Your search keyword '"NAV1.2 Voltage-Gated Sodium Channel genetics"' showing total 216 results

101. Scn2a haploinsufficient mice display a spectrum of phenotypes affecting anxiety, sociability, memory flexibility and ampakine CX516 rescues their hyperactivity.

Author

Tatsukawa T, Raveau M, Ogiwara I, Hattori S, Miyamoto H, Mazaki E, Itohara S, Miyakawa T, Montal M, and Yamakawa K

Subjects

Animals, Anxiety drug therapy, Autism Spectrum Disorder drug therapy, Dioxoles therapeutic use, Gamma Rhythm, Haploinsufficiency, Male, Membrane Transport Modulators therapeutic use, Mice, Mice, Inbred C57BL, Phenotype, Piperidines therapeutic use, Prefrontal Cortex drug effects, Prefrontal Cortex physiopathology, Psychomotor Agitation drug therapy, Anxiety genetics, Autism Spectrum Disorder genetics, Memory, NAV1.2 Voltage-Gated Sodium Channel genetics, Psychomotor Agitation genetics, Social Behavior

Abstract

Background: Mutations of the SCN2A gene encoding a voltage-gated sodium channel alpha-II subunit Nav1.2 are associated with neurological disorders such as epilepsy, autism spectrum disorders, intellectual disability, and schizophrenia. However, causal relationships and pathogenic mechanisms underlying these neurological defects, especially social and psychiatric features, remain to be elucidated., Methods: We investigated the behavior of mice with a conventional or conditional deletion of Scn2a in a comprehensive test battery including open field, elevated plus maze, light-dark box, three chambers, social dominance tube, resident-intruder, ultrasonic vocalization, and fear conditioning tests. We further monitored the effects of the positive allosteric modulator of AMPA receptors CX516 on these model mice., Results: Conventional heterozygous Scn2a knockout mice ( Scn2a KO/+ ) displayed novelty-induced exploratory hyperactivity and increased rearing. The increased vertical activity was reproduced by heterozygous inactivation of Scn2a in dorsal-telencephalic excitatory neurons but not in inhibitory neurons. Moreover, these phenotypes were rescued by treating Scn2a KO/+ mice with CX516. Additionally, Scn2a KO/+ mice displayed mild social behavior impairment, enhanced fear conditioning, and deficient fear extinction. Neuronal activity was intensified in the medial prefrontal cortex of Scn2a KO/+ mice, with an increase in the gamma band., Conclusions: Scn2a KO/+ mice exhibit a spectrum of phenotypes commonly observed in models of schizophrenia and autism spectrum disorder. Treatment with the CX516 ampakine, which ameliorates hyperactivity in these mice, could be a potential therapeutic strategy to rescue some of the disease phenotypes., Competing Interests: All animal breeding and experimental procedures were performed in accordance with the guidelines of the Animal Experiment Committee of RIKEN Center for Brain Science and Fujita Health University.Not applicable.The authors declare that they have no competing interests.Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.

Published

2019

102. Comparison of oxcarbazepine efficacy and MHD concentrations relative to age and BMI: Associations among ABCB1, ABCC2, UGT2B7, and SCN2A polymorphisms.

Author

Yang X, Yan Y, Fang S, Zeng S, Ma H, Qian L, Chen X, Wei J, Gong Z, and Xu Z

Subjects

ATP Binding Cassette Transporter, Subfamily B genetics, Adolescent, Adult, Age Factors, Asian People, Body Mass Index, Carbamazepine analogs & derivatives, Carbamazepine blood, Child, Child, Preschool, China, Female, Genotype, Glucuronosyltransferase genetics, Humans, Infant, Male, Middle Aged, Multidrug Resistance-Associated Protein 2, Multidrug Resistance-Associated Proteins genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, Polymorphism, Single Nucleotide, Young Adult, Anticonvulsants pharmacokinetics, Anticonvulsants therapeutic use, Epilepsy drug therapy, Oxcarbazepine pharmacokinetics, Oxcarbazepine therapeutic use

Abstract

Genetic polymorphisms are related to the concentration and efficacy of oxcarbazepine (OXC). 10-Hydroxycarbazepine (MHD) is the major pharmacologically active metabolite of OXC, and it exerts an antiepileptic effect. This study aimed to explore the connection between the MHD concentration and genes such as ATP-binding cassette B1 (ABCB1), ATP-binding cassette C2 (ABCC2), UDP-glucuronosyltransferase-2B7 and sodium voltage-gated channel alpha subunit 2 (SCN2A), which participate in the antiepileptic function of OXC.Total 218 Chinese epileptic patients, were stratified into different groups according to their age, body mass index (BMI) and OXC efficacy. The genotypes of 7 single nucleotide polymorphisms in all subjects were determined by polymerase chain reaction-improved multiple ligase detection reaction assay. The MHD plasma concentration was detected by high-performance liquid chromatography and then standardized through dosage and body weight.In general, the ABCC2 rs2273697 mutant (P = .026) required a significantly higher standardized MHD concentration. For age groups, carriers of the ABCC2 rs2273697 mutant showed a significantly higher standardized MHD concentration than noncarriers in the juvenile group (P = .033). In terms of BMI, a significantly higher standardized MHD concentration was found in the ABCB1 rs2032582 mutant of the normal weight group (P = .026). The SCN2A rs17183814 mutant required a significantly higher OXC maintenance (P = .014) in the low-weight group, while lower OXC maintenance dose (P = .044) and higher standardized MHD concentration (P = .007) in the overweight group.The ABCC2 rs2273697 polymorphism was significantly associated with MHD plasma concentration in the whole patient cohort and in patients stratified by different ages, this finding provides potential theoretical guidance for the rational and safe clinical use of OXC.

