Your search keyword '"Yu-ichi Goto"' showing total 667 results

51. Re-evaluation of soluble APP-α and APP-β in cerebrospinal fluid as potential biomarkers for early diagnosis of dementia disorders

Author

Kazutomi Kanemaru, Kenji Ishii, Yuko Saito, Masuhiro Sakata, Kotaro Hattori, Wataru Araki, Masahiro Nagao, Yoshie Omachi, Yuma Yokoi, Hidehiro Mizusawa, Hiroshi Matsuda, Yumiko M. Araki, Sumiko Yoshida, Shigeo Murayama, Yu-ichi Goto, Harumasa Takano, Utako Nagaoka, Hiroshi Kunugi, Hisateru Tachimori, Tadashi Tsukamoto, Kunimasa Arima, Takashi Komori, and Miho Murata

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, Pathology, Clinical Biochemistry, Disease, 03 medical and health sciences, Dementia disorders, Soluble amyloid precursor protein, 0302 clinical medicine, Cerebrospinal fluid, Internal medicine, mental disorders, Amyloid precursor protein, Medicine, Dementia, Pathological, biology, business.industry, Research, Biochemistry (medical), lcsh:RM1-950, Mild cognitive impairment, Biomarker, medicine.disease, 030104 developmental biology, lcsh:Therapeutics. Pharmacology, Potential biomarkers, biology.protein, Molecular Medicine, Biomarker (medicine), Tau, business, Alzheimer’s disease, 030217 neurology & neurosurgery

Abstract

Background Because soluble (or secreted) amyloid precursor protein-β (sAPPβ) and -α (sAPPα) possibly reflect pathological features of Alzheimer’s disease (AD), they are potential biomarker candidates for dementia disorders, including AD and mild cognitive impairment (MCI) due to AD (MCI-AD). However, controversial results have been reported regarding their alterations in the cerebrospinal fluid (CSF) of AD and MCI-AD patients. In this study, we re-assessed the utility of sAPPα and sAPPβ in CSF as diagnostic biomarkers of dementia disorders. Methods We used a modified and sensitive detection method to analyze sAPPs levels in CSF in four groups of patients: AD (N = 33), MCI-AD (N = 17), non-AD dementia (N = 27), and disease controls (N = 19). Phosphorylated tau (p-tau), total tau, and Aβ42 were also analyzed using standard methods. Results A strong correlation was observed between sAPPα and sAPPβ, consistent with previous reports. Both sAPPα and sAPPβ were highly correlated with p-tau and total tau, suggesting that sAPPs possibly reflect neuropathological changes in the brain. Levels of sAPPα were significantly higher in MCI-AD cases compared with non-AD and disease control cases, and those of sAPPβ were also significantly higher in MCI-AD and AD cases relative to other cases. A logistic regression analysis indicated that sAPPα and sAPPβ have good discriminative power for the diagnosis of MCI-AD. Conclusions Our findings collectively suggest that both sAPPs are pathologically relevant and potentially useful biomarkers for early and accurate diagnosis of dementia disorders. We also suggest that careful measurement is important in assessing the diagnostic utility of CSF sAPPs. Electronic supplementary material The online version of this article (10.1186/s40364-017-0108-5) contains supplementary material, which is available to authorized users.

Published

2017

52. PTPRQ as a potential biomarker for idiopathic normal pressure hydrocephalus

Author

Kotaro Hattori, Sumiko Yoshida, Yuki Nagata, Shumpei Niida, Saiko Sugiura, Masahiro Kamita, Masaya Ono, Yu-ichi Goto, Katsuya Urakami, and Masahiko Bundo

Subjects

0301 basic medicine, Male, Cancer Research, Pathology, medicine.medical_specialty, Urinary incontinence, Disease, Biology, Biochemistry, Gastroenterology, cerebrospinal fluid, 03 medical and health sciences, Mice, 0302 clinical medicine, Cerebrospinal fluid, Hearing, Internal medicine, Genetics, medicine, Dementia, Animals, Humans, Molecular Biology, PTPRQ, Aged, diagnostic marker, Receptor-Like Protein Tyrosine Phosphatases, Class 3, Brain, Reproducibility of Results, Articles, medicine.disease, Hydrocephalus, Normal Pressure, Hydrocephalus, shunt non-responder, 030104 developmental biology, Oncology, Potential biomarkers, (Idiopathic) normal pressure hydrocephalus, Molecular Medicine, Biomarker (medicine), Audiometry, Pure-Tone, Female, medicine.symptom, idiopathic normal pressure hydrocephalus, 030217 neurology & neurosurgery, Biomarkers

Abstract

Idiopathic normal pressure hydrocephalus (iNPH) is caused by the accumulation of cerebrospinal fluid (CSF) and is characterized by gait disturbance, urinary incontinence, and dementia. iNPH dementia is treatable by shunt operation; however, since the cognitive symptoms of iNPH are often similar to those of other dementias, including Alzheimer's disease (AD), accurate diagnosis of iNPH is difficult. To overcome this problem, the identification of novel diagnostic markers to distinguish iNPH and AD is warranted. Using comparative proteomic analysis of CSF from patients with iNPH and AD, protein tyrosine phosphatase receptor type Q (PTPRQ) was identified as a candidate biomarker protein for discriminating iNPH from AD. ELISA analysis indicated that the PTPRQ concentration in the CSF was significantly higher in patients with iNPH compared with those with AD. In addition, the PTPRQ concentration in the CSF of non-responders to shunt operation (SNRs) tended to be relatively lower compared with that in the responders. PTPRQ may be a useful biomarker for discriminating between patients with iNPH and AD, and may be a potential companion biomarker to identify SNRs among patients with iNPH. Additional large-scale analysis may aid in understanding the novel aspects of iNPH.

Published

2017

53. Pathologic Active mTOR Mutation in Brain Malformation with Intractable Epilepsy Leads to Cell-Autonomous Migration Delay

Author

Shin-ichi Horike, Kenji Sugai, Yuko Saito, Masayuki Itoh, Taisuke Otsuki, Yu-ichi Goto, Mikio Hoshino, Masayuki Sasaki, Tomoo Owa, Schuichi Koizumi, Akio Takahashi, Sae Hanai, Eiji Nakagawa, Naoki Ikegaya, Sayuri Sukigara, Takashi Saito, Noriko Sato, Takanobu Kaido, and Hongmei Dai

Subjects

0301 basic medicine, Drug Resistant Epilepsy, Pathology, medicine.medical_specialty, Hemimegalencephaly, Biology, Transfection, medicine.disease_cause, Pathology and Forensic Medicine, Mice, 03 medical and health sciences, Tuberous sclerosis, 0302 clinical medicine, Germline mutation, Positron Emission Tomography Computed Tomography, medicine, Animals, Humans, Mutation frequency, Cells, Cultured, PI3K/AKT/mTOR pathway, Mutation, TOR Serine-Threonine Kinases, Infant, Electroencephalography, Cell migration, Cortical dysplasia, medicine.disease, Up-Regulation, 030104 developmental biology, Female, Malformations of Cortical Development, Group II, 030217 neurology & neurosurgery

Abstract

The activation of phosphatidylinositol 3-kinase–AKTs–mammalian target of rapamycin cell signaling pathway leads to cell overgrowth and abnormal migration and results in various types of cortical malformations, such as hemimegalencephaly (HME), focal cortical dysplasia, and tuberous sclerosis complex. However, the pathomechanism underlying abnormal cell migration remains unknown. With the use of fetal mouse brain, we performed causative gene analysis of the resected brain tissues from a patient with HME and investigated the pathogenesis. We obtained a novel somatic mutation of the MTOR gene, having approximately 11% and 7% mutation frequency in the resected brain tissues. Moreover, we revealed that the MTOR mutation resulted in hyperphosphorylation of its downstream molecules, S6 and 4E-binding protein 1, and delayed cell migration on the radial glial fiber and did not affect other cells. We suspect cell-autonomous migration arrest on the radial glial foot by the active MTOR mutation and offer potential explanations for why this may lead to cortical malformations such as HME.

Published

2017

54. Respiratory Chain Complex Disorganization Impairs Mitochondrial and Cellular Integrity

Author

Hideyuki Hatakeyama and Yu-ichi Goto

Subjects

0301 basic medicine, biology, Respiratory chain complex, Skeletal muscle, Mitochondrion, medicine.disease_cause, Pathology and Forensic Medicine, Cell biology, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, Mitochondrial respiratory chain, Biochemistry, medicine, biology.protein, DNAJA3, Myocyte, Cytochrome c oxidase, Oxidative stress

Abstract

The relationships between the molecular abnormalities in mitochondrial respiratory chain complexes and their negative contributions to mitochondrial and cellular functions have been proved to be essential for better understandings in mitochondrial medicine. Herein, we established the method to identify disease phenotypic differences among patients with muscle histopathological cytochrome c oxidase (COX) deficiency, as one of the representative clinical features in mitochondrial diseases, by using patients' myoblasts that are derived from biopsied skeletal muscle tissues. We identified two obviously different severities in molecular diagnostic criteria of COX deficiency among patients: structurally stable, but functionally mild/moderate defect and severe functional defect with the disrupted COX holoenzyme structure. COX holoenzyme disorganization actually triggered several mitochondrial dysfunctions, including the decreased ATP level, the increased oxidative stress level, and the damaged membrane potential level, all of which lead to the deteriorated cellular growth, the accelerated cellular senescence, and the induced apoptotic cell death. Our cell-based in vitro diagnostic approaches would be widely applicable to understanding patient-specific pathomechanism in various types of mitochondrial diseases, including other respiratory chain complex deficiencies and other mitochondrial metabolic enzyme deficiencies.

Published

2017

55. Correction to: DNA analysis of benign adult familial myoclonic epilepsy reveals associations between the pathogenic TTTCA repeat insertion in SAMD12 and the nonpathogenic TTTTA repeat expansion in TNRC6A

Author

Teiichi Onuma, Shin-Ichi Niwa, Akira Sano, Sunao Kaneko, Izumi Yokoyama, Yu-ichi Goto, Takeshi Yasuda, Yuko Yamagishi, Misa Nakano, Rumiko Kan, Yoshihiko Furusawa, Akane Terasaki, Ohiko Hashimoto, Kazumaru Wada, Hanae Hiwatashi, Masayuki Nakamura, Osamu Komure, and Yuka Urata

Subjects

0301 basic medicine, Genetics, Benign adult familial myoclonic epilepsy, business.industry, Autosomal dominant trait, 030105 genetics & heredity, Genetic analysis, 03 medical and health sciences, 030104 developmental biology, Anticipation (genetics), medicine, Allele, medicine.symptom, Trinucleotide repeat expansion, business, Myoclonus, Genetics (clinical), Southern blot

Abstract

Benign adult familial myoclonic epilepsy (BAFME) is an autosomal dominant disease characterized by adult-onset tremulous hand movement, myoclonus, and infrequent epileptic seizures. Recently, intronic expansion of unstable TTTCA/TTTTA pentanucleotide repeats in SAMD12, TNRC6A, or RAPGEF2 was identified as pathological mutations in Japanese BAFME pedigrees. To confirm these mutations, we performed a genetic analysis on 12 Japanese BAFME pedigrees. A total of 143 participants, including 43 familial patients, 5 suspected patients, 3 sporadic nonfamilial patients, 22 unaffected familial members, and 70 unrelated controls, were screened for expanded abnormal pentanucleotide repeats in SAMD12, TNRC6A, RAPGEF2, YEAT2, MARCH6, and STARD7. DNA samples were analyzed using Southern blotting, long-range polymerase chain reaction (PCR), repeat-primed PCR, and long-range PCR followed by Southern blotting. Of the 51 individuals with clinically diagnosed or suspected BAFME, 49 carried a SAMD12 allele with an expanded TTTCA/TTTTA pentanucleotide repeat. Genetic and clinical anticipation was observed. As in previous reports, the one patient with homozygous mutant alleles showed more severe symptoms than the heterozygous carriers. In addition, screening for expanded pentanucleotide repeats in TNRC6A revealed that the frequency of expanded TTTTA repeat alleles in the BAFME group was significantly higher than in the control group. All patients who were clinically diagnosed with BAFME, including those in the original family reported by Yasuda, carried abnormally expanded TTTCA/TTTTA repeat alleles of SAMD12. Patients with BAFME also frequently carried a TTTTA repeat expansion in TNRC6A, suggesting that there may be unknown factors in the ancestry of patients with BAFME that make pentanucleotide repeats unstable.

