Your search keyword '"Tsurusaki Y"' showing total 298 results

151. Japanese familial case of myoclonus-dystonia syndrome with a splicing mutation in SGCE.

Author

Wada T, Takano K, Tsurusaki Y, Miyake N, Nakashima M, Saitsu H, Matsumoto N, and Osaka H

Subjects

Asian People, Child, Dystonic Disorders genetics, Humans, Male, Pedigree, Dystonic Disorders diagnosis, Mutation, Sarcoglycans genetics

Abstract

Myoclonus-dystonia syndrome (MDS) is a rare autosomal-dominant movement disorder characterized by brief, frequently alcohol-responsive myoclonic jerks that begin in childhood or early adolescence, caused by mutations in the ε-sarcoglycan gene (SGCE). The patient was a 6-year-old boy. At 2 years 8 months, he had abnormal movement when he ran due to dystonia of his left leg. At 3 years 5 months, he exhibited dystonia and myoclonic movement of his arms when eating. Myoclonus was likely to develop when he felt anxiety or exhaustion. Genomic DNA showed a heterozygous mutation in SGCE (c.109 + 1 G > T). His father and uncle with the same mutation also experienced milder dystonia or myoclonic movements. SGCE mutation can cause a broad range of clinical symptoms between and within families. We should consider MDS as a differential diagnosis for patients with paroxysmal walking abnormalities and/or myoclonic movements., (© 2015 Japan Pediatric Society.)

Published

2015

152. Mutations in the glutaminyl-tRNA synthetase gene cause early-onset epileptic encephalopathy.

Author

Kodera H, Osaka H, Iai M, Aida N, Yamashita A, Tsurusaki Y, Nakashima M, Miyake N, Saitsu H, and Matsumoto N

Subjects

Adolescent, Age of Onset, Brain Diseases diagnosis, Child, DNA Mutational Analysis, Electroencephalography, Epilepsy diagnosis, Exome genetics, Family Health, Humans, Magnetic Resonance Imaging, Male, Siblings, Amino Acyl-tRNA Synthetases genetics, Brain Diseases genetics, Epilepsy genetics, Mutation

Abstract

Aminoacylation is the process of attaching amino acids to their cognate tRNA, and thus is essential for the translation of mRNA into protein. This direct interaction of tRNA with amino acids is catalyzed by aminoacyl-tRNA synthetases. Using whole-exome sequencing, we identified compound heterozygous mutations [c.169T>C (p.Tyr57His) and c.1485dup (p.Lys496*)] in QARS, which encodes glutaminyl-tRNA synthetase, in two siblings with early-onset epileptic encephalopathy (EOEE). Recessive mutations in QARS, including the loss-of-function missense mutation p.Tyr57His, have been reported to cause intractable seizures with progressive microcephaly. The p.Lys496* mutation is novel and causes truncation of the QARS protein, leading to a deletion of part of the catalytic domain and the entire anticodon-binding domain. Transient expression of the p.Lys496* mutant in neuroblastoma 2A cells revealed diminished and aberrantly aggregated expression, indicating the loss-of-function nature of this mutant. Together with the previous report, our data suggest that abnormal aminoacylation is one of the underlying pathologies of EOEE.

Published

2015

153. The somatic GNAQ mutation c.548G>A (p.R183Q) is consistently found in Sturge-Weber syndrome.

Author

Nakashima M, Miyajima M, Sugano H, Iimura Y, Kato M, Tsurusaki Y, Miyake N, Saitsu H, Arai H, and Matsumoto N

Subjects

Age of Onset, Child, Child, Preschool, Female, GTP-Binding Protein alpha Subunits, Gq-G11, Genome, Human, High-Throughput Nucleotide Sequencing, Humans, Male, Mutation, Port-Wine Stain physiopathology, Sturge-Weber Syndrome physiopathology, GTP-Binding Protein alpha Subunits genetics, Port-Wine Stain genetics, Sturge-Weber Syndrome genetics

Abstract

Sturge-Weber syndrome (SWS) is a neurocutaneous disorder characterized by capillary malformation (port-wine stains), and choroidal and leptomeningeal vascular malformations. Previously, the recurrent somatic mutation c.548G>A (p.R183Q) in the G-α q gene (GNAQ) was identified as causative in SWS and non-syndromic port-wine stain patients using whole-genome sequencing. In this study, we investigated somatic mutations in GNAQ by next-generation sequencing. We first performed targeted amplicon sequencing of 15 blood-brain-paired samples in sporadic SWS and identified the recurrent somatic c.548G>A mutation in 80% of patients (12 of 15). The percentage of mutant alleles in brain tissues of these 12 patients ranged from 3.6 to 8.9%. We found no other somatic mutations in any of the seven GNAQ exons in the remaining three patients without c.548G>A. These findings suggest that the recurrent somatic GNAQ mutation c.548G>A is the major determinant genetic factor for SWS and imply that other mutated candidate gene(s) may exist in SWS.

Published

2014

154. Compound heterozygous BRAT1 mutations cause familial Ohtahara syndrome with hypertonia and microcephaly.

Author

Saitsu H, Yamashita S, Tanaka Y, Tsurusaki Y, Nakashima M, Miyake N, and Matsumoto N

Subjects

Epilepsy physiopathology, Female, Frameshift Mutation, Heterozygote, Humans, Infant, Infant, Newborn, Male, Microcephaly mortality, Microcephaly physiopathology, Muscle Hypertonia mortality, Muscle Hypertonia physiopathology, Siblings, Epilepsy genetics, Microcephaly genetics, Muscle Hypertonia genetics, Nuclear Proteins genetics

Abstract

Homozygous frameshift BRAT1 mutations were found in patients with lethal neonatal rigidity and multifocal seizure syndrome (MIM# 614498). Here, we report on two siblings with compound heterozygous mutations in BRAT1. They had intractable seizures from neonatal period, dysmorphic features and hypertonia. Progressive microcephaly was also observed. Initial electroencephalogram showed a suppression-burst pattern, leading to a diagnosis of Ohtahara syndrome. They both died from pneumonia at 1 year and 3 months, respectively. Whole-exome sequencing of one patient revealed a compound heterozygous BRAT1 mutations (c.176T>C (p.Leu59Pro) and c.962_963del (p.Leu321Profs*81)). We are unable to obtain DNA from another patient. The p.Leu59Pro mutation occurred at an evolutionarily conserved amino acid in a CIDE-N (N-terminal of an cell death-inducing DFF45-like effector) domain, which has a regulatory role in the DNA fragmentation pathway of apoptosis. Our results further support that mutations of BRAT1 could lead to epileptic encephalopathy.

Published

2014

155. Precise detection of chromosomal translocation or inversion breakpoints by whole-genome sequencing.

Author

Suzuki T, Tsurusaki Y, Nakashima M, Miyake N, Saitsu H, Takeda S, and Matsumoto N

Subjects

Chromosome Breakpoints, Chromosome Deletion, Chromosome Inversion genetics, Genome, Human, Humans, Genomics, High-Throughput Nucleotide Sequencing, Sequence Analysis, DNA, Translocation, Genetic genetics

Abstract

Structural variations (SVs), including translocations, inversions, deletions and duplications, are potentially associated with Mendelian diseases and contiguous gene syndromes. Determination of SV-related breakpoints at the nucleotide level is important to reveal the genetic causes for diseases. Whole-genome sequencing (WGS) by next-generation sequencers is expected to determine structural abnormalities more directly and efficiently than conventional methods. In this study, 14 SVs (9 balanced translocations, 1 inversion and 4 microdeletions) in 9 patients were analyzed by WGS with a shallow (5 × ) to moderate read coverage (20 × ). Among 28 breakpoints (as each SV has two breakpoints), 19 SV breakpoints had been determined previously at the nucleotide level by any other methods and 9 were uncharacterized. BreakDancer and Integrative Genomics Viewer determined 20 breakpoints (16 translocation, 2 inversion and 2 deletion breakpoints), but did not detect 8 breakpoints (2 translocation and 6 deletion breakpoints). These data indicate the efficacy of WGS for the precise determination of translocation and inversion breakpoints.

Published

2014

156. Late-onset spastic ataxia phenotype in a patient with a homozygous DDHD2 mutation.

Author

Doi H, Ushiyama M, Baba T, Tani K, Shiina M, Ogata K, Miyatake S, Fukuda-Yuzawa Y, Tsuji S, Nakashima M, Tsurusaki Y, Miyake N, Saitsu H, Ikeda S, Tanaka F, Matsumoto N, and Yoshida K

Subjects

Age of Onset, Aged, Brain diagnostic imaging, Female, Gene Frequency, Homozygote, Humans, Intellectual Disability pathology, Magnetic Resonance Imaging, Middle Aged, Muscle Spasticity pathology, Mutation, Missense, Optic Atrophy pathology, Pedigree, Phenotype, Phospholipases chemistry, Polymorphism, Single Nucleotide, Protein Structure, Tertiary, Radiography, Sequence Analysis, DNA, Spinocerebellar Ataxias pathology, Intellectual Disability epidemiology, Intellectual Disability genetics, Muscle Spasticity epidemiology, Muscle Spasticity genetics, Optic Atrophy epidemiology, Optic Atrophy genetics, Phospholipases genetics, Spinocerebellar Ataxias epidemiology, Spinocerebellar Ataxias genetics

Abstract

Autosomal recessive cerebellar ataxias and autosomal recessive hereditary spastic paraplegias (ARHSPs) are clinically and genetically heterogeneous neurological disorders. Herein we describe Japanese siblings with a midlife-onset, slowly progressive type of cerebellar ataxia and spastic paraplegia, without intellectual disability. Using whole exome sequencing, we identified a homozygous missense mutation in DDHD2, whose mutations were recently identified as the cause of early-onset ARHSP with intellectual disability. Brain MRI of the patient showed a thin corpus callosum. Cerebral proton magnetic resonance spectroscopy revealed an abnormal lipid peak in the basal ganglia, which has been reported as the hallmark of DDHD2-related ARHSP (SPG 54). The mutation caused a marked reduction of phospholipase A1 activity, supporting that this mutation is the cause of SPG54. Our cases indicate that the possibility of SPG54 should also be considered when patients show a combination of adult-onset spastic ataxia and a thin corpus callosum. Magnetic resonance spectroscopy may be helpful in the differential diagnosis of patients with spastic ataxia phenotype.

Published

2014

157. A girl with West syndrome and autistic features harboring a de novo TBL1XR1 mutation.

Author

Saitsu H, Tohyama J, Walsh T, Kato M, Kobayashi Y, Lee M, Tsurusaki Y, Miyake N, Goto Y, Nishino I, Ohtake A, King MC, and Matsumoto N

Subjects

Autistic Disorder diagnosis, DNA Mutational Analysis, Exons, Female, Humans, Infant, Rett Syndrome diagnosis, Spasms, Infantile diagnosis, Autistic Disorder genetics, Mutation, Missense, Nuclear Proteins genetics, Receptors, Cytoplasmic and Nuclear genetics, Repressor Proteins genetics, Rett Syndrome genetics, Spasms, Infantile genetics

Abstract

Recently, de novo mutations in TBL1XR1 were found in two patients with autism spectrum disorders. Here, we report on a Japanese girl presenting with West syndrome, Rett syndrome-like and autistic features. Her initial development was normal until she developed a series of spasms at 5 months of age. Electroencephalogram at 7 months showed a pattern of hypsarrhythmia, which led to a diagnosis of West syndrome. Stereotypic hand movements appeared at 8 months of age, and autistic features such as deficits in communication, hyperactivity and excitability were observed later, at 4 years and 9 months. Whole exome sequencing of the patient and her parents revealed a de novo TBL1XR1 mutation [c.209 G>A (p.Gly70Asp)] occurring at an evolutionarily conserved amino acid in an F-box-like domain. Our report expands the clinical spectrum of TBL1XR1 mutations to West syndrome with Rett-like features, together with autistic features.