Published

2019

103. Novel SCN2A mutation in a family associated with juvenile-onset myoclonus: Case report.

Author

Huang Q, Yu L, Ma M, Qi H, and Wu Y

Subjects

Adult, Anticonvulsants administration & dosage, Anticonvulsants adverse effects, Ataxia diagnosis, Ataxia etiology, Disease Progression, Drug Resistant Epilepsy diagnosis, Drug Resistant Epilepsy drug therapy, Drug Resistant Epilepsy genetics, Electroencephalography methods, Female, Genetic Testing methods, Humans, Male, Medical History Taking, Mutation, Neurologic Examination methods, Oxcarbazepine administration & dosage, Oxcarbazepine adverse effects, Pedigree, Valproic Acid administration & dosage, Valproic Acid adverse effects, Carbamazepine administration & dosage, Carbamazepine adverse effects, Myoclonic Epilepsy, Juvenile diagnosis, Myoclonic Epilepsy, Juvenile drug therapy, Myoclonic Epilepsy, Juvenile genetics, NAV1.2 Voltage-Gated Sodium Channel genetics

Abstract

Rationale: The phenotypic spectrum caused by SCN2A mutations includes benign neonatal/infantile seizures, Ohtahara syndrome, infantile spasms, West syndrome, and other unclassified epileptic phenotypes. Mutations in SCN2A have been implicated in neonatal seizure cases. Here, we described a Chinese family with 2 members having juvenile-onset myoclonus and identified a novel SCN2A point mutation within this family., Patient Concerns: The 21-year-old male proband suffered from frequent myoclonus at 11 years old with subsequent progressive ataxia. His elder maternal half-sister also experienced myoclonus. Genomic DNA of the patients was extracted from the peripheral blood cells of the proband, elder maternal half-sister, parents, and uncle of the proband. Targeted next-generation sequencing was used to screen gene mutations in the proband. The potential functional effects of mutations within SCN2A were predicted In silico analyses., Diagnoses: Genetic testing revealed a novel SCN2A variant, c.T4820C, which contains a highly conserved amino acid substitution within segment S5 (p.V1607A). This mutation was predicted to produce a dysfunctional Nav1.2 protein by Mutation Taster and Protein Variation Effect Analyzer (PROVEAN). Genotype-phenotype correlation showed an incomplete penetrance of p.V1607A., Interventions: The proband was treated by multiple antiepileptic drugs. These included carbamazepine, oxcarbazepine, valproate, and topiramate., Outcomes: The duration of follow up was 2 years, and the proband developed drug-resistant epilepsy., Lessons: The case gives us the lesson that SCN2A mutation can contribute to juvenile-onset myoclonus. Our findings extend the spectrums of SCN2A mutations and the clinical features of patients with SCN2A mutations.

Published

2019

104. Replicated associations of FADS1, MAD1L1, and a rare variant at 10q26.13 with bipolar disorder in Chinese population.

Author

Zhao L, Chang H, Zhou DS, Cai J, Fan W, Tang W, Tang W, Li X, Liu W, Liu F, He Y, Bai Y, Sun Y, Dai J, Li L, Xiao X, Zhang C, and Li M

Subjects

Asian People genetics, Bipolar Disorder epidemiology, China epidemiology, Delta-5 Fatty Acid Desaturase, Depressive Disorder, Major epidemiology, Depressive Disorder, Major genetics, Female, Genetic Predisposition to Disease, Genome-Wide Association Study, Haplotypes, Humans, Male, NAV1.2 Voltage-Gated Sodium Channel genetics, Nerve Tissue Proteins genetics, Polymorphism, Single Nucleotide, Reproducibility of Results, Risk Factors, Bipolar Disorder genetics, Cell Cycle Proteins genetics, Fatty Acid Desaturases genetics, Nuclear Proteins genetics

