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1. Minocycline prevents early age-related cognitive decline in a mouse model of intellectual disability caused by ZBTB18/RP58 haploinsufficiency

Author

Tomoko Tanaka, Shinobu Hirai, Hiroyuki Manabe, Kentaro Endo, Hiroko Shimbo, Yasumasa Nishito, Junjiro Horiuchi, Hikari Yoshitane, and Haruo Okado

Subjects
Intellectual disability, Cognitive decline, DNA damage, DNA repair, Inflammation, ZBTB18/RP58, Neurology. Diseases of the nervous system, RC346-429
Abstract

Abstract Haploinsufficiency of the transcriptional repressor ZBTB18/RP58 is associated with intellectual disability. However, the mechanisms causing this disability are unknown, and preventative measures and treatments are not available. Here, we assessed multiple behaviors in Zbtb18/Rp58 heterozygous-knockout mice, and examined local field potentials, DNA fragmentation, mitochondrial morphology, and performed histochemical and transcriptome analyses in the hippocampus to evaluate chronic inflammation. In wild-type mice, object location memory was present at a similar level at 2 and 4–5 months of age, and became impaired at 12–18 months. In contrast, Zbtb18/Rp58 heterozygous-knockout mice displayed early onset impairments in object location memory by 4–5 months of age. These mice also exhibited earlier accumulation of DNA and mitochondrial damage, and activated microglia in the dentate gyrus, which are associated with defective DNA repair. Notably, chronic minocycline therapy, which has neuroprotective and anti-inflammatory effects, attenuated age-related phenotypes, including accumulation of DNA damage, increased microglial activation, and impairment of object location memory. Our results suggest that Zbtb18/Rp58 activity is required for DNA repair and its reduction results in DNA and mitochondrial damage, increased activation of microglia, and inflammation, leading to accelerated declines in cognitive functions. Minocycline has potential as a therapeutic agent for the treatment of ZBTB18/RP58 haploinsufficiency-associated cognitive dysfunction.

Published
2024
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2. Serotonergic neurons control cortical neuronal intracellular energy dynamics by modulating astrocyte-neuron lactate shuttle

Author

Akiyo Natsubori, Shinobu Hirai, Soojin Kwon, Daisuke Ono, Fei Deng, Jinxia Wan, Momoka Miyazawa, Takashi Kojima, Haruo Okado, Akihiro Karashima, Yulong Li, Kenji F. Tanaka, and Makoto Honda

Subjects
Biological sciences, Neuroscience, molecular neuroscience, Science
Abstract

Summary: The central serotonergic system has multiple roles in animal physiology and behavior, including sleep-wake control. However, its function in controlling brain energy metabolism according to the state of animals remains undetermined. Through in vivo monitoring of energy metabolites and signaling, we demonstrated that optogenetic activation of raphe serotonergic neurons increased cortical neuronal intracellular concentration of ATP, an indispensable cellular energy molecule, which was suppressed by inhibiting neuronal uptake of lactate derived from astrocytes. Raphe serotonergic neuronal activation induced cortical astrocytic Ca2+ and cAMP surges and increased extracellular lactate concentrations, suggesting the facilitation of lactate release from astrocytes. Furthermore, chemogenetic inhibition of raphe serotonergic neurons partly attenuated the increase in cortical neuronal intracellular ATP levels as arousal increased in mice. Serotonergic neuronal activation promoted an increase in cortical neuronal intracellular ATP levels, partly mediated by the facilitation of the astrocyte-neuron lactate shuttle, contributing to state-dependent optimization of neuronal intracellular energy levels.

Published
2023
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3. RP58 Regulates the Multipolar-Bipolar Transition of Newborn Neurons in the Developing Cerebral Cortex

Author

Chiaki Ohtaka-Maruyama, Shinobu Hirai, Akiko Miwa, Julian Ik-Tsen Heng, Hiroshi Shitara, Rie Ishii, Choji Taya, Hitoshi Kawano, Masataka Kasai, Kazunori Nakajima, and Haruo Okado

Subjects
Biology (General), QH301-705.5
Abstract

Accumulating evidence suggests that many brain diseases are associated with defects in neuronal migration, suggesting that this step of neurogenesis is critical for brain organization. However, the molecular mechanisms underlying neuronal migration remain largely unknown. Here, we identified the zinc-finger transcriptional repressor RP58 as a key regulator of neuronal migration via multipolar-to-bipolar transition. RP58−/− neurons exhibited severe defects in the formation of leading processes and never shifted to the locomotion mode. Cre-mediated deletion of RP58 using in utero electroporation in RP58flox/flox mice revealed that RP58 functions in cell-autonomous multipolar-to-bipolar transition, independent of cell-cycle exit. Finally, we found that RP58 represses Ngn2 transcription to regulate the Ngn2-Rnd2 pathway; Ngn2 knockdown rescued migration defects of the RP58−/− neurons. Our findings highlight the critical role of RP58 in multipolar-to-bipolar transition via suppression of the Ngn2-Rnd2 pathway in the developing cerebral cortex.

Published
2013
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4. Methamphetamine increases locomotion and dopamine transporter activity in dopamine d5 receptor-deficient mice.

Author

Seiji Hayashizaki, Shinobu Hirai, Yumi Ito, Yoshiko Honda, Yosefu Arime, Ichiro Sora, Haruo Okado, Tohru Kodama, and Masahiko Takada

Subjects
Medicine, Science
Abstract

Dopamine regulates the psychomotor stimulant activities of amphetamine-like substances in the brain. The effects of dopamine are mediated through five known dopamine receptor subtypes in mammals. The functional relevance of D5 dopamine receptors in the central nervous system is not well understood. To determine the functional relevance of D5 dopamine receptors, we created D5 dopamine receptor-deficient mice and then used these mice to assess the roles of D5 dopamine receptors in the behavioral response to methamphetamine. Interestingly, D5 dopamine receptor-deficient mice displayed increased ambulation in response to methamphetamine. Furthermore, dopamine transporter threonine phosphorylation levels, which regulate amphetamine-induced dopamine release, were elevated in D5 dopamine receptor-deficient mice. The increase in methamphetamine-induced locomotor activity was eliminated by pretreatment with the dopamine transporter blocker GBR12909. Taken together, these results suggest that dopamine transporter activity and threonine phosphorylation levels are regulated by D5 dopamine receptors.