Published

2014

158. 'Cortical cerebellar atrophy' dwindles away in the era of next-generation sequencing.

Author

Yoshida K, Miyatake S, Kinoshita T, Doi H, Tsurusaki Y, Miyake N, Saitsu H, and Matsumoto N

Subjects

Atrophy, High-Throughput Nucleotide Sequencing, Humans, Male, Middle Aged, Sequence Analysis, DNA, Cerebellar Cortex pathology

Published

2014

159. Whole exome analysis identifies frequent CNGA1 mutations in Japanese population with autosomal recessive retinitis pigmentosa.

Author

Katagiri S, Akahori M, Sergeev Y, Yoshitake K, Ikeo K, Furuno M, Hayashi T, Kondo M, Ueno S, Tsunoda K, Shinoda K, Kuniyoshi K, Tsurusaki Y, Matsumoto N, Tsuneoka H, and Iwata T

Subjects

Adult, Aged, Asian People, Base Sequence, Exons, Extracellular Matrix Proteins genetics, Eye Proteins genetics, Female, Genes, Recessive, High-Throughput Nucleotide Sequencing, Homozygote, Humans, Male, Middle Aged, Molecular Sequence Data, Pedigree, Phosphotransferases (Alcohol Group Acceptor) genetics, Retinitis Pigmentosa ethnology, Retinitis Pigmentosa pathology, Cyclic Nucleotide-Gated Cation Channels genetics, Exome, Mutation Rate, Retinitis Pigmentosa genetics

Abstract

Objective: The purpose of this study was to investigate frequent disease-causing gene mutations in autosomal recessive retinitis pigmentosa (arRP) in the Japanese population., Methods: In total, 99 Japanese patients with non-syndromic and unrelated arRP or sporadic RP (spRP) were recruited in this study and ophthalmic examinations were conducted for the diagnosis of RP. Among these patients, whole exome sequencing analysis of 30 RP patients and direct sequencing screening of all CNGA1 exons of the other 69 RP patients were performed., Results: Whole exome sequencing of 30 arRP/spRP patients identified disease-causing gene mutations of CNGA1 (four patients), EYS (three patients) and SAG (one patient) in eight patients and potential disease-causing gene variants of USH2A (two patients), EYS (one patient), TULP1 (one patient) and C2orf71 (one patient) in five patients. Screening of an additional 69 arRP/spRP patients for the CNGA1 gene mutation revealed one patient with a homozygous mutation., Conclusions: This is the first identification of CNGA1 mutations in arRP Japanese patients. The frequency of CNGA1 gene mutation was 5.1% (5/99 patients). CNGA1 mutations are one of the most frequent arRP-causing mutations in Japanese patients.

Published

2014

160. Severe manifestations of hand-foot-genital syndrome associated with a novel HOXA13 mutation.

Author

Imagawa E, Kayserili H, Nishimura G, Nakashima M, Tsurusaki Y, Saitsu H, Ikegawa S, Matsumoto N, and Miyake N

Subjects

Abnormalities, Multiple diagnostic imaging, Amino Acid Sequence, Base Sequence, Child, Female, Foot Deformities, Congenital diagnostic imaging, Hand Deformities, Congenital diagnostic imaging, Homeodomain Proteins chemistry, Humans, Infant, Infant, Newborn, Molecular Sequence Data, Radiography, Urogenital Abnormalities diagnostic imaging, Abnormalities, Multiple genetics, Abnormalities, Multiple pathology, Foot Deformities, Congenital genetics, Foot Deformities, Congenital pathology, Genetic Predisposition to Disease, Hand Deformities, Congenital genetics, Hand Deformities, Congenital pathology, Homeodomain Proteins genetics, Mutation genetics, Urogenital Abnormalities genetics, Urogenital Abnormalities pathology

Abstract

We report on a girl with absent nails, short/absent distal phalanges of the second to fifth fingers and toes, short thumbs, absent halluces, and carpo-tarsal coalition who also had genitourinary malformations. Trio-based whole exome sequencing identified a novel de novo mutation (c.1102A>T, p.Ile368Phe) in the HOXA13 gene. Heterozygous HOXA13 mutations have been previously reported in hand-foot-genital syndrome and Guttmacher syndrome, which are variably associated with small nails, short distal and middle phalanges, short thumbs and halluces, but not absent nails. Considering the molecular data, the phenotype in the present patient was defined as the severe end of hand-foot-genital and Guttmacher syndrome spectrum. Our observation expands the clinical spectrum caused by heterozygous HOXA13 mutations and reinforces the difficulty of differential diagnosis on clinical grounds for the disorders with short distal phalanges, short thumbs, and short halluces., (© 2014 Wiley Periodicals, Inc.)

Published

2014

161. Numerous BAF complex genes are mutated in Coffin-Siris syndrome.

Author

Miyake N, Tsurusaki Y, and Matsumoto N

Subjects

Carrier Proteins genetics, Chromosomal Proteins, Non-Histone genetics, Cohort Studies, DNA Helicases genetics, DNA-Binding Proteins genetics, Epilepsy genetics, Exome, Facies, Fingers abnormalities, Foot Deformities, Congenital genetics, Genetic Association Studies, Growth Disorders genetics, Humans, Hypogonadism genetics, Hypotrichosis genetics, Mental Retardation, X-Linked genetics, Mutation Rate, Nuclear Proteins genetics, Obesity genetics, Repressor Proteins, SMARCB1 Protein, Transcription Factors genetics, Abnormalities, Multiple genetics, Face abnormalities, Hand Deformities, Congenital genetics, Intellectual Disability genetics, Micrognathism genetics, Mutation, Neck abnormalities

Abstract

Coffin-Siris syndrome (CSS; OMIM#135900) is a rare congenital anomaly syndrome characterized by intellectual disability, coarse face, hypertrichosis, and absence/hypoplasia of the fifth digits' nails. As the majority of patients are sporadic, an autosomal dominant inheritance model has been postulated. Recently, whole exome sequencing (WES) emerged as a comprehensive analytical method for rare variants. We applied WES on five CSS patients and found two de novo mutations in SMARCB1. SMARCB1 was completely sequenced in 23 CSS patients and the mutations were found in two more patients. As SMARCB1 encodes a subunit of the BAF complex functioning as a chromatin remodeling factor, mutations in 15 other subunit genes may cause CSS and thus were analyzed in 23 CSS patients. We identified heterozygous mutations in either of six genes (SMARCA4, SMARCB1, SMARCA2, SMARCE1, ARID1A, and ARID1B) in 20 out of 23 CSS patients. The patient with a SMARCA2 mutation was re-evaluated and identified as having Nicolaides-Baraitser syndrome (OMIM#601358), which is similar to but different from CSS. Additionally, 49 more CSS patients were analyzed as a second cohort. Together with the first cohort, 37 out of 71 (22 plus 49) patients were found to have a mutation in either one of five BAF complex genes. Furthermore, two CSS patients were reported to have a PHF6 abnormality, which can also cause Borjeson-Forssman-Lehmann syndrome (OMIM#301900), an X-linked intellectual disability syndrome with epilepsy and endocrine abnormalities. The current list of mutated genes in CSS is far from being complete and analysis of more patients is required., (© 2014 Wiley Periodicals, Inc.)

Published

2014

162. Duplication of the NPHP1 gene in patients with autism spectrum disorder and normal intellectual ability: a case series.

Author

Yasuda Y, Hashimoto R, Fukai R, Okamoto N, Hiraki Y, Yamamori H, Fujimoto M, Ohi K, Taniike M, Mohri I, Nakashima M, Tsurusaki Y, Saitsu H, Matsumoto N, Miyake N, and Takeda M

Abstract

Autism spectrum disorder is a neurodevelopmental disorder characterized by impairments in social interactions, reduced verbal communication abilities, stereotyped repetitive behaviors, and restricted interests. It is a complex condition caused by genetic and environmental factors; the high heritability of this disorder supports the presence of a significant genetic contribution. Many studies have suggested that copy-number variants contribute to the etiology of autism spectrum disorder. Recently, copy-number variants of the nephronophthisis 1 gene have been reported in patients with autism spectrum disorder. To the best of our knowledge, only six autism spectrum disorder cases with duplications of the nephronophthisis 1 gene have been reported. These patients exhibited intellectual dysfunction, including verbal dysfunction in one patient, below-average verbal intellectual ability in one patient, and intellectual disability in four patients. In this study, we identified nephronophthisis 1 duplications in two unrelated Japanese patients with autism spectrum disorder using a high-resolution single-nucleotide polymorphism array. This report is the first to describe a nephronophthisis 1 duplication in an autism spectrum disorder patient with an average verbal intelligence quotient and an average performance intelligence quotient. However, the second autism spectrum disorder patient with a nephronophthisis 1 duplication had a below-average performance intelligence quotient. Neither patient exhibited physical dysfunction, motor developmental delay, or neurological abnormalities. This study supports the clinical observation of nephronophthisis 1 duplication in autism spectrum disorder cases and might contribute to our understanding of the clinical phenotype that arises from this duplication.

Published

2014

163. Causative novel PNKP mutations and concomitant PCDH15 mutations in a patient with microcephaly with early-onset seizures and developmental delay syndrome and hearing loss.

Author

Nakashima M, Takano K, Osaka H, Aida N, Tsurusaki Y, Miyake N, Saitsu H, and Matsumoto N

Subjects

Cadherin Related Proteins, Heterozygote, Humans, Infant, Male, Mutation, Sequence Analysis, DNA, Usher Syndromes genetics, Cadherins genetics, DNA Repair Enzymes genetics, Developmental Disabilities genetics, Hearing Loss genetics, Microcephaly genetics, Phosphotransferases (Alcohol Group Acceptor) genetics, Seizures genetics

Abstract

We report on a 1-year-old boy with microcephaly with a simplified gyral pattern, early-onset seizures, congenital hearing loss and a severe developmental delay. Trio-based whole-exome sequencing identified candidate compound heterozygous mutations in two genes: c.163G>T (p.Ala55Ser) and c.874G>A (p.Gly292Arg) in polynucleotide kinase 3'-phosphatase gene (PNKP), and c.195G>A (p.Met65Ile) and c.1210A>C (p.Ser404Arg) in PCDH15. PNKP and PCDH15 mutations have been reported in autosomal recessive microcephaly with early-onset seizures and developmental delay syndrome, and Usher syndrome type 1F, respectively. Our patient showed neurological features similar to reported cases of both syndromes that could be explained by the observed mutations in both PNKP and PCDH15, which therefore appear to be pathogenic in this case.

