Identification of Candidate Genes for Generalized Tonic–Clonic Seizures in Noda Epileptic Rat

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; Serikawa, Tadao

doi:10.1007/s10519-017-9870-2

Cited by 13 publications

(11 citation statements)

References 30 publications

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“…Specifically, Kir4.1 expression was significantly reduced in Noda epileptic rats (NER), a hereditary epilepsy model ( Table 1) (89). NER exhibited frequent spontaneous GTCSs associated with two genetic loci, chromosome (Chr) 1q32-33 and Chr5q22, including cholecystokinin B receptor (Cckbr), suppressor of tumorigenicity 5 (St5), and PHD finger protein 24 (Phf24) (90)(91)(92)(93)(94)(95). In NER, Kir4.1 expression was region-specifically reduced in the amygdala, where the expression of Fos protein, a biological marker of neural excitation, significantly elevated (89).…”

Section: Kir41 Channels In Animal Epilepsy Modelsmentioning

confidence: 99%

Role of Astrocytic Inwardly Rectifying Potassium (Kir) 4.1 Channels in Epileptogenesis

2020

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Astrocytes regulate potassium and glutamate homeostasis via inwardly rectifying potassium (Kir) 4.1 channels in synapses, maintaining normal neural excitability. Numerous studies have shown that dysfunction of astrocytic Kir4.1 channels is involved in epileptogenesis in humans and animal models of epilepsy. Specifically, Kir4.1 channel inhibition by KCNJ10 gene mutation or expressional down-regulation increases the extracellular levels of potassium ions and glutamate in synapses and causes hyperexcitation of neurons. Moreover, recent investigations demonstrated that inhibition of Kir4.1 channels facilitates the expression of brain-derived neurotrophic factor (BDNF), an important modulator of epileptogenesis, in astrocytes. In this review, we summarize the current understanding on the role of astrocytic Kir4.1 channels in epileptogenesis, with a focus on functional and expressional changes in Kir4.1 channels and their regulation of BDNF secretion. We also discuss the potential of Kir4.1 channels as a therapeutic target for the prevention of epilepsy.

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Section: Kir41 Channels In Animal Epilepsy Modelsmentioning

confidence: 99%

Role of Astrocytic Inwardly Rectifying Potassium (Kir) 4.1 Channels in Epileptogenesis

2020

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“…We used the genomic sequences corresponding to the coding regions of 25 inbred rat strains (DDBJ Sequence Read Archive accession number: DRA004543; DDBJ/EMBL/ GenBank accession number: PRJDB4648) obtained from our previous studies (Yoshihara et al 2016a, b;Kuramoto et al 2017) (Table 1). These 25 strains were selected according to the following three categories: representative inbred strains (F344/DuCrlCrlj, F344/Jcl, F344/NSlc, and F344/ Stm), those originating from wild populations (BN/SsNSlc, DOB/Oda, IS/Kyo, IS-Tlk/Kyo, LE/Stm, LEC/Tj, and NIG-III/Hok), and disease models derived from selective breeding (BDIX/NemOda, BDIX.Cg-Tal/NemOda, BUF/ MNa, HTX/Kyo, HWY/Slc, KFRS3B/Kyo, KFRS4/Kyo, NER/Kyo, PVG/Seac, RCS/Kyo, WTC/Kyo, WTC-swh/ Kyo, ZF, and ZFDM).…”

Section: Data Setmentioning

confidence: 99%

“…The advent of genome editing technologies, however, has enabled the genetic manipulation of rats (Mashimo et al 2013), and genetic analyses in rats will be greatly advanced in the future. Currently, more than 800 inbred rat strains are registered in the National BioResource Project-Rat (NBRP-Rat) at Kyoto University, one of the largest repositories for rat strains, as live animals, embryos, or sperm (Serikawa et al 2009), and we have determined the protein coding genes and non-coding conserved sequences of some representative rat strains registered in NBRP-Rat (Yoshihara et al 2016a, b;Kuramoto et al 2017).…”

