Your search keyword '"Shimozawa, Nobuyuki"' showing total 12 results

1. Ataxic form of autosomal recessive PEX10-related peroxisome biogenesis disorders with a novel compound heterozygous gene mutation and characteristic clinical phenotype.

Author

Yamashita T, Mitsui J, Shimozawa N, Takashima S, Umemura H, Sato K, Takemoto M, Hishikawa N, Ohta Y, Matsukawa T, Ishiura H, Yoshimura J, Doi K, Morishita S, Tsuji S, and Abe K

Subjects

Adult, Cerebellar Ataxia complications, Cerebellar Ataxia diagnostic imaging, DNA Mutational Analysis, Female, Humans, Magnetic Resonance Imaging, Male, Peroxins, Peroxisomal Disorders complications, Peroxisomal Disorders diagnostic imaging, Phenotype, Cerebellar Ataxia genetics, Family Health, Mutation genetics, Peroxisomal Disorders genetics, Receptors, Cytoplasmic and Nuclear genetics

Abstract

Peroxisome biogenesis factor 10 (PEX10) is involved in the import of peroxisomal matrix proteins, and the mutation of this gene causes 3 subtypes of peroxisome biogenesis disorders, namely Zellweger syndrome (severe), neonatal adrenoleukodystrophy (moderate) and an ataxic form (mild). Here, we report 3 siblings of the ataxic form with cerebellar ataxia, mild mental retardation, and 3 additional characteristic features: mydriasis, hyperreflexia and involuntary head movement. All 3 siblings are compound heterozygous for a previously reported mutation, c.2T>C (p.M1T), and a novel mutation, c.920G>A, causing a missense change (p.C307Y) located in the RING finger domain of PEX10. The present cases suggest that these PEX10 mutations involve not only cerebellar but also more multiple nervous systems including pupillary autonomic, pyramidal and extrapyramidal systems., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

2. First Japanese case of Zellweger syndrome with a mutation in PEX14.

Author

Komatsuzaki S, Ogawa E, Shimozawa N, Sakamoto O, Haginoya K, Uematsu M, Hasegawa Y, Matsubara Y, and Ohura T

Subjects

DNA Mutational Analysis, Fatal Outcome, Humans, Infant, Newborn, Japan, Male, Membrane Proteins metabolism, Repressor Proteins metabolism, Zellweger Syndrome metabolism, DNA genetics, Membrane Proteins genetics, Mutation, Repressor Proteins genetics, Zellweger Syndrome genetics

Abstract

Zellweger syndrome, one of the peroxisome biogenesis disorders, is an autosomal recessive disease caused by mutations in PEX genes. It is characterized by severe hypotonia, failure to thrive, psychomotor retardation, liver dysfunction, and sensorineural hearing impairment. Most of the patients with this disease die before the age of 1 year. PEX14 is the 13th PEX gene responsible for peroxisome biogenesis disorders. Thus far, only two patients with PEX14 deficiency have been reported. Here, we report the first case of a Japanese patient with a PEX14 mutation who showed severe hypotonia, psychomotor retardation, demyelination, and developed rickets at the age of 5 months. An increased excretion of 3,6-epoxydicarboxylic acids leads to the diagnosis of Zellweger syndrome and a mutation analysis of PEX14 revealed a homozygous mutation of c.538C>T (p.Q180X). The patient survived for a prolonged period of time but died of liver failure at the age of 46 months., (© 2015 Japan Pediatric Society.)

Published

2015

3. Evaluation of SLC20A2 mutations that cause idiopathic basal ganglia calcification in Japan.

Author

Yamada M, Tanaka M, Takagi M, Kobayashi S, Taguchi Y, Takashima S, Tanaka K, Touge T, Hatsuta H, Murayama S, Hayashi Y, Kaneko M, Ishiura H, Mitsui J, Atsuta N, Sobue G, Shimozawa N, Inuzuka T, Tsuji S, and Hozumi I