Published

2020

56. Myoclonic Epilepsy with Ragged-red Fibers with Intranuclear Inclusions.

Author

Tomoya Kawazoe, Shinsuke Tobisawa, Keizo Sugaya, Akinori Uruha, Kazuhito Miyamoto, Takashi Komori, Yu-ichi Goto, Ichizo Nishino, Hiroshi Yoshihashi, Takeshi Mizuguchi, Naomichi Matsumoto, Naohiro Egawa, Akihiro Kawata, and Eiji Isozaki

Published

2022

57. Altered Expression of Astrocyte-Related Receptors and Channels Correlates With Epileptogenesis in Hippocampal Sclerosis

Author

Yu-ichi Goto, Taisuke Otsuki, Takanobu Kaido, Yoshinori Aoki, Sayuri Sukigara, Akira Oka, Sae Hanai, Kenji Sugai, Takashi Saito, Akio Takahashi, Yuu Kaneko, Masayuki Sasaki, Naoki Ikegaya, Eiji Nakagawa, Masaki Iwasaki, and Masayuki Itoh

Subjects

0301 basic medicine, Adult, Male, Potassium Channels, Adolescent, Immunoblotting, Intractable epilepsy, Receptors, Metabotropic Glutamate, Epileptogenesis, Hippocampus, Pathology and Forensic Medicine, 03 medical and health sciences, Young Adult, 0302 clinical medicine, medicine, Humans, Receptor, Child, Hippocampal sclerosis, Epilepsy, Sclerosis, business.industry, General Medicine, medicine.disease, Immunohistochemistry, Astrogliosis, Up-Regulation, 030104 developmental biology, medicine.anatomical_structure, Astrocytes, Case-Control Studies, Child, Preschool, Receptors, Purinergic P2Y, Pediatrics, Perinatology and Child Health, business, Neuroscience, 030217 neurology & neurosurgery, Biomarkers, Astrocyte, Signal Transduction

Abstract

Background Hippocampal sclerosis (HS) is one of the major causes of intractable epilepsy. Astrogliosis in epileptic brain is a peculiar condition showing epileptogenesis and is thought to be different from the other pathological conditions. The aim of this study is to investigate the altered expression of astrocytic receptors, which contribute to neurotransmission in the synapse, and channels in HS lesions. Methods We performed immunohistochemical and immunoblotting analyses of the P2RY1, P2RY2, P2RY4, Kir4.1, Kv4.2, mGluR1, and mGluR5 receptors and channels with the brain samples of 20 HS patients and 4 controls and evaluated the ratio of immunopositive cells and those expression levels. Results The ratio of each immunopositive cell per glial fibrillary acidic protein-positive astrocytes and the expression levels of all 7 astrocytic receptors and channels in HS lesions were significantly increased. We previously described unique astrogliosis in epileptic lesions similar to what was observed in this study. Conclusion This phenomenon is considered to trigger activation of the related signaling pathways and then contribute to epileptogenesis. Thus, astrocytes in epileptic lesion may show self-hyperexcitability and contribute to epileptogenesis through the endogenous astrocytic receptors and channels. These findings may suggest novel astrocytic receptor-related targets for the pharmacological treatment of epilepsy.

Published

2019

58. Gene suppressing therapy for Pelizaeus-Merzbacher disease using artificial microRNA

Author

Kazuhisa Sakai, Hitomi Izumi, Hironori Okada, Ken Inoue, Sadafumi Suzuki, Yu-ichi Goto, Noritaka Ichinohe, Yukiko Matsushima, Heng Li, and Takashi Okada

Subjects

0301 basic medicine, Proteolipid protein 1, Pelizaeus-Merzbacher Disease, Genetic enhancement, Gene Dosage, Gene Expression, Mice, Transgenic, Biology, Mice, 03 medical and health sciences, Myelin, 0302 clinical medicine, Gene duplication, microRNA, Gene expression, medicine, Animals, Humans, Myelin Proteolipid Protein, Gene, Base Sequence, Cell Death, Brain, Pelizaeus–Merzbacher disease, General Medicine, medicine.disease, Cell biology, Disease Models, Animal, MicroRNAs, Oligodendroglia, Phenotype, 030104 developmental biology, medicine.anatomical_structure, Gene Knockdown Techniques, 030220 oncology & carcinogenesis, Research Article

Abstract

Copy number increase or decrease of certain dosage-sensitive genes may cause genetic diseases with distinct phenotypes, conceptually termed genomic disorders. The most common cause of Pelizaeus-Merzbacher disease (PMD), an X-linked hypomyelinating leukodystrophy, is genomic duplication encompassing the entire proteolipid protein 1 (PLP1) gene. Although the exact molecular and cellular mechanisms underlying PLP1 duplication, which causes severe hypomyelination in the central nervous system, remain largely elusive, PLP1 overexpression is likely the fundamental cause of this devastating disease. Here, we investigated if adeno-associated virus–mediated (AAV-mediated) gene-specific suppression may serve as a potential cure for PMD by correcting quantitative aberrations in gene products. We developed an oligodendrocyte-specific Plp1 gene suppression therapy using artificial microRNA under the control of human CNP promoter in a self-complementary AAV (scAAV) platform. A single direct brain injection achieved widespread oligodendrocyte-specific Plp1 suppression in the white matter of WT mice. AAV treatment in Plp1-transgenic mice, a PLP1 duplication model, ameliorated cytoplasmic accumulation of Plp1, preserved mature oligodendrocytes from degradation, restored myelin structure and gene expression, and improved survival and neurological phenotypes. Together, our results provide evidence that AAV-mediated gene suppression therapy can serve as a potential cure for PMD resulting from PLP1 duplication and possibly for other genomic disorders.

Published

2019

59. A novel compound heterozygous variant of ECHS1 identified in a Japanese patient with Leigh syndrome

Author

Atsushi Sato, Masakazu Mimaki, Yu-ichi Goto, Shumpei Uchino, Aritoshi Iida, Ichizo Nishino, and Keiko Ishikawa

Subjects

chemistry.chemical_classification, 0303 health sciences, lcsh:QH426-470, Disease genetics, 030305 genetics & heredity, lcsh:Life, Metabolism, Mitochondrion, Compound heterozygosity, Biochemistry, Molecular biology, Amino acid, lcsh:Genetics, lcsh:QH501-531, 03 medical and health sciences, chemistry, ECHS1, Genetics research, Genetics, Data Report, Molecular Biology, Exome sequencing, 030304 developmental biology

Abstract

Leigh syndrome (LS) is a heterogeneous neurodegenerative disorder caused by mitochondrial dysfunction. Certain LS cases have mutations in ECHS1, which encodes a short-chain enoyl-CoA hydratase involved in the metabolism of fatty acids and branched-chain amino acids in mitochondria. Using exome sequencing, we diagnosed a Japanese patient with LS and identified the patient as a compound heterozygote for a novel variant of ECHS1, consisting of NM_004092.4:c.23T>C (p.Leu8Pro) and NM_004092.4:c.176A>G (p.Asn59Ser).

Published

2019

60. A unique Japanese CPEO family with a novel homozygous m.14819 T G (p. S25A) substitution

Author

Yu ichi Goto, Yasuyuki Ohta, Ryo Sasaki, Mami Takemoto, Koji Abe, Yoshiaki Takahashi, Nozomi Hishikawa, Toru Yamashita, Kota Sato, Emi Nomura, and Koh Tadokoro

Subjects

Aged, 80 and over, Male, Mitochondrial DNA, Ophthalmoplegia, Chronic Progressive External, Substitution (logic), Homozygote, Biology, Middle Aged, Molecular biology, DNA, Mitochondrial, Pedigree, CPEO, chemistry.chemical_compound, Neurology, chemistry, Japan, Humans, Female, Neurology (clinical), Homozygous, DNA

Published

2019

61. Chemical reversal of abnormalities in cells carrying mitochondrial DNA mutations

Author

Hiroyuki Osada, Yu-ichi Goto, Haruna Nishimura, Minoru Yoshida, Yuri Tomabechi, Hiroki Kobayashi, Mikako Shirouzu, Hideyuki Hatakeyama, Sadafumi Suzuki, Mutsumi Yokota, and Masakazu Mimaki

Subjects

Mitochondrial DNA, Mitochondrial Diseases, Mitochondrial disease, Phosphofructokinase-1, Mutant, Cell Respiration, Induced Pluripotent Stem Cells, Oxidative phosphorylation, Mitochondrion, AMP-Activated Protein Kinases, medicine.disease_cause, DNA, Mitochondrial, Oxidative Phosphorylation, Pentose Phosphate Pathway, 03 medical and health sciences, medicine, Humans, Glycolysis, Induced pluripotent stem cell, Molecular Biology, 030304 developmental biology, Neurons, 0303 health sciences, Mutation, Chemistry, Chimera, 030302 biochemistry & molecular biology, Cell Differentiation, Cell Biology, Fibroblasts, medicine.disease, Amides, Cell biology, Mitochondria, HEK293 Cells, Gene Expression Regulation, Carbolines, HeLa Cells

Abstract

Mitochondrial DNA (mtDNA) mutations are the major cause of mitochondrial diseases. Cells harboring disease-related mtDNA mutations exhibit various phenotypic abnormalities, such as reduced respiration and elevated lactic acid production. Induced pluripotent stem cell (iPSC) lines derived from patients with mitochondrial disease, with high proportions of mutated mtDNA, exhibit defects in maturation into neurons or cardiomyocytes. In this study, we have discovered a small-molecule compound, which we name tryptolinamide (TLAM), that activates mitochondrial respiration in cybrids generated from patient-derived mitochondria and fibroblasts from patient-derived iPSCs. We found that TLAM inhibits phosphofructokinase-1 (PFK1), which in turn activates AMPK-mediated fatty-acid oxidation to promote oxidative phosphorylation, and redirects carbon flow from glycolysis toward the pentose phosphate pathway to reinforce anti-oxidative potential. Finally, we found that TLAM rescued the defect in neuronal differentiation of iPSCs carrying a high ratio of mutant mtDNA, suggesting that PFK1 represents a potential therapeutic target for mitochondrial diseases.

Published

2019

62. Different X-linkedKDM5Cmutations in affected male siblings: is maternal reversion error involved?

Author

Naomichi Matsumoto, Yasuo Hachiya, Yu-ichi Goto, Ken Inoue, Eiji Kurihara, Eiji Nakagawa, Atsushi Fujita, Eri Takeshita, Chikako Waga, Satoko Kumada, Satoko Miyatake, Noriko Miyake, Hirotomo Saitsu, Yoshinori Tsurusaki, and Mitsuko Nakashima

Subjects

0301 basic medicine, Genetics, Early embryonic stage, Somatic cell, Haplotype, Reversion, Biology, medicine.disease, Germline, 03 medical and health sciences, 030104 developmental biology, Germline mutation, Intellectual disability, medicine, Gene, Genetics (clinical)

Abstract

Genetic reversion is the phenomenon of spontaneous gene correction by which gene function is partially or completely rescued. However, it is unknown whether this mechanism always correctly repairs mutations, or is prone to error. We investigated a family of three boys with intellectual disability, and among them we identified two different mutations in KDM5C, located at Xp11.22, using whole-exome sequencing. Two affected boys have c.633delG and the other has c.631delC. We also confirmed de novo germline (c.631delC) and low-prevalence somatic (c.633delG) mutations in their mother. The two mutations are present on the same maternal haplotype, suggesting that a postzygotic somatic mutation or a reversion error occurred at an early embryonic stage in the mother, leading to switched KDM5C mutations in the affected siblings. This event is extremely unlikely to arise spontaneously (with an estimated probability of 0.39-7.5 × 10(-28) ), thus a possible reversion error is proposed here to explain this event. This study provides evidence for reversion error as a novel mechanism for the generation of somatic mutations in human diseases.

Published

2016

63. Concise Review: Heteroplasmic Mitochondrial DNA Mutations and Mitochondrial Diseases: Toward iPSC-Based Disease Modeling, Drug Discovery, and Regenerative Therapeutics

Author

Yu-ichi Goto and Hideyuki Hatakeyama

Subjects

0301 basic medicine, Mitochondrial DNA, Mitochondrial Diseases, Patients, Mitochondrial disease, Induced Pluripotent Stem Cells, Mitochondrion, Biology, DNA, Mitochondrial, Genome, Human mitochondrial genetics, 03 medical and health sciences, medicine, Humans, Genetics, Homoplasmy, Genetic Therapy, Cell Biology, medicine.disease, Heteroplasmy, Mitochondria, 030104 developmental biology, mitochondrial fusion, Genome, Mitochondrial, Mutation, Molecular Medicine, Developmental Biology

Abstract

Mitochondria contain multiple copies of their own genome (mitochondrial DNA; mtDNA). Once mitochondria are damaged by mutant mtDNA, mitochondrial dysfunction is strongly induced, followed by symptomatic appearance of mitochondrial diseases. Major genetic causes of mitochondrial diseases are defects in mtDNA, and the others are defects of mitochondria-associating genes that are encoded in nuclear DNA (nDNA). Numerous pathogenic mutations responsible for various types of mitochondrial diseases have been identified in mtDNA; however, it remains uncertain why mitochondrial diseases present a wide variety of clinical spectrum even among patients carrying the same mtDNA mutations (e.g., variations in age of onset, in affected tissues and organs, or in disease progression and phenotypic severity). Disease-relevant induced pluripotent stem cells (iPSCs) derived from mitochondrial disease patients have therefore opened new avenues for understanding the definitive genotype-phenotype relationship of affected tissues and organs in various types of mitochondrial diseases triggered by mtDNA mutations. In this concise review, we briefly summarize several recent approaches using patient-derived iPSCs and their derivatives carrying various mtDNA mutations for applications in human mitochondrial disease modeling, drug discovery, and future regenerative therapeutics.

