Your search keyword '"Kazunari, Monma"' showing total 7 results

1. Novel pathogenic

Author

Yoshiaki, Nishida, Masayuki, Nakamura, Yuka, Urata, Kei, Kasamo, Hanae, Hiwatashi, Izumi, Yokoyama, Masahiro, Mizobuchi, Kotaro, Sakurai, Yasushi, Osaki, Yukari, Morita, Masako, Watanabe, Kenji, Yoshida, Kiyomi, Yamane, Natsuki, Miyakoshi, Ryouichi, Okiyama, Takehiro, Ueda, Noritaka, Wakasugi, Yuji, Saitoh, Takashi, Sakamoto, Yuji, Takahashi, Ken, Shibano, Hideki, Tokuoka, Atsushi, Hara, Kazunari, Monma, Katsuhisa, Ogata, Keita, Kakuda, Hideki, Mochizuki, Takeo, Arai, Manabu, Araki, Takeshi, Fujii, Kazuto, Tsukita, Haruhi, Sakamaki-Tsukita, and Akira, Sano

Subjects

Article

Abstract

Objective To identify mutations in vacuolar protein sorting 13A (VPS13A) for Japanese patients with suspected chorea-acanthocytosis (ChAc). Methods We performed a comprehensive mutation screen, including sequencing and copy number variation (CNV) analysis of the VPS13A gene, and chorein Western blotting of erythrocyte ghosts. As the results of the analysis, 17 patients were molecularly diagnosed with ChAc. In addition, we investigated the distribution of VPS13A gene mutations and clinical symptoms in a total of 39 molecularly diagnosed Japanese patients with ChAc, including 22 previously reported cases. Results We identified 11 novel pathogenic mutations, including 1 novel CNV. Excluding 5 patients with the unknown symptoms, 97.1% of patients displayed various neuropsychiatric symptoms or forms of cognitive dysfunction during the course of disease. The patients carrying the 2 major mutations representing over half of the mutations, exon 60–61 deletion and exon 37 c.4411C>T (R1471X), were localized in western Japan. Conclusions We identified 13 different mutations in VPS13A, including 11 novel mutations, and verified the clinical manifestations in 39 Japanese patients with ChAc.

Published

2018

2. Novel pathogenic VPS13A gene mutations in Japanese patients with chorea-acanthocytosis

Author

Masako Watanabe, Kenji Yoshida, Kazuto Tsukita, Noritaka Wakasugi, Hideki Mochizuki, Ryouichi Okiyama, Yasushi Osaki, Atsushi Hara, Kiyomi Yamane, Katsuhisa Ogata, Kotaro Sakurai, Kei Kasamo, Yuka Urata, Kazunari Monma, Ken Shibano, Yukari Morita, Takehiro Ueda, Yuji Saitoh, Hanae Hiwatashi, Manabu Araki, Yuji Takahashi, Natsuki Miyakoshi, Masahiro Mizobuchi, Keita Kakuda, Akira Sano, Masayuki Nakamura, Haruhi Sakamaki-Tsukita, Takashi Sakamoto, Takeo Arai, Yoshiaki Nishida, Izumi Yokoyama, Takeshi Fujii, and Hideki Tokuoka

Subjects

0301 basic medicine, Vacuolar protein sorting, Genetics, Mutation, business.industry, Gene mutation, medicine.disease_cause, medicine.disease, Blot, 03 medical and health sciences, Exon, 030104 developmental biology, 0302 clinical medicine, Medicine, Neurology (clinical), Copy-number variation, business, Gene, 030217 neurology & neurosurgery, Genetics (clinical), Chorea acanthocytosis

Abstract

ObjectiveTo identify mutations in vacuolar protein sorting 13A (VPS13A) for Japanese patients with suspected chorea-acanthocytosis (ChAc).MethodsWe performed a comprehensive mutation screen, including sequencing and copy number variation (CNV) analysis of the VPS13A gene, and chorein Western blotting of erythrocyte ghosts. As the results of the analysis, 17 patients were molecularly diagnosed with ChAc. In addition, we investigated the distribution of VPS13A gene mutations and clinical symptoms in a total of 39 molecularly diagnosed Japanese patients with ChAc, including 22 previously reported cases.ResultsWe identified 11 novel pathogenic mutations, including 1 novel CNV. Excluding 5 patients with the unknown symptoms, 97.1% of patients displayed various neuropsychiatric symptoms or forms of cognitive dysfunction during the course of disease. The patients carrying the 2 major mutations representing over half of the mutations, exon 60–61 deletion and exon 37 c.4411C>T (R1471X), were localized in western Japan.ConclusionsWe identified 13 different mutations in VPS13A, including 11 novel mutations, and verified the clinical manifestations in 39 Japanese patients with ChAc.