Subjects

Adult, Aged, DNA Mutational Analysis methods, Female, Genetic Linkage genetics, Humans, Japan, Male, Middle Aged, Pedigree, Young Adult, Basal Ganglia Diseases genetics, Brain pathology, Calcinosis genetics, Genetic Predisposition to Disease, Mutation genetics, Neurodegenerative Diseases genetics, Sodium-Phosphate Cotransporter Proteins, Type III genetics

Abstract

Objective: To investigate the clinical, genetic, and neuroradiologic presentations of idiopathic basal ganglia calcification (IBGC) in a nationwide study in Japan., Methods: We documented clinical and neuroimaging data of a total of 69 subjects including 23 subjects from 10 families and 46 subjects in sporadic cases of IBGC in Japan. Mutational analysis of SLC20A2 was performed., Results: Six new mutations in SLC20A2 were found in patients with IBGC: 4 missense mutations, 1 nonsense mutation, and 1 frameshift mutation. Four of them were familial cases and 2 were sporadic cases in our survey. The frequency of families with mutations in SLC20A2 in Japan was 50%, which was as high as in a previous report on other regions. The clinical features varied widely among the patients with SLC20A2 mutations. However, 2 distinct families have the same mutation of S637R in SLC20A2 and they have similar characteristics in the clinical course, symptoms, neurologic findings, and neuroimaging. In our study, all the patients with SLC20A2 mutations showed calcification. In familial cases, there were symptomatic and asymptomatic patients in the same family., Conclusion: SLC20A2 mutations are a major cause of familial IBGC in Japan. The members in the families with the same mutation had similar patterns of calcification in the brain and the affected members showed similar clinical manifestations.

Published

2014

4. Diagnostic utility of whole exome sequencing in patients showing cerebellar and/or vermis atrophy in childhood.

Author

Ohba C, Osaka H, Iai M, Yamashita S, Suzuki Y, Aida N, Shimozawa N, Takamura A, Doi H, Tomita-Katsumoto A, Nishiyama K, Tsurusaki Y, Nakashima M, Miyake N, Eto Y, Tanaka F, Matsumoto N, and Saitsu H

Subjects

Adolescent, Atrophy diagnosis, Atrophy genetics, Child, Child, Preschool, DNA Mutational Analysis, Exome, Humans, Male, Tripeptidyl-Peptidase 1, Young Adult, Cerebellum pathology, Mutation

Abstract

Cerebellar and/or vermis atrophy is recognized in various types of childhood disorders with clinical and genetic heterogeneity. Although careful evaluation of clinical features and neuroimaging can lead to correct diagnosis of disorders, their diagnosis is sometimes difficult because clinical features can overlap with each other. In this study, we performed family-based whole exome sequencing of 23 families including 25 patients with cerebellar and/or vermis atrophy in childhood, who were unable to be diagnosed solely by clinical examination. Pathological mutations of seven genes were found in ten patients from nine families (9/23, 39.1 %): compound heterozygous mutations in FOLR1, C5orf42, POLG, TPP1, PEX16, and de novo mutations in CACNA1A, and ITPR1. Patient 1A with FOLR1 mutations showed extremely low concentration of 5-methyltetrahydrofolate in the cerebrospinal fluid and serum, and Patient 6 with TPP1 mutations demonstrated markedly lowered tripeptidyl peptidase 1 activity in leukocytes. Furthermore, Patient 8 with PEX16 mutations presented a mild increase of very long chain fatty acids in the serum as supportive data for genetic diagnosis. The main clinical features of these ten patients were nonspecific and mixed, and included developmental delay, intellectual disability, ataxia, hypotonia, and epilepsy. Brain MRI revealed both cerebellar and vermis atrophy in eight patients (8/10, 80 %), vermis atrophy/hypoplasia in two patients (2/10, 20 %), and brainstem atrophy in one patient (1/10, 10 %). Our data clearly demonstrate the utility of whole exome sequencing for genetic diagnosis of childhood cerebellar and/or vermis atrophy.