Published

2016

64. Reactive oxygen species stimulate mitochondrial allele segregation toward homoplasmy in human cells

Author

Hideyuki Hatakeyama, Rong Niu, Yu-ichi Goto, Feng Ling, Minoru Yoshida, and Takehiko Shibata

Subjects

0301 basic medicine, DNA Replication, Mitochondrial DNA, Cell division, Concatemer, Primary Cell Culture, Mitochondrion, Biology, DNA, Mitochondrial, Chromosome segregation, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Chromosome Segregation, MELAS Syndrome, Humans, Molecular Biology, Alleles, Homoplasmy, DNA replication, Cell Biology, Articles, Fibroblasts, Molecular biology, Heteroplasmy, Signaling, Mitochondria, 030104 developmental biology, Genes, Mitochondrial, chemistry, Genome, Mitochondrial, Mutation, Reactive Oxygen Species, 030217 neurology & neurosurgery

Abstract

Use of heteroplasmic m.3243A > G primary fibroblast cells derived from a patient with the mitochondrial disease MELAS shows that ROS trigger vegetative segregation of heteroplasmy toward wild-type and mutant mitochondrial DNA homoplasmy via the formation of linear head-to-tail multimers (concatemers)., Mitochondria that contain a mixture of mutant and wild-type mitochondrial (mt) DNA copies are heteroplasmic. In humans, homoplasmy is restored during early oogenesis and reprogramming of somatic cells, but the mechanism of mt-allele segregation remains unknown. In budding yeast, homoplasmy is restored by head-to-tail concatemer formation in mother cells by reactive oxygen species (ROS)–induced rolling-circle replication and selective transmission of concatemers to daughter cells, but this mechanism is not obvious in higher eukaryotes. Here, using heteroplasmic m.3243A > G primary fibroblast cells derived from MELAS patients treated with hydrogen peroxide (H2O2), we show that an optimal ROS level promotes mt-allele segregation toward wild-type and mutant mtDNA homoplasmy. Enhanced ROS level reduced the amount of intact mtDNA replication templates but increased linear tandem multimers linked by head-to-tail unit-sized mtDNA (mtDNA concatemers). ROS-triggered mt-allele segregation correlated with mtDNA-concatemer production and enabled transmission of multiple identical mt-genome copies as a single unit. Our results support a mechanism by which mt-allele segregation toward mt-homoplasmy is mediated by concatemers.

Published

2016

65. Mitochondrial diseases

Author

Yu-ichi Goto

Subjects

Otorhinolaryngology, Neurology (clinical)

Published

2016

66. A novel homoplasmic mitochondrial DNA mutation (m.13376T>C, p.I347T) of MELAS presenting characteristic medial temporal lobe atrophy

Author

Mami Takemoto, Eisaku Morimoto, Yasuyuki Ohta, Emi Nomura, Koh Tadokoro, Yoshio Omote, Sanae Teshigawara, Noriko Hatanaka, Jun Wada, Yu ichi Goto, Toru Yamashita, Nozomi Hishikawa, Jingwei Shang, Ryo Sasaki, and Koji Abe

Subjects

Mitochondrial DNA, Neurology, business.industry, Mutation (genetic algorithm), Medial temporal atrophy, Medicine, Neurology (clinical), business, Molecular biology

Published

2020

67. Leukoencephalopathy with a case of heterozygous POLG mutation mimicking mitochondrial neurogastrointestinal encephalomyopathy (MNGIE)

Author

Yu-ichi Goto, Kenji Yoshinaga, Ryosuke Takahashi, Michikazu Nakamura, Ryo Ohtani, Ken Yasuda, and Nagako Murase

Subjects

Adult, Male, Pathology, medicine.medical_specialty, Heterozygote, medicine.disease_cause, Leukoencephalopathy, 03 medical and health sciences, 0302 clinical medicine, Ptosis, Muscular Dystrophy, Oculopharyngeal, Leukoencephalopathies, Mitochondrial Encephalomyopathies, Physiology (medical), medicine, Humans, Demyelinating polyneuropathy, Heterozygous mutation, Mutation, Ophthalmoplegia, business.industry, External ophthalmoplegia, Intestinal Pseudo-Obstruction, General Medicine, medicine.disease, Phenotype, Magnetic Resonance Imaging, DNA Polymerase gamma, Peripheral neuropathy, Neurology, 030220 oncology & carcinogenesis, Surgery, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

Diseases due to mutations of polymerase γ (POLG) usually present with progressive external ophthalmoplegia. However, a few studies have been reported on POLG1 mutations with the mitochondrial neurogastrointestinal encephalomyopathy (MNGIE)-like phenotype. All cases with POLG1 mutations mimicking MNGIE have never shown leukoencephalopathy on brain magnetic resonance imaging (MRI) or demyelinating polyneuropathy. We present a 26-year-old male with gait disturbance, recurrent bowel obstruction, peripheral neuropathy, ophthalmoplegia or ptosis, which represented MNGIE phenotype. Though he displayed demyelinating peripheral neuropathy or leukoencephalopathy on brain MRI, genetic analysis revealed heterozygous mutation in POLG1 gene. We report for the first time two newly characteristics in our patient with heterozygous POLG1 mutations with the MNGIE-like phenotype: leukoencephalopathy and demyelinating polyneuropathy.

Published

2018

68. CO2-sensitive tRNA modification associated with human mitochondrial disease

Author

Hideki Yagasaki, Tai Harada, Kaori Yanaka, Kenjyo Miyauchi, Huan Lin, Shinichi Nakagawa, Yu-ichi Goto, Tsutomu Suzuki, Ryo Okita, Hirofumi Komaki, Yuriko Sakaguchi, Eri Takeshita, and Kaoru Fujioka

Subjects

0301 basic medicine, TRNA modification, Mitochondrial translation, Science, Mitochondrial disease, Bicarbonate, General Physics and Astronomy, Mitochondrion, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, medicine, Protein biosynthesis, lcsh:Science, Multidisciplinary, Chemistry, RNA, General Chemistry, medicine.disease, Cell biology, 030104 developmental biology, Transfer RNA, lcsh:Q, 030217 neurology & neurosurgery

Abstract

It has been generally thought that tRNA modifications are stable and static, and their frequencies are rarely regulated. N6-threonylcarbamoyladenosine (t6A) occurs at position 37 of five mitochondrial (mt-)tRNA species. We show that YRDC and OSGEPL1 are responsible for t6A37 formation, utilizing L-threonine, ATP, and CO2/bicarbonate as substrates. OSGEPL1-knockout cells exhibit respiratory defects and reduced mitochondrial translation. We find low level of t6A37 in mutant mt-tRNA isolated from the MERRF-like patient’s cells, indicating that lack of t6A37 results in pathological consequences. Kinetic measurements of t6A37 formation reveal that the Km value of CO2/bicarbonate is extremely high (31 mM), suggesting that CO2/bicarbonate is a rate-limiting factor for t6A37 formation. Consistent with this, we observe a low frequency of t6A37 in mt-tRNAs isolated from human cells cultured without bicarbonate. These findings indicate that t6A37 is regulated by sensing intracellular CO2/bicarbonate concentration, implying that mitochondrial translation is modulated in a codon-specific manner under physiological conditions.

Published

2018

69. P.89Infantile-onset lipid storage myopathy

Author

Mariko Okubo, Luh Ari Indrawati, Yoshihiko Saito, Hideo Sugie, Tokiko Fukuda, Aritoshi Iida, Ichizo Nishino, Theerawat Kumutpongpanich, Satoru Noguchi, Masashi Ogasawara, Yu-ichi Goto, Shinichiro Hayashi, Michio Inoue, and Jantima Tanboon

Subjects

Neutral lipid, medicine.medical_specialty, Endocrinology, Neurology, Chemistry, Internal medicine, Pediatrics, Perinatology and Child Health, medicine, Neurology (clinical), Genetics (clinical)

Published

2019

70. Additive dominant effect of a SOX10 mutation underlies a complex phenotype of PCWH

Author

Ken Inoue, Yu-ichi Goto, Youhei W. Terakawa, Shoko Nakamura, Chihiro Akazawa, Takayoshi Inoue, Naoko Inoue, Yoshiki Matsuda, Yukiko Ito, Masumi Inagaki, Shinichi Kohsaka, Yukiko U. Inoue, Junko Asami, and Takahiro Ohkubo

Subjects

Genetically modified mouse, BAC transgenic mouse, Lineage (genetic), Transgene, Mutant, SOX10, Mice, Transgenic, Haploinsufficiency, Biology, medicine.disease_cause, Corpus Callosum, lcsh:RC321-571, Mice, medicine, Animals, Humans, Waardenburg Syndrome, Hirschsprung Disease, Mutant SOX10, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Genes, Dominant, Genetics, Mutation, Waardenburg syndrome, SOXE Transcription Factors, Brain, medicine.disease, Sciatic Nerve, Disease Models, Animal, Phenotype, Neurology, Neural Crest, embryonic structures, Schwann Cells, PCWH, Demyelinating Diseases

Abstract

Distinct classes of SOX10 mutations result in peripheral demyelinating neuropathy, central dysmyelinating leukodystrophy, Waardenburg syndrome, and Hirschsprung disease, collectively known as PCWH. Meanwhile, SOX10 haploinsufficiency caused by allelic loss-of-function mutations leads to a milder non-neurological disorder, Waardenburg-Hirschsprung disease. The cellular pathogenesis of more complex PCWH phenotypes in vivo has not been thoroughly understood. To determine the pathogenesis of PCWH, we have established a transgenic mouse model. A known PCWH-causing SOX10 mutation, c.1400del12, was introduced into mouse Sox10-expressing cells by means of bacterial artificial chromosome (BAC) transgenesis. By crossing the multiple transgenic lines, we examined the effects produced by various copy numbers of the mutant transgene. Within the nervous systems, transgenic mice revealed a delay in the incorporation of Schwann cells in the sciatic nerve and the terminal differentiation of oligodendrocytes in the spinal cord. Transgenic mice also showed defects in melanocytes presenting as neurosensory deafness and abnormal skin pigmentation, and a loss of the enteric nervous system. Phenotypes in each lineage were more severe in mice carrying higher copy numbers, suggesting a gene dosage effect for mutant SOX10. By uncoupling the effects of gain-of-function and haploinsufficiency in vivo, we have demonstrated that the effect of a PCWH-causing SOX10 mutation is solely pathogenic in each SOX10-expressing cellular lineage in a dosage-dependent manner. In both the peripheral and central nervous systems, the primary consequence of SOX10 mutations is hypomyelination. The complex neurological phenotypes in PCWH patients likely result from a combination of haploinsufficiency and additive dominant effect.

Published

2015

71. Mitochondrial respiratory dysfunction caused by a heteroplasmic mitochondrial DNA mutation blocks cellular reprogramming

Author

Saki Okabe, Mutsumi Yokota, Yasuha Ono, Hideyuki Hatakeyama, and Yu-ichi Goto

Subjects

Male, Mitochondrial DNA, Mitochondrial Diseases, Induced Pluripotent Stem Cells, Mutant, General Medicine, Mitochondrion, Biology, Cellular Reprogramming, DNA, Mitochondrial, Molecular biology, Human mitochondrial genetics, Embryonic stem cell, Heteroplasmy, RNA, Transfer, Mutation, Genetics, Humans, Female, Induced pluripotent stem cell, Molecular Biology, Reprogramming, Genetics (clinical)

Abstract

Mitochondrial dysfunction caused by pathogenic mutations in mitochondrial tRNA genes emerges only when mutant mitochondrial DNA (mtDNA) proportions exceed intrinsic pathogenic thresholds; however, little is known about the actual proportions of mutant mtDNA that can affect particular cellular lineage-determining processes. Here, we mainly focused on the effects of mitochondrial respiratory dysfunction caused by m.3243A>G heteroplasmy in MT-TL1 gene on cellular reprogramming. We found that generation of induced pluripotent stem cells (iPSCs) was drastically depressed only by high proportions of mutant mtDNA (≥ 90% m.3243A>G), and these proportions were strongly associated with the degree of induced mitochondrial respiratory dysfunction. Nevertheless, all established iPSCs, even those carrying ∼ 100% m.3243A>G, exhibited an embryonic stem cell-like pluripotent state. Therefore, our findings clearly demonstrate that loss of physiological integrity in mitochondria triggered by mutant mtDNA constitute a roadblock to cellular rejuvenation, but do not affect the maintenance of the pluripotent state.