Published
2013
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7. GAD67-mediated GABA Synthesis and Signaling Impinges on Directing Basket Cell Axonal Projections Toward Purkinje Cells in the Cerebellum

Author

Masahiko Watanabe, Haruo Okado, Shinobu Hirai, Ken Kobayashi, Mitsuhiko Yamada, Hideki Miwa, and Yuchio Yanagawa

Subjects
Mice, Knockout, Cerebellum, Glutamate Decarboxylase, Chemistry, Central nervous system, Glutamate decarboxylase, gamma-Aminobutyric acid, Cell biology, Motor coordination, Mice, Purkinje Cells, Parvalbumins, medicine.anatomical_structure, nervous system, Neurology, Basket cell, FLOX, medicine, Biological neural network, Animals, Neurology (clinical), gamma-Aminobutyric Acid, medicine.drug
Abstract

Gamma-aminobutyric acid (GABA) is a major inhibitory neurotransmitter in the central nervous system, synthesized by two isoforms of glutamate decarboxylase (GAD): GAD65 and GAD67. GABA may act as a trophic factor during brain development, but its contribution to the development and maturation of cerebellar neural circuits is not known. To understand the roles of GABA in cerebellar organization and associated functions in motor coordination and balance, we examined GAD65 conventional knock out (KO) mice and mice in which GAD67 was eliminated in parvalbumin-expressing neurons (PV-Cre; GAD67flox/flox mice). We found aberrant subcellular localization of the Shaker-type K channel Kv1.1 in basket cell collaterals of PV-Cre; GAD67 flox/flox mice and abnormal projections from basket cells to Purkinje cells in both mouse strains. We also found that altered synaptic properties of basket cell terminals to Purkinje cells in PV-Cre; GAD67flox/flox mice. Furthermore, PV-Cre; GAD67 flox/flox mice exhibited abnormal motor coordination in the rotarod test. These results indicate that GABA signaling in the cerebellum is critical for establishing appropriate connections between basket cells and Purkinje cells and is associated with motor coordination in mice.

Published
2021

9. High-sucrose diets contribute to brain angiopathy with impaired glucose uptake and psychosis-related higher brain dysfunctions in mice

Author

Takuya Sakamoto, Hiroko Shimbo, Seiji Shioda, Tomoya Nakamachi, Yasumasa Nishito, Hideki Miwa, Junjiro Horiuchi, Toshio Miyata, Yasuto Kunii, Atsuko Nagaoka, Toshifumi Tomoda, Mitsuhiro Miyashita, Takatoshi Hikida, Hirooki Yabe, Haruo Okado, Takashi Dan, Ryuta Izumi, Makoto Arai, Masanari Itokawa, Kazuhiro Suzuki, Mizuki Hino, Kazuya Toriumi, Tomoko Tanaka, and Shinobu Hirai

Subjects
High sucrose, Psychosis, medicine.medical_specialty, Multidisciplinary, business.industry, Glucose uptake, Brain dysfunction, SciAdv r-articles, Life Sciences, macromolecular substances, medicine.disease, Angiopathy, Pathogenesis, Endocrinology, Internal medicine, mental disorders, medicine, business, Research Article, Neuroscience
Abstract

Description, High-sugar diet in adolescence induces neural angiopathy and multiple psychiatric endophenotypes with impaired glucose logistics., Metabolic dysfunction is thought to contribute to the severity of psychiatric disorders; however, it has been unclear whether current high–simple sugar diets contribute to pathogenesis of these diseases. Here, we demonstrate that a high-sucrose diet during adolescence induces psychosis-related behavioral endophenotypes, including hyperactivity, poor working memory, impaired sensory gating, and disrupted interneuron function in mice deficient for glyoxalase-1 (GLO1), an enzyme involved in detoxification of sucrose metabolites. Furthermore, the high-sucrose diet induced microcapillary impairments and reduced brain glucose uptake in brains of Glo1-deficient mice. Aspirin protected against this angiopathy, enhancing brain glucose uptake and preventing abnormal behavioral phenotypes. Similar vascular damage to our model mice was found in the brains of randomly collected schizophrenia and bipolar disorder patients, suggesting that psychiatric disorders are associated with angiopathy in the brain caused by various environmental stresses, including metabolic stress.

Published
2021

10. A tetracycline antibiotic minocycline prevents early aging phenotypes in mice heterozygous for RP58

Author

Tomoko Tanaka, Shinobu Hirai, Hiroyuki Manabe, Kentaro Endo, Yasumasa Nishito, Hiroko Shimbo, Hikari Yoshitane, and Haruo Okado

Subjects
Microglia, DNA damage, DNA repair, Hippocampus, Endogeny, DNA Repair Pathway, Biology, Cell biology, chemistry.chemical_compound, medicine.anatomical_structure, chemistry, Cerebral cortex, medicine, DNA
Abstract

SummaryIn humans, cognitive and motor functions develop in association with maturation, followed by a decline in advancing age. In this study, we aimed to provide a method for extending healthy lifespan by preventing age-related phenomena. Therefore, we focused on RP58, a transcriptional repressor, whose expression is reduced during aging in the human cortex. In the Rp58 hetero-knockout (KO) mice, object location memory was impaired even at 4–5 months, while it was normal in the wild-type mice at 4–5 months but was impaired at 12–18 months. These results indicate an early onset of impaired spatial memory in the mutant mice. As the underlying mechanism, the Rp58 hetero-KO mice showed early onset of DNA damage accumulation and microglial activation in the dentate gyrus due to a DNA repair defect that is generally observed with aging. As another hallmark of aging, we focused on mitochondrial function and detected mitochondrial abnormalities in the Rp58 hetero-KO mice at 4–5 months. Notably, continuous treatments with minocycline, a neuroprotective and anti-inflammatory antibiotic, prevented the facilitation of age-related phenomena in the Rp58 hetero-KO mice. These results suggest the availability of the Rp58 hetero-KO mice as a novel mouse model of human-like early aging and provide a therapeutic strategy to prevent age-related phenomena using minocycline.HighlightRp58 hetero-KO mice exhibit early aging phenotypes including impairment of spatial cognitionRp58 hetero-KO mice show early accumulation of DNA damage due to a defect in the DNA repair systemTreatment with minocycline prevented cognitive dysfunction observed in Rp58 hetero-KO mice

