Your search keyword '"Serikawa, Tadao"' showing total 35 results

1. Identification of Candidate Genes for Generalized Tonic-Clonic Seizures in Noda Epileptic Rat.

Author

Kuramoto, Takashi, Voigt, Birger, Nakanishi, Satoshi, Kitada, Kazuhiro, Nakamura, Tadashi, Wakamatsu, Kaori, Yoshihara, Minako, Suyama, Mikita, Uemura, Risa, Tanaka, Miyuu, Kuwamura, Mitsuru, Shimizu, Saki, Ohno, Yukihiro, Sasa, Masashi, and Serikawa, Tadao

Subjects

GENETICS of epilepsy, LABORATORY rats, CHOLECYSTOKININ receptors, PROGENY tests (Botany), PENTOBARBITAL, THERAPEUTICS

Abstract

The Noda epileptic rat (NER) exhibits generalized tonic-clonic seizures (GTCS). A genetic linkage analysis identified two GTCS-associated loci, Ner1 on Chr 1 and Ner3 on Chr 5. The wild-type Ner1 and Ner3 alleles suppressed GTCS when combined in double-locus congenic lines, but not when present in single-locus congenic lines. Global expression analysis revealed that cholecystokinin B receptor ( Cckbr) and suppressor of tumorigenicity 5 ( St5), which map within Ner1, and PHD finger protein 24 ( Phf24), which maps within Ner3, were significantly downregulated in NER. De novo BAC sequencing detected an insertion of an endogenous retrovirus sequence in intron 2 of the Phf24 gene in the NER genome, and PHF24 protein was almost absent in the NER brain. Phf24 encodes a G-interacting protein involved in GABA receptor signaling pathway. Based on these findings, we conclude that Cckbr, St5, and Phf24 are strong candidate genes for GTCS in NER. [ABSTRACT FROM AUTHOR]

Published

2017

2. Fat Mass Reduction With Adipocyte Hypertrophy and Insulin Resistance in Heterozygous PPARγ Mutant Rats.

Author

Gumbilai, Valentino, Ebihara, Ken, Aizawa-Abe, Megumi, Ebihara, Chihiro, Mingming Zhao, Yuji Yamamoto, Tomoji Mashimo, Kiminori Hosoda, Tadao Serikawa, Kazuwa Nakao, Zhao, Mingming, Yamamoto, Yuji, Mashimo, Tomoji, Hosoda, Kiminori, Serikawa, Tadao, and Nakao, Kazuwa

Subjects

PEROXISOME proliferator-activated receptors, LABORATORY rats, FAT cells, ALLELES, CELL analysis, MATHEMATICAL models, PHYSIOLOGY, PROTEIN metabolism, ADIPOSE tissues, ANIMAL experimentation, BLOOD sugar, BODY composition, HYPOGLYCEMIC agents, INSULIN resistance, GENETIC mutation, PROTEINS, RATS, TRANSGENIC animals, CYTOMETRY, GENETIC carriers, THIAZOLIDINEDIONES, CELL size, LIPODYSTROPHY, PHARMACODYNAMICS

Abstract

Agonist-induced activation of peroxisome proliferator-activated receptor-γ (PPARγ) stimulates adipocyte differentiation and insulin sensitivity. Patients with heterozygous PPARγ dominant-negative mutation develop partial lipodystrophy and insulin resistance. Inconsistent with this evidence in humans, it was reported that heterozygous PPARγ knockout mice have increased insulin sensitivity and that mice with heterozygous PPARγ dominant-negative mutation have normal insulin sensitivity and improved glucose tolerance. In the context of the interspecies intranslatability of PPARγ-related findings, we generated a PPARγ mutant rat with a loss-of-function mutation (Pparg(mkyo)) without dominant-negative activity by using the ENU (N-ethyl-N-nitrosourea) mutagenesis method. Heterozygous Pparg(mkyo/+) rats showed reduced fat mass with adipocyte hypertrophy and insulin resistance, which were highly predictable from known actions of PPARγ agonists and phenotypes of patients with the PPARγ mutation. This report is the first in our knowledge to clearly demonstrate that both alleles of PPARγ are required for normal adipocyte development and insulin sensitivity in vivo. Furthermore, the study indicates that PPARγ regulates mainly adipocyte number rather than adipocyte size in vivo. The choice of appropriate species as experimental models is critical, especially for the study of PPARγ. [ABSTRACT FROM AUTHOR]

Published

2016

3. Novel ENU-Induced Mutation in Tbx6 Causes Dominant Spondylocostal Dysostosis-Like Vertebral Malformations in the Rat.

Author

Abe, Koichiro, Takamatsu, Nobuhiko, Ishikawa, Kumiko, Tsurumi, Toshiko, Tanimoto, Sho, Sakurai, Yukina, Lisse, Thomas, Imai, Kenji, Serikawa, Tadao, and Mashimo, Tomoji

Subjects

GENETIC mutation, EMBRYOLOGY, LABORATORY rats, SEGMENTATION (Biology), MICROSATELLITE repeats, DNA-binding proteins

Abstract

Congenital vertebral malformations caused by embryonic segmentation defects are relatively common in humans and domestic animals. Although reverse genetics approaches in mice have provided information on the molecular mechanisms of embryonic somite segmentation, hypothesis-driven approaches cannot adequately reflect human dysmorphology within the population. In a N-ethyl-N-nitrosourea (ENU) mutagenesis project in Kyoto, the Oune mutant rat strain was isolated due to a short and kinked caudal vertebra phenotype. Skeletal staining of heterozygous rats showed partial loss of the cervical vertebrae as well as hemivertebrae and fused vertebral blocks in lumbar and sacral vertebrae. In homozygous embryos, severe displacement of the whole vertebrae was observed. The Oune locus was genetically mapped to rat chromosome 1 using 202 backcross animals and 50 genome-wide microsatellite markers. Subsequently, a miss-sense mutation in the Tbx6 gene was identified in the critical region. Although the mutation is located within the T-box domain near a predicted dimmer-interface, in vitro experiments revealed that the Tbx6 variant retains normal DNA binding ability and translational efficiency. However, the variant has decreased transcriptional activation potential in response to Notch-mediated signaling. Recently, it was reported that a dominant type of familial spondylocostal dysostosis is caused by a stoploss mutation in TBX6. Thus, we propose that partial dysfunction of Tbx6 leads to similar congenital vertebral malformations in both humans and rats. The Oune strain could be a unique animal model for dominant spondylocostal dysostosis and is useful for molecular dissection of the pathology of congenital vertebral malformations in humans. [ABSTRACT FROM AUTHOR]

Published

2015

4. Hcn1 Is a Tremorgenic Genetic Component in a Rat Model of Essential Tremor.

Author

Ohno, Yukihiro, Shimizu, Saki, Tatara, Ayaka, Imaoku, Takuji, Ishii, Takahiro, Sasa, Masashi, Serikawa, Tadao, and Kuramoto, Takashi

Subjects

ESSENTIAL tremor, KAINIC acid, LABORATORY rats, DISEASE incidence, PHYSIOLOGIC strain

Abstract

Genetic factors are thought to play a major role in the etiology of essential tremor (ET); however, few genetic changes that induce ET have been identified to date. In the present study, to find genes responsible for the development of ET, we employed a rat model system consisting of a tremulous mutant strain, TRM/Kyo (TRM), and its substrain TRMR/Kyo (TRMR). The TRM rat is homozygous for the tremor (tm) mutation and shows spontaneous tremors resembling human ET. The TRMR rat also carries a homozygous tm mutation but shows no tremor, leading us to hypothesize that TRM rats carry one or more genes implicated in the development of ET in addition to the tm mutation. We used a positional cloning approach and found a missense mutation (c. 1061 C>T, p. A354V) in the hyperpolarization-activated cyclic nucleotide-gated 1 channel (Hcn1) gene. The A354V HCN1 failed to conduct hyperpolarization-activated currents in vitro, implicating it as a loss-of-function mutation. Blocking HCN1 channels with ZD7288 in vivo evoked kinetic tremors in nontremulous TRMR rats. We also found neuronal activation of the inferior olive (IO) in both ZD7288-treated TRMR and non-treated TRM rats and a reduced incidence of tremor in the IO-lesioned TRM rats, suggesting a critical role of the IO in tremorgenesis. A rat strain carrying the A354V mutation alone on a genetic background identical to that of the TRM rats showed no tremor. Together, these data indicate that body tremors emerge when the two mutant loci, tm and Hcn1A354V, are combined in a rat model of ET. In this model, HCN1 channels play an important role in the tremorgenesis of ET. We propose that oligogenic, most probably digenic, inheritance is responsible for the genetic heterogeneity of ET. [ABSTRACT FROM AUTHOR]