Published

2015

72. Isolated mitochondrial stroke-like episodes in an elderly patient with theMT-ND3gene mutation

Author

Yu-ichi Goto, Masako Mukai, Kota Bokuda, Keizo Sugaya, Tadashi Ozawa, Shiro Matsubara, Akira Yagishita, Akinori Miyakoshi, and Imaharu Nakano

Subjects

Pathology, medicine.medical_specialty, Mitochondrial DNA, business.industry, Mitochondrial disease, Encephalopathy, Gene mutation, medicine.disease, Neurology, Mitochondrial myopathy, Lactic acidosis, Immunology, medicine, Neurology (clinical), medicine.symptom, MT-ND3, Myopathy, business

Abstract

Stroke-like episode represents a clinical hallmark of mitochondrial myopathy, encephalopathy, lactic acidosis, and stroke-like episodes. Mitochondrial myopathy, encephalopathy, lactic acidosis, and stroke-like episodes are usually suspected based on clinical symptoms, such as lactic acidosis, deafness, diabetes, short stature, myopathy, and cognitive decline, often with a maternal inheritance pattern of family history. We describe an elderly woman with recurrent stroke-like episodes, who had only a faint concomitant signs, but no family history of mitochondrial disease. Sequence analysis of the mitochondrial genome extracted from biopsied muscle showed a heteroplasmic 10158T>C mutation in the mitochondrial complex I subunit gene, MT-ND3. This is the first adult-onset case harboring the m.10158T>C mutation, which is known to cause lethal infant-onset Leigh syndrome. The unique manifestations of sporadic, elderly-onset, and isolated stroke-like episodes suggest that it is an important differential diagnosis for ischemic stroke and extend the clinical and mutational spectrum of mitochondrial stroke-like episodes.

Published

2015

73. Higd1a is a positive regulator of cytochrome c oxidase

Author

Hisakazu Kato, Shinya Yoshikawa, Takaharu Hayashi, Issei Komuro, Tetsuo Minamino, Ken Matsuoka, Yu-ichi Goto, Yasushi Sakata, Takashi Ogura, Hiroshi Aoyama, Masanori Asakura, Masafumi Kitakaze, Seiji Takashima, Kazuaki Takafuji, Osamu Tsukamoto, Kyoko Shinzawa-Itoh, Tomitake Tsukihara, Atsushi Nakano, Hidetaka Kioka, Hiroshi Asanuma, Yasunori Shintani, Yoshihiro Asano, Masahide Hikita, Satoru Yamazaki, and Shuichiro Higo

Subjects

Protein Conformation, macromolecular substances, Oxidative phosphorylation, Mitochondrion, Oxidative Phosphorylation, Electron Transport Complex IV, chemistry.chemical_compound, Adenosine Triphosphate, Fluorescence Resonance Energy Transfer, Animals, Cytochrome c oxidase, Hypoxia, Electrochemical gradient, HIGD1A, Multidisciplinary, ATP synthase, biology, Biological Sciences, Hypoxia-Inducible Factor 1, alpha Subunit, Mitochondria, Heme A, chemistry, Biochemistry, biology.protein, Cattle, Adenosine triphosphate

Abstract

Cytochrome c oxidase (CcO) is the only enzyme that uses oxygen to produce a proton gradient for ATP production during mitochondrial oxidative phosphorylation. Although CcO activity increases in response to hypoxia, the underlying regulatory mechanism remains elusive. By screening for hypoxia-inducible genes in cardiomyocytes, we identified hypoxia inducible domain family, member 1A (Higd1a) as a positive regulator of CcO. Recombinant Higd1a directly integrated into highly purified CcO and increased its activity. Resonance Raman analysis revealed that Higd1a caused structural changes around heme a, the active center that drives the proton pump. Using a mitochondria-targeted ATP biosensor, we showed that knockdown of endogenous Higd1a reduced oxygen consumption and subsequent mitochondrial ATP synthesis, leading to increased cell death in response to hypoxia; all of these phenotypes were rescued by exogenous Higd1a. These results suggest that Higd1a is a previously unidentified regulatory component of CcO, and represents a therapeutic target for diseases associated with reduced CcO activity.

Published

2015

74. NDUFAF3 variants that disrupt mitochondrial complex I assembly may associate with cavitating leukoencephalopathy

Author

Yu-ichi Goto, Shumpei Uchino, Akihiko Ishiyama, C. Sakai, Masakazu Mimaki, Tomomi Ogata, Hirofumi Komaki, Masayuki Sasaki, E. Suzuki, Nishiki Makioka, Kazuhiro Muramatsu, Yuichi Matsushima, and Ichizo Nishino

Subjects

0301 basic medicine, NDUFB11, Substantia nigra, NDUFA9, NDUFB10, Leukoencephalopathy, Mitochondrial Proteins, 03 medical and health sciences, 0302 clinical medicine, Leukoencephalopathies, Exome Sequencing, Genetics, medicine, Humans, Genetic Predisposition to Disease, Genetics (clinical), Electron Transport Complex I, Chemistry, NDUFS2, Respiratory infection, Infant, medicine.disease, Molecular biology, Respiratory enzyme, Mitochondria, 030104 developmental biology, Mutation, Female, 030217 neurology & neurosurgery

Abstract

Genetic abnormalities in mitochondrial complex assembling factors are associated with leukoencephalopathy. We present a 1-year-old girl with consciousness disturbance after a respiratory infection. Brain MRI revealed leukoencephalopathy with bilaterally symmetrical hyperintensity in the substantia nigra, medial thalamic nuclei, and basal nuclei, as well as cavities in the cerebral white matter and corpus callosum. Lactate levels in the spinal fluid were high, while magnetic resonance spectroscopy of the cerebral white matter and basal nuclei showed high peak lactate levels, suggesting mitochondrial dysfunction. The respiratory enzyme activity of complex I was reduced to 17% to 21% in skeletal muscle. Whole exome sequencing identified compound heterozygous variations in NDUFAF3, involved in the assembly of mitochondrial complex I (c.342_343insGTG:p.117Valdup, c.505C > A:p.Pro169Thr). Two-dimensional, blue-native polyacrylamide gel electrophoresis (PAGE) and sodium dodecyl sulfate-PAGE revealed reductions in Q-module (NDUFS2, NDUFS3, and NDUFA9) and P-module (NDUFB10 and NDUFB11) subunits, indicating disruption of mitochondrial complex I assembly. Our report expands the spectrum of clinical phenotypes associated with pathogenic variants of NDUFAF3.

Published

2017

75. Interleukin-1beta (IL-1β)-induced Notch ligand Jagged1 suppresses mitogenic action of IL-1β on human dystrophic myogenic cells

Author

Tohru Kiyono, Masafumi Matsuo, Madoka Ikemoto-Uezumi, Kikuo Okamura, Naohiro Hashimoto, Yuki Nagata, and Yu-ichi Goto

Subjects

0301 basic medicine, Heredity, Genetic Linkage, medicine.medical_treatment, Cellular differentiation, Duchenne muscular dystrophy, Interleukin-1beta, lcsh:Medicine, Gene Expression, Duchenne Muscular Dystrophy, Muscle Development, Muscular Dystrophies, Spectrum Analysis Techniques, Animal Cells, Morphogenesis, Medicine and Health Sciences, Muscular dystrophy, lcsh:Science, Receptor, Notch3, Musculoskeletal System, Cells, Cultured, Gene knockdown, Multidisciplinary, Chemistry, Reverse Transcriptase Polymerase Chain Reaction, Muscles, Cell Differentiation, Muscle Differentiation, Flow Cytometry, Cell biology, Cytokine, Neurology, X-Linked Traits, Sex Linkage, Spectrophotometry, Cytophotometry, Anatomy, Cellular Types, Muscle Regeneration, Research Article, musculoskeletal diseases, congenital, hereditary, and neonatal diseases and abnormalities, Cell Physiology, Muscle Tissue, Muscle disorder, Research and Analysis Methods, 03 medical and health sciences, Downregulation and upregulation, medicine, Genetics, Humans, Regeneration, Clinical Genetics, Muscle Cells, lcsh:R, Biology and Life Sciences, Cell Biology, medicine.disease, Muscular Dystrophy, Duchenne, 030104 developmental biology, Biological Tissue, Skeletal Muscles, lcsh:Q, Neural cell adhesion molecule, Cell Immortalization, Organism Development, Jagged-1 Protein, Developmental Biology

Abstract

Duchenne muscular dystrophy (DMD) is a severe X-linked recessive muscle disorder caused by mutations in the dystrophin gene. Nonetheless, secondary processes involving perturbation of muscle regeneration probably exacerbate disease progression, resulting in the fatal loss of muscle in DMD patients. A dysfunction of undifferentiated myogenic cells is the most likely cause for the reduction of regenerative capacity of muscle. To clarify molecular mechanisms in perturbation of the regenerative capacity of DMD muscle, we have established several NCAM (CD56)-positive immortalized human dystrophic and non-dystrophic myogenic cell lines from DMD and healthy muscles. A pro-inflammatory cytokine, IL-1β, promoted cell cycle progression of non-dystrophic myogenic cells but not DMD myogenic cells. In contrast, IL-1β upregulated the Notch ligand Jagged1 gene in DMD myogenic cells but not in non-dystrophic myogenic cells. Knockdown of Jagged1 in DMD myogenic cells restored the IL-1β-promoted cell cycle progression. Conversely, enforced expression of Jagged1-blocked IL-1β promoted proliferation of non-dystrophic myogenic cells. In addition, IL-1β prevented myogenic differentiation of DMD myogenic cells depending on Jagged1 but not of non-dystrophic myogenic cells. These results demonstrate that Jagged1 induced by IL-1β in DMD myogenic cells modified the action of IL-1β and reduced the ability to proliferate and differentiate. IL-1β induced Jagged1 gene expression may be a feedback response to excess stimulation with this cytokine because high IL-1β (200-1000 pg/ml) induced Jagged1 gene expression even in non-dystrophic myogenic cells. DMD myogenic cells are likely to acquire the susceptibility of the Jagged1 gene to IL-1β under the microcircumstances in DMD muscles. The present results suggest that Jagged1 induced by IL-1β plays a crucial role in the loss of muscle regeneration capacity of DMD muscles. The IL-1β/Jagged1 pathway may be a new therapeutic target to ameliorate exacerbation of muscular dystrophy in a dystrophin-independent manner.

Published

2017

76. Arima syndrome caused by CEP290 specific variant and accompanied with pathological cilium; clinical comparison with Joubert syndrome and its related diseases

Author

Yu-ichi Goto, Takashi Saito, Takeki Furue, Keishi Narita, Hirotsugu Kitayama, Keiko Maeda, Eihiko Takahashi, Shinji Yamakura, Shuhei Ide, Yuji Iwasaki, Sen Takeda, Kiyoshi Matsui, Hongmei Dai, Masayuki Itoh, and Masataka Arima

Subjects

0301 basic medicine, Pathology, Cell Cycle Proteins, 030105 genetics & heredity, Compound heterozygosity, Cerebellum, Eye Abnormalities, Cells, Cultured, Sanger sequencing, Polycystic Kidney Diseases, Cilium, General Medicine, Kidney Diseases, Cystic, Immunohistochemistry, Neoplasm Proteins, Coloboma, symbols, Female, Adult, medicine.medical_specialty, Adolescent, Biology, Joubert syndrome, Retina, 03 medical and health sciences, symbols.namesake, Young Adult, Developmental Neuroscience, Microscopy, Electron, Transmission, Antigens, Neoplasm, Cerebellar Diseases, Ciliogenesis, Exome Sequencing, medicine, Humans, Abnormalities, Multiple, Family, Cilia, Gene, Ciliary membrane, Centrosome, Fibroblasts, medicine.disease, Molecular Weight, Cytoskeletal Proteins, 030104 developmental biology, Pediatrics, Perinatology and Child Health, Mutation, Neurology (clinical)

Abstract

Objective Arima syndrome (AS) is a rare disease and its clinical features mimic those of Joubert syndrome or Joubert syndrome-related diseases (JSRD). Recently, we clarified the AS diagnostic criteria and its severe phenotype. However, genetic evidence of AS remains unknown. We explored causative genes of AS and compared the clinical and genetic features of AS with the other JSRD. Patients and methods We performed genetic analyses of 4 AS patients of 3 families with combination of whole-exome sequencing and Sanger sequencing. Furthermore, we studied cell biology with the cultured fibroblasts of 3 AS patients. Results All patients had a specific homozygous variant (c.6012-12T>A, p.Arg2004Serfs*7) or compound heterozygous variants (c.1711+1G>A; c.6012-12T>A, p.Gly570Aspfs*19;Arg2004Serfs*7) in centrosomal protein 290 kDa (CEP290) gene. These unique variants lead to abnormal splicing and premature termination. Morphological analysis of cultured fibroblasts from AS patients revealed a marked decrease of the CEP290-positive cell number with significantly longer cilium and naked and protruded ciliary axoneme without ciliary membrane into the cytoplasm. Conclusion AS resulted in cilia dysfunction from centrosome disruption. The unique variant of CEP290 could be strongly linked to AS pathology. Here, we provided AS specific genetic evidence, which steers the structure and functions of centrosome that is responsible for normal ciliogenesis. This is the first report that has demonstrated the molecular basis of Arima syndrome.