Published
2021

11. Roles of GABA Signaling in Directing Basket Cell Axonal Projections Toward Purkinje Cells in the Cerebellum

Author

Ken Kobayashi, Masahiko Watanabe, Mitsuhiko Yamada, Shinobu Hirai, Yuchio Yanagawa, Hideki Miwa, and Haruo Okado

Subjects
Cerebellum, medicine.anatomical_structure, nervous system, Basket cell, medicine, Biology, Neuroscience
Abstract

Gamma-aminobutyric acid (GABA) is a major inhibitory neurotransmitter in the central nervous system, synthesized by two isoforms of glutamate decarboxylase (GAD): GAD65 and GAD67. GABA may act as a trophic factor during brain development, but its contribution to the development and maturation of cerebellar neural circuits is not known. To understand the roles of GABA in cerebellar development and associated functions in motor coordination and balance, we examined GAD65 conventional knock out (KO) mice and mice in which GAD67 was eliminated in parvalbumin-expressing neurons ( PV-Cre ; GAD67 flox/flox mice). We found aberrant subcellular localization of the Shaker-type K channel Kv1.1 in basket cell collaterals of PV-Cre ; GAD67 flox/flox mice and abnormal projections from basket cells to Purkinje cells in both mouse strains. Furthermore, PV-Cre ; GAD67 flox/flox mice exhibited abnormal motor coordination in the rotarod test. These results indicate that GABA signaling in the cerebellum during development is critical for establishing appropriate connections between basket cells and Purkinje cells and is associated with motor coordination in mice.

Published
2020

12. Early-life stress facilitates the development of Alzheimer’s disease pathology via angiopathy

Author

Masato Hosokawa, Shinobu Hirai, Tomoko Tanaka, Masato Hasegawa, Takashi Saito, Haruo Okado, Takaomi C. Saido, and Hiroshi Sakuma

Subjects
Pathology, medicine.medical_specialty, Mutation, biology, Microglia, business.industry, medicine.disease, medicine.disease_cause, Angiopathy, Pathogenesis, medicine.anatomical_structure, Amyloid precursor protein, biology.protein, Medicine, Immunohistochemistry, Fear conditioning, business, Prefrontal cortex
Abstract

BackgroundAlzheimer’s disease (AD), a progressive neurodegenerative disorder, is a serious social problem. Recently, several early-life factors have been associated with an increased risk of a clinical diagnosis of AD.MethodsWe investigated the involvement of early-life stress in AD pathogenesis using heterozygous the amyloid precursor protein (APP) mutant mice (AppNL-G-F/wt) and wild-type (Appwt/wt) mice. Maternal separation was used as an animal paradigm for early-life stress. Object location and fear conditioning tests were performed to measure cognitive functions, in addition to biochemical tests. Immunohistochemical analyses were performed after the behavioral tests.ResultsWe found that maternal-separated Appwt/wt mice showed narrowing of vessels and decreased pericyte coverage of capillaries in prefrontal cortex, while maternal-separated AppNL-G-F/wt mice additionally showed impairment of cognitive function, and earlier formation of Aβ plaques and disruption of the blood–brain barrier. Severe activation of microglia was detected in the maternal-separated AppNL-G-F/wt mice and maternal-separated Appwt/wt mice. At the early stage, morphological changes and inflammatory responses were observed in the microglia of the maternal-separated AppNL-G-F/wt mice and maternal-separated Appwt/wt mice, as well as morphological changes in the microglia of the non-maternal-separated AppNL-G-F/wt mice.ConclusionsMicroglia activation induced by maternal separation in combination with the APP mutation may impairs the vascular system, leading to AD progression. These findings therefore suggest that maternal separation causes early induction of AD pathology via angiopathy.

Published
2020

13. High Sucrose Diets Contribute to Brain Angiopathy with Impaired Glucose Uptake, and Psychosis-related Higher Brain Dysfunctions in Mice

Author

Mizuki Hino, Toshifumi Tomoda, Shinobu Hirai, Mitsuhiro Miyashita, Haruo Okado, Yasuto Kunii, Takeshi Dan, Masanori Itokawa, Kazuya Toriumi, Tomoko Tanaka, Hirooki Yabe, Junjiro Horiuchi, Hikida Takatoshi, Makoto Arai, Hideki Miwa, Seiji Shioda, Atsuko Nagaoka, Ryuta Izumi, Toshio Miyata, Takuya Sakamoto, Kazuhiro Suzuki, Tomoya Nakamachi, Yasumasa Nishito, and Hiroko Shimbo

Subjects
medicine.medical_specialty, Psychosis, Sensory gating, Interneuron, business.industry, Glucose uptake, medicine.disease, Angiopathy, medicine.anatomical_structure, Endocrinology, Schizophrenia, Internal medicine, Endophenotype, medicine, Bipolar disorder, business
Abstract

Metabolic dysfunction is thought to contribute to the severity of psychiatric disorders; however, it has been unclear whether current high-simple-sugar diets contribute to pathogenesis of these diseases. Here we demonstrate that a high-sucrose diet during adolescence induces psychosis-related behavioral endophenotypes, including hyperactivity, poor working memory, impaired sensory gating, and disrupted interneuron function in mice deficient for glyoxalase-1 (Glo1), an enzyme involved in detoxification of sucrose metabolites. Further, the high-sucrose diet induced microcapillary impairments and reduced brain glucose uptake in brains of Glo1 deficient mice. Aspirin protected against this angiopathy, enhancing brain glucose uptake, and preventing abnormal behavioral phenotypes. Similar vascular damage to our model mice was found in the brains of randomly collected schizophrenia and bipolar disorder patients, suggesting that psychiatric disorders are associated with angiopathy in the brain caused by various environmental stresses, including metabolic stress.

