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3. Peripheral nerves are involved in hypomyelinating leukodystrophy-3 caused by a homozygous AIMP1 variant

Author

Shogo Ito, Minoru Kokubo, Daisuke Ieda, Kohei Aoyama, Ikumi Hori, Shinji Saitoh, Yuji Nakamura, Seimi Ebe, Kei Ohashi, and Ayako Hattori

Subjects
Cerebral atrophy, Pathology, medicine.medical_specialty, Microcephaly, medicine.diagnostic_test, business.industry, Neurodegeneration, Central nervous system, General Medicine, medicine.disease, 03 medical and health sciences, 0302 clinical medicine, Peripheral neuropathy, medicine.anatomical_structure, Developmental Neuroscience, Pediatrics, Perinatology and Child Health, Failure to thrive, Nerve conduction study, medicine, Neurology (clinical), Spasticity, medicine.symptom, business, 030217 neurology & neurosurgery
Abstract

Introduction Aminoacyl-tRNA synthetase-interacting multifunctional protein 1 (AIMP1) is a non-catalytic component of the multi-tRNA synthetase complex that catalyzes the ligation of amino acids to their correct tRNAs. Bi-allelic truncating variants in the AIMP1 gene have been associated with hypomyelinating leukodystrophy-3 (HLD3; MIM 260600), which is characterized by hypomyelination, microcephaly, seizures and decreased life expectancy. Although peripheral nerve involvement has been assumed for HLD3, no compelling evidence is available to date. Case report The case was a first-born Filipino male. He showed profound developmental delay, failure to thrive, and spasticity in his limbs. At three months of age he developed refractory epilepsy. Serial magnetic resonance imaging (MRIs) showed profound myelination delay and progressive cerebral atrophy. He showed abnormal nerve conduction studies. Genetic testing revealed a homozygous pathogenic variant in the AIMP1 gene (NM_004757.3: c.115C > T: p.Gln39*). The parents were heterozygous for the same variant. Conclusion Here, we report a patient with a homozygous nonsense AIMP1 variant showing peripheral neuropathy as well as HLD3. Our case suggests that AIMP1 plays a pivotal role in the peripheral nerve as well as the central nervous system.

Published
2021
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5. Angelman syndrome with mosaic paternal uniparental disomy suggestive of mitotic nondisjunction

Author

Masanori Fujimoto, Yuji Nakamura, Toshihiko Iwaki, Emi Sato, Daisuke Ieda, Ayako Hattori, Anna Shiraki, Seiji Mizuno, and Shinji Saitoh

Subjects
Genetics, Genetics (clinical)
Abstract

Angelman syndrome (AS) is caused by the functional absence of the maternal ubiquitin-protein ligase E3A (UBE3A) gene. Approximately 5% of AS is caused by paternal uniparental disomy of chromosome 15 (UPD(15)pat), most of which is considered to result from monosomy rescue. However, little attention has focused on how UPD(15)pat occurs. We suggest the mitotic nondisjunction mechanism as a cause of UPD(15)pat in a six-year-old patient presenting with distinctive characteristics in line with AS. DNA methylation screening of 15q11-q13 showed a paternal band and a faint maternal band, suggestive of mosaic status. By trio-based microsatellite analysis, we confirmed a large proportion of UPD(15)pat cells and a small proportion of cells of biparental origin. Single nucleotide polymorphism (SNP) microarray revealed isodisomy of the entire chromosome 15. These results suggest that the UPD(15)pat of the patient resulted from mitotic nondisjunction, which may also be the cause of other cases of AS with UPD(15)pat.

Published
2022

6. CTCFdeletion syndrome: clinical features and epigenetic delineation

Author

Shinji Saitoh, Ikumi Hori, Keiko Wakui, Rie Kawamura, Junko Tomikawa, Kenji Kurosawa, Ken Higashimoto, Kei Ohashi, Yutaka Negishi, Kazuhiko Nakabayashi, Kenichiro Hata, Daisuke Ieda, Hidetaka Watanabe, Yoshitsugu Sugio, Ayako Hattori, and Hidenobu Soejima

Subjects
0301 basic medicine, Genetics, Candidate gene, Microdeletion syndrome, Biology, Phenotype, X-inactivation, 03 medical and health sciences, 030104 developmental biology, CTCF, DNA methylation, Epigenetics, Haploinsufficiency, Genetics (clinical)
Abstract