Section: Introductionmentioning

confidence: 99%

“…In this study, using the genomic sequences of all protein coding genes of 25 inbred rat strains that we recently sequenced (Yoshihara et al 2016a, b;Kuramoto et al 2017), we first analyzed the phylogenetic relationship among them, and then comprehensively identified variant sites that showed discordant mutation patterns. We found that discordant sites are not uniformly distributed along chromosomes, but are concentrated at certain genomic loci.…”

Section: Introductionmentioning

confidence: 99%

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Comparative genomic analysis of inbred rat strains reveals the existence of ancestral polymorphisms

2020

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In an alignment of closely related genomic sequences, the existence of discordant mutation sites, which do not reflect the phylogenetic relationship of the genomes, is often observed. Although these discordant mutation sites are thought to have emerged by ancestral polymorphism or gene flow, their frequency and distribution in the genome have not yet been analyzed in detail. Using the genome sequences of all protein coding genes of 25 inbred rat strains, we analyzed the frequency and genome-wide distribution of the discordant mutation sites. From the comparison of different substrains, it was found that these loci are not substrain specific, but are common among different groups of substrains, suggesting that the discordant sites might have mainly emerged through ancestral polymorphism. It was also revealed that the discordant sites are not uniformly distributed along chromosomes, but are concentrated at certain genomic loci, such as RT1, major histocompatibility complex of rats, and olfactory receptors, indicating that genes known to be highly polymorphic tend to have more discordant sites. Our results also showed that loci with a high density of discordant sites are also rich in heterozygous variants, even though these are inbred strains.

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“…Three candidate genes were identified to contribute to the epileptogenesis of NER [5,6]. PHD finger protein 24 (Phf24) was identified as a major candidate gene; lack of PHF24 expression was considered to be related to epileptogenesis of NER [6]. PHF24 is a key modulator of peripherally evoked GABAB-receptor signaling [7].…”

Section: Introductionmentioning

confidence: 99%

PHF24 is expressed in the inhibitory interneurons in rats

et al. 2021

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Noda epileptic rat (NER) is a mutant model for epilepsy that exhibits spontaneous generalized tonic-clonic seizure. Epileptogenesis of NER remains to be elucidated; but it is detected an insertion of an endogenous retrovirus sequence in intron 2 of the PHD finger protein 24 (Phf24) gene, encoding Gαi-interacting protein (GINIP). Phf24 is a strong candidate gene for epileptogenesis in NER. PHF24 modulates GABA B signaling through interacting with Gαi protein. To clarify the epileptogenesis of NER, we investigated a distribution of PHF24-expressing cells in the central nerve system (CNS). While broad expression of PHF24 was observed in the CNS, characteristic expression was noted in the periglomerular layer of the olfactory bulb and the lamina II of the spinal cord in the control rats. These cells showed co-expression with calbindin or calretinin, inhibitory interneuron markers. In the olfactory bulb, 15.6% and 41.2 % of PHF24-positive neurons co-expressed calbindin and calretinin, respectively. Immunoelectron microscopy revealed that PHF24 was located in the presynaptic terminals, synaptic membranes and cytoplasmic matrix of neuronal soma. Our data suggested PHF24 is expressed in the inhibitory interneurons and may play important roles in modulation of the GABA B signaling.

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Identification of Candidate Genes for Generalized Tonic–Clonic Seizures in Noda Epileptic Rat

Cited by 13 publications

References 30 publications

Role of Astrocytic Inwardly Rectifying Potassium (Kir) 4.1 Channels in Epileptogenesis

Role of Astrocytic Inwardly Rectifying Potassium (Kir) 4.1 Channels in Epileptogenesis

Comparative genomic analysis of inbred rat strains reveals the existence of ancestral polymorphisms

PHF24 is expressed in the inhibitory interneurons in rats

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