Published

2014

164. Novel compound heterozygous PIGT mutations caused multiple congenital anomalies-hypotonia-seizures syndrome 3.

Author

Nakashima M, Kashii H, Murakami Y, Kato M, Tsurusaki Y, Miyake N, Kubota M, Kinoshita T, Saitsu H, and Matsumoto N

Subjects

Abnormalities, Multiple pathology, Acyltransferases metabolism, Female, Glycosylphosphatidylinositols metabolism, Granulocytes metabolism, Heterozygote, Humans, Muscle Hypotonia complications, Pedigree, Seizures complications, Syndrome, Abnormalities, Multiple genetics, Acyltransferases genetics, Muscle Hypotonia genetics, Mutation, Seizures genetics

Abstract

Recessive mutations in genes of the glycosylphosphatidylinositol (GPI)-anchor synthesis pathway have been demonstrated as causative of GPI deficiency disorders associated with intellectual disability, seizures, and diverse congenital anomalies. We performed whole exome sequencing in a patient with progressive encephalopathies and multiple dysmorphism with hypophosphatasia and identified novel compound heterozygous mutations, c.250G>T (p. Glu84*) and c.1342C>T (p. Arg488Trp), in PIGT encoding a subunit of the GPI transamidase complex. The surface expression of GPI-anchored proteins (GPI-APs) on patient granulocytes was lower than that of healthy controls. Transfection of the Arg488Trp mutant PIGT construct, but not the Glu84* mutant, into PIGT-deficient cells partially restored the expression of GPI-APs DAF and CD59. These results indicate that PIGT mutations caused neurological impairment and multiple congenital anomalies in this patient.

Published

2014

165. A novel PITX2 mutation causing iris hypoplasia.

Author

Kimura M, Tokita Y, Machida J, Shibata A, Tatematsu T, Tsurusaki Y, Miyake N, Saitsu H, Miyachi H, Shimozato K, Matsumoto N, and Nakashima M

Abstract

Iris hypoplasia (IH) is rare autosomal dominant disorder characterized by a poorly developed iris stroma and malformations of the eyes and umbilicus. This disorder is caused by mutation of the paired-like homeodomain 2 (PITX2) gene. Here, we describe a novel PITX2 mutation (c.205C>T) in an IH family presenting with very mild eye features but with tooth agenesis as the most obvious clinical feature.

Published

2014

166. Early onset epileptic encephalopathy caused by de novo SCN8A mutations.

Author

Ohba C, Kato M, Takahashi S, Lerman-Sagie T, Lev D, Terashima H, Kubota M, Kawawaki H, Matsufuji M, Kojima Y, Tateno A, Goldberg-Stern H, Straussberg R, Marom D, Leshinsky-Silver E, Nakashima M, Nishiyama K, Tsurusaki Y, Miyake N, Tanaka F, Matsumoto N, and Saitsu H

Subjects

Adolescent, Child, Child, Preschool, Early Diagnosis, Electroencephalography methods, Epilepsy complications, Epilepsy diagnosis, Epilepsy genetics, Female, Humans, Infant, Intellectual Disability diagnosis, Intellectual Disability etiology, Intellectual Disability genetics, Male, Phenotype, Spasms, Infantile complications, Mutation, Missense genetics, NAV1.6 Voltage-Gated Sodium Channel genetics, Spasms, Infantile diagnosis, Spasms, Infantile genetics

Abstract

Objective: De novo SCN8A mutations have been reported in patients with epileptic encephalopathy. Herein we report seven patients with de novo heterozygous SCN8A mutations, which were found in our comprehensive genetic analysis (target capture or whole-exome sequencing) for early onset epileptic encephalopathies (EOEEs)., Methods: A total of 163 patients with EOEEs without mutations in known genes, including 6 with malignant migrating partial seizures in infancy (MMPSI), and 60 with unclassified EOEEs, were analyzed by target capture (28 samples) or whole-exome sequencing (135 samples)., Results: We identified de novo SCN8A mutations in 7 patients: 6 of 60 unclassified EOEEs (10.0%), and one of 6 MMPSI cases (16.7%). The mutations were scattered through the entire gene: four mutations were located in linker regions, two in the fourth transmembrane segments, and one in the C-terminal domain. The type of the initial seizures was variable including generalized tonic-clonic, atypical absence, partial, apneic attack, febrile convulsion, and loss of tone and consciousness. Onset of seizures was during the neonatal period in two patients, and between 3 and 7 months of age in five patients. Brain magnetic resonance imaging (MRI) showed cerebellar and cerebral atrophy in one and six patients, respectively. All patients with SCN8A missense mutations showed initially uncontrollable seizures by any drugs, but eventually one was seizure-free and three were controlled at the last examination. All patients showed developmental delay or regression in infancy, resulting in severe intellectual disability., Significance: Our data reveal that SCN8A mutations can cause variable phenotypes, most of which can be diagnosed as unclassified EOEEs, and rarely as MMPSI. Together with previous reports, our study further indicates that genetic testing of SCN8A should be considered in children with unclassified severe epilepsy., (Wiley Periodicals, Inc. © 2014 International League Against Epilepsy.)

Published

2014

167. Deep sequencing detects very-low-grade somatic mosaicism in the unaffected mother of siblings with nemaline myopathy.

Author

Miyatake S, Koshimizu E, Hayashi YK, Miya K, Shiina M, Nakashima M, Tsurusaki Y, Miyake N, Saitsu H, Ogata K, Nishino I, and Matsumoto N

Subjects

Child, Child, Preschool, DNA Mutational Analysis, Fathers, Female, Humans, Male, Models, Genetic, Mothers, Muscles metabolism, Muscles pathology, Myopathies, Nemaline pathology, Pedigree, Siblings, Mosaicism, Mutation, Myopathies, Nemaline genetics, Myopathies, Nemaline metabolism

Abstract

When an expected mutation in a particular disease-causing gene is not identified in a suspected carrier, it is usually assumed to be due to germline mosaicism. We report here very-low-grade somatic mosaicism in ACTA1 in an unaffected mother of two siblings affected with a neonatal form of nemaline myopathy. The mosaicism was detected by deep resequencing using a next-generation sequencer. We identified a novel heterozygous mutation in ACTA1, c.448A>G (p.Thr150Ala), in the affected siblings. Three-dimensional structural modeling suggested that this mutation may affect polymerization and/or actin's interactions with other proteins. In this family, we expected autosomal dominant inheritance with either parent demonstrating germline or somatic mosaicism. Sanger sequencing identified no mutation. However, further deep resequencing of this mutation on a next-generation sequencer identified very-low-grade somatic mosaicism in the mother: 0.4%, 1.1%, and 8.3% in the saliva, blood leukocytes, and nails, respectively. Our study demonstrates the possibility of very-low-grade somatic mosaicism in suspected carriers, rather than germline mosaicism., (Copyright © 2014 Elsevier B.V. All rights reserved.)

Published

2014

168. Expanding the phenotypic spectrum of TUBB4A-associated hypomyelinating leukoencephalopathies.

Author

Miyatake S, Osaka H, Shiina M, Sasaki M, Takanashi J, Haginoya K, Wada T, Morimoto M, Ando N, Ikuta Y, Nakashima M, Tsurusaki Y, Miyake N, Ogata K, Matsumoto N, and Saitsu H

Subjects

Adolescent, Adult, Basal Ganglia pathology, Cerebellum pathology, Child, Child, Preschool, DNA Mutational Analysis, Demyelinating Diseases complications, Exome genetics, Female, Humans, Infant, Leukoencephalopathies complications, Male, Models, Molecular, Phenotype, Young Adult, Demyelinating Diseases genetics, Genetic Predisposition to Disease, Leukoencephalopathies genetics, Mutation genetics, Tubulin genetics

Abstract

Objective: We performed whole-exome sequencing analysis of patients with genetically unsolved hypomyelinating leukoencephalopathies, identifying 8 patients with TUBB4A mutations and allowing the phenotypic spectrum of TUBB4A mutations to be investigated., Methods: Fourteen patients with hypomyelinating leukoencephalopathies, 7 clinically diagnosed with hypomyelination with atrophy of the basal ganglia and cerebellum (H-ABC), and 7 with unclassified hypomyelinating leukoencephalopathy, were analyzed by whole-exome sequencing. The effect of the mutations on microtubule assembly was examined by mapping altered amino acids onto 3-dimensional models of the αβ-tubulin heterodimer., Results: Six heterozygous missense mutations in TUBB4A, 5 of which are novel, were identified in 8 patients (6/7 patients with H-ABC [the remaining patient is an atypical case] and 2/7 patients with unclassified hypomyelinating leukoencephalopathy). In 4 cases with parental samples available, the mutations occurred de novo. Analysis of 3-dimensional models revealed that the p.Glu410Lys mutation, identified in patients with unclassified hypomyelinating leukoencephalopathy, directly impairs motor protein and/or microtubule-associated protein interactions with microtubules, whereas the other mutations affect longitudinal interactions for maintaining αβ-tubulin structure, suggesting different mechanisms in tubulin function impairment. In patients with the p.Glu410Lys mutation, basal ganglia atrophy was unobserved or minimal although extrapyramidal features were detected, suggesting its functional impairment., Conclusions: TUBB4A mutations cause typical H-ABC. Furthermore, TUBB4A mutations associate cases of unclassified hypomyelinating leukoencephalopathies with morphologically retained but functionally impaired basal ganglia, suggesting that TUBB4A-related hypomyelinating leukoencephalopathies encompass a broader clinical spectrum than previously expected. Extrapyramidal findings may be a key for consideration of TUBB4A mutations in hypomyelinating leukoencephalopathies., (© 2014 American Academy of Neurology.)

Published

2014

169. De novo SOX11 mutations cause Coffin-Siris syndrome.

Author

Tsurusaki Y, Koshimizu E, Ohashi H, Phadke S, Kou I, Shiina M, Suzuki T, Okamoto N, Imamura S, Yamashita M, Watanabe S, Yoshiura K, Kodera H, Miyatake S, Nakashima M, Saitsu H, Ogata K, Ikegawa S, Miyake N, and Matsumoto N

Subjects

Adolescent, Animals, Child, Preschool, Cohort Studies, Female, Gene Knockdown Techniques, Humans, Mice, Mutation, Zebrafish, Abnormalities, Multiple genetics, Face abnormalities, Hand Deformities, Congenital genetics, Intellectual Disability genetics, Micrognathism genetics, Neck abnormalities, SOX Transcription Factors genetics, SOXC Transcription Factors genetics, Zebrafish Proteins genetics

Abstract

Coffin-Siris syndrome (CSS) is a congenital disorder characterized by growth deficiency, intellectual disability, microcephaly, characteristic facial features and hypoplastic nails of the fifth fingers and/or toes. We previously identified mutations in five genes encoding subunits of the BAF complex, in 55% of CSS patients. Here we perform whole-exome sequencing in additional CSS patients, identifying de novo SOX11 mutations in two patients with a mild CSS phenotype. sox11a/b knockdown in zebrafish causes brain abnormalities, potentially explaining the brain phenotype of CSS. SOX11 is the downstream transcriptional factor of the PAX6-BAF complex, highlighting the importance of the BAF complex and SOX11 transcriptional network in brain development.

Published

2014

170. PIGN mutations cause congenital anomalies, developmental delay, hypotonia, epilepsy, and progressive cerebellar atrophy.