Background Heterozygous mutations in CTCF have been reported in patients with distinct clinical features including intellectual disability. However, the precise pathomechanism underlying the phenotype remains to be uncovered, partly because of the diverse function of CTCF. Here we describe extensive clinical and genetic investigation for two patients with a microdeletion encompassing CTCF . Methods We performed genetic examination including comprehensive investigation of X chromosome inactivation and DNA methylation profiling at imprinted loci and genome-wide. Results Two patients showed comparable clinical features to those in a previous report, indicating that haploinsufficiency of CTCF was the major determinant of the microdeletion syndrome. Despite the haploinsufficiency of CTCF, X chromosome inactivation was normal. DNA methylation at imprinted loci was normal, but hypermethylation at CTCF binding sites was demonstrated, of which PRKCZ and FGFR2 were identified as candidate genes. Conclusions This study confirms that haploinsufficiency of CTCF causes distinct clinical features, and that a microdeletion encompassing CTCF could cause a recognisable CTCF deletion syndrome. Perturbed DNA methylation at CTCF binding sites, not at imprinted loci, may underlie the pathomechanism of the syndrome.

Published
2017
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7. Schaaf-Yang syndrome shows a Prader-Willi syndrome-like phenotype during infancy

Author

Takanori Yamagata, Keisuke Nagasaki, Yutaka Negishi, Hirofumi Komaki, Shinji Saitoh, Jun Tohyama, Yasuyuki Nozaki, Ikumi Hori, Hiroko Tada, and Daisuke Ieda

Subjects
Male, Pediatrics, medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, Neurological deterioration, lcsh:Medicine, MAGEL2, symbols.namesake, Genomic Imprinting, SCHAAF-YANG SYNDROME, Medicine, Humans, Pharmacology (medical), Genetics (clinical), Retrospective Studies, Sanger sequencing, Arthrogryposis, business.industry, Research, lcsh:R, Proteins, General Medicine, Phenotype, Human genetics, Neonatal hypotonia, Schaaf-Yang syndrome, symbols, Female, medicine.symptom, Complication, business, Genomic imprinting, Prader-Willi Syndrome
Abstract

BackgroundSchaaf-Yang syndrome (SYS) is a newly recognized imprinting related syndrome, which is caused by a truncating variant in maternally imprintedMAGEL2located in 15q11-q13.Yet, precise pathomechanism remains to be solved. We sequencedMAGEL2in patients suspected Prader-Willi syndrome (PWS) to delineate clinical presentation of SYS. We examined 105 patients with clinically suspected PWS but without a specific PWS genetic alteration. Sanger sequencing of the entireMAGEL2gene and methylation-specific restriction enzyme treatment to detect the parent of origin were performed. Clinical presentation was retrospectively assessed in detail.ResultsTruncating variants inMAGEL2were detected in six patients (5.7%), including a pair of siblings. All truncating variants in affected patients were on the paternally derived chromosome, while the healthy father of the affected siblings inherited the variant from his mother. Patients withMAGEL2variants shared several features with PWS, such as neonatal hypotonia, poor suck, and obesity; however, there were also unique features, including arthrogryposis and a failure to acquire meaningful words. Additionally, an episode of neurological deterioration following febrile illness was confirmed in four of the six patients, which caused severe neurological sequalae.ConclusionsSYS can be present in infants suspected with PWS but some unique features, such as arthrogryposis, can help discriminate between the two syndromes. An episode of neurological deterioration following febrile illness should be recognized as an important complication.

Published
2019

8. Molecular genetic analysis of 30 families with Joubert syndrome

Author

Kenji Ichinomiya, Yoshihiko Shitara, Yasunari Sakai, Aya Inaba, Nobuhiko Okamoto, Kazuyori Yagyu, Naomichi Matsumoto, Kiyoko Sameshima, Adila Al-Kindy, Satoru Takeda, Yumi Habata, Masataka Hisano, Kunimasa Yan, Noriko Miyake, Toshifumi Suzuki, Masato Hiyane, Yasuko Kobayashi, Shuichi Ito, Hideaki Shiraishi, Mai Sato, Kazuhiro Haginoya, Seiji Mizuno, Noboru Fueki, Konomi Shimoda, Yuki Ueda, Kazuhiro Muramatsu, Yumiko Komatsu, Shigemi Kimura, Yu Tsuyusaki, Daisuke Ieda, Hiroshi Suzumura, Hirotomo Saitsu, Yoshinori Tsurusaki, Mitsuko Nakashima, Midori Nakajima, Shinji Saitoh, Kenji Kurosawa, and Chikage Yoshizawa