Published

2013

5. Newly identified milder phenotype of peroxisome biogenesis disorder caused by mutated PEX3 gene.

Author

Matsui S, Funahashi M, Honda A, and Shimozawa N

Subjects

Adult, Brain pathology, Catalase metabolism, Fibroblasts metabolism, Genetic Predisposition to Disease genetics, Homozygote, Humans, Male, Peroxins, Peroxisomal Disorders diagnosis, Peroxisomal Disorders metabolism, Phenotype, Catalase genetics, Lipoproteins genetics, Membrane Proteins genetics, Mutation genetics, Peroxisomal Disorders genetics

Abstract

We identified the first patient with infantile Refsum disease (IRD), a milder phenotype of peroxisome biogenesis disorder (PBD) caused by a mutated PEX3, and investigated the clinical, molecular and cellular characterization in this patient. The patient presented psychomotor regression, late-onset leukodystrophy, peripheral neuropathy, hearing impairment, a renal cyst, and renal hypertension and survived until the age of 36. Furthermore, fibroblasts from the patient indicated a mosaic pattern of catalase-positive particles (peroxisomes) and numerous peroxisomal membrane structures. Molecular analysis was homozygous for the D347Y mutation and reduced gene expression of PEX3 which encodes a peroxisomal membrane protein, pex3p, involved in peroxisome assembly at the early stage of peroxisomal membrane vesicle formation, therefore, patients with a mutated PEX3 gene have been reported to have only a severe phenotype of Zellweger syndrome and no or less peroxisomal remnant membrane structure. This is not only a newly identified milder PBD caused by a mutated PEX3 gene but also the first report of a Japanese patient with IRD who had not been diagnosed until over 30years of age, which suggests there must be more variant PBD in patients with degenerative neurologic disorder, and to bring them to light is necessary., (Copyright © 2012 The Japanese Society of Child Neurology. Published by Elsevier B.V. All rights reserved.)

Published

2013

6. Molecular mechanism of a temperature-sensitive phenotype in peroxisomal biogenesis disorder.

Author

Hashimoto K, Kato Z, Nagase T, Shimozawa N, Kuwata K, Omoya K, Li A, Matsukuma E, Yamamoto Y, Ohnishi H, Tochio H, Shirakawa M, Suzuki Y, Wanders RJ, and Kondo N

Subjects

Amino Acid Motifs, Amino Acid Sequence, Circular Dichroism, Fibroblasts metabolism, Genotype, Homozygote, Humans, Infant, Isoleucine chemistry, Male, Microscopy, Fluorescence, Models, Molecular, Molecular Sequence Data, Peptides chemistry, Phenotype, Protein Conformation, Protein Folding, Protein Structure, Secondary, Protein Structure, Tertiary, Recombinant Proteins chemistry, Temperature, Tryptophan chemistry, src Homology Domains, Membrane Proteins chemistry, Mutation, Peroxisomal Disorders diagnosis, Peroxisomal Disorders genetics

Abstract

Peroxisomal biogenesis disorders include Zellweger syndrome and milder phenotypes, such as neonatal adrenoleukodystrophy (NALD). Our previous study of a NALD patient with a marked deterioration by a fever revealed a mutation (Ile326Thr) within a SH3 domain of PEX13 protein (Pex13p), showing a temperature-sensitive (TS) phenotype in peroxisomal biogenesis. Clinical TS phenotypes also have been reported in several genetic diseases, but the molecular mechanisms still remain to be clarified. The immunofluorescent staining with anti-Pex13p antibody also revealed TS phenotype of the I326T mutant protein itself in the patient cells. Protease digestion of the recombinant Pex13p-SH3 domain showed an increase of protease susceptibility, suggesting a problem of mutant protein fold. Conformational analyses against urea denaturation using urea gradient gel electrophoresis or fluorescence emission from tryptophan residue revealed that the mutant protein should be easily unfolded. Far-UV circular dichroism (CD) spectra demonstrated that both wild-type and the mutant protein have antiparallel beta-sheets as their secondary structure with slightly different extent. The thermal unfolding profiles measured by CD showed a marked lower melting temperature for I326T protein compared with that of wild-type protein. Analysis of the protein 3D-structure indicated that the Ile326 should be a core residue for folding kinetics and the substitution of Ile326 by threonine should directly alter the kinetic equilibrium, suggesting a marked increase of the unfolded molecules when the patient had a high fever. Structural analyses of the protein in the other genetic diseases could provide an avenue for better understanding of genotype-phenotype correlations.