Author

Ohba C, Okamoto N, Murakami Y, Suzuki Y, Tsurusaki Y, Nakashima M, Miyake N, Tanaka F, Kinoshita T, Matsumoto N, and Saitsu H

Subjects

Brain abnormalities, CD24 Antigen metabolism, Cerebellar Diseases genetics, Cerebellar Diseases pathology, Child, Child, Preschool, Congenital Abnormalities genetics, Developmental Disabilities genetics, Epilepsy genetics, Female, GPI-Linked Proteins metabolism, Heterozygote, Humans, Male, Muscle Hypotonia genetics, Pedigree, Receptors, IgG metabolism, Abnormalities, Multiple genetics, Mutation, Phosphotransferases genetics

Abstract

Defects of the human glycosylphosphatidylinositol (GPI) anchor biosynthetic pathway show a broad range of clinical phenotypes. A homozygous mutation in PIGN, a member of genes involved in the GPI anchor-synthesis pathway, was previously reported to cause dysmorphic features, multiple congenital anomalies, severe neurological impairment, and seizure in a consanguineous family. Here, we report two affected siblings with compound heterozygous PIGN mutations [c.808T >C (p.Ser270Pro) and c.963G >A] showing congenital anomalies, developmental delay, hypotonia, epilepsy, and progressive cerebellar atrophy. The c.808C >T mutation altered an evolutionarily conserved amino acid residue (Ser270), while reverse transcription-PCR and sequencing demonstrated that c.963G >A led to aberrant splicing, in which two mutant transcripts with premature stop codons (p.Ala322Valfs*24 and p.Glu308Glyfs*2) were generated. Expression of GPI-anchored proteins such as CD16 and CD24 on granulocytes from affected siblings was significantly decreased, and expression of the GPI-anchored protein CD59 in PIGN-knockout human embryonic kidney 293 cells was partially or hardly restored by transient expression of p.Ser270Pro and p.Glu308Glyfs*2 mutants, respectively, suggesting severe and complete loss of PIGN activity. Our findings confirm that developmental delay, hypotonia, and epilepsy combined with congenital anomalies are common phenotypes of PIGN mutations and add progressive cerebellar atrophy to this clinical spectrum.

Published

2014

171. De novo WDR45 mutation in a patient showing clinically Rett syndrome with childhood iron deposition in brain.

Author

Ohba C, Nabatame S, Iijima Y, Nishiyama K, Tsurusaki Y, Nakashima M, Miyake N, Tanaka F, Ozono K, Saitsu H, and Matsumoto N

Subjects

Adolescent, Alleles, Alternative Splicing, Brain pathology, DNA Mutational Analysis, Exome, Female, High-Throughput Nucleotide Sequencing, Humans, Magnetic Resonance Imaging, Rett Syndrome diagnosis, Brain metabolism, Carrier Proteins genetics, Iron metabolism, Mutation, Rett Syndrome genetics, Rett Syndrome metabolism

Abstract

Rett syndrome (RTT) is a neurodevelopmental disorder mostly caused by MECP2 mutations. We identified a de novo WDR45 mutation, which caused a subtype of neurodegeneration with brain iron accumulation, in a patient showing clinically typical RTT. The mutation (c.830+1G>A) led to aberrant splicing in lymphoblastoid cells. Sequential brain magnetic resonance imaging demonstrated that iron deposition in the globus pallidus and the substantia nigra was observed as early as at 11 years of age. Because the patient showed four of the main RTT diagnostic criteria, WDR45 should be investigated in patients with RTT without MECP2 mutations.

Published

2014

172. A novel homozygous YARS2 mutation causes severe myopathy, lactic acidosis, and sideroblastic anemia 2.

Author

Nakajima J, Eminoglu TF, Vatansever G, Nakashima M, Tsurusaki Y, Saitsu H, Kawashima H, Matsumoto N, and Miyake N

Subjects

Acidosis, Lactic complications, Adolescent, Adult, Anemia, Sideroblastic complications, Child, Child, Preschool, Fatal Outcome, Female, Homozygote, Humans, Infant, Infant, Newborn, Male, Muscular Diseases complications, Pedigree, Young Adult, Acidosis, Lactic genetics, Anemia, Sideroblastic genetics, Muscular Diseases genetics, Mutation, Tyrosine-tRNA Ligase genetics

Abstract

Mitochondrial diseases are associated with defects of adenosine triphosphate production and energy supply to organs as a result of dysfunctions of the mitochondrial respiratory chain. Biallelic mutations in the YARS2 gene encoding mitochondrial tyrosyl-tRNA synthetase cause myopathy, lactic acidosis, and sideroblastic anemia 2 (MLASA2), a type of mitochondrial disease. Here, we report a consanguineous Turkish family with two siblings showing severe metabolic decompensation including recurrent hypoglycemia, lactic acidosis, and transfusion-dependent anemia. Using whole-exome sequencing of the proband and his parents, we identified a novel YARS2 mutation (c.1303A>G, p.Ser435Gly) that was homozygous in the patient and heterozygous in his parents. This mutation is located at the ribosomal protein S4-like domain of the gene, while other reported YARS2 mutations are all within the catalytic domain. Interestingly, the proband showed more severe symptoms and an earlier onset than previously reported patients, suggesting the functional importance of the S4-like domain in tyrosyl-tRNA synthetase.

Published

2014

173. A novel WTX mutation in a female patient with osteopathia striata with cranial sclerosis and hepatoblastoma.

Author

Fujita A, Ochi N, Fujimaki H, Muramatsu H, Takahashi Y, Natsume J, Kojima S, Nakashima M, Tsurusaki Y, Saitsu H, Matsumoto N, and Miyake N

Subjects

Child, Female, Genetic Predisposition to Disease, Humans, Adaptor Proteins, Signal Transducing genetics, Hepatoblastoma genetics, Liver Neoplasms genetics, Mutation, Osteosclerosis genetics, Tumor Suppressor Proteins genetics

Abstract

Osteopathia striata with cranial sclerosis (OSCS) is an X-linked dominant sclerosing bone dysplasia. Typically affected females show macrocephaly, characteristic facial appearance, cleft palate, mild learning difficulties, hearing loss, sclerosis of the long bones and skull, and longitudinal striations visible on radiographs of the long bones, pelvis and scapulae. Typically affected males usually die at the fetal or early neonatal stage. Because of its variable expressivity, which ranges from asymptomatic to fetal death, clinical diagnosis of OSCS can be difficult. Here, we identify a unique female patient presenting with severe macrocephaly, characteristic facial appearance, developmental delay, and hepatoblastoma. Exome sequencing identified a novel de novo nonsense mutation (c.1045C>T, p.Glu349*) in the WTX gene associated with OSCS. The OSCS diagnosis was confirmed in this patient based on the hallmark appearance of longitudinal striations in long bones when viewed by X-ray. WTX is also known as a tumor suppressor gene, and somatic mutations in that gene have been identified in Wilms tumors. In addition to this patient, although two patients with OSCS have been reported to have colorectal cancer or ovarian cancer, Wilms tumor has never been reported in association with this disorder. Tumor susceptibility in patients with OSCS is discussed., (© 2014 Wiley Periodicals, Inc.)

Published

2014

174. A de novo 1.4-Mb deletion at 21q22.11 in a boy with developmental delay.

Author

Fukai R, Hiraki Y, Nishimura G, Nakashima M, Tsurusaki Y, Saitsu H, Matsumoto N, and Miyake N

Subjects

Adaptor Proteins, Vesicular Transport genetics, Chromosome Deletion, Humans, Infant, Male, Phenotype, Chromosomes, Human, Pair 21 genetics, Developmental Disabilities genetics

Abstract

Monosomy 21 is a very rare chromosomal abnormality. At least 45 patients with partial deletion involving 21q11 have been reported. Here, we report a Japanese boy who presented with pre- and postnatal growth delays, psychomotor developmental delay, microcephaly, and iris coloboma. Cytogenetic analysis revealed a de novo 1.4-Mb deletion at 21q22.11 containing 19 protein-coding RefSeq genes. We compared the clinical phenotypes between the present patient and 16 previously reported patients with a deleted region associated with postnatal growth delay and psychomotor developmental delay. Interestingly, ITSN1 was the only gene deleted or disrupted in all cases; this gene is known to be associated with intellectual disability. Microcephaly and brain structural abnormalities including polymicrogyria and agenesis/hypoplasia of the corpus callosum may also result from haploinsufficiency of ITSN1, highlighting its clinical significance for the neurological features of patients with monosomy 21., (© 2014 Wiley Periodicals, Inc.)

Published

2014

175. A de novo CASK mutation in pontocerebellar hypoplasia type 3 with early myoclonic epilepsy and tetralogy of Fallot.

Author

Nakamura K, Nishiyama K, Kodera H, Nakashima M, Tsurusaki Y, Miyake N, Matsumoto N, Saitsu H, Jinnou H, Ohki S, Yokochi K, Okanishi T, and Enoki H

Subjects

Epilepsies, Myoclonic complications, Humans, Male, Olivopontocerebellar Atrophies complications, Tetralogy of Fallot complications, Epilepsies, Myoclonic genetics, Frameshift Mutation, Guanylate Kinases genetics, Olivopontocerebellar Atrophies genetics, Tetralogy of Fallot genetics

Published

2014

176. A hemizygous GYG2 mutation and Leigh syndrome: a possible link?

Author

Imagawa E, Osaka H, Yamashita A, Shiina M, Takahashi E, Sugie H, Nakashima M, Tsurusaki Y, Saitsu H, Ogata K, Matsumoto N, and Miyake N

Subjects

Adult, Amino Acid Sequence, DNA Mutational Analysis, Exome, Glucosyltransferases chemistry, Glycoproteins chemistry, Glycoproteins genetics, Hemizygote, Humans, Isoenzymes, Japan, Male, Molecular Sequence Data, Mutation, Missense, Pedigree, Phenotype, Sequence Alignment, Sequence Analysis, DNA, Young Adult, Glucosyltransferases genetics, Glycogen metabolism, Leigh Disease genetics, Models, Molecular

Abstract

Leigh syndrome (LS) is an early-onset progressive neurodegenerative disorder characterized by unique, bilateral neuropathological findings in brainstem, basal ganglia, cerebellum and spinal cord. LS is genetically heterogeneous, with the majority of the causative genes affecting mitochondrial malfunction, and many cases still remain unsolved. Here, we report male sibs affected with LS showing ketonemia, but no marked elevation of lactate and pyruvate. To identify their genetic cause, we performed whole exome sequencing. Candidate variants were narrowed down based on autosomal recessive and X-linked recessive models. Only one hemizygous missense mutation (c.665G>C, p.W222S) in glycogenin-2 (GYG2) (isoform a: NM_001079855) in both affected sibs and a heterozygous change in their mother were identified, being consistent with the X-linked recessive trait. GYG2 encodes glycogenin-2 (GYG2) protein, which plays an important role in the initiation of glycogen synthesis. Based on the structural modeling, the mutation can destabilize the structure and result in protein malfunctioning. Furthermore, in vitro experiments showed mutant GYG2 was unable to undergo the self-glucosylation, which is observed in wild-type GYG2. This is the first report of GYG2 mutation in human, implying a possible link between GYG2 abnormality and LS.

Published

2014

177. PIGO mutations in intractable epilepsy and severe developmental delay with mild elevation of alkaline phosphatase levels.