Subjects
Male, 0301 basic medicine, Oman, BBS1, TMEM67, Cell Cycle Proteins, Biology, Retina, Joubert syndrome, Genetic Heterogeneity, 03 medical and health sciences, Japan, Antigens, Neoplasm, Cerebellum, Genetics, medicine, Humans, Abnormalities, Multiple, Genetic Predisposition to Disease, Eye Abnormalities, Allele, Alleles, Genetics (clinical), Adaptor Proteins, Signal Transducing, Membrane Proteins, Aplasia, Kidney Diseases, Cystic, medicine.disease, Hypoplasia, Neoplasm Proteins, Pedigree, Cytoskeletal Proteins, 030104 developmental biology, RPGRIP1L, Mutation, Cerebellar vermis, Female, Microtubule-Associated Proteins
Abstract

Joubert syndrome (JS) is rare recessive disorders characterized by the combination of hypoplasia/aplasia of the cerebellar vermis, thickened and elongated superior cerebellar peduncles, and a deep interpeduncular fossa which is defined by neuroimaging and is termed the 'molar tooth sign'. JS is genetically highly heterogeneous, with at least 29 disease genes being involved. To further understand the genetic causes of JS, we performed whole-exome sequencing in 24 newly recruited JS families. Together with six previously reported families, we identified causative mutations in 25 out of 30 (24 + 6) families (83.3%). We identified eight mutated genes in 27 (21 + 6) Japanese families, TMEM67 (7/27, 25.9%) and CEP290 (6/27, 22.2%) were the most commonly mutated. Interestingly, 9 of 12 CEP290 disease alleles were c.6012-12T>A (75.0%), an allele that has not been reported in non-Japanese populations. Therefore c.6012-12T>A is a common allele in the Japanese population. Importantly, one Japanese and one Omani families carried compound biallelic mutations in two distinct genes (TMEM67/RPGRIP1L and TMEM138/BBS1, respectively). BBS1 is the causative gene in Bardet-Biedl syndrome. These concomitant mutations led to severe and/or complex clinical features in the patients, suggesting combined effects of different mutant genes.

Published
2016
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9. A novel missense mutation in the HECT domain of NEDD4L identified in a girl with periventricular nodular heterotopia, polymicrogyria and cleft palate

Author

Yonehiro Kanemura, Mitsuhiro Kato, Ikumi Hori, Mami Yamasaki, Shinji Saitoh, Yutaka Negishi, Fuyuki Miya, Kenjiro Kosaki, Nobuhiko Okamoto, Tatsuhiko Tsunoda, Ayako Hattori, Koji Kato, Kei Ohashi, and Daisuke Ieda

Subjects
0301 basic medicine, HECT domain, medicine.medical_specialty, Nedd4 Ubiquitin Protein Ligases, DNA Mutational Analysis, Mutation, Missense, Biology, medicine.disease_cause, 03 medical and health sciences, 0302 clinical medicine, Periventricular Nodular Heterotopia, Protein Domains, Molecular genetics, Genetics, medicine, Polymicrogyria, Humans, Missense mutation, FLNA, Syndactyly, Global developmental delay, Genetic Association Studies, Genetics (clinical), Mutation, Brain, medicine.disease, Magnetic Resonance Imaging, Cleft Palate, 030104 developmental biology, Child, Preschool, Cancer research, Female, 030217 neurology & neurosurgery
Abstract

We identified a novel de novo heterozygous missense mutation in the NEDD4L gene (NM_015277: c.2617G>A; p.Glu873Lys) through whole-exome sequencing in a 3-year-old girl showing severe global developmental delay, infantile spasms, cleft palate, periventricular nodular heterotopia and polymicrogyria. Mutations in the HECT domain of NEDD4L have been reported in patients with a neurodevelopmental disorder along with similar brain malformations. All patients reported with NEDD4L HECT domain mutations showed periventricular nodular heterotopia, and most had seizures, cortex anomalies, cleft palate and syndactyly. The unique constellation of clinical features in patients with NEDD4L mutations might help clinically distinguish them from patients with other genetic mutations including FLNA, which is a well-known causative gene of periventricular nodular heterotopia. Although mutations in the HECT domain of NEDD4L that lead to AKT-mTOR pathway deregulation in forced expression system were reported, our western blot analysis did not show an increased level of AKT-mTOR activity in lymphoblastoid cell lines (LCLs) derived from the patient. In contrast to the forced overexpression system, AKT-mTOR pathway deregulation in LCLs derived from our patient seems to be subtle.