Published

2005

7. Mutational and structural analysis of Japanese patients with mucopolysaccharidosis type II.

Author

Kato T, Kato Z, Kuratsubo I, Tanaka N, Ishigami T, Kajihara JI, Sukegawa-Hayasaka K, Orii K, Isogai K, Fukao T, Shimozawa N, Orii T, Kondo N, and Suzuki Y

Subjects

Adolescent, Adult, Alternative Splicing, Amino Acid Sequence, Base Sequence, Binding Sites, Child, Child, Preschool, Codon, Nonsense, Frameshift Mutation, Humans, Iduronate Sulfatase chemistry, Japan, Models, Molecular, Mutation, Missense, Protein Structure, Tertiary, Sequence Deletion, DNA Mutational Analysis, Iduronate Sulfatase genetics, Mucopolysaccharidosis II genetics, Mutation

Abstract

We investigated mutations of the iduronate-2-sulfatase (I2S) gene and structural characteristics of I2S to clarify genotype/phenotype relationships in 18 Japanese patients with mucopolysaccharidosis type II. The I2S gene was analyzed in five patients with a severe phenotype and in 13 patients with an attenuated phenotype. The tertiary structural model of the human I2S was constructed by homology modeling using the arylsulfatase structure as a template. We identified four missense mutations and a nonsense mutation in the severe phenotype; four missense, two nonsense, three frame shifts, and one each of splice and amino acid deletion in the attenuated phenotype. Seven of them (L73del, Q75X, G140R, C171R, V401 fs, C422 fs, and H441 fs) were novel mutations. Structural analysis indicated that the residues of the mutations found in the severe phenotype would have direct interactions with the active site residues or should break the hydrophobic core domain of I2S, whereas residues of the missense mutations found in the attenuated phenotype were located in the peripheral region. In addition, effects by deletion or frameshift mutations could also be interpreted by the structure. Structural analysis of mutant proteins would help in understanding the genotype/phenotype relationships of Hunter disease.

Published

2005

8. Identification of a new complementation group of the peroxisome biogenesis disorders and PEX14 as the mutated gene.

Author

Shimozawa N, Tsukamoto T, Nagase T, Takemoto Y, Koyama N, Suzuki Y, Komori M, Osumi T, Jeannette G, Wanders RJ, and Kondo N

Subjects

Animals, Cells, Cultured, Fibroblasts, Genetic Complementation Test, Humans, Infant, Newborn, Peroxisomal Targeting Signal 2 Receptor, Peroxisome-Targeting Signal 1 Receptor, Rats, Receptors, Cytoplasmic and Nuclear metabolism, Zellweger Syndrome genetics, Mutation, Peroxisomal Disorders genetics

Abstract

Peroxisome biogenesis disorders (PBD) are lethal hereditary diseases caused by abnormalities in the biogenesis of peroxisomes. At present, 12 different complementation groups have been identified and to date, all genes responsible for each of these complementation groups have been identified. The peroxisomal membrane protein PEX14 is a key component of the peroxisomal import machinery and may be the initial docking site for the two import receptors PEX5 and PEX7. Although PEX14 mutants have been identified in yeasts and CHO-cells, human PEX14 deficiency has apparently not been documented. We now report the identification of a new complementation group of the peroxisome biogenesis disorders with PEX14 as the defective gene. Indeed, human PEX14 rescues the import of a PTS1-dependent as well as a PTS2-dependent protein into the peroxisomes in fibroblasts from a patient with Zellweger syndrome belonging to the new complementation group. This patient was homozygous for a nonsense mutation in a putative coiled-coil region of PEX14, c.553C>T (p.Q185X). Furthermore, we showed that the patient's fibroblasts lacked PEX14 as determined by immunocytochemical analysis. These findings indicate that there are 13 genotypes in PBD and that the role of PEX14 is also essential in humans., (Copyright 2004 Wiley-Liss, Inc.)