Published

2017

77. Plasma Nervonic Acid Is a Potential Biomarker for Major Depressive Disorder: A Pilot Study

Author

Kenji Kuroda, Kotaro Hattori, Sumiko Yoshida, Yuki Kageyama, Yasuhiko Deguchi, Tadafumi Kato, Koki Inoue, Yu-ichi Goto, Munehide Tani, Takemichi Nakamura, and Takaoki Kasahara

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Pilot Projects, Gastroenterology, Regular Research Articles, nervonic acid, Cohort Studies, Fatty Acids, Monounsaturated, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Internal medicine, Metabolome, medicine, Humans, Pharmacology (medical), Bipolar disorder, Pharmacology, bipolar disorder, Depressive Disorder, Major, Psychotropic Drugs, major depressive disorder, business.industry, Reproducibility of Results, Middle Aged, medicine.disease, metabolomics, Cortisone, Psychiatry and Mental health, 030104 developmental biology, chemistry, Schizophrenia, Cohort, Biomarker (medicine), Major depressive disorder, biomarker, Female, business, 030217 neurology & neurosurgery, Nervonic acid, Biomarkers, Cohort study

Abstract

Background Diagnostic biomarkers of major depressive disorder, bipolar disorder, and schizophrenia are urgently needed, because none are currently available. Methods We performed a comprehensive metabolome analysis of plasma samples from drug-free patients with major depressive disorder (n=9), bipolar disorder (n=6), schizophrenia (n=17), and matched healthy controls (n=19) (cohort 1) using liquid chromatography time-of-flight mass spectrometry. A significant effect of diagnosis was found for 2 metabolites: nervonic acid and cortisone, with nervonic acid being the most significantly altered. The reproducibility of the results and effects of psychotropic medication on nervonic acid were verified in cohort 2, an independent sample set of medicated patients [major depressive disorder (n=45), bipolar disorder (n=71), schizophrenia (n=115)], and controls (n=90) using gas chromatography time-of-flight mass spectrometry. Results The increased levels of nervonic acid in patients with major depressive disorder compared with controls and patients with bipolar disorder in cohort 1 were replicated in the independent sample set (cohort 2). In cohort 2, plasma nervonic acid levels were also increased in the patients with major depressive disorder compared with the patients with schizophrenia. In cohort 2, nervonic acid levels were increased in the depressive state in patients with major depressive disorder compared with the levels in the remission state in patients with major depressive disorder and the depressive state in patients with bipolar disorder. Conclusion These results suggested that plasma nervonic acid is a good candidate biomarker for the depressive state of major depressive disorder.

Published

2017

78. CO

Author

Huan, Lin, Kenjyo, Miyauchi, Tai, Harada, Ryo, Okita, Eri, Takeshita, Hirofumi, Komaki, Kaoru, Fujioka, Hideki, Yagasaki, Yu-Ichi, Goto, Kaori, Yanaka, Shinichi, Nakagawa, Yuriko, Sakaguchi, and Tsutomu, Suzuki

Subjects

Adenosine, Cell Respiration, Proteins, RNA-Binding Proteins, Carbon Dioxide, Fibroblasts, Models, Biological, MERRF Syndrome, Article, Cell Line, Mitochondria, Myoblasts, Bicarbonates, HEK293 Cells, RNA, Transfer, GTP-Binding Proteins, Humans, Nucleic Acid Conformation, CRISPR-Cas Systems, RNA Processing, Post-Transcriptional, Apoptosis Regulatory Proteins, Base Pairing, HT29 Cells, Gene Deletion, HeLa Cells

Abstract

It has been generally thought that tRNA modifications are stable and static, and their frequencies are rarely regulated. N6-threonylcarbamoyladenosine (t6A) occurs at position 37 of five mitochondrial (mt-)tRNA species. We show that YRDC and OSGEPL1 are responsible for t6A37 formation, utilizing L-threonine, ATP, and CO2/bicarbonate as substrates. OSGEPL1-knockout cells exhibit respiratory defects and reduced mitochondrial translation. We find low level of t6A37 in mutant mt-tRNA isolated from the MERRF-like patient’s cells, indicating that lack of t6A37 results in pathological consequences. Kinetic measurements of t6A37 formation reveal that the Km value of CO2/bicarbonate is extremely high (31 mM), suggesting that CO2/bicarbonate is a rate-limiting factor for t6A37 formation. Consistent with this, we observe a low frequency of t6A37 in mt-tRNAs isolated from human cells cultured without bicarbonate. These findings indicate that t6A37 is regulated by sensing intracellular CO2/bicarbonate concentration, implying that mitochondrial translation is modulated in a codon-specific manner under physiological conditions., Transfer RNA modifications play critical roles in protein synthesis. Here the authors reveal the t6A37 tRNA modification is dynamically regulated by sensing intracellular CO2 concentration in mitochondria, implying metabolic regulation of protein synthesis.

Published

2017

79. Induction of Pluripotent Stem Cells from a Manifesting Carrier of Duchenne Muscular Dystrophy and Characterization of Their X-Inactivation Status

Author

Fusako Takemura, Narihiro Minami, Shin'ichi Takeda, Takashi Nishiyama, Satoru Masuda, Miho Nakamura, Yu-ichi Goto, Hirofumi Komaki, Yuko Miyagoe-Suzuki, Kumiko Murayama, and Asako Narita

Subjects

0301 basic medicine, musculoskeletal diseases, lcsh:Internal medicine, biology, Article Subject, Duchenne muscular dystrophy, Cell Biology, medicine.disease, Embryonic stem cell, Molecular biology, X-inactivation, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine, biology.protein, Muscular dystrophy, Dystrophin, Induced pluripotent stem cell, lcsh:RC31-1245, Molecular Biology, Reprogramming, 030217 neurology & neurosurgery, X chromosome, Research Article

Abstract

Three to eight percent of female carriers of Duchenne muscular dystrophy (DMD) develop dystrophic symptoms ranging from mild muscle weakness to a rapidly progressive DMD-like muscular dystrophy due to skewed inactivation of X chromosomes during early development. Here, we generated human induced pluripotent stem cells (hiPSCs) from a manifesting female carrier using retroviral or Sendai viral (SeV) vectors and determined their X-inactivation status. Although manifesting carrier-derived iPS cells showed normal expression of human embryonic stem cell markers and formed well-differentiated teratomas in vivo, many hiPS clones showed bi-allelic expression of the androgen receptor (AR) gene and loss of X-inactivation-specific transcript and trimethyl-histone H3 (Lys27) signals on X chromosomes, suggesting that both X chromosomes of the hiPS cells are in an active state. Importantly, normal dystrophin was expressed in multinucleated myotubes differentiated from a manifesting carrier of DMD-hiPS cells with XaXa pattern. AR transcripts were also equally transcribed from both alleles in induced myotubes. Our results indicated that the inactivated X chromosome in the patient’s fibroblasts was activated during reprogramming, and XCI occurred randomly during differentiation.

Published

2017

80. Dominant mutations in ORAI1 cause tubular aggregate myopathy with hypocalcemia via constitutive activation of store-operated Ca2+ channels

Author

Kazushi Motomura, Satoru Noguchi, Sumimasa Yamashita, Rika Kizu, Yukari Endo, Naomichi Matsumoto, Yu-ichi Goto, Nobuyuki Murakami, Yuji Hara, Satoko Miyatake, Ikuya Nonaka, Satsuki Tanaka, Yukiko K. Hayashi, Ichizo Nishino, and Masahiro Bamba

Subjects

medicine.medical_specialty, Mutation, ORAI1, Endoplasmic reticulum, Skeletal muscle, STIM1, General Medicine, Biology, Muscle disorder, medicine.disease_cause, Cell biology, Endocrinology, medicine.anatomical_structure, Internal medicine, Genetics, medicine, medicine.symptom, Myopathy, Molecular Biology, Genetics (clinical), Homeostasis

Abstract

The store-operated Ca(2+) release-activated Ca(2+) (CRAC) channel is activated by diminished luminal Ca(2+) levels in the endoplasmic reticulum and sarcoplasmic reticulum (SR), and constitutes one of the major Ca(2+) entry pathways in various tissues. Tubular aggregates (TAs) are abnormal structures in the skeletal muscle, and although their mechanism of formation has not been clarified, altered Ca(2+) homeostasis related to a disordered SR is suggested to be one of the main contributing factors. TA myopathy is a hereditary muscle disorder that is pathologically characterized by the presence of TAs. Recently, dominant mutations in the STIM1 gene, encoding a Ca(2+) sensor that controls CRAC channels, have been identified to cause tubular aggregate myopathy (TAM). Here, we identified heterozygous missense mutations in the ORAI1 gene, encoding the CRAC channel itself, in three families affected by dominantly inherited TAM with hypocalcemia. Skeletal myotubes from an affected individual and HEK293 cells expressing mutated ORAI1 proteins displayed spontaneous extracellular Ca(2+) entry into cells without diminishment of luminal Ca(2+) or the association with STIM1. Our results indicate that STIM1-independent activation of CRAC channels induced by dominant mutations in ORAI1 cause altered Ca(2+) homeostasis, resulting in TAM with hypocalcemia.

Published

2014

81. A rapid screening with direct sequencing from blood samples for the diagnosis of Leigh syndrome

Author

Mizue Iai, Kyoko Takano, Mitsuko Okuda, Akira Ohtake, Kei Murayama, Hitoshi Osaka, Yu-ichi Goto, Hiroko Shimbo, Mariko Takagi, Sumimasa Yamashita, Noriko Aida, and Yu Tsuyusaki

Subjects

Genetics, Sanger sequencing, lcsh:R5-920, Direct sequencing, mDNA mutation, Respiratory chain, Complex I deficiency, Biology, Pyruvate dehydrogenase complex, Heteroplasmy, Molecular biology, Leigh syndrome, symbols.namesake, Endocrinology, lcsh:Biology (General), Cohort, symbols, SURF1, lcsh:Medicine (General), Molecular Biology, Gene, lcsh:QH301-705.5, Research Paper

Abstract

Large numbers of genes are responsible for Leigh syndrome (LS), making genetic confirmation of LS difficult. We screened our patients with LS using a limited set of 21 primers encompassing the frequently reported gene for the respiratory chain complexes I (ND1–ND6, and ND4L), IV(SURF1), and V(ATP6) and the pyruvate dehydrogenase E1α-subunit. Of 18 LS patients, we identified mutations in 11 patients, including 7 in mDNA (two with ATP6), 4 in nuclear (three with SURF1). Overall, we identified mutations in 61% of LS patients (11/18 individuals) in this cohort. Sanger sequencing with our limited set of primers allowed us a rapid genetic confirmation of more than half of the LS patients and it appears to be efficient as a primary genetic screening in this cohort.

Published

2014

82. METABOLIC DISTURBANCES IN NEUROMUSCULAR DISEASES

Author

L. Van Lommel, Michio Inoue, Shinichiro Hayashi, Shumpei Uchino, Takuya Yoshizawa, Hirofumi Komaki, Satoru Noguchi, Ikuya Nonaka, Masakazu Mimaki, Eri Takeshita, Ichizo Nishino, F. Schuit, Tatsuji Takahashi, Aritoshi Iida, Katsunori Fujii, and Yu-ichi Goto

Subjects

Neurology, Pediatrics, Perinatology and Child Health, Neurology (clinical), Genetics (clinical)

Published

2019

83. Identification of two novelShank3transcripts in the developing mouse neocortex

Author

Hirotsugu Asano, Masayuki Itoh, Shigeo Uchino, Akiko Tsuchiya, Yasuko Nakamura, Tomomi Sanagi, Chikako Waga, Yu-ichi Goto, Shinichi Kohsaka, and Eri Suzuki

Subjects

Male, Gene isoform, Transcription, Genetic, Methyl-CpG-Binding Protein 2, Mice, Transgenic, Neocortex, Nerve Tissue Proteins, Rett syndrome, Epigenetics of autism, Biology, Methylation, Biochemistry, Cell Line, MECP2, Mice, Cellular and Molecular Neuroscience, Neurodevelopmental disorder, medicine, Animals, Humans, Protein Isoforms, Epigenetics, Neurons, Genetics, Mice, Inbred ICR, Microfilament Proteins, Intron, medicine.disease, Introns, Mice, Inbred C57BL, DNA methylation, CpG Islands, Female, Transcription Initiation Site, Protein Binding

Abstract

SHANK3 is a synaptic scaffolding protein enriched in the post-synaptic density of excitatory synapses. Since several SHANK3 mutations have been identified in a particular phenotypic group of patients with autism spectrum disorder (ASD), SHANK3 is strongly suspected of being involved in the pathogenesis and neuropathology of ASD. Several SHANK3 isoforms are known to be produced in the developing brain, but they have not been fully investigated. Here, we identified two different amino-terminus truncated Shank3 transcripts. One transcript, designated as Shank3c-3, produces an isoform that contains the entire carboxyl-terminus, but the other transcript, designated as Shank3c-4, produces a carboxyl-terminus truncated isoform. During development, expression of the novel Shank3 transcripts increased after birth, transiently decreased at P14 and then gradually increased again thereafter. We also determined that methyl CpG-binding protein 2 (MeCP2) is involved in regulating expression of the novel Shank3 transcripts. MeCP2 is a transcriptional regulator that has been identified as the causative molecule of Rett syndrome, a neurodevelopmental disorder that includes autistic behavior. We demonstrated a difference between the expression of the novel Shank3 transcripts in wild-type mice and Mecp2-deficient mice. These findings suggest that the SHANK3 isoforms may be implicated in the synaptic abnormality in Rett syndrome. SHANK3 is a synaptic scaffolding protein and is suspected of being implicated in the pathogenesis and neuropathology of ASD. We here identified two different amino-terminus truncated Shank3 transcripts, Shank3c-3 and Shank3c-4, expressed from the intron 10 of the Shank3 gene, and also suggested the epigenetic regulation of their expression via methyl CpG-binding protein 2 (MeCP2) that has been identified as the causative molecule of Rett syndrome.