Author

Nakamura K, Osaka H, Murakami Y, Anzai R, Nishiyama K, Kodera H, Nakashima M, Tsurusaki Y, Miyake N, Kinoshita T, Matsumoto N, and Saitsu H

Subjects

Abnormalities, Multiple diagnosis, Child, Developmental Disabilities blood, Developmental Disabilities diagnosis, Developmental Disabilities genetics, Epilepsy diagnosis, Fatal Outcome, Female, Glycosylphosphatidylinositols blood, Glycosylphosphatidylinositols deficiency, Hemoglobinuria, Paroxysmal blood, Hemoglobinuria, Paroxysmal diagnosis, Humans, Infant, Intellectual Disability diagnosis, Male, Membrane Proteins blood, Mutation genetics, Pedigree, Phosphorus Metabolism Disorders diagnosis, Seizures, Severity of Illness Index, Abnormalities, Multiple blood, Abnormalities, Multiple genetics, Alkaline Phosphatase blood, Epilepsy blood, Epilepsy genetics, Intellectual Disability blood, Intellectual Disability genetics, Membrane Proteins genetics, Phosphorus Metabolism Disorders blood, Phosphorus Metabolism Disorders genetics

Abstract

Aberrations in the glycosylphosphatidylinositol (GPI)-anchor biosynthesis pathway constitute a subclass of congenital disorders of glycosylation, and mutations in seven genes involved in this pathway have been identified. Among them, mutations in PIGV and PIGO, which are involved in the late stages of GPI-anchor synthesis, and PGAP2, which is involved in fatty-acid GPI-anchor remodeling, are all causative for hyperphosphatasia with mental retardation syndrome (HPMRS). Using whole exome sequencing, we identified novel compound heterozygous PIGO mutations (c.389C>A [p.Thr130Asn] and c.1288C>T [p.Gln430*]) in two siblings, one of them having epileptic encephalopathy. GPI-anchored proteins (CD16 and CD24) on blood granulocytes were slightly decreased compared with a control and his mother. Our patients lacked the characteristic features of HPMRS, such as facial dysmorphology (showing only a tented mouth) and hypoplasia of distal phalanges, and had only a mild elevation of serum alkaline phosphatase (ALP). Our findings therefore expand the clinical spectrum of GPI-anchor deficiencies involving PIGO mutations to include epileptic encephalopathy with mild elevation of ALP., (Wiley Periodicals, Inc. © 2014 International League Against Epilepsy.)

Published

2014

178. Aortic aneurysm and craniosynostosis in a family with Cantu syndrome.

Author

Hiraki Y, Miyatake S, Hayashidani M, Nishimura Y, Matsuura H, Kamada M, Kawagoe T, Yunoki K, Okamoto N, Yofune H, Nakashima M, Tsurusaki Y, Satisu H, Murakami A, Miyake N, Nishimura G, and Matsumoto N

Subjects

Adult, Amino Acid Sequence, Aortic Aneurysm genetics, Aortic Aneurysm, Thoracic diagnostic imaging, Aortic Aneurysm, Thoracic pathology, Base Sequence, Brain pathology, Cardiomegaly diagnostic imaging, Cardiomegaly genetics, Child, Preschool, Craniosynostoses genetics, DNA Mutational Analysis, Facies, Genetic Diseases, X-Linked genetics, Humans, Hypertrichosis genetics, Magnetic Resonance Imaging, Male, Mutation, Mutation, Missense, Osteochondrodysplasias genetics, Phenotype, Radiography, Sulfonylurea Receptors chemistry, Sulfonylurea Receptors genetics, Syndrome, Aortic Aneurysm diagnosis, Cardiomegaly diagnosis, Craniosynostoses diagnosis, Genetic Diseases, X-Linked diagnosis, Hypertrichosis diagnosis, Osteochondrodysplasias diagnosis

Abstract

Cantu syndrome is an autosomal dominant overgrowth syndrome associated with facial dysmorphism, congenital hypertrichosis, and cardiomegaly. Some affected individuals show bone undermodeling of variable severity. Recent investigations revealed that the disorder is caused by a mutation in ABCC9, encoding a regulatory SUR2 subunit of an ATP-sensitive potassium channel mainly expressed in cardiac and skeletal muscle as well as vascular smooth muscle. We report here on a Japanese family with this syndrome. An affected boy and his father had a novel missense mutation in ABCC9. Each patient had a coarse face and hypertrichosis. However, cardiomegaly was seen only in the boy, and macrosomia only in the father. Skeletal changes were not evident in either patient. Craniosynostosis in the boy and the development of aortic aneurysm in the father are previously undescribed associations with Cantu syndrome., (© 2013 Wiley Periodicals, Inc.)

Published

2014

179. [Impact of comprehensive stroke team combined with vascular neurologist, neurosurgeon and endovascular interventionist for acute stroke].

Author

Okada Y, Sambongi Y, Tsurusaki Y, Tsumoto T, Nagata S, and Yasaka M

Subjects

Comprehensive Health Care organization & administration, Humans, Japan, Patient Care Team organization & administration, Patient Care Team trends, Physicians, Comprehensive Health Care trends, Endovascular Procedures methods, Endovascular Procedures trends, Interdisciplinary Communication, Neurosurgery, Stroke therapy

Abstract

The stroke center with endovascular intervention has been developed with advances in acute stroke therapy. Vascular neurologists who intend to perform endovascular intervention should receive advanced clinical training in a neurosurgical department, as well as experience in cardiovascular medicine for a prescribed period. A stroke team combined with vascular neurologists, neurosurgeons, and endovascular interventionists would be essential for a regional core comprehensive stroke center in the future.

Published

2014

180. Novel FIG4 mutations in Yunis-Varon syndrome.

Author

Nakajima J, Okamoto N, Shiraishi J, Nishimura G, Nakashima M, Tsurusaki Y, Saitsu H, Kawashima H, Matsumoto N, and Miyake N

Subjects

Child, Preschool, Female, Humans, Phosphoric Monoester Hydrolases, Cleidocranial Dysplasia genetics, Ectodermal Dysplasia genetics, Flavoproteins genetics, Limb Deformities, Congenital genetics, Micrognathism genetics, Mutation genetics

Abstract

Yunis-Varon syndrome (YVS, MIM 216340) is a rare autosomal recessive disorder characterized by skeletal abnormalities and severe neurological impairment with vacuolation of the central nervous system, skeletal muscles and cartilages. Very recently, mutations of the FIG4 (FIG4 homolog, SAC1 lipid phosphatase domain containing (Saccharomyces cerevisiae)) gene, which encodes a 5'-phosphoinositide phosphatase essential for endosome/lysosome function have been identified as the cause for YVS. Interestingly, FIG4 mutations were previously reported to be responsible for other neurodegenerative diseases such as autosomal recessive Charcot-Marie-Tooth disease type 4J and autosomal dominant amyotrophic lateral sclerosis/primary lateral sclerosis. We analyzed a YVS patient using whole-exome sequencing, and identified novel biallelic FIG4 mutations: c.1750+1delG and c.2284_2285delCT (p.S762Wfs*3). These two mutations were mutations supposed to have null function. To our knowledge, this is the second report of FIG4 mutations in YVS and our result supports the idea that biallelic null mutations of FIG4 cause YVS in human.

Published

2013

181. De novo mutations in SLC35A2 encoding a UDP-galactose transporter cause early-onset epileptic encephalopathy.

Author

Kodera H, Nakamura K, Osaka H, Maegaki Y, Haginoya K, Mizumoto S, Kato M, Okamoto N, Iai M, Kondo Y, Nishiyama K, Tsurusaki Y, Nakashima M, Miyake N, Hayasaka K, Sugahara K, Yuasa I, Wada Y, Matsumoto N, and Saitsu H

Subjects

Age of Onset, Animals, Brain pathology, Brain physiopathology, Cell Line, Child, DNA Mutational Analysis, Electroencephalography, Exome, Facies, Female, Gene Expression, Gene Order, High-Throughput Nucleotide Sequencing, Humans, Infant, Infant, Newborn, Magnetic Resonance Imaging, Mice, Monosaccharide Transport Proteins chemistry, Phenotype, Protein Transport, RNA Isoforms, Monosaccharide Transport Proteins genetics, Mutation, Spasms, Infantile diagnosis, Spasms, Infantile genetics

Abstract

Early-onset epileptic encephalopathies (EOEE) are severe neurological disorders characterized by frequent seizures accompanied by developmental regression or retardation. Whole-exome sequencing of 12 patients together with five pairs of parents and subsequent Sanger sequencing in additional 328 EOEE patients identified two de novo frameshift and one missense mutations in SLC35A2 at Xp11.23, respectively. The three patients are all females. X-inactivation analysis of blood leukocyte DNA and mRNA analysis using lymphoblastoid cells derived from two patients with a frameshift mutation indicated that only the wild-type SLC35A2 allele was expressed in these cell types, at least in part likely as a consequence of skewed X-inactivation. SLC35A2 encodes a UDP-galactose transporter (UGT), which selectively supplies UDP-galactose from the cytosol to the Golgi lumen. Transient expression experiments revealed that the missense mutant protein was correctly localized in the Golgi apparatus. In contrast, the two frameshift mutant proteins were not properly expressed, suggesting that their function is severely impaired. Defects in the UGT can cause congenital disorders of glycosylation. Of note, no abnormalities of glycosylation were observed in three serum glycoproteins, which is consistent with favorably skewed X-inactivation. We hypothesize that a substantial number of neurons might express the mutant SLC35A2 allele and suffer from defective galactosylation, resulting in EOEE., (© 2013 WILEY PERIODICALS, INC.)

Published

2013

182. 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

183. Co-occurrence of 22q11 deletion syndrome and HDR syndrome.

Author

Fukai R, Ochi N, Murakami A, Nakashima M, Tsurusaki Y, Saitsu H, Matsumoto N, and Miyake N

Subjects

22q11 Deletion Syndrome diagnosis, Abnormalities, Multiple diagnosis, Base Sequence, Chromosome Breakpoints, Chromosome Deletion, Chromosomes, Human, Pair 10, Chromosomes, Human, Pair 22, Comparative Genomic Hybridization, Facies, Hearing Loss, Sensorineural diagnosis, Humans, Hypoparathyroidism diagnosis, In Situ Hybridization, Fluorescence, Male, Nephrosis diagnosis, Phenotype, Young Adult, 22q11 Deletion Syndrome complications, Hearing Loss, Sensorineural complications, Hypoparathyroidism complications, Nephrosis complications

Abstract

22q11 deletion syndrome is one of the most common chromosomal deletion syndromes and is usually caused by a 1.5-3.0 Mb deletion at chromosome 22q11.2. It is characterized by hypocalcemia resulting from hypoplasia of the parathyroid glands, hypoplasia of the thymus, and defects of the cardiac outflow tract. We encountered a Japanese boy presenting with an unusually severe phenotype of 22q11 deletion syndrome, including progressive renal failure and severe intellectual disabilities. Diagnostic testing using fluorescent in situ hybridization revealed deletion of the 22q11 region, but this did not explain the additional complications. Copy number analysis was therefore performed using whole genome single nucleotide polymorphism (SNP) assay, which identified an additional de novo deletion at 10p14. This region is the locus for hypoparathyroidism, deafness, and renal dysplasia (HDR) syndrome caused by haploinsufficiency of GATA3. Together, these two syndromes sufficiently explain the patient's phenotype. This is the first known case report of the co-occurrence of 22q11 deletion syndrome and HDR syndrome. As the two syndromes overlap clinically, this study indicates the importance of carrying out careful clinical and genetic assessment of patients with atypical clinical phenotypes or unique complications. Unbiased genetic analysis using whole genome copy number SNP arrays is especially useful for detecting such rare double mutations., (Copyright © 2013 Wiley Periodicals, Inc.)

Published

2013

184. Performance comparison of bench-top next generation sequencers using microdroplet PCR-based enrichment for targeted sequencing in patients with autism spectrum disorder.