Published

2015

5. Generation and Characterization of Severe Combined Immunodeficiency Rats

Author

Mashimo, Tomoji, Takizawa, Akiko, Kobayashi, Junya, Kunihiro, Yayoi, Yoshimi, Kazuto, Ishida, Saeko, Tanabe, Koji, Yanagi, Ami, Tachibana, Asato, Hirose, Jun, Yomoda, Jun-ichiro, Morimoto, Shiho, Kuramoto, Takashi, Voigt, Birger, Watanabe, Takeshi, Hiai, Hiroshi, Tateno, Chise, Komatsu, Kenshi, and Serikawa, Tadao

Subjects

GENE therapy, SEVERE combined immunodeficiency, LABORATORY rats, LYMPHOCYTES, TRANSPLANTATION of organs, tissues, etc., ZINC-finger proteins, XENOGRAFTS, KNOCKOUT mice

Abstract

Summary: Severe combined immunodeficiency (SCID) mice, the most widely used animal model of DNA-PKcs (Prkdc) deficiency, have contributed enormously to our understanding of immunodeficiency, lymphocyte development, and DNA-repair mechanisms, and they are ideal hosts for allogeneic and xenogeneic tissue transplantation. Here, we use zinc-finger nucleases to generate rats that lack either the Prkdc gene (SCID) or the Prkdc and Il2rg genes (referred to as F344-scid gamma [FSG] rats). SCID rats show several phenotypic differences from SCID mice, including growth retardation, premature senescence, and a more severe immunodeficiency without “leaky” phenotypes. Double-knockout FSG rats show an even more immunocompromised phenotype, such as the abolishment of natural killer cells. Finally, xenotransplantation of human induced pluripotent stem cells, ovarian cancer cells, and hepatocytes shows that SCID and FSG rats can act as hosts for xenogeneic tissue grafts and stem cell transplantation and may be useful for preclinical testing of new drugs. [ABSTRACT FROM AUTHOR]

Published

2012

6. Origins of Albino and Hooded Rats: Implications from Molecular Genetic Analysis across Modern Laboratory Rat Strains.

Author

Kuramoto, Takashi, Nakanishi, Satoshi, Ochiai, Masako, Nakagama, Hitoshi, Voigt, Birger, Serikawa, Tadao, and Laudet, Vincent

Subjects

LABORATORY rats, ANIMAL mutation, PHENOTYPES, PHENOL oxidase, MISSENSE mutation, ENDOGENOUS retroviruses

Abstract

Albino and hooded (or piebald) rats are one of the most frequently used laboratory animals for the past 150 years. Despite this fact, the origin of the albino mutation as well as the genetic basis of the hooded phenotype remained unclear. Recently, the albino mutation has been identified as the Arg299His missense mutation in the Tyrosinase gene and the hooded (H) locus has been mapped to the ,460-kb region in which only the Kit gene exists. Here, we surveyed 172 laboratory rat strains for the albino mutation and the hooded (h) mutation that we identified by positional cloning approach to investigate possible genetic roots and relationships of albino and hooded rats. All of 117 existing laboratory albino rats shared the same albino missense mutation, indicating they had only one single ancestor. Genetic fine mapping followed by de novo sequencing of BAC inserts covering the H locus revealed that an endogenous retrovirus (ERV) element was inserted into the first intron of the Kit gene where the hooded allele maps. A solitary long terminal repeat (LTR) was found at the same position to the ERV insertion in another allele of the H locus, which causes the so called Irish (hi) phenotype. The ERV and the solitary LTR insertions were completely associated with the hooded and Irish coat patterns, respectively, across all colored rat strains examined. Interestingly, all 117 albino rat strains shared the ERV insertion without any exception, which strongly suggests that the albino mutation had originally occurred in hooded rats. [ABSTRACT FROM AUTHOR]

Published

2012

7. Therapy for hyperthermia-induced seizures in Scn1a mutant rats.

Author

Hayashi, Keiichiro, Ueshima, Satoshi, Ouchida, Mamoru, Mashimo, Tomoji, Nishiki, Teiichi, Sendo, Toshiaki, Serikawa, Tadao, Matsui, Hideki, and Ohmori, Iori

Subjects

FEBRILE seizures, ANIMAL models in research, INFANTILE spasms, GENETIC mutation, CARBAMAZEPINE, HOT water, LABORATORY rats, THERAPEUTICS

Abstract

Mutations in the SCN1A gene, which encodes the α1 subunit of voltage-gated sodium channels, cause generalized epilepsy with febrile seizures plus (GEFS+) and severe myoclonic epilepsy of infancy (SMEI). N1417H- Scn1a mutant rats are considered to be an animal model of human FS+ or GEFS+. To assess the pharmacologic validity of this model, we compared the efficacies of eight different antiepileptic drugs (AEDs) for the treatment of hyperthermia-induced seizures using N1417H- Scn1a mutant rats. AEDs used in this study included valproate, carbamazepine (CBZ), phenobarbital, gabapentin, acetazolamide, diazepam (DZP), topiramate, and potassium bromide (KBr). The effects of these AEDs were evaluated using the hot water model, which is a model of experimental FS. Five-week-old rats were pretreated with each AED and immersed in water at 45°C to induce hyperthermia-induced seizures. The seizure manifestations and video-electroencephalographic recordings were evaluated. Furthermore, the effects of each AED on motor coordination and balance were assessed using the balance-beam test. KBr significantly reduced seizure durations, and its anticonvulsant effects were comparable to those of DZP. On the other hand, CBZ decreased the seizure threshold. In addition, DZP and not KBr showed significant impairment in motor coordination and balance. DZP and KBr showed potent inhibitory effects against hyperthermia-induced seizures in the Scn1a mutant rats, whereas CBZ exhibited adverse effects. These responses to hyperthermia-induced seizures were similar to those in patients with GEFS+ and SMEI. N1417H- Scn1a mutant rats may, therefore, be useful for testing the efficacy of new AEDs against FS in GEFS+ and SMEI patients. [ABSTRACT FROM AUTHOR]

Published

2011

8. A Mutation in the Gene Encoding Mitochondrial Mg2+ Channel MRS2 Results in Demyelination in the Rat.

Author

Kuramoto, Takashi, Kuwamura, Mitsuru, Tokuda, Satoko, Izawa, Takeshi, Nakane, Yoshifumi, Kitada, Kazuhiro, Akao, Masaharu, Guénet, Jean-Louis, and Serikawa, Tadao

Subjects

ANIMAL mutation, GENETIC code, MITOCHONDRIA, MAGNESIUM compounds, DEMYELINATION, LABORATORY rats, ANIMAL genetics

Published

2011

9. Identification of the Rat Rex Mutation as a 7-bp Deletion at Splicing Acceptor Site of the Krt71 Gene.

Author

KURAMOTO, Takashi, HIRANO, Ryuji, KUWAMURA, Mitsuru, and SERIKAWA, Tadao

Subjects

LABORATORY rats, HAIR follicles, GENETIC mutation, ANIMAL mutation, CHROMOSOMES, KERATIN, NUCLEOTIDES

Abstract

The article presents a study which examined morphologically the rat Rex (Re) mutation on chromosome 7 at splicing acceptor site of the keratin 71 (Krt71) gene which plays an important role in hair formation. The authors found dilatation of the hair follicle in rats as stated by the histopathological examination of dorsal skin samples with the dilated cyst lined by a flattened squamous epithelium with a granular cell layer. It states the need to amplify the exon 1-nitron 1 boundary to identify genomic nucleotide alteration of the Krt71 gene.