Published

2013

84. Neuromelanin MRI in a family with mitochondrial parkinsonism harboring a Y955C mutation in POLG1

Author

Masako Mukai, Huaying Cai, Hidenao Sasaki, Kazuhito Miyamoto, Ichiro Yabe, Keizo Sugaya, Yu-ichi Goto, Shiro Matsubara, and Fusako Yokochi

Subjects

Ophthalmoplegia, Chronic Progressive External, Mitochondrial DNA, Pathology, medicine.medical_specialty, Substantia nigra, DNA-Directed DNA Polymerase, medicine.disease_cause, DNA, Mitochondrial, Parkinsonian Disorders, Neuromelanin, medicine, Humans, Aged, Melanins, Mutation, medicine.diagnostic_test, business.industry, Parkinsonism, Locus Ceruleus, Magnetic resonance imaging, medicine.disease, Magnetic Resonance Imaging, DNA Polymerase gamma, Mitochondria, Pedigree, Neurology, Female, Neurology (clinical), Geriatrics and Gerontology, Multiple mtDNA deletions, business

Abstract

Background Progressive external ophthalmoplegia (PEO) and parkinsonism can be caused by genetic mutations that affect mitochondrial DNA (mtDNA) maintenance. We characterized parkinsonism in a family with dominantly inherited PEO. Methods We conducted clinical, histological and genetic analyses on two affected members suffering from PEO and parkinsonism, and reviewed the cases in the literature. To clarify parkinsonism related to multiple mtDNA deletions, we used 3-T neuromelanin magnetic resonance imaging (MRI) to assess signal changes in the substantia nigra (SN) and locus ceruleus (LC) in our patients, and compared the results to those observed in idiopathic Parkinson's disease (iPD) ( n = 35). Results We report the first case of a Japanese family harboring a heterozygous p.Y955C mutation in POLG1 . The clinical features of parkinsonism related to the Y955C mutation in a total of 16 patients, including our two cases, are indistinguishable from iPD. However, neuromelanin MRI showed a distinct pattern in our cases compared to iPD. The neuromelanin imaging results were consistent with the neuropathological findings reported in cases of POLG1 mutations, in which neurons of the SN were profoundly affected while those in the LC were preserved. Conclusions Our results suggest that 3-T neuromelanin MRI may be useful for differentiating POLG1 mutation-associated parkinsonism from iPD, and that POLG1 mutations may cause selective neuronal loss in the SN via a mechanism different from that of iPD.

Published

2013

85. Behavioral and cortical EEG evaluations confirm the roles of both CCKA and CCKB receptors in mouse CCK-induced anxiety

Author

Yu-ichi Goto, Hidenobu Ohta, Yukiko Matsushima, Hitomi Izumi, Misaki Akiyama, Heng Li, Makiko Kaga, Takako Toda, Yoshiki Matsuda, Mika Seki, and Masumi Inagaki

Subjects

Male, medicine.medical_specialty, Indoles, medicine.drug_class, Devazepide, Anxiety, Amygdala, Tetragastrin, Mice, Behavioral Neuroscience, Meglumine, Internal medicine, medicine, Animals, CCK-4, Maze Learning, Receptor, Injections, Intraventricular, Cholecystokinin, Analysis of Variance, Brain Mapping, Behavior, Animal, Dose-Response Relationship, Drug, Spectrum Analysis, Brain, Electroencephalography, Receptor antagonist, Adaptation, Physiological, Brain Waves, Receptor, Cholecystokinin B, Receptor, Cholecystokinin A, Cortex (botany), Mice, Inbred C57BL, Disease Models, Animal, medicine.anatomical_structure, Endocrinology, Gene Expression Regulation, Neuron, Psychology, Neuroscience, hormones, hormone substitutes, and hormone antagonists, medicine.drug

Abstract

This study investigated the roles of cholecystokinin (CCK)(A) and CCK(B) receptors on CCK-4-induced anxiety-like behaviors in mice through behavioral and neural evaluations. Anxiety-like behaviors in mice were induced by an intracerebroventricular (i.c.v.) administration of CCK-4, which can bind to both CCK(A) and CCK(B) receptors. The effects of CCK(A) and CCK(B) receptor antagonists (devazepide and CI-988, respectively) were examined using mouse anxiety tests (elevated-plus maze and light-dark box) and also by examining neuronal activities through EEG monitoring and c-Fos immunohistochemistry in the cortex and amygdala. CCK-4 (3 μg/kg of body weight i.c.v.) significantly induced mouse anxiety-like behaviors in the anxiety tests and also affected their EEG patterns with respect to pre-drug tracing, resulting in increase in spectral power in relative power distribution in the delta and theta bands (0.5-5 Hz frequency bands) and also in increase in c-Fos immunopositive neuron counts. These CCK-4 effects were completely suppressed by 1.0mg/kg CCK(B) receptor antagonist, CI-988, while the same amount of CCK(A) receptor antagonist, devazepide was partly able to suppress the same effects. These findings indicated that not only CCK(B) receptors but also CCK(A) receptors in the brain play important roles in regulating anxiety-like behaviors in mice. The present study also proposed a possibility that cortical EEG is useful for assessing anxiety.

Published

2013

86. Low dose resveratrol ameliorates mitochondrial respiratory dysfunction and enhances cellular reprogramming

Author

Yuki Mizuguchi, Kou Sueoka, Mamoru Tanaka, Yu-ichi Goto, and Hideyuki Hatakeyama

Subjects

0301 basic medicine, Pluripotent Stem Cells, Mitochondrial DNA, Mitochondrial disease, Mutant, Cell Respiration, Resveratrol, Biology, Antioxidants, 03 medical and health sciences, chemistry.chemical_compound, Stilbenes, medicine, Humans, Induced pluripotent stem cell, Molecular Biology, Cells, Cultured, Respiratory dysfunction, Cell Biology, Fibroblasts, medicine.disease, Cellular Reprogramming, Molecular biology, Heteroplasmy, Mitochondria, 030104 developmental biology, chemistry, Cancer research, Molecular Medicine, Reprogramming

Abstract

Mitochondrial disease is associated with a wide variety of clinical presentations, even among patients carrying heteroplasmic mitochondrial DNA (mtDNA) mutations, probably because of variations in mutant mtDNA proportions at the tissue and organ levels. Although several case reports and clinical trials have assessed the effectiveness of various types of drugs and supplements for the treatment of mitochondrial diseases, there are currently no cures for these conditions. In this study, we demonstrated for the first time that low dose resveratrol (RSV) ameliorated mitochondrial respiratory dysfunction in patient-derived fibroblasts carrying homoplasmic mtDNA mutations. Furthermore, low dose RSV also facilitated efficient cellular reprogramming of the patient-derived fibroblasts into induced pluripotent stem cells, partly due to improved cellular viability. Our results highlight the potential of RSV as a new therapeutic drug candidate for the treatment of mitochondrial diseases.

Published

2016

87. Respiratory Chain Complex Disorganization Impairs Mitochondrial and Cellular Integrity: Phenotypic Variation in Cytochrome c Oxidase Deficiency

Author

Hideyuki, Hatakeyama and Yu-Ichi, Goto

Subjects

Electron Transport Complex IV, Phenotype, Mutation, Cytochrome-c Oxidase Deficiency, Homeostasis, Humans, RNA, Messenger, Holoenzymes, Muscle Development, Muscle, Skeletal, Models, Biological, Mitochondria

Abstract

The relationships between the molecular abnormalities in mitochondrial respiratory chain complexes and their negative contributions to mitochondrial and cellular functions have been proved to be essential for better understandings in mitochondrial medicine. Herein, we established the method to identify disease phenotypic differences among patients with muscle histopathological cytochrome c oxidase (COX) deficiency, as one of the representative clinical features in mitochondrial diseases, by using patients' myoblasts that are derived from biopsied skeletal muscle tissues. We identified two obviously different severities in molecular diagnostic criteria of COX deficiency among patients: structurally stable, but functionally mild/moderate defect and severe functional defect with the disrupted COX holoenzyme structure. COX holoenzyme disorganization actually triggered several mitochondrial dysfunctions, including the decreased ATP level, the increased oxidative stress level, and the damaged membrane potential level, all of which lead to the deteriorated cellular growth, the accelerated cellular senescence, and the induced apoptotic cell death. Our cell-based in vitro diagnostic approaches would be widely applicable to understanding patient-specific pathomechanism in various types of mitochondrial diseases, including other respiratory chain complex deficiencies and other mitochondrial metabolic enzyme deficiencies.

Published

2016

88. Novel TK2 mutations as a cause of delayed muscle maturation in mtDNA depletion syndrome

Author

Hiroshi Suzumura, Satomi Mitsuhashi, Seito Hisamatsu, Osamu Arisaka, Satoru Noguchi, Ishiyama Akihiko, Noriko Sumitomo, Thanes Termglinchan, George Imataka, Masayuki Sasaki, Ikuya Nonaka, Yu-ichi Goto, Nobuyuki Murakami, Junko Ohmori, Ichizo Nishino, and Narihiro Minami

Subjects

0301 basic medicine, Genetics, MtDNA depletion, Biology, medicine.disease, Early infancy, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Muscle fiber immaturity, Mitochondrial DNA depletion syndrome, medicine, Neurology (clinical), medicine.symptom, Myopathy, Clinical/Scientific Notes, 030217 neurology & neurosurgery, Genetics (clinical)

Abstract

Recessive mutations in TK2 cause a severe mitochondrial DNA depletion syndrome (MDS),(1) characterized by severe myopathy from early infancy. Recent reports have suggested a wider clinical spectrum including encephalomyopathic form.(1,2) We report a patient with infantile-onset fatal encephalomyopathy presenting with extreme muscle fiber immaturity.

Published

2016

89. Early Onset of Diabetes Mellitus Accelerates Cognitive Decline in Japanese Patients with Mitochondrial Myopathy, Encephalopathy, Lactic Acidosis, and Stroke-Like Episodes

Author

Shin Yonemitsu, Daita Kaneda, Yu-ichi Goto, Seiji Muro, Yuya Shinoto, Takaaki Murakami, Yasutoshi Koga, and Shogo Oki

Subjects

Male, medicine.medical_specialty, Mitochondrial disease, Encephalopathy, Hypoglycemia, MELAS syndrome, General Biochemistry, Genetics and Molecular Biology, Diabetes Complications, 03 medical and health sciences, 0302 clinical medicine, Mitochondrial myopathy, Internal medicine, Diabetes mellitus, medicine, Diabetes Mellitus, MELAS Syndrome, Humans, 030212 general & internal medicine, Cognitive decline, Age of Onset, Retrospective Studies, business.industry, General Medicine, Middle Aged, medicine.disease, Endocrinology, Lactic acidosis, Mutation, Female, business, Cognition Disorders, 030217 neurology & neurosurgery

Abstract

Approximately 80% of patients with mitochondrial myopathy, encephalopathy, lactic acidosis, and stroke-like episodes (MELAS) carry the A3243G mutation in the mitochondrial tRNALeu (UUR) gene. Conversely, this mutation has also been identified as one of the most prevalent genetic abnormalities in patients with diabetes mellitus. Mitochondrial diabetes mellitus complicated with MELAS is relatively common, and 12.5% of patients with the A3243G mutation develop MELAS after being diagnosed with diabetes mellitus. However, the clinical impact of diabetes mellitus in MELAS patients remains unclear. Therefore, we retrospectively studied 14 Japanese MELAS patients with the A3243G mutation: three men and eleven women, with the mean age of 48.0 (± 15.4) years. Eight patients had been diagnosed with diabetes mellitus prior to the diagnosis of mitochondrial disease, and all of them were treated with insulin. The other six included four patients with concurrent diagnosis of diabetes and mitochondrial disease, one patient diagnosed with diabetes after the diagnosis of mitochondrial disease, and one patient without developing diabetes currently. We thus compared the patients' characteristics between those with and without early onset of diabetes mellitus. Cognitive decline (75.0% vs. 0%; p = 0.03) and poor glycemic control with severe hypoglycemic events (75.0% vs. 16.7%; p = 0.05) were more common in MELAS patients with a prior diagnosis of diabetes than in those without the prior diagnosis of diabetes. Our data suggest that the latent progress of cognitive decline is accelerated because of early onset of diabetes mellitus in MELAS patients.