Published
2020

14. Early-life stress induces the development of Alzheimer's disease pathology via angiopathy

Author

Shinobu Hirai, Takaomi C. Saido, Hiroshi Sakuma, Haruo Okado, Masato Hasegawa, Takashi Saito, Tomoko Tanaka, and Masato Hosokawa

Subjects
Male, 0301 basic medicine, Pathology, medicine.medical_specialty, Amyloid beta, Prefrontal Cortex, Mice, Transgenic, medicine.disease_cause, Angiopathy, Pathogenesis, Mice, Amyloid beta-Protein Precursor, 03 medical and health sciences, Cognition, 0302 clinical medicine, Immune system, Developmental Neuroscience, Alzheimer Disease, Amyloid precursor protein, Animals, Medicine, Gene Knock-In Techniques, Prefrontal cortex, Mutation, Behavior, Animal, Microglia, biology, business.industry, Maternal Deprivation, medicine.disease, Capillaries, Mice, Inbred C57BL, Cerebral Amyloid Angiopathy, 030104 developmental biology, medicine.anatomical_structure, Neurology, Blood-Brain Barrier, biology.protein, Blood Vessels, Female, Corticosterone, Pericytes, business, Stress, Psychological, 030217 neurology & neurosurgery
Abstract

Alzheimer's disease (AD), a progressive neurodegenerative disorder, is a major societal, scientific, and economic problem. Several early-life factors associated with an increased risk for the clinical diagnosis of AD have recently been identified. In the present study, we investigated the involvement of early-life stress in the pathogenesis of AD using heterozygous amyloid precursor protein (APP) mutant mice (AppNL-G-F/wt) and wild-type (Appwt/wt) mice. We found that maternal-separated Appwt/wt mice showed narrowing of vessels and decreased pericyte coverage of capillaries in the prefrontal cortex, while maternal-separated AppNL-G-F/wt mice additionally showed the impairment of cognitive function, earlier formation of Aβ plaques, increased vessel-associated microglia, and disruption of the blood-brain barrier. Substantial activation of microglia was detected in the maternal-separated AppNL-G-F/wt mice and maternal-separated Appwt/wt mice. At an early stage, morphological changes and inflammatory responses were observed in the microglia of the maternal-separated AppNL-G-F/wt mice and maternal-separated Appwt/wt mice, and morphological changes in the microglia were observed in the non-maternal-separated AppNL-G-F/wt mice. Microglia activation induced by maternal separation in combination with the APP mutation may impair the vascular system, leading to AD progression. These findings therefore suggest that maternal separation results in the early induction of AD-related pathology via angiopathy.

Published
2021

15. High-sucrose diets contribute to brain angiopathy with impaired glucose uptake and psychosis-related higher brain dysfunctions in mice.

Author

Shinobu Hirai, Hideki Miwa, Tomoko Tanaka, Kazuya Toriumi, Yasuto Kunii, Hiroko Shimbo, Takuya Sakamoto, Mizuki Hino, Ryuta Izumi, Atsuko Nagaoka, Hirooki Yabe, Tomoya Nakamachi, Seiji Shioda, Takashi Dan, Toshio Miyata, Yasumasa Nishito, Kazuhiro Suzuki, Mitsuhiro Miyashita, Toshifumi Tomoda, and Takatoshi Hikida

Subjects
*ASPIRIN, *DOPAMINE, *FIBRIN, *MEDICAL sciences, *MICE
Abstract

The article focuses on high-sucrose diets contribute to brain angiopathy with impaired glucose uptake and psychosis-related higher brain dysfunctions in mice. Topics include the metabolic dysfunction is thought to contribute to the severity of psychiatric disorders, the unclear whether high–simple sugar diets contribute to pathogenesis of these diseases, and the demonstrate that a high-sucrose diet during adolescence induces psychosis-related behavioral endophenotypes.

Published
2021
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16. C9ORF72 dipeptide repeat poly-GA inclusions promote intracellular aggregation of phosphorylated TDP-43

Author

Shinobu Hirai, Masato Hosokawa, Takashi Nonaka, Masami Masuda-Suzukake, Masato Hasegawa, Aki Shimozawa, and Haruo Okado

Subjects
0301 basic medicine, Repetitive Sequences, Amino Acid, tau Proteins, Biology, Protein aggregation, 03 medical and health sciences, 0302 clinical medicine, C9orf72, mental disorders, Genetics, Humans, Phosphorylation, Molecular Biology, Genetics (clinical), Cells, Cultured, DNA Repeat Expansion, C9orf72 Protein, Amyotrophic Lateral Sclerosis, nutritional and metabolic diseases, RNA, General Medicine, Dipeptides, nervous system diseases, Cell biology, DNA-Binding Proteins, Open reading frame, 030104 developmental biology, Polyglutamic Acid, alpha-Synuclein, Frontotemporal Lobar Degeneration, Trinucleotide repeat expansion, 030217 neurology & neurosurgery, Intracellular
Abstract

Amyotrophic lateral sclerosis and frontotemporal lobar degeneration are neurodegenerative diseases characterized by accumulation of insoluble aggregates of phosphorylated 43 kDa TAR DNA-binding protein (TDP-43) and linked with abnormal expansion of a hexanucleotide repeat in an intron of chromosome 9 open reading frame 72 (C9ORF72). However, the relationship between C9ORF72 mutations and TDP-43 aggregation remains unknown. Non-ATG-dependent translation of C9ORF72 repeats produces dipeptide repeat proteins, which form p62-positive aggregates in cerebral cortex and cerebellum of patients. Here, we show that the formation of poly-GA protein inclusions induced intracellular aggregation of endogenous and exogenous TDP-43 in cultured cells. Poly-GA aggregation preceded accumulation of phosphorylated TDP-43. These inclusions induced intracellular aggregation of phosphorylated TDP-43, but not tau or α-synuclein. Formation of phosphorylated TDP-43 aggregates depends on the number of poly-GA repeats. Detergent-insoluble fraction from cells co-expressing poly-GA and TDP-43 could function as seeds for further TDP-43 aggregation. These findings suggest a novel pathogenic mechanism that poly-GA protein aggregation directly promotes pathogenic changes of TDP-43 without the formation of nuclear RNA foci containing GGGGCC repeat expansion or loss-of-function of the C9ORF72 protein.