Published

2019

3. Mutation profile of the GNE gene in Japanese patients with distal myopathy with rimmed vacuoles (GNE myopathy)

Author

Anna Cho, Ikuya Nonaka, Yukiko K. Hayashi, Satoru Noguchi, Ichizo Nishino, Kazunari Monma, and Yasushi Oya

Subjects

Adult, Male, Genotype, DNA Mutational Analysis, Nonsense mutation, Biology, Compound heterozygosity, medicine.disease_cause, Young Adult, Japan, medicine, Humans, Missense mutation, Age of Onset, Muscle, Skeletal, Myopathy, Allele frequency, Alleles, Retrospective Studies, Genetics, Mutation, Hereditary inclusion body myopathy, DNA, Middle Aged, medicine.disease, DNA Fingerprinting, Distal Myopathies, Psychiatry and Mental health, Phenotype, Female, Surgery, Neurology (clinical), medicine.symptom, Carbohydrate Epimerases

Abstract

Background GNE myopathy (also called distal myopathy with rimmed vacuoles or hereditary inclusion body myopathy) is an autosomal recessive myopathy characterised by skeletal muscle atrophy and weakness that preferentially involve the distal muscles. It is caused by mutations in the gene encoding a key enzyme in sialic acid biosynthesis, UDP- N -acetylglucosamine 2-epimerase/ N -acetylmannosamine kinase (GNE). Methods We analysed the GNE gene in 212 Japanese GNE myopathy patients. A retrospective medical record review was carried out to explore genotype–phenotype correlation. Results Sixty-three different mutations including 25 novel mutations were identified: 50 missense mutations, 2 nonsense mutations, 1 insertion, 4 deletions, 5 intronic mutations and 1 single exon deletion. The most frequent mutation in the Japanese population is c.1714G>C (p.Val572Leu), which accounts for 48.3% of total alleles. Homozygosity for this mutation results in more severe phenotypes with earlier onset and faster progression of the disease. In contrast, the second most common mutation, c.527A>T (p.Asp176Val), seems to be a mild mutation as the onset of the disease is much later in the compound heterozygotes with this mutation and c.1714G>C than the patients homozygous for c.1714G>C. Although the allele frequency is 22.4%, there are only three homozygotes for c.527A>T, raising a possibility that a significant number of c.527A>T homozygotes may not develop an apparent disease. Conclusions Here, we report the mutation profile of the GNE gene in 212 Japanese GNE myopathy patients, which is the largest single-ethnic cohort for this ultra-orphan disease. We confirmed the clinical difference between mutation groups. However, we should note that the statistical summary cannot predict clinical course of every patient.

Published

2013

4. Heterozygous UDP-GlcNAc 2-epimerase and N-acetylmannosamine kinase domain mutations in the GNE gene result in a less severe GNE myopathy phenotype compared to homozygous N-acetylmannosamine kinase domain mutations

Author

Masahiro Sonoo, Miho Murata, Yasushi Oya, Jun Shimizu, Madoka Mori-Yoshimura, Naoki Suzuki, Kazuma Sugie, Masashi Aoki, Keiko Tanaka, Ichizo Nishino, Yukiko K. Hayashi, May Christine V. Malicdan, Satoru Noguchi, Toshihide Kumamoto, Harumasa Nakamura, Hiroyuki Tomimitsu, Satoshi Nakano, and Kazunari Monma

Subjects

Adult, Male, Heterozygote, medicine.medical_specialty, Adolescent, Biology, medicine.disease_cause, Compound heterozygosity, Severity of Illness Index, Young Adult, Multienzyme Complexes, Internal medicine, Genotype, medicine, Humans, Myopathy, Aged, Genetics, Mutation, Hereditary inclusion body myopathy, Kinase, Homozygote, Heterozygote advantage, Middle Aged, medicine.disease, Phenotype, Protein Structure, Tertiary, Phosphotransferases (Alcohol Group Acceptor), Endocrinology, Neurology, Female, Neurology (clinical), medicine.symptom, Carbohydrate Epimerases

Abstract

Background Glucosamine (UDP-N-acetyl)-2-epimerase/ N -acetylmannosamine kinase (GNE) myopathy, also called distal myopathy with rimmed vacuoles (DMRV) or hereditary inclusion body myopathy (HIBM), is a rare, progressive autosomal recessive disorder caused by mutations in the GNE gene. Here, we examined the relationship between genotype and clinical phenotype in participants with GNE myopathy. Methods Participants with GNE myopathy were asked to complete a questionnaire regarding medical history and current symptoms. Results A total of 71 participants with genetically confirmed GNE myopathy (27 males and 44 females; mean age, 43.1±13.0 (mean±SD) years) completed the questionnaire. Initial symptoms ( e.g. , foot drop and lower limb weakness) appeared at a mean age of 24.8±8.3years. Among the 71 participants, 11 (15.5%) had the ability to walk, with a median time to loss of ambulation of 17.0±2.1years after disease onset. Participants with a homozygous mutation (p.V572L) in the N -acetylmannosamine kinase domain (KD/KD participants) had an earlier disease onset compared to compound heterozygous participants with mutations in the uridine diphosphate-N-acetylglucosamine (UDP-GlcNAc) 2-epimerase and N -acetylmannosamine kinase domains (ED/KD participants; 26.3±7.3 vs. 21.2±11.1years, respectively). KD/KD participants were more frequently non-ambulatory compared to ED/KD participants at the time of survey (80% vs. 50%). Data were verified using medical records available from 17 outpatient participants. Conclusions Homozygous KD/KD participants exhibited a more severe phenotype compared to heterozygous ED/KD participants.