Published

2010

10. Genetic Quality Control of the Rat Strains at the National Bio Resource Project - Rat.

Author

Kuramoto, Takashi, Nakanishi, Satoshi, Yamasaki, Ken-ichi, Kumafuji, Kenta, Sakakibara, Yuichi, Neoda, Yuki, Takizawa, Akiko, Kaneko, Takehito, Otsuki, Mito, Hashimoto, Ryoko, Voigt, Birger, Mashimo, Tomoji, and Serikawa, Tadao

Subjects

LABORATORY rats, RATTUS norvegicus, GENETIC research, GENETIC markers, EMBRYOS, HUMAN chromosome abnormality diagnosis

Abstract

The National Bio Resource Project-Rat (NBRP-Rat) comprises the largest bank of laboratory rat (Rattus norvegicus) strains in the world. Its main focus is to develop infrastructure that will facilitate the systematic collection, preservation, and provision of rat strains. To breed effectively more than 180 rat strains in living stock, we establish the genetic control system in which a systematic set of genetic diagnoses and genetic monitoring are included. Genetic monitoring is performed by using 20 polymorphic markers. Monitoring is carried out when a living animal stock is re-established by using cryopreserved embryos or sperm or when a rat strain is first introduced to the NBRP-Rat by a depositor. Additional monitoring is then carried out on each strain every two years. Genetic diagnosis is performed largely by employing the Amp-FTA method. Protocols which detail how to perform a genetic diagnosis of 11 transgenes and 24 mutations have been made. Among the mutations, nine can be detected by simple gel electrophoresis of the PCR products, 11 by restriction enzyme treatment of the PCR products, and four by direct PCR product sequencing. Using this genetic control system, the NBRP-Rat can guarantee the genetic quality of its rat strains. [ABSTRACT FROM AUTHOR]

Published

2010

11. Generation of Knockout Rats with X-Linked Severe Combined Immunodeficiency (X-SCID) Using Zinc-Finger Nucleases.

Author

Mashimo, Tomoji, Takizawa, Akiko, Voigt, Birger, Yoshimi, Kazuto, Hiai, Hiroshi, Kuramoto, Takashi, and Serikawa, Tadao

Subjects

MURIDAE, GENETIC engineering, LABORATORY rats, IMMUNODEFICIENCY, GENE therapy, LOCUS (Genetics), FRUIT flies, GENE targeting, DRUG therapy

Abstract

Background: Although the rat is extensively used as a laboratory model, the inability to utilize germ line-competent rat embryonic stem (ES) cells has been a major drawback for studies that aim to elucidate gene functions. Recently, zinc-finger nucleases (ZFNs) were successfully used to create genome-specific double-stranded breaks and thereby induce targeted gene mutations in a wide variety of organisms including plants, drosophila, zebrafish, etc. Methodology/Principal Findings: We report here on ZFN-induced gene targeting of the rat interleukin 2 receptor gamma (Il2rg) locus, where orthologous human andmouse mutations cause X-linked severe combined immune deficiency (X-SCID). Co-injection of mRNAs encoding custom-designed ZFNs into the pronucleus of fertilized oocytes yielded genetically modified offspring at rates greater than 20%, which possessed a wide variety of deletion/insertion mutations. ZFN-modified founders faithfully transmitted their genetic changes to the next generation along with the severe combined immune deficiency phenotype. Conclusions and Significance: The efficient and rapid generation of gene knockout rats shows that using ZFN technology is a new strategy for creating gene-targeted rat models of human diseases. In addition, the X-SCID rats that were established in this study will be valuable in vivo tools for evaluating drug treatment or gene therapy as well as model systems for examining the treatment of xenotransplanted malignancies. [ABSTRACT FROM AUTHOR]

Published

2010

12. An informative set of SSLP markers and genomic profiles in the rat MHC, the RT1 complex.

Author

Takagi, Yumie, Kuramoto, Takashi, Voigt, Birger, Tsurumi, Toshiko, Nakanishi, Satoshi, Mashimo, Tomoji, Masui, Norio, and Serikawa, Tadao

Subjects

NUCLEOTIDES, GENETIC polymorphisms, HISTOCOMPATIBILITY, LABORATORY rats, GENETIC markers

Abstract

Almost 10,000 single nucleotide polymorphisms (SNPs) had been identified in the RT1 complex, the major histocompatibility complex of the rat, but less than ∼0.5% have been characterized. In the context of the incomplete characterization of most SNPs, simple sequence length polymorphism (SSLP) marker development is still valuable for understanding the involvement of genes in the RT1 in controlling disease susceptibility, since SSLPs are user-friendly and cost-effective genetic markers in rat genome analysis. In this study, we developed a set of 67 SSLP markers, including 57 novel markers, to cover the entire RT1 complex and then created genetic profiles across 67 rat strains. These markers are located almost every 50 kb in the RT1 complex and show comparable polymorphism; the average number of alleles was 8.04 ± 3.44 and the average polymorphic rate was 71 ± 23%. Interestingly, markers failing to amplify polymerase chain reaction products were highly observed in all strains except for BN/SsNHsd, which suggests the existence of highly variable genomic sequences or genomic rearrangements in the RT1 region across rat strains. Based on the phylogenic tree and individual genotyping data, we identified 28 SSLP marker haplotypes in the RT1 region that roughly consisted of three genomic regions. These findings provided new insight into the genomic organization of the RT1 complex and we recognized the need of additional RT1 genome sequences in different strains. Owing to the accuracy and ease of determination, PCR-based SSLP genotyping could replace serological typing in genetic analyses and characterization of rat major histocompatibility. [ABSTRACT FROM AUTHOR]

Published

2009

13. A set of highly informative rat simple sequence length polymorphism (SSLP) markers and genetically defined rat strains.

Author

Mashimo, Tomoji, Voigt, Birger, Tsurumi, Toshiko, Naoi, Kuniko, Nakanishi, Satoshi, Yamasaki, Ken-ichi, Kuramoto, Takashi, and Serikawa, Tadao

Subjects

RATS, GENETIC polymorphisms, TRANSGENIC organisms, LABORATORY rats, GENETICS

Abstract

Background: The National Bio Resource Project for the Rat in Japan (NBRP-Rat) is focusing on collecting, preserving and distributing various rat strains, including spontaneous mutant, transgenic, congenic, and recombinant inbred (RI) strains. To evaluate their value as models of human diseases, we are characterizing them using 109 phenotypic parameters, such as clinical measurements, internal anatomy, metabolic parameters, and behavioral tests, as part of the Rat Phenome Project. Here, we report on a set of 357 simple sequence length polymorphism (SSLP) markers and 122 rat strains, which were genotyped by the marker set. Results: The SSLP markers were selected according to their distribution patterns throughout the whole rat genome with an average spacing of 7.59 Mb. The average number of informative markers between all possible pairs of strains was 259 (72.5% of 357 markers), showing their high degree of polymorphism. From the genetic profile of these rat inbred strains, we constructed a rat family tree to clarify their genetic background. Conclusion: These highly informative SSLP markers as well as genetically and phenotypically defined rat strains are useful for designing experiments for quantitative trait loci (QTL) analysis and to choose strategies for developing new genetic resources. The data and resources are freely available at the NBRP-Rat web site [1]. [ABSTRACT FROM AUTHOR]

Published

2006

14. Activation by N -Acetyl-l-Aspartate of Acutely Dissociated Hippocampal Neurons in Rats via Metabotropic Glutamate Receptors.