Author

Koshimizu E, Miyatake S, Okamoto N, Nakashima M, Tsurusaki Y, Miyake N, Saitsu H, and Matsumoto N

Subjects

Humans, Child Development Disorders, Pervasive genetics, High-Throughput Nucleotide Sequencing methods, Polymerase Chain Reaction methods

Abstract

Next-generation sequencing (NGS) combined with enrichment of target genes enables highly efficient and low-cost sequencing of multiple genes for genetic diseases. The aim of this study was to validate the accuracy and sensitivity of our method for comprehensive mutation detection in autism spectrum disorder (ASD). We assessed the performance of the bench-top Ion Torrent PGM and Illumina MiSeq platforms as optimized solutions for mutation detection, using microdroplet PCR-based enrichment of 62 ASD associated genes. Ten patients with known mutations were sequenced using NGS to validate the sensitivity of our method. The overall read quality was better with MiSeq, largely because of the increased indel-related error associated with PGM. The sensitivity of SNV detection was similar between the two platforms, suggesting they are both suitable for SNV detection in the human genome. Next, we used these methods to analyze 28 patients with ASD, and identified 22 novel variants in genes associated with ASD, with one mutation detected by MiSeq only. Thus, our results support the combination of target gene enrichment and NGS as a valuable molecular method for investigating rare variants in ASD.

Published

2013

185. De Novo mutations in GNAO1, encoding a Gαo subunit of heterotrimeric G proteins, cause epileptic encephalopathy.

Author

Nakamura K, Kodera H, Akita T, Shiina M, Kato M, Hoshino H, Terashima H, Osaka H, Nakamura S, Tohyama J, Kumada T, Furukawa T, Iwata S, Shiihara T, Kubota M, Miyatake S, Koshimizu E, Nishiyama K, Nakashima M, Tsurusaki Y, Miyake N, Hayasaka K, Ogata K, Fukuda A, Matsumoto N, and Saitsu H

Subjects

Amino Acid Sequence, Amino Acid Substitution genetics, Animals, Calcium metabolism, Child, Child, Preschool, Electroencephalography, Epilepsy pathology, Epilepsy physiopathology, Exome genetics, Female, GTP-Binding Protein alpha Subunits, Gi-Go chemistry, Humans, Infant, Magnetic Resonance Imaging, Mice, Models, Molecular, Molecular Sequence Data, Mutant Proteins chemistry, Mutant Proteins genetics, Mutant Proteins metabolism, Phenotype, Protein Transport, Sequence Analysis, DNA, Signal Transduction genetics, Epilepsy genetics, GTP-Binding Protein alpha Subunits, Gi-Go genetics, Genetic Predisposition to Disease, Mutation genetics

Abstract

Heterotrimeric G proteins, composed of α, β, and γ subunits, can transduce a variety of signals from seven-transmembrane-type receptors to intracellular effectors. By whole-exome sequencing and subsequent mutation screening, we identified de novo heterozygous mutations in GNAO1, which encodes a Gαo subunit of heterotrimeric G proteins, in four individuals with epileptic encephalopathy. Two of the affected individuals also showed involuntary movements. Somatic mosaicism (approximately 35% to 50% of cells, distributed across multiple cell types, harbored the mutation) was shown in one individual. By mapping the mutation onto three-dimensional models of the Gα subunit in three different complexed states, we found that the three mutants (c.521A>G [p.Asp174Gly], c.836T>A [p.Ile279Asn], and c.572_592del [p.Thr191_Phe197del]) are predicted to destabilize the Gα subunit fold. A fourth mutant (c.607G>A), in which the Gly203 residue located within the highly conserved switch II region is substituted to Arg, is predicted to impair GTP binding and/or activation of downstream effectors, although the p.Gly203Arg substitution might not interfere with Gα binding to G-protein-coupled receptors. Transient-expression experiments suggested that localization to the plasma membrane was variably impaired in the three putatively destabilized mutants. Electrophysiological analysis showed that Gαo-mediated inhibition of calcium currents by norepinephrine tended to be lower in three of the four Gαo mutants. These data suggest that aberrant Gαo signaling can cause multiple neurodevelopmental phenotypes, including epileptic encephalopathy and involuntary movements., (Copyright © 2013 The American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2013

186. MLL2 and KDM6A mutations in patients with Kabuki syndrome.

Author

Miyake N, Koshimizu E, Okamoto N, Mizuno S, Ogata T, Nagai T, Kosho T, Ohashi H, Kato M, Sasaki G, Mabe H, Watanabe Y, Yoshino M, Matsuishi T, Takanashi J, Shotelersuk V, Tekin M, Ochi N, Kubota M, Ito N, Ihara K, Hara T, Tonoki H, Ohta T, Saito K, Matsuo M, Urano M, Enokizono T, Sato A, Tanaka H, Ogawa A, Fujita T, Hiraki Y, Kitanaka S, Matsubara Y, Makita T, Taguri M, Nakashima M, Tsurusaki Y, Saitsu H, Yoshiura K, Matsumoto N, and Niikawa N

Subjects

Abnormalities, Multiple diagnosis, Adolescent, Adult, Amino Acid Substitution, Child, Child, Preschool, Exome, Facies, Female, Genetic Association Studies, Hematologic Diseases diagnosis, High-Throughput Nucleotide Sequencing, Humans, Infant, Infant, Newborn, Male, Mutation Rate, Phenotype, Vestibular Diseases diagnosis, X Chromosome Inactivation, Young Adult, Abnormalities, Multiple genetics, DNA-Binding Proteins genetics, Face abnormalities, Hematologic Diseases genetics, Histone Demethylases genetics, Mutation, Neoplasm Proteins genetics, Nuclear Proteins genetics, Vestibular Diseases genetics

Abstract

Kabuki syndrome is a congenital anomaly syndrome characterized by developmental delay, intellectual disability, specific facial features including long palpebral fissures and ectropion of the lateral third of the lower eyelids, prominent digit pads, and skeletal and visceral abnormalities. Mutations in MLL2 and KDM6A cause Kabuki syndrome. We screened 81 individuals with Kabuki syndrome for mutations in these genes by conventional methods (n = 58) and/or targeted resequencing (n = 45) or whole exome sequencing (n = 5). We identified a mutation in MLL2 or KDM6A in 50 (61.7%) and 5 (6.2%) cases, respectively. Thirty-five MLL2 mutations and two KDM6A mutations were novel. Non-protein truncating-type MLL2 mutations were mainly located around functional domains, while truncating-type mutations were scattered through the entire coding region. The facial features of patients in the MLL2 truncating-type mutation group were typical based on those of the 10 originally reported patients with Kabuki syndrome; those of the other groups were less typical. High arched eyebrows, short fifth finger, and hypotonia in infancy were more frequent in the MLL2 mutation group than in the KDM6A mutation group. Short stature and postnatal growth retardation were observed in all individuals with KDM6A mutations, but in only half of the group with MLL2 mutations., (Copyright © 2013 Wiley Periodicals, Inc.)

Published

2013

187. A unique case of de novo 5q33.3-q34 triplication with uniparental isodisomy of 5q34-qter.

Author

Fujita A, Suzumura H, Nakashima M, Tsurusaki Y, Saitsu H, Harada N, Matsumoto N, and Miyake N

Subjects

Adult, Female, Genome, Human, Gestational Age, Humans, Karyotyping, Male, Pregnancy, Real-Time Polymerase Chain Reaction, Chromosome Duplication, Chromosomes, Human, Pair 5 genetics, DNA Copy Number Variations genetics, Polymorphism, Single Nucleotide genetics, Uniparental Disomy genetics

Abstract

De novo triplication together with uniparental disomy (UPD) is a rare genomic rearrangement, and, to our knowledge, co-occurrence has previously only been reported in two individuals. We encountered a patient with a suspected karyotype of 46,XX,del(5)(q33.1q33.3),dup(5)(q31.3q33.3) or (q33.1q35.1). Genetic analysis revealed tetrasomy of 5q33.3-q34 caused by de novo middle inverted triplication and uniparental isodisomy of 5q34-qter. Most clinical features in the patient were observed in previously reported cases of duplication overlapping with 5q33.3-q34, with the exception of hearing loss. The FOXI1 gene, which causes autosomal recessive deafness (OMIM 600791, DFNB4) when mutated, was contained within the uniparental isodisomy region (5q34-qter). However, no mutations were identified following Sanger sequencing of FOXI1. This is the first report of a patient with de novo triplication together with uniparental isodisomy of chromosome 5q. As segmental isodisomy is a post-fertilization error, it is thought to have occurred during mitosis just after fertilization via a U-type exchange, while inverted duplication could have occurred during meiosis or mitosis. This study reaffirms that the single nucleotide polymorphism (SNP) array is a powerful tool to screen for UPD in a single experiment, especially in cases of isodisomy., (Copyright © 2013 Wiley Periodicals, Inc.)

Published

2013

188. Mutations in KLHL40 are a frequent cause of severe autosomal-recessive nemaline myopathy.

Author

Ravenscroft G, Miyatake S, Lehtokari VL, Todd EJ, Vornanen P, Yau KS, Hayashi YK, Miyake N, Tsurusaki Y, Doi H, Saitsu H, Osaka H, Yamashita S, Ohya T, Sakamoto Y, Koshimizu E, Imamura S, Yamashita M, Ogata K, Shiina M, Bryson-Richardson RJ, Vaz R, Ceyhan O, Brownstein CA, Swanson LC, Monnot S, Romero NB, Amthor H, Kresoje N, Sivadorai P, Kiraly-Borri C, Haliloglu G, Talim B, Orhan D, Kale G, Charles AK, Fabian VA, Davis MR, Lammens M, Sewry CA, Manzur A, Muntoni F, Clarke NF, North KN, Bertini E, Nevo Y, Willichowski E, Silberg IE, Topaloglu H, Beggs AH, Allcock RJ, Nishino I, Wallgren-Pettersson C, Matsumoto N, and Laing NG

Subjects

Amino Acid Substitution, Animals, Asian People genetics, Cohort Studies, Frameshift Mutation, Genes, Recessive, Genetic Association Studies, Genetic Predisposition to Disease, Humans, Muscle Proteins genetics, Myopathies, Nemaline ethnology, Myopathies, Nemaline pathology, Pedigree, Polymorphism, Single Nucleotide, Severity of Illness Index, Zebrafish genetics, Muscle Proteins metabolism, Muscle, Skeletal pathology, Mutation, Missense, Myopathies, Nemaline genetics

Abstract

Nemaline myopathy (NEM) is a common congenital myopathy. At the very severe end of the NEM clinical spectrum are genetically unresolved cases of autosomal-recessive fetal akinesia sequence. We studied a multinational cohort of 143 severe-NEM-affected families lacking genetic diagnosis. We performed whole-exome sequencing of six families and targeted gene sequencing of additional families. We identified 19 mutations in KLHL40 (kelch-like family member 40) in 28 apparently unrelated NEM kindreds of various ethnicities. Accounting for up to 28% of the tested individuals in the Japanese cohort, KLHL40 mutations were found to be the most common cause of this severe form of NEM. Clinical features of affected individuals were severe and distinctive and included fetal akinesia or hypokinesia and contractures, fractures, respiratory failure, and swallowing difficulties at birth. Molecular modeling suggested that the missense substitutions would destabilize the protein. Protein studies showed that KLHL40 is a striated-muscle-specific protein that is absent in KLHL40-associated NEM skeletal muscle. In zebrafish, klhl40a and klhl40b expression is largely confined to the myotome and skeletal muscle, and knockdown of these isoforms results in disruption of muscle structure and loss of movement. We identified KLHL40 mutations as a frequent cause of severe autosomal-recessive NEM and showed that it plays a key role in muscle development and function. Screening of KLHL40 should be a priority in individuals who are affected by autosomal-recessive NEM and who present with prenatal symptoms and/or contractures and in all Japanese individuals with severe NEM., (Copyright © 2013 The American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2013