Published

2012

5. Acid phosphatase-positive globular inclusions is a good diagnostic marker for two patients with adult-onset Pompe disease lacking disease specific pathology

Author

Hideo Sugie, Yasushi Oya, Tokiko Fukuda, Ichizo Nishino, Kazunari Monma, Rie Tsuburaya, Ikuya Nonaka, Yukiko K. Hayashi, and T. Nakayama

Subjects

Disease specific, Adult, Genetic Markers, Male, Pathology, medicine.medical_specialty, Acid Phosphatase, DNA Mutational Analysis, Disease, Biology, Vacuolated fibers, Muscle pathology, medicine, Humans, Muscular dystrophy, Age of Onset, Muscle, Skeletal, Genetics (clinical), Inclusion Bodies, Glycogen Storage Disease Type II, Acid phosphatase, Skeletal muscle, Diagnostic marker, alpha-Glucosidases, Middle Aged, medicine.disease, medicine.anatomical_structure, Neurology, Pediatrics, Perinatology and Child Health, Mutation, biology.protein, Female, Neurology (clinical)

Abstract

Diagnosis of adult-onset Pompe disease is sometimes challenging because of its clinical similarities to muscular dystrophy and the paucity of disease-specific vacuolated fibers in the skeletal muscle pathology. We describe two patients with adult-onset Pompe disease whose muscle pathology showed no typical vacuolated fibers but did show unique globular inclusions with acid phosphatase activity. The acid phosphatase-positive globular inclusions may be a useful diagnostic marker for adult-onset Pompe disease even when typical vacuolated fibers are absent.

Published

2011

6. G.P.11.08 Cytoplasmic body with acid phosphatase activity – Hallmark of adult-onset Pompe disease on muscle pathology

Author

Satoru Noguchi, Ikuya Nonaka, Ichizo Nishino, Kazunari Monma, Yuichi Hayashi, and Yasushi Oya

Subjects

Pathology, medicine.medical_specialty, Cytoplasmic body, biology, business.industry, Acid phosphatase, Disease, Muscle pathology, Neurology, Pediatrics, Perinatology and Child Health, medicine, biology.protein, Neurology (clinical), business, Genetics (clinical)

Published

2008

7. Mutation profile of the GNE gene in Japanese patients with distal myopathy with rimmed vacuoles (GNE myopathy).

Author

Anna Cho, Hayashi, Yukiko K., Kazunari Monma, Yasushi Oya, Satoru Noguchi, Ikuya Nonaka, and Ichizo Nishino

Subjects

MUSCLE diseases, HUMAN genes, GENETIC mutation, JAPANESE people, SKELETAL muscle, DISEASE progression, GENETICS, DISEASES

Abstract

Background: GNE myopathy (also called distal myopathy with rimmed vacuoles or hereditary inclusion body myopathy) is an autosomal recessive myopathy characterised by skeletal muscle atrophy and weakness that preferentially involve the distal muscles. It is caused by mutations in the gene encoding a key enzyme in sialic acid biosynthesis, UDP-N-acetylglucosamine 2-epimerase/Nacetylmannosamine kinase (GNE). Methods: We analysed the GNE gene in 212 Japanese GNE myopathy patients. A retrospective medical record review was carried out to explore genotype-phenotype correlation. Results: Sixty-three different mutations including 25 novel mutations were identified: 50 missense mutations, 2 nonsense mutations, 1 insertion, 4 deletions, 5 intronic mutations and 1 single exon deletion. The most frequent mutation in the Japanese population is c.1714G>C (p. Val572Leu), which accounts for 48.3% of total alleles. Homozygosity for this mutation results in more severe phenotypes with earlier onset and faster progression of the disease. In contrast, the second most common mutation, c.527A>T (p.Asp176Val), seems to be a mild mutation as the onset of the disease is much later in the compound heterozygotes with this mutation and c.1714G>C than the patients homozygous for c.1714G>C. Although the allele frequency is 22.4%, there are only three homozygotes for c.527A>T, raising a possibility that a significant number of c.527A>T homozygotes may not develop an apparent disease. Conclusions: Here, we report the mutation profile of the GNE gene in 212 Japanese GNE myopathy patients, which is the largest single-ethnic cohort for this ultra-orphan disease. We confirmed the clinical difference between mutation groups. However, we should note that the statistical summary cannot predict clinical course of every patient. [ABSTRACT FROM AUTHOR]

Published

2014