Author

Hai-Dun Yan, Ishihara, Kumatoshi, Serikawa, Tadao, and Sasa, Masashj

Subjects

ASPARTATE aminotransferase, PEOPLE with epilepsy, NEURONS, HIPPOCAMPUS (Brain), LABORATORY rats

Abstract

Summary: Purpose: We previously reported that an increase in the N -acetyl-l-aspartate (NAA) level due to the lack of aspartoacylase gene was found in the brain of the tremor rat (tm/tm ), which is a mutant with a causative gene named tm that shows epileptic seizures. Therefore, NAA is suggested to be one of the factors involved in the induction of epileptic seizures. Patch-clamp studies were performed to determine whether NAA produces an excitatory effect on acutely dissociated rat hippocampal neurons. Methods: Acutely dissociated hippocampal neurons were prepared from normal Wistar rats aged 3–4 weeks. NAA-induced currents were investigated by using the whole-cell voltage-clamp recording technique. Results: Application of NAA at concentrations of 100 nM to 1 mM through a U-tube for 2 s produced an inward current in a concentration-dependent manner at a holding potential of –60 mV. When the current–voltage relation was examined, the reversal potential of the NAA-induced current was found to be ∼0 mV. The NAA-induced current was inhibited by bath application of the metabotropic glutamate receptor (mGluR) antagonist (±)-α-methyl-4-carboxyphenylglycine (MCPG) and by intracellular application of guanosine 5′-O -(2-thiodiphosphate) (GDP-βS), a nonhydrolyzable GDP analogue. However, the NAA-induced current remained unaffected by glutamic acid diethyl ester, a non–N -methyl-d-aspartate (NMDA)-subtype ionotropic glutamate receptor antagonist, or the voltage-dependent ion channel blockers tetrodotoxin, CdCl[sub 2] , and tetraethylammonium-chloride. Conversely, the mGluR agonist, trans -(1S,3R)-1-amino-1,3-cyclopentanedicarboxylic acid (ACPD) also induced an inward current, with a reversal potential of 0 mV. The ACPD-induced current also was inhibited by MCPG. Conclusions: These results suggest that NAA acts on the G protein-coupled mGluRs to induce an inward current that results in excitation of the neurons, thereby contributing to the occurrence of epileptic seizures. [ABSTRACT FROM AUTHOR]

Published

2003

15. Genetic analysis of cataract in Ihara epileptic rat.

Author

Yokoyama, Masao, Amano, Shigeru, Tsuji, Atsushi, Sasahara, Masakiyo, Serikawa, Tadao, Ihara, Nobuo, Matsuda, Masayuki, Hazama, Fumitada, and Handa, Jyoji

Subjects

GENETICS, CATARACT, LABORATORY rats, CHROMOSOMES, LINKAGE (Genetics), CROSSING over (Genetics)

Abstract

We analyzed the mode of inheritance of cataract in the Ihara epileptic rat (IER) by crossing experiments, and mapped cataract-related genes by linkage analysis. Cataract did not develop in the F1 animals, but it developed in both male and female animals of backcross and F2. The occurrence rate of cataract was 48.5% in the backcross progeny and 19.4% in the F2 progeny. Thus, the character was considered to be inherited by the autosomal recessive mode. We found two groups that differed according to the time of onset among the backcross and F2 progeny: an early-onset group (EOG), in which cataracts developed by about 4 months after birth, and a late-onset group (LOG), in which cataracts developed 8 months or more after birth. Linkage analysis indicated the presence of one cataract gene each on Chromosome (Chr) 8 and Chr 15, and the cataract was demonstrated to be governed by more than one gene. The gene on Chr 8 was named Cati1, and that on Chr 15, Cati2. Cati1 was involved in the occurrence of cataract, and the conditions required for cataract to develop were Cati1i/Cati1i or Cati1i/Cati1w. However, in the cataract rats with Cati1i/Cati1w, the allele of Cati2 was always Cati2i/Cati2i. Cati2 was involved in the timing of onset of the cataract, and the precondition for early onset was Cati2i/Cati2i. [ABSTRACT FROM AUTHOR]

Published

2001

16. Genetic mapping of the rat mutation creeping and evaluation of its positional candidate gene reelin.

Author

Yokoi, Norihide, Shimizu, Seiko, Ishibashi, Kotaro, Kitada, Kazuhiro, Iwama, Hiroyuki, Namae, Misako, Sugawara, Moriyuki, Serikawa, Tadao, and Komeda, Kajuro

Subjects

LABORATORY rats, GENE mapping, GENETIC mutation, BIOLOGICAL models, CHROMOSOMES, GENETICS

Abstract

We have previously described a rat autosomal recessive mutation, creeping (cre), causing severe ataxia and disarrangement of neuronal cells in the central nervous system. The mutant strain has recently been successfully inbred, named Komeda Zucker creeping (KZC) rat. In the present study, we have performed a genetic analysis of the creeping mutation, and mapped it to rat Chromosome (Chr) 4. Comparative mapping, together with the similarity of the phenotype, suggested that the creeping mutation is homologous to the mouse reeler mutation. In fact, reelin expression was markedly reduced in the homozygous mutant (cre/cre) animals compared with the normal littermates. Thus, the KZC rat should become a useful biological model with a novel mutation in the reelin gene. [ABSTRACT FROM AUTHOR]

Published

2000

17. Down-Regulation of Astrocytic Kir4.1 Channels during the Audiogenic Epileptogenesis in Leucine-Rich Glioma-Inactivated 1 (Lgi1) Mutant Rats.

Author

Kinboshi, Masato, Shimizu, Saki, Mashimo, Tomoji, Serikawa, Tadao, Ito, Hidefumi, Ikeda, Akio, Takahashi, Ryosuke, and Ohno, Yukihiro

Subjects

SPASMS, LABORATORY rats, GENETIC regulation, ASTROCYTES, EPILEPSY, CEREBRAL cortex

Abstract

The dysfunction of astrocytic inwardly rectifying potassium (Kir) 4.1 channels, which mediate the spatial potassium-buffering function of astrocytes, is known to be involved in the development of epilepsy. Here, we analyzed the Kir4.1 expressional changes in Leucine-Rich Glioma-Inactivated 1 (Lgi1) mutant rats, which is a model of autosomal dominant lateral temporal lobe epilepsy in humans, to clarify the role of astrocytic Kir4.1 channels in Lgi1-related epileptogenesis. Priming acoustic stimulation (at postnatal day 16) conferred seizure susceptibility on Lgi1 mutant rats, which evoked audiogenic seizures with test stimulation at eight weeks. In the seizure-susceptible Lgi1 mutant rats (before test stimulation), astrocytic Kir4.1 expression was down-regulated region-specifically in the cerebral cortex, hippocampus, and amygdala. In addition, prophylactic treatments of Lgi1 mutant rats with valproic acid (VPA, 30 mg/kg and 200 mg/kg) for two weeks prevented both the development of seizure susceptibility and the down-regulation of Kir4.1 expression in astrocytes. The present study demonstrated for the first time that the astrocytic Kir4.1 expression was reduced in the Lgi1-related seizure model, suggesting that the down-regulation of Kir4.1 channels in astrocytes is involved in audiogenic epileptogenesis caused by Lgi1 mutation. In addition, VPA seemed to have a prophylactic effect on Lgi1-related seizures. [ABSTRACT FROM AUTHOR]

Published

2019

18. Correction: Novel ENU-Induced Mutation in Tbx6 Causes Dominant Spondylocostal Dysostosis-Like Vertebral Malformations in the Rat.

