminidase blood, Hyaluronoglucosaminidase genetics, Mucopolysaccharidoses enzymology

Abstract

Hyaluronidases are endo-glycosidases that degrade both hyaluronan (hyaluronic acid) (HA) and chondroitin sulfates. Deficiency of hyaluronidase activity has been predicted to result in a phenotype similar to that observed in mucopolysaccharidosis (MPS). In the present study, we surveyed a variety of patients with phenotypes similar to those observed in MPS, but without significant mucopolysacchariduria to determine if some are based on aberrations in serum hyaluronidase (Hyal-1) activity. The study included patients with well-characterized dysmorphic disorders occurring on genetic basis, as well as those of unkown etiology. The purpose of the study was to establish how wide spread were abnormalities in levels of circulating Hyal-1 activity. A simple and sensitive semi-quantitative zymographic procedure was used for the determination of activity. Levels of both beta-N-acetylglucosaminidase and beta-glucuronidase whose activities contribute to the total breakdown of hyaluronan (HA) were also measured, as well as the concentration of circulating HA. Among 48 patients with bone or connective tissue abnormalities, low levels of Hyal-1 activity were found in six patients compared to levels in 100 healthy donors (2.0-3.2 units/microL vs 6(+/- 1 SE) units/microL). These six patients exhibited a wide spectrum of clinical abnormalities, in particular shortened extremities: they included three patients with unknown causes of clinical symptoms, one patient with Sanfilippo disease, one of the seven patients with achondroplasia, and one with hypophosphotemic rickets. Normal levels of serum Hyal-1 activities were found in patients with Morquio disease, GM1 gangliosidosis, I cell-disease, 6 of the 7 patients with achondroplasia, Marfan's-syndrome and Ehlers-Danlos syndrome. No patient totally lacked serum Hyal-1 activity. Serum HA concentration was elevated in patients with Sanfilippo A and I-cell disease. Determination of serum and leukocyte Hyal-1 and serum HA may be useful to evaluate patients with metabolic and morphogenetic disorders.

Published

2005

49. Mucolipidosis II is caused by mutations in GNPTA encoding the alpha/beta GlcNAc-1-phosphotransferase.

Author

Tiede S, Storch S, Lübke T, Henrissat B, Bargal R, Raas-Rothschild A, and Braulke T

Subjects

Amino Acid Sequence, Fibroblasts, Humans, Molecular Sequence Data, Mucolipidoses enzymology, Sequence Homology, Amino Acid, Transferases (Other Substituted Phosphate Groups) genetics, Mucolipidoses genetics, Mutation genetics, Transferases (Other Substituted Phosphate Groups) biosynthesis

Abstract

Mucolipidosis II (ML II) is a fatal lysosomal storage disorder resulting from defects in the multimeric GlcNAc-1-phosphotransferase responsible for the initial step in the generation of the mannose 6-phosphate (M6P) recognition marker. M6P residues on oligosaccharides of newly synthesized lysosomal enzymes are essential for efficient receptor-mediated transport to lysosomes. We used the recombinant GlcNAc-1-phosphotransferase gamma subunit as an affinity matrix to purify an unknown protein identified as the product of GNPTA (encoding GNPTA, previously known as MGC4170). The cDNA encodes a protein of 1,256 amino acids with two putative transmembrane domains and a complex preserved modular structure comprising at least six domains. The N-terminal domain of GNPTA, interrupted by a long insertion, shows similarities to bacterial capsule biosynthesis proteins. We identified seven mutations in GNPTA that lead to premature translational termination in six individuals with ML II. Retroviral transduction of fibroblasts from an individual with ML II resulted in the expression and localization of GNPTA in the Golgi apparatus, accompanied by the correction of hypersecretion of lysosomal enzymes. Our results provide evidence that GNPTA encodes a subunit of GlcNAc-1-phosphotransferase defective in individuals with ML II.

Published

2005

50. Missense mutations in N-acetylglucosamine-1-phosphotransferase alpha/beta subunit gene in a patient with mucolipidosis III and a mild clinical phenotype.

Author

Tiede S, Muschol N, Reutter G, Cantz M, Ullrich K, and Braulke T

Subjects

Adolescent, Cells, Cultured, Contracture pathology, DNA Mutational Analysis, Fibroblasts cytology, Fibroblasts enzymology, Fingers abnormalities, Humans, Joint Diseases pathology, Lysosomes enzymology, Male, Microscopy, Fluorescence, Mucolipidoses enzymology, Mucolipidoses genetics, Phenotype, Protein Subunits genetics, RNA, Messenger genetics, RNA, Messenger metabolism, Mucolipidoses pathology, Mutation, Missense, Transferases (Other Substituted Phosphate Groups) genetics

Abstract

Mucolipidosis type III (ML III, pseudo-Hurler polydystrophy), an autosomal recessive inherited disorder of lysosomal enzyme targeting is due to a defective N-acetylglucosamine 1-phosphotransferase (phosphotransferase) activity and leads to the impaired formation of mannose 6-phosphate markers in soluble lysosomal enzymes followed by their increased excretion into the serum. Mutations in the phosphotransferase gamma subunit gene (GNPTAG) have been reported to be responsible for ML III. Here we report on a 14-year-old adolescent with a mild clinical phenotype of ML III. He presented with progressive joint stiffness and swelling. Urinary oligosaccharide and mucopolysaccharide excretion was normal. Lysosomal enzyme activities were significantly elevated in the serum and decreased in cultured fibroblasts. Impaired trafficking of the lysosomal protease cathepsin D (CtsD) was confirmed by metabolic labeling of the patient's fibroblasts. Neither mutations in the GNPTAG gene nor alterations in the GNPTAG mRNA level were detected whereas the steady state concentration of the 97 kDa GNPTAG dimer was reduced. Most importantly, the patient is homozygous for a pathogenic nucleotide substitution and a polymorphism in the phosphotransferase alpha/beta subunit gene (GNPTA). The data indicate that defects in genes other than GNPTAG can be linked to ML III contributing to the variability of the phenotype., ((c) 2005 Wiley-Liss, Inc.)

Published

2005