Published

2004

9. Mutations in novel peroxin gene PEX26 that cause peroxisome-biogenesis disorders of complementation group 8 provide a genotype-phenotype correlation.

Author

Matsumoto N, Tamura S, Furuki S, Miyata N, Moser A, Shimozawa N, Moser HW, Suzuki Y, Kondo N, and Fujiki Y

Subjects

Amino Acid Sequence, Animals, CHO Cells, Catalase metabolism, Cell Line, Cricetinae, DNA genetics, DNA Mutational Analysis, Female, Gene Expression, Genetic Complementation Test, Genotype, Humans, Membrane Proteins deficiency, Mice, Molecular Sequence Data, Peroxisomal Disorders classification, Peroxisomal Disorders metabolism, Peroxisome-Targeting Signal 1 Receptor, Phenotype, Pregnancy, RNA, Messenger genetics, RNA, Messenger metabolism, Receptors, Cytoplasmic and Nuclear metabolism, Sequence Homology, Amino Acid, Temperature, Tissue Distribution, Transfection, Zellweger Syndrome genetics, Zellweger Syndrome metabolism, Membrane Proteins genetics, Mutation, Peroxisomal Disorders genetics

Abstract

The human disorders of peroxisome biogenesis (PBDs) are subdivided into 12 complementation groups (CGs). CG8 is one of the more common of these and is associated with varying phenotypes, ranging from the most severe, Zellweger syndrome (ZS), to the milder neonatal adrenoleukodystrophy (NALD) and infantile Refsum disease (IRD). PEX26, encoding the 305-amino-acid membrane peroxin, has been shown to be deficient in CG8. We studied the PEX26 genotype in fibroblasts of eight CG8 patients--four with the ZS phenotype, two with NALD, and two with IRD. Catalase was mostly cytosolic in all these cell lines, but import of the proteins that contained PTS1, the SKL peroxisome targeting sequence, was normal. Expression of PEX26 reestablished peroxisomes in all eight cell lines, confirming that PEX26 defects are pathogenic in CG8 patients. When cells were cultured at 30 degrees C, catalase import was restored in the cell lines from patients with the NALD and IRD phenotypes, but to a much lesser extent in those with the ZS phenotype, indicating that temperature sensitivity varied inversely with the severity of the clinical phenotype. Several types of mutations were identified, including homozygous G89R mutations in two patients with ZS. Expression of these PEX26 mutations in pex26 Chinese hamster ovary cells resulted in cell phenotypes similar to those in the human cell lines. These findings confirm that the degree of temperature sensitivity in pex26 cell lines is predictive of the clinical phenotype in patients with PEX26 deficiency.

Published

2003

10. Genetic heterogeneity of peroxisome biogenesis disorders among Japanese patients: evidence for a founder haplotype for the most common PEX10 gene mutation.

Author

Shimozawa N, Nagase T, Takemoto Y, Ohura T, Suzuki Y, and Kondo N

Subjects

ATPases Associated with Diverse Cellular Activities, Adenosine Triphosphatases genetics, Adrenoleukodystrophy genetics, Alleles, Chondrodysplasia Punctata genetics, DNA, Complementary metabolism, Female, Genotype, Homozygote, Humans, Japan, Male, Membrane Proteins genetics, Peroxins, Peroxisomal Biogenesis Factor 2, Peroxisomal Targeting Signal 2 Receptor, Phenotype, Polymorphism, Genetic, Zellweger Syndrome genetics, Founder Effect, Haplotypes, Mutation, Peroxisomal Disorders genetics, Peroxisomes metabolism, Receptors, Cytoplasmic and Nuclear genetics