Author

Abe, Koichiro, Takamatsu, Nobuhiko, Ishikawa, Kumiko, Tsurumi, Toshiko, Tanimoto, Sho, Sakurai, Yukina, Lisse, Thomas S., Imai, Kenji, Serikawa, Tadao, and Mashimo, Tomoji

Subjects

DYSOSTOSIS, SPONDYLOSIS, GENETIC mutation, HUMAN abnormalities, LABORATORY rats, MEDICAL research

Published

2015

19. Effects of levetiracetam on hippocampal kindling in Noda epileptic rats

Author

Ishimaru, Yuji, Chiba, Shigeru, Serikawa, Tadao, Sasa, Masashi, Inaba, Hiroko, Tamura, Yoshiyuki, Ishimoto, Takahiro, Takasaki, Hideki, Sakamoto, Kazutaka, and Yamaguchi, Kazuhide

Subjects

*PHARMACODYNAMICS, *ANTICONVULSANTS, *HIPPOCAMPUS (Brain), *TREATMENT of epilepsy, *ELECTRIC stimulation, *NEUROLOGICAL disorders, *GENETICS of disease susceptibility, *LABORATORY rats

Abstract

Abstract: In order to clarify the seizure susceptibility of Noda epileptic rat (NER) and the antiepileptic effects of levetiracetam (LEV), we performed electrical hippocampal kindling in NERs compared with Wistar rats (experiment 1), and hippocampal kindling in NERs with LEV administration (experiment 2). In experiment 1, electrical stimulation was administered to the right dorsal hippocampus of NERs and Wistar rats once per day. In experiment 2, NERs were randomly assigned to group L (LEV administration) and C (saline administration). Following daily administration of LEV (240 mg/kg, i.p.) to group L and saline to group C, hippocampal kindling was performed from the 5th day of consecutive LEV or saline administration. As a result of experiment 1, all NERs exhibited stage 5 (falling) or stage 6 seizure (running/jumping, subsequent seizure) from the first electrical stimulation. In experiment 2, LEV suppressed development of hippocampal kindling, increased the afterdischarge threshold of the hippocampus and inhibited stage 6 seizures in NER. Although LEV prolonged the afterdischarge duration at the first stage 5 seizure significantly, there was a tendency to prolong the latency to generalization by LEV. These findings indicate that NER is susceptible not only to limbic seizures but also to brainstem seizures. Furthermore, LEV may have inhibitory effects not only on the hippocampus but also on other neuronal pathways to secondary generalization in this rat model. [Copyright &y& Elsevier]

Published

2010

20. Atopic dermatitis-like skin lesions with IgE hyperproduction and pruritus in KFRS4/Kyo rats.

Author

Kuramoto, Takashi, Yokoe, Mayuko, Tanaka, Daisuke, Yuri, Azusa, Nishitani, Ai, Higuchi, Yuki, Yoshimi, Kazuto, Tanaka, Miyuu, Kuwamura, Mitsuru, Hiai, Hiroshi, Kabashima, Kenji, and Serikawa, Tadao

Subjects

*ATOPIC dermatitis, *IMMUNOGLOBULIN E, *ITCHING, *LABORATORY rats, *SYMPTOMS

Abstract

Background Rats showing spontaneous atopic dermatitis (AD)-like skin lesions were observed in the Kyoto Fancy Rat Stock 4 (KFRS4) strain breeding colony. Objective To establish the KFRS4 rat as a model of AD. Methods The clinical symptoms of AD-like skin lesions were assessed by scoring the degree of dermatitis and examining scratching behavior. The transepidermal water loss was measured to evaluate skin barrier function. Cells infiltrating the skin lesions were identified using histological and immunohistological analyses. IgE and cytokine levels were measured to examine immune status. An ointment treatment experiment was carried out to characterize dermatitis in the KFRS4 rats. Results Dermatitis initially appeared around 4 months of age and rapidly worsened from 6 to 8 months of age. The skin lesions accompanied scratching behavior and were predominantly observed in females. The increased transepidermal water loss indicated skin barrier dysfunction. Extensive infiltration of eosinophils, mast cells and lymphocytes was observed in the skin lesions. The plasma IgE level increased in accord with increasing severity of dermatitis. The Th2 and Th17 cytokine mRNA levels were significantly higher in the skin-draining lymph nodes than those in the non-skin-draining lymph nodes. It was demonstrated that betamethasone improved the symptoms of dermatitis. These findings demonstrated that dermatitis in the KFRS4 rats closely resembled that seen in human AD. Conclusion Female KFRS4 rats have the potential to serve as an animal model of human AD. [ABSTRACT FROM AUTHOR]

Published

2015

21. Evaluation of seizure foci and genes in the Lgi1 L385R/+ mutant rat.

Author

Fumoto, Naohiro, Mashimo, Tomoji, Masui, Atsushi, Ishida, Saeko, Mizuguchi, Yuto, Minamimoto, Shoko, Ikeda, Akio, Takahashi, Ryosuke, Serikawa, Tadao, and Ohno, Yukihiro

Subjects

*GENETIC mutation, *TEMPORAL lobe, *AUDITORY cortex, *SPASMS, *ELECTROENCEPHALOGRAPHY, *EPILEPSY, *LABORATORY rats

Abstract

Highlights: [•] EEG Lgi1 L385R/+ rats showed patterns that corresponded to seizure behavior. [•] Neural activity is increased in the lateral temporal lobe, including auditory cortex. [•] Microarray analysis identified candidate genes responsible for audiogenic seizures. [Copyright &y& Elsevier]

Published

2014

22. Expressional analysis of inwardly rectifying Kir4.1 channels in Noda epileptic rat (NER).

Author

Harada, Yuya, Nagao, Yuki, Shimizu, Saki, Serikawa, Tadao, Terada, Ryo, Fujimoto, Megumi, Okuda, Aoi, Mukai, Takahiro, Sasa, Masashi, Kurachi, Yoshihisa, and Ohno, Yukihiro

Subjects

*PEOPLE with epilepsy, *LABORATORY rats, *ASTROCYTES, *POTASSIUM channels, *PATHOLOGICAL physiology, *OCCIPITAL lobe

Abstract

Abstract: The inwardly rectifying potassium channel subunit Kir4.1 is expressed in brain astrocytes and involved in spatial K+ buffering, regulating neural activity. To explore the pathophysiological alterations of Kir4.1 channels in epileptic disorders, we analyzed interictal expressional levels of Kir4.1 in the Noda epileptic rat (NER), a hereditary animal model for generalized tonic-clonic (GTC) seizures. Western blot analysis showed that Kir4.1 expression in NERs was significantly reduced in the occipito-temporal cortical region and thalamus. However, the expression of Kir5.1, another Kir subunit mediating spatial K+ buffering, remained unaltered in any brain regions examined. Immunohistochemical analysis revealed that Kir4.1 was primarily expressed in glial fibrillary acidic protein (GFAP)-positive astrocytes (somata) and foot processes clustered around neurons proved with anti-neuronal nuclear antigen (NeuN) antibody. In NERs, Kir4.1 expression in astrocytic processes was region-selectively diminished in the amygdaloid nuclei (i.e., medial amygdaloid nucleus and basomedial amygdaloid nucleus) while Kir4.1 expression in astrocytic somata was unchanged. Furthermore, the amygdala regions with reduced Kir4.1 expression showed a marked elevation of Fos protein expression following GTC seizures. The present results suggest that reduced activity of astrocytic Kir4.1 channels in the amygdala is involved in limbic hyperexcitability in NERs. [Copyright &y& Elsevier]

Published

2013

23. Inhibitory effects of levetiracetam on the high-voltage-activated L-type Ca2+ channels in hippocampal CA3 neurons of spontaneously epileptic rat (SER)

Author

Yan, Hai-Dun, Ishihara, Kumatoshi, Seki, Takahiro, Hanaya, Ryosuke, Kurisu, Kaoru, Arita, Kazunori, Serikawa, Tadao, and Sasa, Masashi

Subjects

*HIGH voltages, *CALCIUM channels, *PEOPLE with epilepsy, *LABORATORY rats, *HIPPOCAMPUS (Brain), *NEURONS, *EPILEPSY, *ANTICONVULSANTS