Published
2018

17. Developmental Roles and Evolutionary Significance of AMPA-Type Glutamate Receptors

Author

Shinobu Hirai, Haruo Okado, and Kohji Hotta

Subjects
0301 basic medicine, Nervous system, Chemistry, Organogenesis, Central nervous system, Glutamate receptor, Metamorphosis, Biological, Glutamic Acid, AMPA receptor, General Biochemistry, Genetics and Molecular Biology, Cell biology, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, Receptors, Glutamate, Extracellular, medicine, Excitatory postsynaptic potential, Animals, Humans, Calcium, Receptors, AMPA, Signal transduction, Receptor
Abstract

Organogenesis and metamorphosis require the intricate orchestration of multiple types of cellular interactions and signaling pathways. Glutamate (Glu) is an excitatory extracellular signaling molecule in the nervous system, while Ca2+ is a major intracellular signaling molecule. The first Glu receptors to be cloned are Ca2+ -permeable receptors in mammalian brains. Although recent studies have focused on Glu signaling in synaptic mechanisms of the mammalian central nervous system, it is unclear how this signaling functions in development. Our recent article demonstrated that Ca2+ -permeable AMPA-type Glu receptors (GluAs) are essential for formation of a photosensitive organ, development of some neurons, and metamorphosis, including tail absorption and body axis rotation, in ascidian embryos. Based on findings in these embryos and mammalian brains, we formed several hypotheses regarding the evolution of GluAs, the non-synaptic function of Glu, the origin of GluA-positive neurons, and the neuronal network that controls metamorphosis in ascidians.

Published
2018

18. Benzodiazepines induce sequelae in immature mice with inflammation-induced status epilepticus

Author

Haruo Okado, Tomohiro Morio, Shinobu Hirai, and Keisuke Nakajima

Subjects
Male, Agonist, medicine.drug_class, Midazolam, Apoptosis, Convulsants, Inflammation, Status epilepticus, Pharmacology, Benzodiazepines, Mice, Behavioral Neuroscience, Epilepsy, Status Epilepticus, Seizures, medicine, Animals, GABA Agonists, Neurons, Benzodiazepine, GABAA receptor, business.industry, Pilocarpine, Receptors, GABA-A, medicine.disease, Mice, Inbred C57BL, Parvalbumins, Poly I-C, Neurology, Anesthesia, Exploratory Behavior, Anticonvulsants, Neurology (clinical), medicine.symptom, business, medicine.drug
Abstract

Objective Since benzodiazepines (BZPs) became clinically available for the treatment of status epilepticus (SE) in children, the incidence of neurological sequelae has increased. However, the cause–effect relationship is poorly understood. In this paper, we examined the effect of BZPs on an inflammation-induced SE (iSE) animal model. Method Inflammation was induced by injecting poly(I:C) (pIC 10 mg/kg, postnatal day 12–14), seizure was induced by injecting pilocarpine hydrochloride (PILO 200 mg/kg, postnatal day 15) into C57BL/6J mice, and the pIC + PILO mice were used as the iSE model (miSE). The GABA-A receptor agonist midazolam (MDL 0.5 mg/kg) was used to inhibit seizures. Sequelae were evaluated by performing behavior and immunohistochemical analyses in the chronic phase. Result The exploratory activity of mice in the miSE plus MDL group increased significantly, indicating that hyperactivity was newly induced by MDL in miSE mice. The contextual fear memory of the miSE mice was also significantly increased and that of miSE treated with MDL returned to the normal level. The parvalbumin-positive GABA neurons were decreased in number by pIC + PILO which was rescued by MDL. Apoptosis marker ssDNA-positive cells were increased by pIC + PILO which could not be rescued by MDL. Therefore, we propose that BZP-dependent therapy for SE needs to be rethought from the perspective of using other treatment approaches.

Published
2015

19. AMPA glutamate receptors are required for sensory-organ formation and morphogenesis in the basal chordate

Author

Atsuo Nishino, Yasushi Okamura, Shinobu Hirai, Haruo Okado, Yoshihiro Kubo, Kohji Hotta, and Shigeo Okabe

Subjects
0301 basic medicine, Male, Xenopus, Central nervous system, Green Fluorescent Proteins, Morphogenesis, Chordate, AMPA receptor, Biology, 03 medical and health sciences, medicine, Animals, Ciona intestinalis, Multidisciplinary, Glutamate receptor, Gene Expression Regulation, Developmental, Sense Organs, Biological Sciences, biology.organism_classification, Ciona, 030104 developmental biology, medicine.anatomical_structure, Amino Acid Substitution, Receptors, Glutamate, Gene Knockdown Techniques, Larva, Excitatory postsynaptic potential, Oocytes, Calcium, Female, Neuroscience
Abstract

AMPA-type glutamate receptors (GluAs) mediate fast excitatory transmission in the vertebrate central nervous system (CNS), and their function has been extensively studied in the mature mammalian brain. However, GluA expression begins very early in developing embryos, suggesting that they may also have unidentified developmental roles. Here, we identify developmental roles for GluAs in the ascidian Ciona intestinalis Mammals express Ca2+-permeable GluAs (Ca-P GluAs) and Ca2+-impermeable GluAs (Ca-I GluAs) by combining subunits derived from four genes. In contrast, ascidians have a single gluA gene. Taking advantage of the simple genomic GluA organization in ascidians, we knocked down (KD) GluAs in Ciona and observed severe impairments in formation of the ocellus, a photoreceptive organ used during the swimming stage, and in resorption of the tail and body axis rotation during metamorphosis to the adult stage. These defects could be rescued by injection of KD-resistant GluAs. GluA KD phenotypes could also be reproduced by expressing a GluA mutant that dominantly inhibits glutamate-evoked currents. These results suggest that, in addition to their role in synaptic communication in mature animals, GluAs also have critical developmental functions.