Published
2017
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10. Two mouse models carrying truncating mutations in Magel2 show distinct phenotypes

Author

Daisuke Ieda, Tomomi Miyamoto, Makoto Nakanishi, Yutaka Negishi, Kohji Kato, Shinya Ugawa, Hisashi Oishi, Natsuko Kumamoto, Shinji Saitoh, Ichiro Miyoshi, and Yoshikazu Johmura

Subjects
Male, 0301 basic medicine, Embryology, 0302 clinical medicine, Neurodevelopmental disorder, Gene Editing, Genetics, Mammalian Genomics, Multidisciplinary, Genetically Modified Organisms, Brain, Animal Models, Genomics, Phenotype, Pedigree, Experimental Organism Systems, Hyperexpression Techniques, Engineering and Technology, Medicine, Epigenetics, Female, Prader-Willi syndrome, Genetic Engineering, Research Article, Biotechnology, Genetically modified mouse, Science, Transgene, Mouse Models, Bioengineering, Mice, Transgenic, Biology, Research and Analysis Methods, Frameshift mutation, Genomic Imprinting, 03 medical and health sciences, Model Organisms, Antigens, Neoplasm, Gene Expression and Vector Techniques, medicine, Animals, Humans, Clinical genetics, RNA, Messenger, Allele, Molecular Biology Techniques, Molecular Biology, Alleles, Medicine and health sciences, Molecular Biology Assays and Analysis Techniques, Genetically Modified Animals, Embryos, Body Weight, Wild type, Biology and Life Sciences, Proteins, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, HEK293 Cells, 030104 developmental biology, Gene Expression Regulation, Animal Genomics, Disorders of imprinting, Genetic Loci, Mutation, Animal Studies, Genomic imprinting, 030217 neurology & neurosurgery, Developmental Biology
Abstract

Schaaf-Yang syndrome (SYS) is a neurodevelopmental disorder caused by truncating variants in the paternal allele of MAGEL2, located in the Prader-Willi critical region, 15q11-q13. Although the phenotypes of SYS overlap those of Prader-Willi syndrome (PWS), including neonatal hypotonia, feeding problems, and developmental delay/intellectual disability, SYS patients show autism spectrum disorder and joint contractures, which are atypical phenotypes for PWS. Therefore, we hypothesized that the truncated Magel2 protein could potentially produce gain-of-function toxic effects. To test the hypothesis, we generated two engineered mouse models; one, an overexpression model that expressed the N-terminal region of Magel2 that was FLAG tagged with a strong ubiquitous promoter, and another, a genome-edited model that carried a truncating variant in Magel2 generated using the CRISPR/Cas9 system. In the overexpression model, all transgenic mice died in the fetal or neonatal period indicating embryonic or neonatal lethality of the transgene. Therefore, overexpression of the truncated Magel2 could show toxic effects. In the genome-edited model, we generated a mouse model carrying a frameshift variant (c.1690_1924del; p(Glu564Serfs*130)) in Magel2. Model mice carrying the frameshift variant in the paternal or maternal allele of Magel2 were termed Magel2P:fs and Magel2M:fs, respectively. The imprinted expression and spatial distribution of truncating Magel2 transcripts in the brain were maintained. Although neonatal Magel2P:fs mice were lighter than wildtype littermates, Magel2P:fs males and females weighed the same as their wildtype littermates by eight and four weeks of age, respectively. Collectively, the overexpression mouse model may recapitulate fetal or neonatal death, which are the severest phenotypes for SYS. In contrast, the genome-edited mouse model maintains genomic imprinting and distribution of truncated Magel2 transcripts in the brain, but only partially recapitulates SYS phenotypes. Therefore, our results imply that simple gain-of-function toxic effects may not explain the patho-mechanism of SYS, but rather suggest a range of effects due to Magel2 variants as in human SYS patients.