Abstract

Abstract: Levetiracetam (LEV) is a widely used antiepileptic agent for partial refractory epilepsy in humans. LEV has unique antiepileptic effects in that it does not inhibit electroshock- or pentylenetetrazol-induced convulsion, but does inhibit seizures in kindling animal and spontaneously epileptic rat (SER: zi/zi, tm/tm) that shows both tonic convulsion and absence-like seizures. LEV also has unique characteristics in terms of its antiepileptic mechanism; it has no activity on Na+ and K+ channels or on glutamate and GABAA receptors. Recently, we found that LEV inhibits the depolarization shift and accompanying repetitive firing induced by mossy fiber stimulation in CA3 neurons of SER hippocampal slices. Therefore, this study was performed to determine whether LEV could inhibit the voltage-activated L-type Ca2+ current of hippocampal CA3 neurons obtained from SER and the non-epileptic Wistar rat. As previously reported, SER CA3 neurons were classified into type 1 and type 2 neurons. The application of LEV (100μM) elevated the threshold for activation of the Ca2+ current, which was lowered in SER type 1 neurons and reduced the current size. Type 2 neurons of SER have a similar current–voltage relationship to Wistar rat neurons and the decay component of Ca2+ current during depolarization pulse in type 2 neurons was found to be smaller than that in Wistar rat neurons. LEV (100μM) also reduced Ca2+ current in SER type 2 neurons. The effects of LEV were examined on such type 2 SER hippocampal CA3 neurons, compared with those on Wistar rat CA3 neurons. Application of LEV (10μM) produced a significant decrease of amplitude of the Ca2+ current in SER neurons, although at this concentration of LEV there was no statistically significant decrease in the amplitude of Ca2+ current in Wistar rat neurons. Furthermore, LEV (100nM–1mM) reduced the Ca2+ current in a concentration-dependent manner in both SER and Wistar rat neurons, but the inhibition was much more potent in the former neurons than in the latter. Under the condition that the Ca2+ current had already been inhibited by LEV (10μM), the addition of nifedipine (10μM) did not cause further inhibition. Conversely, LEV had no effects on the current that had already been decreased by nifedipine (10μM) given before LEV treatment (10μM), indicating that LEV could act on the L-type Ca2+channel. LEV elevated the threshold potential level for activation of the Ca2+ current and reduced the L-type Ca2+ current in type 1 neurons of SER, and the inhibitory action in type 2 neurons was much more potent than that in Wistar rat neurons, suggesting that these effects contribute, at least partly, to the antiepileptic action of LEV. [Copyright &y& Elsevier]

Published

2013

24. Abnormal myelinogenesis in the central nervous system of the VF mutant rat with recoverable tremor

Author

Tanaka, Miyuu, Soma, Katsumi, Izawa, Takeshi, Yamate, Jyoji, Franklin, Robin J.M., Kuramoto, Takashi, Serikawa, Tadao, and Kuwamura, Mitsuru

Subjects

*MYELINATION, *CENTRAL nervous system abnormalities, *LABORATORY rats, *PROTEOLIPIDS, *IN situ hybridization, *CITRATES, *POLYOXYMETHYLENE, *SOMATOMEDIN

Abstract

Abstract: The vacuole formation (VF) rat is an autosomal recessive myelin mutant characterized by generalized tremor and vacuole formation within the myelin of the central nervous system (CNS). The tremor is prominent between 4 and 8 weeks of age but thereafter gradually improves. The present study, aimed at producing a detailed description of how the principal lesions evolve, revealed that the VF rat has abnormal vacuoles in the periaxonal space in the spinal cord and that these vacuoles decreased concurrently with the loss of tremor. However, a degree of hypomyelination persisted throughout the CNS after the resolution of periaxonal vacuoles. In situ hybridization for proteolipid protein (PLP) demonstrated that the number of small, round PLP-positive oligodendrocytes increased in the spinal cord of VF rats between 10 and 20 weeks of age, suggesting a disruption of oligodendrocytes'' maturation. Activated astrocytes and microglia were also found in the VF rats from 4 weeks of age. Our results indicate that the causative genetic defect of the VF rat is likely to be involved in the formation and maintenance of the CNS myelin. [Copyright &y& Elsevier]

Published

2012

25. Hypercholesterolemia and atherosclerosis in low density lipoprotein receptor mutant rats

Author

Asahina, Makoto, Mashimo, Tomoji, Takeyama, Michiyasu, Tozawa, Ryuichi, Hashimoto, Tadatoshi, Takizawa, Akiko, Ueda, Masatsugu, Aoto, Toshihiro, Kuramoto, Takashi, and Serikawa, Tadao

Subjects

*HYPERCHOLESTEREMIA, *ATHEROSCLEROSIS, *LIPOPROTEIN receptors, *LABORATORY rats, *LOW density lipoprotein receptors, *HYPERLIPIDEMIA, *CHOLESTEROL

Abstract

Abstract: To establish low density lipoprotein receptor (LDLR) mutant rats as a hypercholesterolemia and atherosclerosis model, we screened the rat LDLR gene for mutations using an N-ethyl-N-nitrosourea mutagenesis archive of rat gene data, and identified five mutations in its introns and one missense mutation (478T>A) in exon 4. The C160S mutation was located in the ligand binding domain of LDLR and was revealed to be equivalent to mutations (C160Y/G) identified in human familial hypercholesterolemia (FH) patients. The wild type, heterozygous, and homozygous mutant rats were fed a normal chow diet or a high fat high cholesterol (HFHC) diet from the age of 10weeks for 16weeks. The LDLR homozygous mutants fed the normal chow diet showed higher levels of plasma total cholesterol and LDL cholesterol than the wild type rats. When fed the HFHC diet, the homozygous mutant rats exhibited severe hyperlipidemia and significant lipid deposition from the aortic arch to the abdominal aorta as well as in the aortic valves. Furthermore, the female homozygous mutants also developed xanthomatosis in their paws. In conclusion, we suggest that LDLR mutant rats are a useful novel animal model of hypercholesterolemia and atherosclerosis. [Copyright &y& Elsevier]

Published

2012

26. Kcna1-mutant rats dominantly display myokymia, neuromyotonia and spontaneous epileptic seizures

Author

Ishida, Saeko, Sakamoto, Yu, Nishio, Takeshi, Baulac, Stéphanie, Kuwamura, Mitsuru, Ohno, Yukihiro, Takizawa, Akiko, Kaneko, Shuji, Serikawa, Tadao, and Mashimo, Tomoji

Subjects

*SPASMS, *CEREBELLAR ataxia, *POTASSIUM channels, *NEUROLOGY, *PHENOTYPES, *EPILEPSY, *LABORATORY rats

Abstract

Abstract: Mutations in the KCNA1 gene, which encodes for the α subunit of the voltage-gated potassium channel Kv1.1, cause episodic ataxia type 1 (EA1). EA1 is a dominant human neurological disorder characterized by variable phenotypes of brief episodes of ataxia, myokymia, neuromyotonia, and associated epilepsy. Animal models for EA1 include Kcna1-deficient mice, which recessively display severe seizures and die prematurely, and V408A-knock-in mice, which dominantly exhibit stress-induced loss of motor coordination. In the present study, we have identified an N-ethyl-N-nitrosourea-mutagenized rat, named autosomal dominant myokymia and seizures (ADMS), with a missense mutation (S309T) in the voltage-sensor domain, S4, of the Kcna1 gene. ADMS rats dominantly exhibited myokymia, neuromyotonia and generalized tonic–clonic seizures. They also showed cold stress-induced tremor, neuromyotonia, and motor incoordination. Expression studies of homomeric and heteromeric Kv1.1 channels in HEK cells and Xenopus oocytes, showed that, although S309T channels are transferred to the cell membrane surface, they remained non-functional in terms of their biophysical properties, suggesting a dominant-negative effect of the S309T mutation on potassium channel function. ADMS rats provide a new model, distinct from previously reported mouse models, for studying the diverse functions of Kv1.1 in vivo, as well as for understanding the pathology of EA1. [Copyright &y& Elsevier]

Published

2012

27. Neuroprotective effect of levetiracetam on hippocampal sclerosis-like change in spontaneously epileptic rats

Author

Sugata, Sei, Hanaya, Ryosuke, Kumafuji, Kenta, Tokudome, Mai, Serikawa, Tadao, Kurisu, Kaoru, Arita, Kazunori, and Sasa, Masashi

Subjects

*NEUROPROTECTIVE agents, *HIPPOCAMPUS (Brain), *PEOPLE with epilepsy, *LABORATORY rats, *NEURONS, *SEIZURES (Medicine)