Published
2017

20. Distinct pathways leading to TDP-43-induced cellular dysfunctions

Author

Haruhiko Akiyama, Masato Hosokawa, Akiko Miwa, Shinobu Hirai, Makiko Yamashita, Masato Hasegawa, Takashi Nonaka, Haruo Okado, and Tetsuaki Arai

Subjects
Programmed cell death, Sp1 Transcription Factor, Apoptosis, RNA polymerase II, Biology, Cell Line, Tumor, mental disorders, Genetics, Humans, Cytotoxic T cell, Cyclic AMP Response Element-Binding Protein, Molecular Biology, Transcription factor, Genetics (clinical), Neurons, Amyotrophic Lateral Sclerosis, nutritional and metabolic diseases, RNA, General Medicine, Molecular biology, nervous system diseases, DNA-Binding Proteins, G2 Phase Cell Cycle Checkpoints, Gene Expression Regulation, Cell culture, Frontotemporal Dementia, biology.protein, RNA Polymerase II, Peptides, Metabolic Networks and Pathways, Intracellular
Abstract

TAR DNA-binding protein of 43 kDa (TDP-43) is the major component protein of inclusions found in brains of patients with amyotrophic lateral sclerosis (ALS) and frontotemporal lobar degeneration (FTLD-TDP). However, the molecular mechanisms by which TDP-43 causes neuronal dysfunction and death remain unknown. Here, we report distinct cytotoxic effects of full-length TDP-43 (FL-TDP) and its C-terminal fragment (CTF) in SH-SY5Y cells. When FL-TDP was overexpressed in the cells using a lentiviral system, exogenous TDP-43, like endogenous TDP-43, was expressed mainly in nuclei of cells without any intracellular inclusions. However, these cells showed striking cell death, caspase activation and growth arrest at G2/M phase, indicating that even simple overexpression of TDP-43 induces cellular dysfunctions leading to apoptosis. On the other hand, cells expressing TDP-43 CTF showed cytoplasmic aggregates but without significant cell death, compared with cells expressing FL-TDP. Confocal microscopic analyses revealed that RNA polymerase II (RNA pol II) and several transcription factors, such as specificity protein 1 and cAMP-response-element-binding protein, were co-localized with the aggregates of TDP-43 CTF, suggesting that sequestration of these factors into TDP-43 aggregates caused transcriptional dysregulation. Indeed, accumulation of RNA pol II at TDP-43 inclusions was detected in brains of patients with FTLD-TDP. Furthermore, apoptosis was not observed in affected neurons of FTLD-TDP brains containing phosphorylated and aggregated TDP-43 pathology. Our results suggest that different pathways of TDP-43-induced cellular dysfunction may contribute to the degeneration cascades involved in the onset of ALS and FTLD-TDP.

Published
2014

22. RP58 controls neuron and astrocyte differentiation by downregulating the expression ofId1-4genes in the developing cortex

Author

Shigeo Okabe, Akiko Miwa, Haruo Okado, Chiaki Ohtaka-Maruyama, Shinobu Hirai, Masataka Kasai, and Yutaka Hata

Subjects
Regulation of gene expression, Gene knockdown, General Immunology and Microbiology, General Neuroscience, Cellular differentiation, Biology, Molecular biology, General Biochemistry, Genetics and Molecular Biology, Neural stem cell, Cell biology, Astrocyte differentiation, Corticogenesis, medicine.anatomical_structure, Cerebral cortex, medicine, Progenitor cell, Molecular Biology
Abstract

Appropriate number of neurons and glial cells is generated from neural stem cells (NSCs) by the regulation of cell cycle exit and subsequent differentiation. Although the regulatory mechanism remains obscure, Id (inhibitor of differentiation) proteins are known to contribute critically to NSC proliferation by controlling cell cycle. Here, we report that a transcriptional factor, RP58, negatively regulates all four Id genes (Id1–Id4) in developing cerebral cortex. Consistently, Rp58 knockout (KO) mice demonstrated enhanced astrogenesis accompanied with an excess of NSCs. These phenotypes were mimicked by the overexpression of all Id genes in wild-type cortical progenitors. Furthermore, Rp58 KO phenotypes were rescued by the knockdown of all Id genes in mutant cortical progenitors but not by the knockdown of each single Id gene. Finally, we determined p57 as an effector gene of RP58-Id-mediated cell fate control. These findings establish RP58 as a novel key regulator that controls the self-renewal and differentiation of NSCs and restriction of astrogenesis by repressing all Id genes during corticogenesis.

Published
2012

23. Methamphetamine increases locomotion and dopamine transporter activity in dopamine d5 receptor-deficient mice

Author

Tohru Kodama, Yoshiko Honda, Haruo Okado, Yosefu Arime, Ichiro Sora, Masahiko Takada, Yumi Ito, Shinobu Hirai, and Seiji Hayashizaki

Subjects
Dopamine, Dopamine Plasma Membrane Transport Proteins, Science, Pharmacology, Methamphetamine, Mice, Dopamine receptor D1, Dopamine receptor D3, Dopamine receptor D2, medicine, Animals, Receptors, Dopamine D5, Phosphorylation, Dopamine transporter, Mice, Knockout, Multidisciplinary, biology, Chemistry, Dopaminergic, Mice, Inbred C57BL, Dopamine receptor, biology.protein, Medicine, Locomotion, Research Article, medicine.drug
Abstract

Dopamine regulates the psychomotor stimulant activities of amphetamine-like substances in the brain. The effects of dopamine are mediated through five known dopamine receptor subtypes in mammals. The functional relevance of D5 dopamine receptors in the central nervous system is not well understood. To determine the functional relevance of D5 dopamine receptors, we created D5 dopamine receptor-deficient mice and then used these mice to assess the roles of D5 dopamine receptors in the behavioral response to methamphetamine. Interestingly, D5 dopamine receptor-deficient mice displayed increased ambulation in response to methamphetamine. Furthermore, dopamine transporter threonine phosphorylation levels, which regulate amphetamine-induced dopamine release, were elevated in D5 dopamine receptor-deficient mice. The increase in methamphetamine-induced locomotor activity was eliminated by pretreatment with the dopamine transporter blocker GBR12909. Taken together, these results suggest that dopamine transporter activity and threonine phosphorylation levels are regulated by D5 dopamine receptors.