189. Targeted capture and sequencing for detection of mutations causing early onset epileptic encephalopathy.

Author

Kodera H, Kato M, Nord AS, Walsh T, Lee M, Yamanaka G, Tohyama J, Nakamura K, Nakagawa E, Ikeda T, Ben-Zeev B, Lev D, Lerman-Sagie T, Straussberg R, Tanabe S, Ueda K, Amamoto M, Ohta S, Nonoda Y, Nishiyama K, Tsurusaki Y, Nakashima M, Miyake N, Hayasaka K, King MC, Matsumoto N, and Saitsu H

Subjects

Carrier Proteins genetics, Electroencephalography, Female, Genetic Testing, Humans, Male, Microarray Analysis, Microfilament Proteins genetics, Munc18 Proteins genetics, NAV1.1 Voltage-Gated Sodium Channel genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, Sequence Analysis, DNA methods, DNA Copy Number Variations genetics, Mutation genetics, Spasms, Infantile genetics

Abstract

Purpose: Early onset epileptic encephalopathies (EOEEs) are heterogeneous epileptic disorders caused by various abnormalities in causative genes including point mutations and copy number variations (CNVs). In this study, we performed targeted capture and sequencing of a subset of genes to detect point mutations and CNVs simultaneously., Methods: We designed complementary RNA oligonucleotide probes against the coding exons of 35 known and potential candidate genes. We tested 68 unrelated patients, including 15 patients with previously detected mutations as positive controls. In addition to mutation detection by the Genome Analysis Toolkit, CNVs were detected by the relative depth of coverage ratio. All detected events were confirmed by Sanger sequencing or genomic microarray analysis., Key Findings: We detected all positive control mutations. In addition, in 53 patients with EOEEs, we detected 12 pathogenic mutations, including 9 point mutations (2 nonsense, 3 splice-site, and 4 missense mutations), 2 frameshift mutations, and one 3.7-Mb microdeletion. Ten of the 12 mutations occurred de novo; the other two had been previously reported as pathogenic. The entire process of targeted capture, sequencing, and analysis required 1 week for the testing of up to 24 patients., Significance: Targeted capture and sequencing enables the identification of mutations of all classes causing EOEEs, highlighting its usefulness for rapid and comprehensive genetic testing., (Wiley Periodicals, Inc. © 2013 International League Against Epilepsy.)

Published

2013

190. Whole-exome sequencing identified a homozygous FNBP4 mutation in a family with a condition similar to microphthalmia with limb anomalies.

Author

Kondo Y, Koshimizu E, Megarbane A, Hamanoue H, Okada I, Nishiyama K, Kodera H, Miyatake S, Tsurusaki Y, Nakashima M, Doi H, Miyake N, Saitsu H, and Matsumoto N

Subjects

Exons, Family, Female, Homozygote, Humans, Intracellular Signaling Peptides and Proteins, Male, Osteonectin genetics, Pedigree, Sequence Analysis methods, Carrier Proteins genetics, Mutation, Waardenburg Syndrome genetics

Abstract

Microphthalmia with limb anomalies (MLA), also known as Waardenburg anophthalmia syndrome or ophthalmoacromelic syndrome, is a rare autosomal recessive disorder. Recently, we and others successfully identified SMOC1 as the causative gene for MLA. However, there are several MLA families without SMOC1 abnormality, suggesting locus heterogeneity in MLA. We aimed to identify a pathogenic mutation in one Lebanese family having an MLA-like condition without SMOC1 mutation by whole-exome sequencing (WES) combined with homozygosity mapping. A c.683C>T (p.Thr228Met) in FNBP4 was found as a primary candidate, drawing the attention that FNBP4 and SMOC1 may potentially modulate BMP signaling., (Copyright © 2013 Wiley Periodicals, Inc.)

Published

2013

191. Clinical spectrum of early onset epileptic encephalopathies caused by KCNQ2 mutation.

Author

Kato M, Yamagata T, Kubota M, Arai H, Yamashita S, Nakagawa T, Fujii T, Sugai K, Imai K, Uster T, Chitayat D, Weiss S, Kashii H, Kusano R, Matsumoto A, Nakamura K, Oyazato Y, Maeno M, Nishiyama K, Kodera H, Nakashima M, Tsurusaki Y, Miyake N, Saito K, Hayasaka K, Matsumoto N, and Saitsu H

Subjects

DNA Mutational Analysis, Electroencephalography, Epilepsy physiopathology, Exons genetics, Female, Genetic Testing, Humans, Infant, Infant, Newborn, Magnetic Resonance Imaging, Male, Tomography, X-Ray Computed, Epilepsy genetics, Genetic Predisposition to Disease genetics, KCNQ2 Potassium Channel genetics, Mutation genetics

Abstract

Purpose: KCNQ2 mutations have been found in patients with benign familial neonatal seizures, myokymia, or early onset epileptic encephalopathy (EOEE). In this study, we aimed to delineate the clinical spectrum of EOEE associated with KCNQ2 mutation., Methods: A total of 239 patients with EOEE, including 51 cases with Ohtahara syndrome and 104 cases with West syndrome, were analyzed by high-resolution melting (HRM) analysis or whole-exome sequencing. Detailed clinical information including electroencephalography (EEG) and brain magnetic resonance imaging (MRI) were collected from patients with KCNQ2 mutation., Key Findings: A total of nine de novo and one inherited mutations were identified (two mutations occurred recurrently). The initial seizures, which were mainly tonic seizures, occurred in the early neonatal period in all 12 patients. A suppression-burst pattern on EEG was found in most. Only three patients showed hypsarrhythmia on EEG; eight patients became seizure free when treated with carbamazepine, zonisamide, phenytoin, topiramate, or valproic acid. Although the seizures were relatively well controlled, moderate-to-profound intellectual disability was found in all except one patient who died at 3 months., Significance: De novo KCNQ2 mutations are involved in EOEE, most of which cases were diagnosed as Ohtahara syndrome. These cases showed distinct features with early neonatal onset, tonic seizures, a suppression-burst EEG pattern, infrequent evolution to West syndrome, and good response to sodium channel blockers, but poor developmental prognosis. Genetic testing for KCNQ2 should be considered for patients with EOEE., (Wiley Periodicals, Inc. © 2013 International League Against Epilepsy.)

Published

2013

192. Mutations in B3GALT6, which encodes a glycosaminoglycan linker region enzyme, cause a spectrum of skeletal and connective tissue disorders.

Author

Nakajima M, Mizumoto S, Miyake N, Kogawa R, Iida A, Ito H, Kitoh H, Hirayama A, Mitsubuchi H, Miyazaki O, Kosaki R, Horikawa R, Lai A, Mendoza-Londono R, Dupuis L, Chitayat D, Howard A, Leal GF, Cavalcanti D, Tsurusaki Y, Saitsu H, Watanabe S, Lausch E, Unger S, Bonafé L, Ohashi H, Superti-Furga A, Matsumoto N, Sugahara K, Nishimura G, and Ikegawa S

Subjects

Adult, Child, Child, Preschool, Female, Genetic Association Studies, Glycosaminoglycans biosynthesis, High-Throughput Nucleotide Sequencing, Humans, Joint Instability enzymology, Male, Osteochondrodysplasias enzymology, Sequence Analysis, DNA, Abnormalities, Multiple genetics, Galactosyltransferases genetics, Joint Instability genetics, Mutation, Missense, Osteochondrodysplasias genetics

Abstract

Proteoglycans (PGs) are a major component of the extracellular matrix in many tissues and function as structural and regulatory molecules. PGs are composed of core proteins and glycosaminoglycan (GAG) side chains. The biosynthesis of GAGs starts with the linker region that consists of four sugar residues and is followed by repeating disaccharide units. By exome sequencing, we found that B3GALT6 encoding an enzyme involved in the biosynthesis of the GAG linker region is responsible for a severe skeletal dysplasia, spondyloepimetaphyseal dysplasia with joint laxity type 1 (SEMD-JL1). B3GALT6 loss-of-function mutations were found in individuals with SEMD-JL1 from seven families. In a subsequent candidate gene study based on the phenotypic similarity, we found that B3GALT6 is also responsible for a connective tissue disease, Ehlers-Danlos syndrome (progeroid form). Recessive loss-of-function mutations in B3GALT6 result in a spectrum of disorders affecting a broad range of skeletal and connective tissues characterized by lax skin, muscle hypotonia, joint dislocation, and spinal deformity. The pleiotropic phenotypes of the disorders indicate that B3GALT6 plays a critical role in a wide range of biological processes in various tissues, including skin, bone, cartilage, tendon, and ligament., (Copyright © 2013 The American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2013

193. Exome sequencing identifies a novel INPPL1 mutation in opsismodysplasia.

Author

Iida A, Okamoto N, Miyake N, Nishimura G, Minami S, Sugimoto T, Nakashima M, Tsurusaki Y, Saitsu H, Shiina M, Ogata K, Watanabe S, Ohashi H, Matsumoto N, and Ikegawa S

Subjects

Amino Acid Sequence, Asian People genetics, Child, Exome, Female, Genetic Heterogeneity, Homozygote, Humans, Japan, Molecular Sequence Data, Pedigree, Phenotype, Phosphatidylinositol-3,4,5-Trisphosphate 5-Phosphatases, Gene Deletion, Osteochondrodysplasias genetics, Phosphoric Monoester Hydrolases genetics, Sequence Analysis, DNA methods

Abstract

Opsismodysplasia is an autosomal recessive skeletal disorder characterized by facial dysmorphism, micromelia, platyspondyly and retarded bone maturation. Recently, mutations in the gene encoding inositol polyphosphate phosphatase-like 1 (INPPL1) are found in several families with opsismodysplasia by a homozygosity mapping, followed by whole genome sequencing. We performed an exome sequencing in two unrelated Japanese families with opsismodysplasia and identified a novel INPPL1 mutation, c.1960_1962delGAG, in one family. The mutation is predicted to result in an in-frame deletion (p.E654del) within the central catalytic 5-phosphate domain. Our results further support that INPPL1 is the disease gene for opsismodysplasia and that opsismodysplasia has genetic heterogeneity.

Published

2013

194. Clinical correlations of mutations affecting six components of the SWI/SNF complex: detailed description of 21 patients and a review of the literature.