Abstract

Abstract: The spontaneously epileptic rat (SER) begins to exhibit both tonic convulsions and absence seizures from 6 weeks of age and SERs have stable seizures after 10 weeks of age. Low-dose administrations of levetiracetam (LEV) for 4- to 5-weeks-old SERs which did not show spontaneous seizures reduced both seizures 5 weeks after termination of administration. The hippocampus of SER exhibited decreased CA3 neurons, sprouting of mossy fibers, and hyperexpression of the brain-derived neurotrophic factor (BDNF). We attempted prophylactic LEV administrations in preseizure-manifesting SERs to evaluate if such a treatment regimen would protect the hippocampal sclerosis-like changes observed in SERs. The osmotic mini-pump administered LEV dissolved in saline to 4-weeks-old SERs for 4 weeks at 2.5μl/h. LEV was administered at 420mg/ml for 4 weeks in Group A. In Group B, LEV was given at 420mg/ml for the first 2 weeks followed by doubling the dosage (840mg/ml) in the following 2 weeks. LEV administrations in preseizure-manifesting SERs reduced the decrease of CA3 neurons and mossy fibers sprouting at 10–11 weeks of age in both group A and B. LEV attenuated BDNF expression in inner molecular layers of the dentate gyrus, striatum radiatum, and CA3 in 10- to 11- and 14- to 15-weeks-old SERs. In group B, LEV decreased BDNF expression in hilus and CA1 of 10- to 11- weeks-old SER. The present results suggest that prophylactic treatment with LEV in preseizure-manifesting SERs inhibits hippocampal sclerosis-like neuronal degeneration and/or regeneration. [Copyright &y& Elsevier]

Published

2011

28. Oligodendroglial pathology in the development of myelin breakdown in the dmy mutant rat

Author

Kuwamura, Mitsuru, Inumaki, Kazuo, Tanaka, Miyuu, Shirai, Makoto, Izawa, Takeshi, Yamate, Jyoji, Franklin, Robin J.M., Kuramoto, Takashi, and Serikawa, Tadao

Subjects

*OLIGODENDROGLIA, *MYELIN genes, *CENTRAL nervous system, *INTRONS, *MITOCHONDRIA, *SPINAL cord, *LABORATORY rats

Abstract

Abstract: The dmy rat is an autosomal recessive mutant that exhibits severe myelin destruction throughout the white matter of the central nervous system. Recently, a point mutation in intron 3 of the Mrs2 has been found in the dmy rat. Mrs2 encodes an essential component of the major electrophoretic Mg2+ influx system in mitochondria of yeast as well as human cells. In this study, we examined the morphological and numerical changes of oligodendroctyes in the development of myelin destruction in the spinal cord of the dmy rat. The number of oligodendrocytes decreases rapidly from 7weeks of age in the dmy rat in accordance with myelin breakdown. Hypertrophic oligodendrocytes were frequently observed, and the cytoplasm was found to be intensely positive for prohibitin and cytochrome oxidase, mitochondrial markers. These data suggest that mitochondrial dysfunction causes a work/compensatory hypertrophy of oligodendrocytes, resulting in direct cell death and leading to myelin destruction. [Copyright &y& Elsevier]

Published

2011

29. Scn1a missense mutation causes limbic hyperexcitability and vulnerability to experimental febrile seizures

Author

Ohno, Yukihiro, Ishihara, Shizuka, Mashimo, Tomoji, Sofue, Nobumasa, Shimizu, Saki, Imaoku, Takuji, Tsurumi, Toshiko, Sasa, Masashi, and Serikawa, Tadao

Subjects

*GENETIC mutation, *LIMBIC system, *EXPERIMENTAL design, *FEBRILE seizures, *ELECTRIC potential, *SODIUM channels, *EPILEPSY, *LABORATORY rats

Abstract

Abstract: Mutations of the voltage-gated sodium (Nav) channel subunit SCN1A have been implicated in the pathogenesis of human febrile seizures including generalized epilepsy with febrile seizures plus (GEFS+) and severe myoclonic epilepsy in infancy (SMEI). Hyperthermia-induced seizure-susceptible (Hiss) rats are the novel rat model carrying a missense mutation (N1417H) of Scn1a, which is located in the third pore-forming region of the Nav1.1 channel. Here, we conducted behavioral and neurochemical studies to clarify the functional relevance of the Scn1a mutation in vivo and the mechanism underlying the vulnerability to hyperthermic seizures. Hiss rats showed markedly high susceptibility to hyperthermic seizures (mainly generalized clonic seizures) which were synchronously associated with paroxysmal epileptiform discharges. Immunohistochemical analysis of brain Fos expression revealed that hyperthermic seizures induced a widespread elevation of Fos-immunoreactivity in the cerebral cortices including the motor area, piriform, and insular cortex. In the subcortical regions, hyperthermic seizures enhanced Fos expression region—specifically in the limbic and paralimbic regions (e.g., hippocampus, amygdala, and perirhinal–entorhinal cortex) without affecting other brain regions (e.g., basal ganglia, diencephalon, and lower brainstem), suggesting a primary involvement of limbic system in the induction of hyperthermic seizures. In addition, Hiss rats showed a significantly lower threshold than the control animals in inducing epileptiform discharges in response to local stimulation of the hippocampus (hippocampal afterdischarges). Furthermore, hyperthermic seizures in Hiss rats were significantly alleviated by the antiepileptic drugs, diazepam and sodium valproate, while phenytoin or ethosuximide were ineffective. The present findings support the notion that Hiss rats are useful as a novel rat model of febrile seizures and suggest that hyperexcitability of limbic neurons associated with Scn1a missense mutation plays a crucial role in the pathogenesis of febrile seizures. [Copyright &y& Elsevier]

Published

2011

30. Inhibitory effects of levetiracetam on absence seizures in a novel absence-like epilepsy animal model, Groggy rat

Author

Tokuda, Satoko, Sofue, Nobumasa, Ohno, Yukihiro, Sasa, Masashi, and Serikawa, Tadao

Subjects

*ANTICONVULSANTS, *DRUG efficacy, *SEIZURES (Medicine), *ANIMAL models in research, *EPILEPSY, *LABORATORY rats, *DRUG dosage, *THERAPEUTICS

Abstract

Abstract: Levetiracetam (LEV) is known to inhibit convulsive seizures and is clinically used for treating both partial and generalized seizures. The study was performed to determine whether LEV possesses an inhibitory effect on absence seizures in a novel genetic animal model of absence epilepsy, Groggy (GRY) rats. Single injections of LEV at doses ranging from 20 to 160mg/kg i.p. markedly inhibited absence seizures in GRY rats. The anti-absence action of LEV was potent and the cumulative duration of spike and wave discharges (SWD) in GRY rats was almost completely suppressed even at 20mg/kg (i.p.). When the time-course of the inhibitory action of LEV (80mg/kg i.p.) was examined up to 24h after the treatment, the appearance of SWD was suppressed for over 6h after injection of LEV in contrast to the action of sodium valproate (200mg/kg i.p.) which had a very short effect (<2h). The maximum level of blood concentration of LEV was attained within 2h after administration, and the drug disappeared from the blood in 24h with T 1/2 of 2.7h. These results revealed that LEV displays potent and relatively long-lasting inhibitory effects on absence seizures in GRY rats. [Copyright &y& Elsevier]

Published

2010

31. Scn1a missense mutation impairs GABAA receptor-mediated synaptic transmission in the rat hippocampus

Author

Ohno, Yukihiro, Sofue, Nobumasa, Ishihara, Shizuka, Mashimo, Tomoji, Sasa, Masashi, and Serikawa, Tadao

Subjects

*GENETIC mutation, *GABA receptors, *NEURAL transmission, *LABORATORY rats, *HIPPOCAMPUS (Brain), *FEBRILE seizures, *SODIUM channels