Published
2013

24. RP58 controls neuron and astrocyte differentiation by downregulating the expression of Id1-4 genes in the developing cortex

Author

Shinobu, Hirai, Akiko, Miwa, Chiaki, Ohtaka-Maruyama, Masataka, Kasai, Shigeo, Okabe, Yutaka, Hata, and Haruo, Okado

Subjects
Cerebral Cortex, Mice, Knockout, Neurons, Repressor Proteins, Mice, Gene Expression Regulation, Astrocytes, Gene Knockdown Techniques, Animals, Gene Expression, Cell Differentiation, Inhibitor of Differentiation Proteins, Article
Abstract

Appropriate number of neurons and glial cells is generated from neural stem cells (NSCs) by the regulation of cell cycle exit and subsequent differentiation. Although the regulatory mechanism remains obscure, Id (inhibitor of differentiation) proteins are known to contribute critically to NSC proliferation by controlling cell cycle. Here, we report that a transcriptional factor, RP58, negatively regulates all four Id genes (Id1-Id4) in developing cerebral cortex. Consistently, Rp58 knockout (KO) mice demonstrated enhanced astrogenesis accompanied with an excess of NSCs. These phenotypes were mimicked by the overexpression of all Id genes in wild-type cortical progenitors. Furthermore, Rp58 KO phenotypes were rescued by the knockdown of all Id genes in mutant cortical progenitors but not by the knockdown of each single Id gene. Finally, we determined p57 as an effector gene of RP58-Id-mediated cell fate control. These findings establish RP58 as a novel key regulator that controls the self-renewal and differentiation of NSCs and restriction of astrogenesis by repressing all Id genes during corticogenesis.

Published
2011

25. The 5'-flanking region of the RP58 coding sequence shows prominent promoter activity in multipolar cells in the subventricular zone during corticogenesis

Author

Chiaki Ohtaka-Maruyama, A. Takahashi, Akiko Miwa, Haruo Okado, and Shinobu Hirai

Subjects
5' Flanking Region, Neurogenesis, 5' flanking region, Cre recombinase, Subventricular zone, Nerve Tissue Proteins, Chick Embryo, Biology, Transfection, Cerebral Ventricles, Mice, Cell Movement, Tubulin, Chlorocebus aethiops, medicine, Basic Helix-Loop-Helix Transcription Factors, Animals, RNA, Messenger, Cells, Cultured, Cerebral Cortex, Homeodomain Proteins, Mice, Knockout, Neocortex, Activator (genetics), General Neuroscience, SOXB1 Transcription Factors, Stem Cells, Gene Expression Regulation, Developmental, Promoter, Cell Differentiation, Embryo, Mammalian, Cell biology, Repressor Proteins, Corticogenesis, Luminescent Proteins, medicine.anatomical_structure, Electroporation, nervous system, Cerebral cortex, Cancer research, Transcription Factors
Abstract

Pyramidal neurons of the neocortex are produced from progenitor cells located in the neocortical ventricular zone (VZ) and subventricular zone (SVZ) during embryogenesis. RP58 is a transcriptional repressor that is strongly expressed in the developing brain and plays an essential role in corticogenesis. The expression of RP58 is strictly regulated in a time-dependent and spatially restricted manner. It is maximally expressed in E15-16 embryonic cerebral cortex, localized specifically to the cortical plate and SVZ of the neocortex, hippocampus, and parts of amygdala during brain development, and found in glutamatergic but not GABAergic neurons. Identification of the promoter activity underlying specific expression patterns provides important clues to their mechanisms of action. Here, we show that the RP58 gene promoter is activated prominently in multipolar migrating cells, the first in vivo analysis of RP58 promoter activity in the brain. The 5.3 kb 5′-flanking genomic DNA of the RP58 coding region demonstrates promoter activity in neurons both in vitro and in vivo . This promoter is highly responsive to the transcription factor neurogenin2 (Ngn2), which is a direct upstream activator of RP58 expression. Using in utero electroporation, we demonstrate that RP58 gene promoter activity is first detected in a subpopulation of pin-like VZ cells, then prominently activated in migrating multipolar cells in the multipolar cell accumulation zone (MAZ) located just above the VZ. In dissociated primary cultured cortical neurons, RP58 promoter activity mimics in vivo expression patterns from a molecular standpoint that RP58 is expressed in a fraction of Sox2-positive progenitor cells, Ngn2-positive neuronal committed cells, and Tuj1-positive young neurons, but not in Dlx2-positive GABAergic neurons. Finally, we show that Cre recombinase expression under the control of the RP58 gene promoter is a feasible tool for conditional gene switching in post-mitotic multipolar migrating young neurons in the developing cerebral cortex.

Published
2011

26. Co-localization of a novel transcriptional repressor simiRP58 with RP58

Author

Shinobu Hirai, Haruo Okado, Shigeo Okabe, Yutaka Hata, Akiyo Takahashi, Akiko Miwa, and Chiaki Ohtaka-Maruyama

Subjects
Male, Biophysics, Cell Biology, In situ hybridization, Biology, Biochemistry, Molecular biology, Spermatozoa, Repressor Proteins, Mice, medicine.anatomical_structure, Krüppel, Cytoplasm, Testis, medicine, Transcriptional Repressor, Animals, Luciferase, Tissue Distribution, Northern blot, Spermatogenesis, Molecular Biology, Nucleus, Cells, Cultured
Abstract

We have cloned a novel transcriptional repressor protein, termed simiRP58, which has high homology to RP58. Both simiRP58 and RP58 belong to the POZ domain and Kruppel Zn finger (POK) family of proteins. Using the luciferase assay system, we found that simiRP58 also has transcriptional repressor activity like RP58. Northern blotting and quantitative RT-PCR showed that simiRP58 was expressed in testes at the highest level. In situ hybridization of testes showed that simiRP58 is expressed by spermatocytes in only a portion of the seminiferous tubules. In contrast, expression of RP58 by spermatocytes was ubiquitous in all seminiferous tubules. Using COS-7 cells, we observed that simiRP58 was localized in the cytoplasm, which is in contrast to RP58 that was localized in the nucleus. Interestingly, co-transfection with simiRP58 and RP58 induced changes in the localization patterns of both proteins.