Published

2016

90. Pyruvate Improved Insulin Secretion Status in a Mitochondrial Diabetes Mellitus Patient

Author

Yu-ichi Goto, Nobuyuki Murakami, Ryoichi Sakuta, Ichizo Nishino, Takeshi Inoue, Yasutoshi Koga, Tadayuki Ayabe, and Yuji Oto

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Mitochondrial Diseases, Endocrinology, Diabetes and Metabolism, Urinary system, medicine.medical_treatment, Clinical Biochemistry, 030209 endocrinology & metabolism, Context (language use), Mitochondrion, Biochemistry, 03 medical and health sciences, Diabetes mellitus genetics, chemistry.chemical_compound, 0302 clinical medicine, Endocrinology, Sodium pyruvate, Internal medicine, Diabetes mellitus, Pyruvic Acid, Diabetes Mellitus, Medicine, Humans, Insulin, C-Peptide, business.industry, Biochemistry (medical), medicine.disease, 030104 developmental biology, Treatment Outcome, chemistry, Mutation, Glycated hemoglobin, business

Abstract

Mitochondrial diabetes is a rare form of diabetes mellitus accounting for up to 1% of all diabetes. Pyruvate therapy has been reported to be a potential therapeutic choice for patients with mitochondrial diseases.Water-based sodium pyruvate solutions (0.5 g/kg, thrice daily) were administrated orally to a 32-year-old Japanese male with mitochondrial diabetes and myopathy caused by m.14709TC mutation. At the age of 20 years, he was diagnosed with diabetes mellitus and started insulin therapy. He tested negative for islet cell and glutamic decarboxylase antibodies. To evaluate favorable therapeutic improvements, we measured the lactate and pyruvate levels in plasma and cerebrospinal fluid; urinary C-peptide, glycated hemoglobin, and glycoalbumin levels; and total daily insulin dose (TDD). The patient experienced no side effects such as diarrhea because of pyruvate therapy. His urinary C-peptide level improved from 4.3 to 17.2 μg/d after 1 day and to 30.2 μg/d after 6 months of pyruvate therapy. TDD decreased from 33 to 20 U/d after 6 months of pyruvate therapy, but the lactate levels of plasma and cerebrospinal fluid and the lactate/pyruvate ratio did not change.Sodium pyruvate improved insulin secretion and resulted in decreased TDD in a patient with mitochondrial diabetes. Pyruvate therapy may be a potential therapeutic choice for patients with mitochondrial diabetes. Clinical trials involving a larger number of patients and long-term evaluation of the therapy are necessary to clarify the efficacy of pyruvate therapy.

Published

2016

91. Plasma Metabolites Predict Severity of Depression and Suicidal Ideation in Psychiatric Patients-A Multicenter Pilot Analysis

Author

Sumiko Yoshida, Daisuke Miura, Hidenaga Yamamori, Yu-ichi Goto, Kotaro Hattori, Dongchon Kang, Takahiro A. Kato, Kohei Hayakawa, Daiki Setoyama, Hiroshi Kunugi, Mina Sato-Kasai, Shigenobu Kanba, Masahiro Ohgidani, Norihiro Shimokawa, Yuka Yasuda, Sachie Kaneko, Ryota Hashimoto, and Noriaki Sagata

Subjects

Metabolic Analysis, Male, Physiology, lcsh:Medicine, Pilot Projects, Biochemistry, Severity of Illness Index, Mass Spectrometry, Machine Learning, 0302 clinical medicine, Drug Metabolism, Hamd, Medicine and Health Sciences, Metabolites, lcsh:Science, Suicidal ideation, gamma-Aminobutyric Acid, Multidisciplinary, 3-Hydroxybutyric Acid, Depression, Hematology, Body Fluids, Suicide, Blood, Bioassays and Physiological Analysis, Creatinine, Female, medicine.symptom, Anatomy, Research Article, medicine.medical_specialty, Research and Analysis Methods, Blood Plasma, Citric Acid, Suicidal Ideation, 03 medical and health sciences, Severity of illness, Mental Health and Psychiatry, Metabolome, medicine, Metabolomics, Humans, Pharmacokinetics, Psychiatry, Pharmacology, Psychiatric Status Rating Scales, business.industry, Mood Disorders, lcsh:R, Hamilton Rating Scale for Depression, Biology and Life Sciences, medicine.disease, 030227 psychiatry, Patient Health Questionnaire, Clinical trial, Betaine, Metabolism, Mood disorders, lcsh:Q, Self Report, business, 030217 neurology & neurosurgery, Biomarkers, Chromatography, Liquid

Abstract

Evaluating the severity of depression (SOD), especially suicidal ideation (SI), is crucial in the treatment of not only patients with mood disorders but also psychiatric patients in general. SOD has been assessed on interviews such as the Hamilton Rating Scale for Depression (HAMD)-17, and/or self-administered questionnaires such as the Patient Health Questionnaire (PHQ)-9. However, these evaluation systems have relied on a person's subjective information, which sometimes lead to difficulties in clinical settings. To resolve this limitation, a more objective SOD evaluation system is needed. Herein, we collected clinical data including HAMD-17/PHQ-9 and blood plasma of psychiatric patients from three independent clinical centers. We performed metabolome analysis of blood plasma using liquid chromatography mass spectrometry (LC-MS), and 123 metabolites were detected. Interestingly, five plasma metabolites (3-hydroxybutyrate (3HB), betaine, citrate, creatinine, and gamma-aminobutyric acid (GABA)) are commonly associated with SOD in all three independent cohort sets regardless of the presence or absence of medication and diagnostic difference. In addition, we have shown several metabolites are independently associated with sub-symptoms of depression including SI. We successfully created a classification model to discriminate depressive patients with or without SI by machine learning technique. Finally, we produced a pilot algorithm to predict a grade of SI with citrate and kynurenine. The above metabolites may have strongly been associated with the underlying novel biological pathophysiology of SOD. We should explore the biological impact of these metabolites on depressive symptoms by utilizing a cross species study model with human and rodents. The present multicenter pilot study offers a potential utility for measuring blood metabolites as a novel objective tool for not only assessing SOD but also evaluating therapeutic efficacy in clinical practice. In addition, modification of these metabolites by diet and/or medications may be a novel therapeutic target for depression. To clarify these aspects, clinical trials measuring metabolites before/after interventions should be conducted. Larger cohort studies including non-clinical subjects are also warranted to clarify our pilot findings.

Published

2016

92. A homozygous mutation ofC12orf65causes spastic paraplegia with optic atrophy and neuropathy (SPG55)

Author

Yuichi Matsushima, Haruo Shimazaki, Shoji Tsuji, Jun Goto, Hideyuki Hatakeyama, Yuji Takahashi, Junko Honda, Yoshihisa Takiyama, Michito Namekawa, Yoko Fukuda, Imaharu Nakano, Hiroyuki Ishiura, Kumi Sakoe, Tametou Naoi, Chika Sakai, and Yu-ichi Goto

Subjects

Adult, Male, DNA Copy Number Variations, Genetic Linkage, Mitochondrial translation, Nonsense mutation, Single-nucleotide polymorphism, Biology, medicine.disease_cause, Mitochondrial Proteins, Atrophy, Genetics, medicine, Humans, Exome, Genetics (clinical), Exome sequencing, Mutation, Base Sequence, Spastic Paraplegia, Hereditary, Homozygote, Peripheral Nervous System Diseases, medicine.disease, Respiratory enzyme, Mitochondria, Pedigree, Optic Atrophy, Peptide Termination Factors

Abstract

Background Autosomal recessive hereditary spastic paraplegias (AR-HSP) constitute a heterogeneous group of neurodegenerative diseases involving pyramidal tracts dysfunction. The genes responsible for many types of AR-HSPs remain unknown. We attempted to identify the gene responsible for AR-HSP with optic atrophy and neuropathy. Methods The present study involved two patients in a consanguineous Japanese family. Neurologic examination and DNA analysis were performed for both patients, and a skin biopsy for one. We performed genome-wide linkage analysis involving single nucleotide polymorphism arrays, copy-number variation analysis, and exome sequencing. To clarify the mitochondrial functional alteration resulting from the identified mutation, we performed immunoblot analysis, mitochondrial protein synthesis assaying, blue native polyacrylamide gel electrophoresis (BN-PAGE) analysis, and respiratory enzyme activity assaying of cultured fibroblasts of the patient and a control. Results We identified a homozygous nonsense mutation (c.394C>T, p.R132X) in C12orf65 in the two patients in this family. This C12orf65 mutation was not found in 74 Japanese AR-HSP index patients without any mutations in previously known HSP genes. This mutation resulted in marked reduction of mitochondrial protein synthesis, followed by functional and structural defects in respiratory complexes I and IV. Conclusions This novel nonsense mutation in C12orf65 could cause AR-HSP with optic atrophy and neuropathy, resulting in a premature stop codon. The truncated C12orf65 protein must lead to a defect in mitochondrial protein synthesis and a reduction in the respiratory complex enzyme activity. Thus, dysfunction of mitochondrial translation could be one of the pathogenic mechanisms underlying HSPs.

Published

2012

93. CRIF1 Is Essential for the Synthesis and Insertion of Oxidative Phosphorylation Polypeptides in the Mammalian Mitochondrial Membrane

Author

Young Suk Jo, Seung-Wook Ryu, Yong Kyung Kim, Min Jeong Ryu, Jongkyeong Chung, Hideyuki Hatakeyama, Yong-Hyeon Yim, Surendar Tadi, Minho Shong, Minchul Kwon, Soung Jung Kim, Chul-Ho Lee, Young-Yun Kong, Jin-Man Kim, Ji-Hoon Park, Gi Ryang Kweon, Yu-ichi Goto, Sang Hee Lee, and Hyo Kyun Chung

Subjects

Physiology, Protein subunit, Blotting, Western, RNA, Cell Cycle Proteins, Translation (biology), Cell Biology, Oxidative phosphorylation, Mitochondrion, Biology, Cell Fractionation, Immunohistochemistry, Oxidative Phosphorylation, Mitochondrial Proteins, Mice, Biochemistry, Ribosomal protein, Mitochondrial Membranes, Animals, Inner membrane, Peptides, Inner mitochondrial membrane, Molecular Biology

Abstract

SummaryAlthough substantial progress has been made in understanding the mechanisms underlying the expression of mtDNA-encoded polypeptides, the regulatory factors involved in mitoribosome-mediated synthesis and simultaneous insertion of mitochondrial oxidative phosphorylation (OXPHOS) polypeptides into the inner membrane of mitochondria are still unclear. In the present study, disruption of the mouse Crif1 gene, which encodes a mitochondrial protein, resulted in a profound deficiency in OXPHOS caused by the disappearance of OXPHOS subunits and complexes in vivo. CRIF1 was associated with large mitoribosomal subunits that were located close to the polypeptide exit tunnel, and the elimination of CRIF1 led to both aberrant synthesis and defective insertion of mtDNA-encoded nascent OXPHOS polypeptides into the inner membrane. CRIF1 interacted with nascent OXPHOS polypeptides and molecular chaperones, e.g., Tid1. Taken together, these results suggest that CRIF1 plays a critical role in the integration of OXPHOS polypeptides into the mitochondrial membrane in mammals.

Published

2012

94. The incidence of hypoplasia of the corpus callosum in patients with dup (X)(q28) involvingMECP2is associated with the location of distal breakpoints

Author

Yu-ichi Goto, Takaya Nakane, Hiroshi Yoshihashi, Nobuhiko Okamoto, Kenji Kurosawa, Mitsuhiro Kato, Shozo Honda, Shin Hayashi, Issei Imoto, Seiji Mizuno, Eiji Nakagawa, Johji Inazawa, and Takeo Kubota

Subjects

Male, Heterozygote, congenital, hereditary, and neonatal diseases and abnormalities, Methyl-CpG-Binding Protein 2, MECP2 duplication syndrome, Neuroimaging, Biology, Bioinformatics, MECP2, Chromosome Breakpoints, X Chromosome Inactivation, Intellectual Disability, Chromosome Duplication, Gene duplication, Genetics, medicine, Humans, Abnormalities, Multiple, Alleles, Genetics (clinical), Genes, Dominant, Chromosomes, Human, X, Comparative Genomic Hybridization, Incidence, Chromosome Mapping, Infant, Chromosome Breakage, Low copy repeats, medicine.disease, Hypoplasia, Pedigree, Xq28, dup, Agenesis of Corpus Callosum, Chromosome breakage

Abstract

Duplications of Xq28 harboring the methyl CpG binding protein 2 (MECP2) gene explain approximately 1% of X-linked intellectual disability (XLID). The common clinical features observed in patients with dup(X)(q28) are severe ID, infantile hypotonia, mild dysmorphic features and a history of recurrent infections, and MECP2 duplication syndrome is now recognized as a clinical entity. While some patients with this syndrome have other characteristic phenotypes, the reason for the spectrum of phenotypes has not been clarified. Since dup(X)(q28) rearrangements vary in size and location, genes other than MECP2 might affect the phenotype. We used a high-density oligonucleotide array to carry out precise mapping in eight Japanese families in which dup(X)(q28) was detected using an in-house bacterial artificial chromosome-based microarray to screen cohorts of individuals with multiple congenital anomalies and intellectual disability (MCA/ID) or with XLID. We hypothesized that the size, gene content, and location of dup(X)(q28) may contribute to variable expressively observed in MECP2 duplication syndrome. Genotype-phenotype correlation in our cases together with cases reported in the literature suggested that copy-number gains between two low copy repeats (LCRK1 and LCRL1) are associated with the incidence of hypoplasia of the corpus callosum. Further studies are necessary to understand the mechanism of this association.