Abstract

Abstract: Mutations of the Nav1.1 channel subunit SCN1A have been implicated in the pathogenesis of human febrile seizures (FS). We have recently developed hyperthermia-induced seizure-susceptible (Hiss) rat, a novel rat model of FS, which carries a missense mutation (N1417H) in Scn1a. Here, we conducted electrophysiological studies to clarify the influences of the Scn1a mutation on the hippocampal synaptic transmission, specifically focusing on the GABAergic system. Hippocampal slices were prepared from Hiss or F344 (control) rats and maintained in artificial cerebrospinal fluid saturated with 95% O2 and 5% CO2 in vitro. Single neuron activity was recorded from CA1 pyramidal neurons and their responses to the test (unconditioned) or paired pulse (PP) stimulation of the Schaffer collateral/commissural fibers were evaluated. Hiss rats were first tested for pentylenetetrazole-induced seizures and confirmed to show high seizure susceptibility to the blockade of GAGAA receptors. The Scn1a mutation in Hiss rats did not directly affect spike generation (i.e., number of evoked spikes and firing threshold) of the CA1 pyramidal neurons elicited by the Schaffer collateral/commissural stimulation. However, GABAA receptor-mediated inhibition of pyramidal neurons by the PP stimulation was significantly disrupted in Hiss rats, yielding a significant increase in the number of PP-induced firings at PP intervals of 32–256ms. The present study shows that the Scn1a missense mutation preferentially impairs GABAA receptor-mediated synaptic transmission without directly altering the excitability of the pyramidal neurons in the hippocampus, which may be linked to the pathogenesis of FS. [ABSTRACT FROM AUTHOR]

Published

2010

32. A novel middle-wavelength opsin (M-opsin) null-mutation in the retinal cone dysfunction rat

Author

Xie, Bei, Nakanishi, Satoshi, Guo, Qun, Xia, Feng, Yan, Guolin, An, Jing, Li, Li, Serikawa, Tadao, Kuramoto, Takashi, and Zhang, Zuoming

Subjects

*THERAPEUTIC use of proteins, *LABORATORY rats, *ANIMAL models in research, *ELECTRORETINOGRAPHY, *GENETIC polymorphisms, *IMMUNOHISTOCHEMISTRY, *GENE mapping

Abstract

Abstract: The disease-causing gene which underlies a naturally occurring X-linked mutant cone dysfunction Sprague–Dawley rat model was investigated. Full-field electroretinogram (ERG) and simple sequence length polymorphism analyses were applied to 441-second filial generation rats that were derived from crossing a mutant rat and a Brown–Norway rat. After identifying a mutation mapping within the telomeric region of chromosome X, a candidate gene related to retinal cone function in this region was further screened using real-time PCR, immunohistochemistry and histological methods. The results showed that a G-to-T substitution at the splice acceptor site of intron 4 was present in the opsin 1, medium-wave sensitive (Opn1mw) gene, thereby causing down-regulated transcription and translation. These changes were consistent with abnormities seen in the ERG response. However, there was no significant histological change in the mutant rat retina. Therefore, we infer from this that the causative gene for the mutation is Opn1mw and consequently term this a middle-wavelength opsin cone dysfunction (MCD) rat model. The deficiency in vision of the MCD rat is similar to the color vision defects that occur in humans with a color vision defect but without recessive retinal degeneration. This rat model may be useful for understanding the mechanism that is responsible for color vision and for developing clinical therapies for several retinal dystrophies caused by cone opsin deficiencies. [Copyright &y& Elsevier]

Published

2010

33. Hippocampal cell loss and propagation of abnormal discharges accompanied with the expression of tonic convulsion in the spontaneously epileptic rat

Author

Hanaya, Ryosuke, Sasa, Masashi, Sugata, Sei, Tokudome, Mai, Serikawa, Tadao, Kurisu, Kaoru, and Arita, Kazunori

Subjects

*HIPPOCAMPUS (Brain), *SEIZURES (Medicine), *LABORATORY rats, *CALCIUM channels, *DENTATE gyrus, *NERVE growth factor, EPILEPSY research

Abstract

Abstract: Spontaneously epileptic rats (SER) are double mutants with both tonic convulsion and absence-like seizures from the age of 8weeks. Hippocampal CA3 neurons in SER display a long-lasting depolarizing shift accompanied by repetitive firing (attributed to abnormalities of the Ca2+ channels) with a single stimulation of the mossy fibers. In the present investigation, we examined if the seizure discharges of SER were correlated with the hippocampal abnormality of SER using electrophysiological and histological methods. In CA1 neurons of seizure-susceptible mature SER, higher-voltage (<8–11V) stimulations induced a long depolarization shift (in 25% of neurons) with repetitive firing (in 12.5% of neurons). However, the tremor rat, one of the parent strains of SER, did not exhibit such abnormal firing in the CA3 region of the hippocampus. The number of CA3 neurons in SER was significantly (p <0.01) lower than that in tremor rats and Wistar rats, although no significant difference was established in the hilus. Sprouting of mossy fiber was observed in the dentate of mature SER; however, negligible staining was spotted in the dentate of both mature tremor and Wistar rats. Interestingly, expression of the brain-derived neurotrophic factor was higher in the hilus, CA3, and granular cell layer of dentate gyrus in SER than normal Wistar rats. The expression levels of TUNEL, bax, and Caspase-3 did not show significant changes between the SER and Wistar rats. SER exhibited hippocampal sclerosis-like changes which did not have enough potential for epileptogenesis. Repetitive tonic seizures and vulnerable CA3 neurons of SER could be involved in the induction of sclerosis-like changes in the hippocampus. [Copyright &y& Elsevier]

Published

2010

34. Regional expression of Fos-like immunoreactivity following seizures in Noda epileptic rat (NER)

Author

Ohno, Yukihiro, Shimizu, Saki, Harada, Yuya, Morishita, Maho, Ishihara, Shizuka, Kumafuji, Kenta, Sasa, Masashi, and Serikawa, Tadao

Subjects

*GENE expression, *SPASMS, *PEOPLE with epilepsy, *EPILEPSY, *BRAIN diseases, *MOTOR cortex, *ANIMAL models in research, *LABORATORY rats

Abstract

Summary: Noda epileptic rat (NER) is a genetic rat model of epilepsy that exhibit spontaneous generalized tonic–clonic (GTC) seizures with paroxysmal discharges. We analyzed the regional expression of Fos-like immunoreactivity (Fos-IR) following GTC seizures in NER to clarify the brain regions involved in the seizure generation. GTC seizures in NER elicited a marked increase in Fos expression in the piriform cortex, perirhinal–entorhinal cortex, insular cortex and other cortices including the motor cortex. In the limbic regions, Fos-IR was highest in the amygdalar nuclei (e.g., basomedial amygdaloid nucleus), followed by the cingulate cortex and hippocampus (i.e., dentate gyrus and CA3). As compared to the above forebrain regions, NER either with or without GTC seizures exhibited only marginal Fos expression in the basal ganglia (e.g., accumbens, striatum and globus pallidus), diencephalon (e.g., thalamus and hypothalamus) and lower brain stem structures (e.g., pons-medulla oblongata). These results suggest that GTC seizures in NER are of forebrain origin and are evoked primarily by activation of the limbic and/or cortical seizure circuits. [Copyright &y& Elsevier]

Published

2009

35. Adenoviral gene transfer of aspartoacylase into the tremor rat, a genetic model of epilepsy, as a trial of gene therapy for inherited epileptic disorder

Author

Seki, Takahiro, Matsubayashi, Hiroaki, Amano, Taku, Kitada, Kazuhiro, Serikawa, Tadao, Sakai, Norio, and Sasa, Masashi

Subjects

*LABORATORY rats, *EPILEPSY

Abstract

The tremor rat (tm/tm) is a genetic model of epilepsy that exhibits absence-like seizures characterized by 5–7 Hz spike–wave-like complexes in cortical and hippocampal electroencephalograms (EEGs). A deletion of the aspartoacylase (ASPA) gene and resultant high levels of N-acetyl-aspartate (NAA) in the brain have been found in tremor rats. We attempted to determine whether gene transfer of ASPA inhibited absence-like seizures in tremor rats using recombinant adenovirus. Recombinant adenovirus (5×107 pfu) carrying the rat ASPA gene (AxASPA) or β-galactosidase gene (AxLacZ), as a control virus, was intracerebroventricularly administered to premature tremor rats aged 7 weeks. Cortical and hippocampal EEG were recorded with chronically implanted electrodes before and after viral administration. The absence-like seizures were increased in AxLacZ-administered control rats with age. However, the increase was significantly inhibited in AxASPA-administered rats at 1 week after treatment. These results suggest that gene transfer of ASPA is effective in inhibiting the generation of absence-like seizures, probably by reducing the NAA level. [Copyright &y& Elsevier]

Published

2002