Published
2008

27. AMPA glutamate receptors are required for sensory-organ formation and morphogenesis in the basal chordate.

Author

Shinobu Hirai, Kohji Hotta, Yoshihiro Kubo, Shigeo Okabe, Yasushi Okamura, and Haruo Okado

Subjects
*CHORDATA genetics, *SEA squirt morphology, *BRAIN physiology, *GENE expression in mammals, *AMPA receptors, *MAMMAL development
Abstract

AMPA-type glutamate receptors (GluAs) mediate fast excitatory transmission in the vertebrate central nervous system (CNS), and their function has been extensively studied in the mature mammalian brain. However, GluA expression begins very early in developing embryos, suggesting that they may also have unidentified developmental roles. Here, we identify developmental roles for GluAs in the ascidian Ciona intestinalis. Mammals express Ca2+-permeable GluAs (Ca-P GluAs) and Ca2+-impermeable GluAs (Ca-I GluAs) by combining subunits derived from four genes. In contrast, ascidians have a single gluA gene. Taking advantage of the simple genomic GluA organization in ascidians, we knocked down (KD) GluAs in Ciona and observed severe impairments in formation of the ocellus, a photoreceptive organ used during the swimming stage, and in resorption of the tail and body axis rotation during metamorphosis to the adult stage. These defects could be rescued by injection of KD-resistant GluAs. GluA KD phenotypes could also be reproduced by expressing a GluA mutant that dominantly inhibits glutamate-evoked currents. These results suggest that, in addition to their role in synaptic communication in mature animals, GluAs also have critical developmental functions. [ABSTRACT FROM AUTHOR]

Published
2017
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28. RP58 represses Id3 gene promoter activity

Author

Chiaki Ohtaka-Maruyama, Shinobu Hirai, Haruo Okado, Akiyo Takahashi, Masataka Kasai, and Akiko Miwa

Subjects
General Neuroscience, Promoter, General Medicine, Biology, Molecular biology
Published
2009

33. The transcriptional repressor RP58 is crucial for cell-division patterning and neuronal survival in the developing cerebral cortex

Author

Shinobu Hirai, Akiyo Takahashi, Masaharu Ogawa, Osamu Suzuki, Masataka Kasai, Akiko Miwa, Toshio Terashima, Yoshinobu Sugitani, Hitoshi Kawano, Keiji Mochida, Chiaki Ohtaka-Maruyama, Reiko Ishida, Haruo Okado, Junichiro Matsuda, Kazunori Nakajima, Yuko Fukuda, Takao Honda, and Katsunori Aoki

Subjects
medicine.anatomical_structure, Cell division, Cerebral cortex, General Neuroscience, Transcriptional Repressor, medicine, General Medicine, Biology, Neuroscience
Published
2009

34. D5 dopamine receptor is involved in the functional modification of dopamine transporter

Author

Yumi Ito, Shinobu Hirai, Yosefu Arime, Haruo Okado, Ichiro Sora, Masahiko Takada, Seiji Hayashizaki, Tohru Kodama, and Yoshiko Honda

Subjects
medicine.medical_specialty, biology, Chemistry, General Neuroscience, Dopaminergic, General Medicine, Endocrinology, Dopamine receptor D1, Dopamine receptor, Dopamine receptor D3, D2-like receptor, Internal medicine, Dopamine receptor D2, Cholecystokinin B receptor, medicine, biology.protein, Dopamine transporter
Published
2009

36. Cloning and characterization of an ascidian AMPA receptor

Author

Shinobu Hirai, Yasushi Okamura, Hiroki Takahashi, Atsuo Nishino, and Haruo Okado

Subjects
Cloning, Chemistry, General Neuroscience, Enzyme-linked receptor, General Medicine, AMPA receptor, Cell biology
Published
2007

38. Phosphorylation of TAR DNA-binding Protein of 43 kDa (TDP-43) by Truncated Casein Kinase 1δ Triggers Mislocalization and Accumulation of TDP-43.

Author

Takashi Nonaka, Genjiro Suzuki, Yoshinori Tanaka, Fuyuki Kametani, Shinobu Hirai, Haruo Okado, Tomoyuki Miyashita, Minoru Saitoe, Haruhiko Akiyama, Hisao Masai, and Masato Hasegawa

Subjects
*DNA-binding proteins, *PHOSPHORYLATION, *CASEIN kinase, *FRONTOTEMPORAL lobar degeneration, *NEUROBLASTOMA
Abstract

Intracellular aggregates of phosphorylated TDP-43 are a major component of ubiquitin-positive inclusions in the brains of patients with frontotemporal lobar degeneration and ALS and are considered a pathological hallmark. Here, to gain insight into the mechanism of intracellular TDP-43 accumulation, we examined the relationship between phosphorylation and aggregation of TDP-43. We found that expression of a hyperactive form of casein kinase 1 δ (CK1δ1-317, a C-terminally truncated form) promotes mislocalization and cytoplasmic accumulation of phosphorylated TDP-43 (ubiquitin- and p62-positive) in cultured neuroblastoma SH-SY5Y cells. Insoluble phosphorylated TDP-43 prepared from cells co-expressing TDP-43 and CK1δ1-317 functioned as seeds for TDP-43 aggregation in cultured cells, indicating that CK1δ1-317-induced aggregated TDP-43 has prion-like properties.Astriking toxicity and alterations of TDP-43 were also observed in yeast expressing TDP-43 and CK1δ1-317. Therefore, abnormal activation of CK1δ causes phosphorylation of TDP-43, leading to the formation of cytoplasmic TDP-43 aggregates, which, in turn, may trigger neurodegeneration. [ABSTRACT FROM AUTHOR]

Published
2016
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