Abstract

We, as the only diagnostic center for peroxisome biogenesis disorders (PBD) in Japan, identified a total of 31 Japanese patients with PBD during the last 20 years. They were 27 patients with Zellweger syndrome (ZS), including two sib cases, three with neonatal adrenoleukodystrophy (NALD) and one with rhizomelic type chondrodysplasia punctata (RCDP). No patient with infantile Refsum disease has been detected. These patients were genetically subdivided into complementation group A (five ZS and one NALD), B (11 ZS), C (four ZS), E (five ZS and two NALD), F (two ZS), and R (one RCDP). They were subjected to mutation analysis of PEX1, PEX2, PEX6, PEX7, and PEX10. All the 11 ZS patients with group-B PBD had a common mutation, i.e., a homozygous 2-base-pair deletion in PEX10. To determine whether this highly frequent mutation is due to a founder effect, we analyzed single nucleotide polymorphisms within PEX10 among patients and Japanese controls. The mutation apparently arose once on an ancestral chromosome in the Japanese population. Based on the value of 24 PBD patients identified during the last 10 years, we estimated the prevalence of PBD in Japan to be approximately one in 500,000 births., (Copyright 2003 Wiley-Liss, Inc.)

Published

2003

11. A novel aberrant splicing mutation of the PEX16 gene in two patients with Zellweger syndrome.

Author

Shimozawa N, Nagase T, Takemoto Y, Suzuki Y, Fujiki Y, Wanders RJ, and Kondo N

Subjects

Base Sequence, Catalase analysis, Catalase immunology, Cell Line, DNA Mutational Analysis, Fibroblasts ultrastructure, Fluorescent Antibody Technique, Humans, Membrane Proteins analysis, Membrane Proteins immunology, Transfection, Zellweger Syndrome pathology, ATP-Binding Cassette Transporters, Alternative Splicing, Fungal Proteins, Membrane Proteins genetics, Mutation, Zellweger Syndrome genetics

Abstract

Human Pex16p, a peroxisomal membrane protein composed of 336 amino acids, plays a central role in peroxisomal membrane biogenesis. A nonsense mutation (R176ter) in the PEX16 gene has been reported in the case of only one patient (D-01) belonging to complementation group D of the peroxisome biogenesis disorders. We have now identified two patients belonging to group D (D-02 and D-03) whose fibroblasts were found to contain no peroxisomal membrane structure ghosts. Molecular analysis of the PEX16 gene revealed aberrant cDNA species lacking 65 bp, corresponding to exon 10 skipping caused by a splice site mutation (IVS10 + 2T -->C). Both patients, although unrelated, were homozygous for this mutation. This mutation changes the amino acid sequence starting from codon 298 and introduces a termination codon at codon 336. As a consequence, the cell's ability to membrane synthesis and protein import is disrupted, which implies that the changed C terminus of the Pex16p in these patients likely affects its function., ((C)2002 Elsevier Science (USA).)

Published

2002

12. Molecular genetic study in Japanese patients with Alexander disease: a novel mutation, R79L

Author

Shiroma, Naohide, Kanazawa, Naomi, Kato, Zenichiro, Shimozawa, Nobuyuki, Imamura, Atsushi, Ito, Masayuki, Ohtani, Kyoich, Oka, Akira, Wakabayashi, Kazuyo, Iai, Mizue, Sugai, Kenji, Sasaki, Masayuki, Kaga, Makiko, Ohta, Takao, and Tsujino, Seiichi

Subjects

*NEUROGLIA, *GENETIC mutation

Abstract

Since the first report by Brenner et al. of mutations in the glial fibrillary acidic protein (GFAP) gene in patients with Alexander disease, several molecular genetic studies have been performed in different ethnic groups. We previously reported a Japanese patient with a mutation, R239C, which is identical to one commonly found in American patients. Here we have analyzed four additional Japanese patients by screening for known mutations or, if no known mutation was found, by sequencing of all exons of the GFAP gene. We detected three missense mutations; one was a novel mutation, R79L, and two were previously reported mutations, R239C and R79C. All of our patients were heterozygous for their mutations. Together with the novel mutation, R79L, four different nucleotide changes altering the R79 residue have been reported, implying that any alternation of this arginine residue can give the GFAP protein a dominant negative effect, leading to accumulation of GFAP as Rosenthal fibers. We conclude that molecular genetic analysis of the GFAP gene is feasible for antemortem diagnosis of Alexander disease in Japanese patients. [Copyright &y& Elsevier]

Published

2003