Author

Kosho T, Okamoto N, Ohashi H, Tsurusaki Y, Imai Y, Hibi-Ko Y, Kawame H, Homma T, Tanabe S, Kato M, Hiraki Y, Yamagata T, Yano S, Sakazume S, Ishii T, Nagai T, Ohta T, Niikawa N, Mizuno S, Kaname T, Naritomi K, Narumi Y, Wakui K, Fukushima Y, Miyatake S, Mizuguchi T, Saitsu H, Miyake N, and Matsumoto N

Subjects

Chromosomal Proteins, Non-Histone genetics, DNA Helicases genetics, DNA-Binding Proteins genetics, Facies, Female, Genetic Association Studies, Humans, Male, Mutation, Nuclear Proteins genetics, SMARCB1 Protein, Syndrome, Abnormalities, Multiple genetics, Chromatin Assembly and Disassembly genetics, Face abnormalities, Foot Deformities, Congenital genetics, Hand Deformities, Congenital genetics, Hypotrichosis genetics, Intellectual Disability genetics, Micrognathism genetics, Neck abnormalities, Transcription Factors genetics

Abstract

Mutations in the components of the SWItch/sucrose nonfermentable (SWI/SNF)-like chromatin remodeling complex have recently been reported to cause Coffin-Siris syndrome (CSS), Nicolaides-Baraitser syndrome (NCBRS), and ARID1B-related intellectual disability (ID) syndrome. We detail here the genotype-phenotype correlations for 85 previously published and one additional patient with mutations in the SWI/SNF complex: four with SMARCB1 mutations, seven with SMARCA4 mutations, 37 with SMARCA2 mutations, one with an SMARCE1 mutation, three with ARID1A mutations, and 33 with ARID1B mutations. The mutations were associated with syndromic ID and speech impairment (severe/profound in SMARCB1, SMARCE1, and ARID1A mutations; variable in SMARCA4, SMARCA2, and ARID1B mutations), which was frequently accompanied by agenesis or hypoplasia of the corpus callosum. SMARCB1 mutations caused "classical" CSS with typical facial "coarseness" and significant digital/nail hypoplasia. SMARCA4 mutations caused CSS without typical facial coarseness and with significant digital/nail hypoplasia. SMARCA2 mutations caused NCBRS, typically with short stature, sparse hair, a thin vermillion of the upper lip, an everted lower lip and prominent finger joints. A SMARCE1 mutation caused CSS without typical facial coarseness and with significant digital/nail hypoplasia. ARID1A mutations caused the most severe CSS with severe physical complications. ARID1B mutations caused CSS without typical facial coarseness and with mild digital/nail hypoplasia, or caused syndromic ID. Because of the common underlying mechanism and overlapping clinical features, we propose that these conditions be referred to collectively as "SWI/SNF-related ID syndromes"., (Copyright © 2013 Wiley Periodicals, Inc.)

Published

2013

195. Increase in the Size of an Intracardiac Thrombus during Dabigatran Therapy (110 mg b.i.d.) in an Acute Cardioembolic Stroke Patient.

Author

Tabata E, Yasaka M, Wakugawa Y, Komori M, Mori K, Tsurusaki Y, Kokuba K, Sambongi Y, Maeda K, and Okada Y

Abstract

We report a case of atrial fibrillation in a patient in whom a mobile thrombus in the left atrial appendage increased in size after low-dose dabigatran therapy. A 74-year-old man was admitted to our hospital because of sudden onset of right hemiplasia and dysarthria. On admission, his National Institutes of Health Stroke Scale score was three. Axial diffusion-weighted magnetic resonance images and magnetic resonance angiography images showed hyperintense signals in the left front-parietal cerebral cortex without any intracranial stenotic lesions, and acute cardioembolic stroke associated with nonvalvular atrial fibrillation was diagnosed. Transesophageal echocardiography revealed a mobile thrombosis (1.0 × 2.2 cm) in the left atrial appendage, and dabigatran therapy (110 mg b.i.d.) was initiated to prevent stroke recurrence. Transesophageal echocardiography performed 6 days later revealed that the size of the thrombus had increased to 1.5 × 3.0 cm. Medication was changed to warfarin, and the thrombosis subsequently decreased in size. The patient did not have a recurrent stroke and was discharged with a National Institutes of Health Stroke Scale score of zero. This case demonstrates that low-dose dabigatran may not be effective in reducing the size of a thrombus.

Published

2013

196. De novo mutations in the autophagy gene WDR45 cause static encephalopathy of childhood with neurodegeneration in adulthood.

Author

Saitsu H, Nishimura T, Muramatsu K, Kodera H, Kumada S, Sugai K, Kasai-Yoshida E, Sawaura N, Nishida H, Hoshino A, Ryujin F, Yoshioka S, Nishiyama K, Kondo Y, Tsurusaki Y, Nakashima M, Miyake N, Arakawa H, Kato M, Mizushima N, and Matsumoto N

Subjects

Adult, Child, Female, High-Throughput Nucleotide Sequencing, Humans, Iron metabolism, Lennox Gastaut Syndrome, Magnetic Resonance Imaging, Phenotype, Autophagy, Carrier Proteins genetics, Exome genetics, Intellectual Disability etiology, Mutation genetics, Neurodegenerative Diseases etiology, Spasms, Infantile etiology

Abstract

Static encephalopathy of childhood with neurodegeneration in adulthood (SENDA) is a recently established subtype of neurodegeneration with brain iron accumulation (NBIA). By exome sequencing, we found de novo heterozygous mutations in WDR45 at Xp11.23 in two individuals with SENDA, and three additional WDR45 mutations were identified in three other subjects by Sanger sequencing. Using lymphoblastoid cell lines (LCLs) derived from the subjects, aberrant splicing was confirmed in two, and protein expression was observed to be severely impaired in all five. WDR45 encodes WD-repeat domain 45 (WDR45). WDR45 (also known as WIPI4) is one of the four mammalian homologs of yeast Atg18, which has an important role in autophagy. Lower autophagic activity and accumulation of aberrant early autophagic structures were demonstrated in the LCLs of the affected subjects. These findings provide direct evidence that an autophagy defect is indeed associated with a neurodegenerative disorder in humans.

Published

2013

197. A novel SCARB2 mutation causing late-onset progressive myoclonus epilepsy.

Author

Higashiyama Y, Doi H, Wakabayashi M, Tsurusaki Y, Miyake N, Saitsu H, Ohba C, Fukai R, Miyatake S, Joki H, Koyano S, Suzuki Y, Tanaka F, Kuroiwa Y, and Matsumoto N

Subjects

Age of Onset, Aged, Female, Genetic Predisposition to Disease, Humans, Male, Middle Aged, Myoclonic Epilepsies, Progressive diagnosis, Pedigree, Lysosomal Membrane Proteins genetics, Mutation genetics, Myoclonic Epilepsies, Progressive genetics, Myoclonus pathology, Receptors, Scavenger genetics

Published

2013

198. Mitochondrial complex III deficiency caused by a homozygous UQCRC2 mutation presenting with neonatal-onset recurrent metabolic decompensation.

Author

Miyake N, Yano S, Sakai C, Hatakeyama H, Matsushima Y, Shiina M, Watanabe Y, Bartley J, Abdenur JE, Wang RY, Chang R, Tsurusaki Y, Doi H, Nakashima M, Saitsu H, Ogata K, Goto Y, and Matsumoto N

Subjects

ATPases Associated with Diverse Cellular Activities, Acidosis, Lactic genetics, Adult, Blotting, Western, Electron Transport Complex III deficiency, Exome, Female, Genetic Linkage, Humans, Hyperammonemia genetics, Hypoglycemia genetics, Ketosis genetics, Male, Membrane Proteins genetics, Mitochondria genetics, Mitochondrial Proteins genetics, Pedigree, Protein Conformation, Sequence Analysis, DNA, Electron Transport Complex III genetics, Homozygote, Mitochondrial Diseases diagnosis, Mitochondrial Diseases genetics, Mutation, Missense

Abstract

Mitochondrial complex III (CIII) deficiency is a relatively rare disease with high clinical and genetic heterogeneity. CIII comprises 11 subunits encoded by one mitochondrial and 10 nuclear genes. Abnormalities of the nuclear genes such as BCS1L and TTC19 encoding mitochondrial assembly factors are well known, but an explanation of the majority of CIII deficiency remains elusive. Here, we report three patients from a consanguineous Mexican family presenting with neonatal onset of hypoglycemia, lactic acidosis, ketosis, and hyperammonemia. We found a homozygous missense mutation in UQCRC2 that encodes mitochondrial ubiquinol-cytochrome c reductase core protein II by whole-exome sequencing combined with linkage analysis. On the basis of structural modeling, the mutation (p.Arg183Trp) was predicted to destabilize the hydrophobic core at the subunit interface of the core protein II homodimer. In vitro studies using fibroblasts from the index patient clearly indicated CIII deficiency, as well as impaired assembly of the supercomplex formed from complexes I, III, and IV. This is the first described human disease caused by a core protein abnormality in mitochondrial CIII., (© 2012 Wiley Periodicals, Inc.)

Published

2013

199. The diagnostic utility of exome sequencing in Joubert syndrome and related disorders.

Author

Tsurusaki Y, Kobayashi Y, Hisano M, Ito S, Doi H, Nakashima M, Saitsu H, Matsumoto N, and Miyake N

Subjects

Abnormalities, Multiple, Cerebellar Diseases genetics, Cerebellum abnormalities, Eye Abnormalities genetics, Female, Humans, Kidney Diseases, Cystic genetics, Magnetic Resonance Imaging, Male, Pedigree, Retina abnormalities, Reverse Transcriptase Polymerase Chain Reaction, Cerebellar Diseases diagnosis, Exome, Eye Abnormalities diagnosis, Kidney Diseases, Cystic diagnosis, Sequence Analysis, DNA

Abstract

Joubert syndrome (JS) and related disorders (JSRD) are autosomal recessive and X-linked disorders characterized by hypoplasia of the cerebellar vermis with a characteristic 'molar tooth sign' on brain imaging and accompanying neurological symptoms including episodic hyperpnoea, abnormal eye movements, ataxia and intellectual disability. JSRD are clinically and genetically heterogeneous, and, to date, a total of 17 causative genes are known. We applied whole-exome sequencing (WES) to five JSRD families and found mutations in all: either CEP290, TMEM67 or INPP5E was mutated. Compared with conventional Sanger sequencing, WES appears to be advantageous with regard to speed and cost, supporting its potential utility in molecular diagnosis.

Published

2013

200. Identification of a novel homozygous SPG7 mutation in a Japanese patient with spastic ataxia: making an efficient diagnosis using exome sequencing for autosomal recessive cerebellar ataxia and spastic paraplegia.

Author

Doi H, Ohba C, Tsurusaki Y, Miyatake S, Miyake N, Saitsu H, Kawamoto Y, Yoshida T, Koyano S, Suzuki Y, Kuroiwa Y, Tanaka F, and Matsumoto N

Subjects

ATPases Associated with Diverse Cellular Activities, Exome genetics, Homozygote, Humans, Intellectual Disability diagnosis, Male, Middle Aged, Muscle Spasticity diagnosis, Optic Atrophy diagnosis, Paraplegia diagnosis, Pedigree, Sequence Analysis, DNA methods, Spastic Paraplegia, Hereditary diagnosis, Spinocerebellar Ataxias diagnosis, Asian People genetics, Intellectual Disability genetics, Metalloendopeptidases genetics, Muscle Spasticity genetics, Mutation genetics, Optic Atrophy genetics, Paraplegia genetics, Spastic Paraplegia, Hereditary genetics, Spinocerebellar Ataxias genetics

Abstract

Autosomal recessive cerebellar ataxias and autosomal recessive hereditary spastic paraplegias are clinically and genetically heterogeneous disorders with diverse neurological and non-neurological features. We herein describe a Japanese patient with a slowly progressive form of ataxia and spastic paraplegia. Using whole exome sequencing, we identified a novel homozygous frameshift mutation in SPG7, encoding paraplegin, in this patient. This is the first report of an SPG7 mutation in the Japanese population. For disorders previously undetected in a particular population, or unrecognized/atypical phenotypes, exome sequencing may facilitate molecular diagnosis.

Published

2013