Published

2012

95. Importance of CAG repeat length in childhood-onset dentatorubral–pallidoluysian atrophy

Author

Yuko Saito, Satoko Kumada, Eiji Nakagawa, Hajime Tanaka, Shinsuke Maruyama, Yoshiaki Saito, Kenji Sugai, Yu-ichi Goto, Masayuki Sasaki, Narihiro Minami, Hirofumi Komaki, and Takashi Saito

Subjects

Adult, Male, medicine.medical_specialty, Pathology, Pediatrics, Neurology, Adolescent, Population, Disease, Epilepsy, Atrophy, Trinucleotide Repeats, medicine, Humans, Child, education, Retrospective Studies, education.field_of_study, Dentatorubral-pallidoluysian atrophy, Retrospective cohort study, Middle Aged, Myoclonic Epilepsies, Progressive, medicine.disease, Female, Neurology (clinical), Trinucleotide repeat expansion, Psychology

Abstract

To elucidate a relationship between CAG repeat expansion length and disease progression history in patients with childhood-onset dentatorubral-pallidoluysian atrophy (DRPLA). We retrospectively evaluated information from nine Japanese patients with disease onset reported as between 6 months and 12 years of age. CAG repeat length in these patients ranged from 62 to 93. A strong correlation was confirmed for the age of disease onset, with the onset of epilepsy and involuntary movements, emergence of regression, and autonomic symptoms. The age at becoming wheelchair-bound and initiation of tube feeding also showed a significant correlation with CAG repeat length. This is the first report detailing this aspect of DRPLA focusing on the childhood-onset population. Earlier disease milestones were revealed compared to the expected age based upon a previous report that contained data from the entire patient population, including adult-onset cases (Hasegawa et al. in Mov Disord 25:1694-1700, 2010). These results provide a basis for predicting the outcome of patients in this particular age group, as well as for assessing the results of future clinical therapeutic trials.

Published

2012

96. Methyl CpG-binding Protein Isoform MeCP2_e2 Is Dispensable for Rett Syndrome Phenotypes but Essential for Embryo Viability and Placenta Development

Author

Toshikuni Sasaoka, Akihiro Kurimasa, Yu-ichi Goto, Akihiro Otsuki, Shuhei Ide, Masayuki Itoh, Candice G.T. Tahimic, Mitsuo Oshimura, and Shigeru Noguchi

Subjects

Protein isoform, congenital, hereditary, and neonatal diseases and abnormalities, Cell Survival, Methyl-CpG-Binding Protein 2, Placenta, Apoptosis, Rett syndrome, Biology, Biochemistry, X-inactivation, Epigenesis, Genetic, MECP2, Mice, Exon, Pregnancy, mental disorders, Rett Syndrome, medicine, Animals, Protein Isoforms, Allele, Molecular Biology, Alleles, Genetics, Alternative splicing, Gene Expression Regulation, Developmental, Molecular Bases of Disease, Cell Biology, medicine.disease, Molecular biology, Null allele, nervous system diseases, Alternative Splicing, Disease Models, Animal, Phenotype, Female, Protein Binding

Abstract

Methyl CpG-binding protein 2 gene (MeCP2) mutations are implicated in Rett syndrome (RTT), one of the common causes of female mental retardation. Two MeCP2 isoforms have been reported: MeCP2_e2 (splicing of all four exons) and MeCP2_e1 (alternative splicing of exons 1, 3, and 4). Their relative expression levels vary among tissues, with MeCP2_e1 being more dominant in adult brain, whereas MeCP2_e2 is expressed more abundantly in placenta, liver, and skeletal muscle. In this study, we performed specific disruption of the MeCP2_e2-defining exon 2 using the Cre-loxP system and examined the consequences of selective loss of MeCP2_e2 function in vivo. We performed behavior evaluation, gene expression analysis, using RT-PCR and real-time quantitative PCR, and histological analysis. We demonstrate that selective deletion of MeCP2_e2 does not result in RTT-associated neurological phenotypes but confers a survival disadvantage to embryos carrying a MeCP2_e2 null allele of maternal origin. In addition, we reveal a specific requirement for MeCP2_e2 function in extraembryonic tissue, where selective loss of MeCP2_e2 results in placenta defects and up-regulation of peg-1, as determined by the parental origin of the mutant allele. Taken together, our findings suggest a novel role for MeCP2 in normal placenta development and illustrate how paternal X chromosome inactivation in extraembryonic tissues confers a survival disadvantage for carriers of a mutant maternal MeCP2_e2 allele. Moreover, our findings provide an explanation for the absence of reports on MeCP2_e2-specific exon 2 mutations in RTT. MeCP2_e2 mutations in humans may result in a phenotype that evades a diagnosis of RTT.

Published

2012

97. Peracetylated N-Acetylmannosamine, a Synthetic Sugar Molecule, Efficiently Rescues Muscle Phenotype and Biochemical Defects in Mouse Model of Sialic Acid-deficient Myopathy

Author

Yu-ichi Goto, Ikuya Nonaka, Satoru Noguchi, Ichizo Nishino, Yukiko K. Hayashi, Tomoharu Tokutomi, and May Christine V. Malicdan

Subjects

Mice, Transgenic, Biology, Biochemistry, Mice, chemistry.chemical_compound, N-Acetylmannosamine, medicine, Animals, Humans, Muscular dystrophy, Muscle, Skeletal, Myopathy, Molecular Biology, Hereditary inclusion body myopathy, Hexosamines, Molecular Bases of Disease, Cell Biology, medicine.disease, Phenotype, N-Acetylneuraminic Acid, Muscle atrophy, Sialic acid, Distal Myopathies, Disease Models, Animal, chemistry, sense organs, medicine.symptom, N-Acetylneuraminic acid

Abstract

Distal myopathy with rimmed vacuoles/hereditary inclusion body myopathy (DMRV/hIBM), characterized by progressive muscle atrophy, weakness, and degeneration, is due to mutations in GNE, a gene encoding a bifunctional enzyme critical in sialic acid biosynthesis. In the DMRV/hIBM mouse model, which exhibits hyposialylation in various tissues in addition to muscle atrophy, weakness, and degeneration, we recently have demonstrated that the myopathic phenotype was prevented by oral administration of N-acetylneuraminic acid, N-acetylmannosamine, and sialyllactose, underscoring the crucial role of hyposialylation in the disease pathomechanism. The choice for the preferred molecule, however, was limited probably by the complex pharmacokinetics of sialic acids and the lack of biomarkers that could clearly show dose response. To address these issues, we screened several synthetic sugar compounds that could increase sialylation more remarkably and allow demonstration of measurable effects in the DMRV/hIBM mice. In this study, we found that tetra-O-acetylated N-acetylmannosamine increased cell sialylation most efficiently, and in vivo evaluation in DMRV/hIBM mice revealed a more dramatic, measurable effect and improvement in muscle phenotype, enabling us to establish analysis of protein biomarkers that can be used for assessing response to treatment. Our results provide a proof of concept in sialic acid-related molecular therapy with synthetic monosaccharides.

Published

2012

98. A case of pyruvate dehydrogenase E1α subunit deficiency with antenatal brain dysgenesis demonstrated by prenatal sonography and magnetic resonance imaging

Author

Jiu Okuno, Shinya Imada, Tsuguhiro Horikoshi, Yu-ichi Goto, Shunsuke Tamaru, Akihiko Kikuchi, Kaori Ishikawa, Shinichi Hirabayashi, and Kimiyo Takagi

Subjects

Adult, Nervous system, medicine.medical_specialty, Pathology, Ultrasonography, Prenatal, Dysgenesis, Pregnancy, Internal medicine, medicine, Humans, Pyruvate Dehydrogenase (Lipoamide), Radiology, Nuclear Medicine and imaging, Fetus, medicine.diagnostic_test, business.industry, Infant, Newborn, Brain, Magnetic resonance imaging, medicine.disease, Pyruvate dehydrogenase complex, Echoencephalography, Magnetic Resonance Imaging, Pyruvate dehydrogenase deficiency, medicine.anatomical_structure, Endocrinology, Female, Leigh Disease, business

Abstract

Prenatal depiction of brain dysgenesis in patients with pyruvate dehydrogenase complex (PDHc) deficiencies has been infrequently reported. As PDHc plays a critical role in the brain that obtains all of the energy from the aerobic oxidation of glucose, its deficiency is a severe inborn disorder of metabolism, which predominantly affects the nervous system. This report describes a case of PDHc deficiency with antenatal brain dysgenesis depicted in detail by fetal ultrasound and magnetic resonance imaging. This is the first case report clearly demonstrating the developing mechanism and time course of antenatal brain lesions in a patient with PDHc deficiency.

Published

2011

99. A loss-of-function mutation in the SLC9A6 gene causes X-linked mental retardation resembling Angelman syndrome

Author

Kayoko Saito, Hiroshi Kanazawa, Yu-ichi Goto, Yumi Takahashi, Shinji Saitoh, Kana Hosoki, Makoto Funatsuka, and Masafumi Matsushita

Subjects

Male, Sodium-Hydrogen Exchangers, DNA Mutational Analysis, Molecular Sequence Data, Nonsense-mediated decay, Down-Regulation, Biology, medicine.disease_cause, Cell Line, Cellular and Molecular Neuroscience, Angelman syndrome, Happy puppet syndrome, medicine, Humans, Amino Acid Sequence, RNA, Messenger, Gene, Genetics (clinical), X chromosome, Genetics, Mutation, Base Sequence, Genome, Human, Reverse Transcriptase Polymerase Chain Reaction, medicine.disease, Phenotype, Human genetics, Nonsense Mediated mRNA Decay, Psychiatry and Mental health, Mental Retardation, X-Linked, Mutant Proteins, Angelman Syndrome

Abstract

SLC9A6 mutations have been reported in families in whom X-linked mental retardation (XMR) mimics Angelman syndrome (AS). However, the relative importance of SLC9A6 mutations in patients with an AS-like phenotype or XMR has not been fully investigated. Here, the involvement of SLC9A6 mutations in 22 males initially suspected to have AS but found on genetic testing not to have AS (AS-like cohort), and 104 male patients with XMR (XMR cohort), was investigated. A novel SLC9A6 mutation (c.441delG, p.S147fs) was identified in one patient in the AS-like cohort, but no mutation was identified in XMR cohort, suggesting mutations in SLC9A6 are not a major cause of the AS-like phenotype or XMR. The patient with the SLC9A6 mutation showed the typical AS phenotype, further demonstrating the similarity between patients with AS and those with SLC9A6 mutations. To clarify the effect of the SLC9A6 mutation, we performed RT-PCR and Western blot analysis on lymphoblastoid cells from the patient. Expression of the mutated transcript was significantly reduced, but was restored by cycloheximide treatment, indicating the presence of nonsense mediated mRNA decay. Western blot analysis demonstrated absence of the normal NHE6 protein encoded for by SLC9A6. Taken together, these findings indicate a loss-of-function mutation in SLC9A6 caused the phenotype in our patient.

Published

2011

100. A new phenotype of mitochondrial disease characterized by familial late-onset predominant axial myopathy and encephalopathy

Author

Hideyuki Hatakeyama, Yoko Sangatsuda, Itsuro Higuchi, Yusuke Sakiyama, Hiroshi Takashima, Yuji Okamoto, Osamu Watanabe, Yu-ichi Goto, Kumiko Michizono, Yukie Inamori, and Kimiyoshi Arimura

Subjects

Proband, Pathology, medicine.medical_specialty, Mitochondrial Diseases, Neuromuscular disease, Mitochondrial disease, DNA Mutational Analysis, Encephalopathy, Clinical Neurology, Case Reports, Late-onset, Biology, DNA, Mitochondrial, Pathology and Forensic Medicine, Electron Transport Complex IV, Cellular and Molecular Neuroscience, Camptocormia, Atrophy, medicine, Humans, Predominant axial myopathy, Muscle, Skeletal, Myopathy, Aged, Aged, 80 and over, Cerebellar ataxia, Neuromuscular Diseases, medicine.disease, Succinate Dehydrogenase, Female, Neurology (clinical), medicine.symptom, Familial case

Abstract

Axial myopathy is a rare neuromuscular disease that is characterized by paraspinal muscle atrophy and abnormal posture, most notably camptocormia (also known as bent spine). The genetic cause of familial axial myopathy is unknown. Described here are the clinical features and cause of late-onset predominant axial myopathy and encephalopathy. A 73-year-old woman presented with a 10-year history of severe paraspinal muscle atrophy and cerebellar ataxia. Her 84-year-old sister also developed late-onset paraspinal muscle atrophy and generalized seizures with encephalopathy. Computed tomography showed severe atrophy and fatty degeneration of their paraspinal muscles. Their mother and maternal aunt also developed bent spines. The existence of many ragged-red fibers and cytochrome c oxidase-negative fibers in the biceps brachii muscle of the proband indicated a mitochondrial abnormality. No significant abnormalities were observed in the respiratory chain enzyme activities; however, the activities of complexes I and IV were relatively low compared with the activities of other complexes. Sequence analysis of the mitochondrial DNA from the muscle revealed a novel heteroplasmic mutation (m.602CT) in the mitochondrial tRNA(Phe) gene. This familial case of late-onset predominant axial myopathy and encephalopathy may represent a new clinical phenotype of a mitochondrial disease.

Published

2011