Published
2020
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11. Author Correction: A missense mutation in the HECT domain of NEDD4L identified in a girl with periventricular nodular heterotopia, polymicrogyria, and cleft palate

Author

Mitsuhiro Kato, Koji Kato, Daisuke Ieda, Kei Ohashi, Ikumi Hori, Yonehiro Kanemura, Yutaka Negishi, Nobuhiko Okamoto, Shinji Saitoh, Kenjiro Kosaki, Mami Yamasaki, Ayako Hattori, Tatsuhiko Tsunoda, and Fuyuki Miya

Subjects
NEDD4L, HECT domain, Pathology, medicine.medical_specialty, media_common.quotation_subject, Periventricular Nodular Heterotopia, Biology, medicine.disease, Human genetics, Genetics, Polymicrogyria, medicine, Missense mutation, Girl, Genetics (clinical), media_common
Published
2019
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12. Distinctive facies, macrocephaly, and developmental delay are signs of a PTEN mutation in childhood

Author

Shinobu Fukumura, Ikumi Hori, Seiji Mizuno, Yutaka Negishi, Ayako Hattori, Daisuke Ieda, Kei Ohashi, Mie Inaba, Shinji Saitoh, Kohji Kato, Naoko Kurahashi, and Koichi Maruyama

Subjects
0301 basic medicine, Oncology, Male, medicine.medical_specialty, Dolichocephaly, Developmental Disabilities, 03 medical and health sciences, Frontal Bossing, 0302 clinical medicine, Germline mutation, Developmental Neuroscience, Internal medicine, medicine, PTEN, Hamartoma, Humans, Child, biology, business.industry, Macrocephaly, PTEN Phosphohydrolase, Cancer, General Medicine, medicine.disease, Megalencephaly, 030104 developmental biology, Phenotype, Child, Preschool, Face, Pediatrics, Perinatology and Child Health, Mutation (genetic algorithm), Mutation, biology.protein, Female, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery
Abstract

Background Germline mutations of the PTEN gene are responsible for several PTEN hamartoma tumor syndromes. They are also implicated as a cause of macrocephaly and mild to severe developmental delay, regardless of the presence or absence of hamartomas in childhood. Nevertheless, because of limited information, the clinical features present during childhood in patients with a PTEN mutation are yet to be elucidated. Methods PTEN mutations were investigated by multiplex targeted sequencing of genomic DNA from 33 children with increased head circumference (>+2 SD) and developmental delay. The clinical features of all the patients with a PTEN mutation were abstracted by dysmorphologists. Results We have identified six children with a PTEN mutation. Clinical dissection of these six patients, in addition to patient reports in the literature, revealed distinctive facial features that included frontal bossing, dolichocephaly, horizontal eyebrows, and a depressed nasal bridge. Macrocephaly (+3.2 to +6.0 SD) was noticeable compared to their height (โˆ’0.8 to +2.1 SD), and the difference in the SD value of head circumference and height was more than 3 SD in all patients. Conclusion The presence of distinctive facies, extreme macrocephaly with normal to mildly high stature, and developmental delay may be useful for identifying patients with a PTEN mutation in childhood. Early identification of patients with a PTEN mutation would help uncover the natural course of tumor development in this group of individuals who have a possible predisposition to cancer, and be important for the development of an optimal surveillance strategy.

Published
2018

13. A novel truncating mutation in FLNA causes periventricular nodular heterotopia, Ehlers-Danlos-like collagenopathy and macrothrombocytopenia

Author

Katsumasa Kitamura, Ikumi Hori, Yutaka Negishi, Tomoki Kawai, Takenori Kato, Osamu Ohara, Ayako Hattori, Sachiko Inukai, Shinji Kunishima, Daisuke Ieda, Shinji Saitoh, Hironori Ohshita, Yuji Nakamura, and Tsutomu Shinohara

Subjects
0301 basic medicine, Pathology, medicine.medical_specialty, Filamins, 030105 genetics & heredity, Filamin, Diagnosis, Differential, 03 medical and health sciences, Epilepsy, Developmental Neuroscience, Periventricular Nodular Heterotopia, Ductus arteriosus, medicine, FLNA, Humans, Platelet, business.industry, General Medicine, medicine.disease, Phenotype, Thrombocytopenia, Xq28, 030104 developmental biology, medicine.anatomical_structure, Child, Preschool, Pediatrics, Perinatology and Child Health, Mutation, Ehlers-Danlos Syndrome, Female, Neurology (clinical), Ligation, business
Abstract

Introduction Filamin A (FLNA) is located in Xq28, and encodes the actin binding protein, filamin A. A mutation in FLNA is the most common cause of periventricular nodular heterotopia (PVNH), but a clear phenotype-genotype correlation has not been established. Indeed, some patients with a FLNA mutation have recently been shown to additionally have Ehlers-Danlos-like collagenopathy or macrothrombocytopenia. In an attempt to establish a clearer correlation between clinical symptoms and genotype, we have investigated a phenotype that involves thrombocytopenia in a patient with a truncation of the FLNA gene. Case report We present the case of a 4-year-old girl who, at birth, showed a ventral hernia. At 2 months of age, she was diagnosed with patent ductus arteriosus (PDA) and aortic valve regurgitation. At 11 months, she underwent ligation of the PDA. She was also diagnosed with diaphragmatic eventration by a preoperative test. At 19 months, motor developmental delay was noted, and brain MRI revealed bilateral PVNH with mega cisterna magna. Presently, there is no evidence of epilepsy, intellectual disability or motor developmental delay. She has chronic, mild thrombocytopenia, and a platelet count that transiently decreases after viral infection. Dilation of the ascending aorta is progressing gradually. Genetic testing revealed a de novo nonsense heterozygous mutation in FLNA (NM_001456.3: c.1621G > T; p.Glu541Ter). Immunofluorescence staining of a peripheral blood smear showed a lack of filamin A expression in 21.1% of her platelets. These filamin A-negative platelets were slightly larger than her normal platelets. Conclusion Our data suggests immunofluorescence staining of peripheral blood smears is a convenient diagnostic approach to identify patients with a FLNA mutation, which will facilitate further investigation of the correlation between FLNA mutations and patient phenotype.

Published
2017

14. A de novo p.Arg756Cys mutation in ATP1A3 causes a distinct phenotype with prolonged weakness and encephalopathy triggered by fever

Author

Yutaka Negishi, Naoki Ando, Mitsuko Nakashima, Naomichi Matsumoto, Ayako Hattori, Ikumi Hori, Daisuke Ieda, Yuji Nakamura, and Shinji Saitoh

Subjects
0301 basic medicine, Male, medicine.medical_specialty, Ataxia, Fever, Encephalopathy, DNA Mutational Analysis, Choreoathetosis, Arginine, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, Developmental Neuroscience, Internal medicine, Dysmetria, medicine, Humans, Cysteine, Genetics, Dystonia, Brain Diseases, Cerebellar ataxia, business.industry, Alternating hemiplegia of childhood, General Medicine, medicine.disease, Hypotonia, 030104 developmental biology, Phenotype, Child, Preschool, Pediatrics, Perinatology and Child Health, Mutation, Neurology (clinical), medicine.symptom, Sodium-Potassium-Exchanging ATPase, business, 030217 neurology & neurosurgery
Abstract

Patients with a mutation at Arg756 in ATP1A3 have been known to exhibit a distinct phenotype, characterized by prolonged weakness and encephalopathy, triggered by febrile illness. With only eight reports published to date, more evidence is required to correlate clinical features with a mutation at Arg756. Here we report an additional case with an Arg756Cys mutation in ATP1A3. A four-year-old boy showed mild developmental delay with recurrent paroxysmal episodes of weakness and encephalopathy from nine months of age. Motor deficits, which included bilateral hypotonia, ataxia, dysmetria, limb incoordination, dysarthria, choreoathetosis, and dystonia, were observed from one year and three months. Whole-exome sequencing detected a heterozygous de novo variant at c.2266C>T (p.Arg756Cys) in ATP1A3. The episodic course and clinical features of this case were consistent with previously reported cases with mutations at Arg756. Furthermore, his phenotype of marked ataxia was more similar to that of an Arg756Cys patient with relapsing encephalopathy and cerebellar ataxia syndrome, than to those with Arg756His and Arg756Leu mutations. This report therefore provides evidence of genotype-phenotype correlations in ATP1A3-related disorders as well as in patients with mutations at Arg756 in ATP1A3.

Published
2017

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