Abstract

Genetic analyses of psychiatric illnesses, such as bipolar disorder (BPD), have revealed essential information regarding the underlying pathological mechanisms. While such studies in populations of European ancestry have achieved prominent success, understanding the genetic risk factors of these illnesses (especially BPD) in Chinese population remains an urgent task. Given the lack of genome-wide association study (GWAS) of BPD in Chinese population from Mainland China, replicating the previously reported GWAS hits in distinct populations will provide valuable information for future GWAS analysis in Han Chinese. In the present study, we have recruited 1146 BPD cases and 1956 controls from Mainland China for genetic analyses, as well as 65 Han Chinese brain amygdala tissues for mRNA expression analyses. Using this clinical sample, one of the largest Han Chinese BPD samples till now, we have conducted replication analyses of 21 single nucleotide polymorphisms (SNPs) extracted from previous GWAS of distinct populations. Among the 21 tested SNPs, 16 showed the same direction of allelic effects in our samples compared with previous studies; 6 SNPs achieved nominal significance (p < 0.05) at one-tailed test, and 2 additional SNPs showed marginal significance (p < 0.10). Aside from replicating previously reported BPD risk SNPs, we herein also report several intriguing findings: (1) the SNP rs174576 was associated with BPD in our Chinese sample and in the overall global meta-analysis, and was significantly correlated with FADS1 mRNA in diverse public RNA-seq datasets as well as our in house collected Chinese amygdala samples; (2) two (partially) independent SNPs in MAD1L1 were both significantly associated with BPD in our Chinese sample, which was also supported by haplotype analysis; (3) a rare SNP rs78089757 in 10q26.13 region was a genome-wide significant variant for BPD in East Asians, and this SNP was near monomorphic in Europeans. In sum, these results confirmed several significant BPD risk genes. We hope this Chinese BPD case-control sample and the current brain amygdala tissues (with continuous increasing sample size in the near future) will provide helpful resources in elucidating the genetic and molecular basis of BPD in this major world population.

Published

2018

105. Relationship of electrophysiological dysfunction and clinical severity in SCN2A-related epilepsies.

Author

Lauxmann S, Verbeek NE, Liu Y, Zaichuk M, Müller S, Lemke JR, van Kempen MJA, Lerche H, and Hedrich UBS

Subjects

Cell Line, Electrophysiological Phenomena, Epileptic Syndromes genetics, Epileptic Syndromes metabolism, Female, Genetic Variation, Humans, Infant, Infant, Newborn, Male, Pedigree, Phenotype, Severity of Illness Index, Amino Acid Substitution, Epileptic Syndromes physiopathology, NAV1.2 Voltage-Gated Sodium Channel genetics, NAV1.2 Voltage-Gated Sodium Channel metabolism

Abstract

Variants in the SCN2A gene cause a broad spectrum of epilepsy syndromes of variable severity including benign neonatal-infantile epilepsy (BFNIE), developmental and epileptic encephalopathies (DEE), and other neuropsychiatric disorders. Here, we studied three newly identified variants, which caused distinct phenotypes observed in nine affected individuals of three families, including BFNIE, and DEE with intractable neonatal seizures. Whole cell patch-clamp recordings of transfected tsA201 cells disclosed an increased current density and an increased subthreshold sodium inward current upon an action potential stimulus (p.(Lys908Glu)), a hyperpolarizing shift of the activation curve (p.(Val208Glu) and p.(Thr773Ile)), and an increased persistent current (p.(Thr773Ile)). To evaluate genotype-phenotype correlations, we next developed scoring systems for both the extent of the electrophysiological dysfunction and the severity of the clinical phenotype and applied those to 21 previously and newly functionally characterized SCN2A variants. All inherited variants were associated with a mild clinical phenotype and a lower electrophysiological score compared to those occurring de novo and causing severe phenotypes. Our results thus reveal a nice correlation between the extent of channel dysfunction and the clinical severity., (© 2018 Wiley Periodicals, Inc.)

Published

2018

106. Dominant SCN2A Mutation Causes Familial Episodic Ataxia and Impairment of Speech Development.

Author

Fazeli W, Becker K, Herkenrath P, Düchting C, Körber F, Landgraf P, Nürnberg P, Altmüller J, Thiele H, Koy A, Liebau MC, Simon T, Dötsch J, and Cirak S

Subjects

Adult, Female, Humans, Infant, Male, Pedigree, Cerebellar Ataxia genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, Speech Disorders genetics

Abstract

Mutations in SCN2A are associated with a heterogeneous clinical spectrum including epilepsy and autism. Here, we have identified a peculiar phenotype associated with vaccination related exacerbations of ataxia. We report the first family with three individuals affected by SCN2A -associated episodic ataxia (EA) with impaired speech development. The index patient manifested his first episode of subacute cerebellar ataxia at the age of 12 months, 3 weeks after vaccinations for measles, mumps, rubella, and varicella. Cranial magnetic resonance imaging showed a lesion of the left cerebellar hemisphere, which was first considered as a potential cause of the ataxia. The patient fully recovered within 3 weeks, but developed three very similar episodes of transient ataxia within the following 24 months. Whole exome sequencing of the index patient revealed a heterozygous autosomal-dominant mutation in SCN2A (NM&#95;021007, c.4949T > C; p.L1650P), which was confirmed in the likewise affected mother, and was then also identified in the younger brother who developed the first episode of ataxia. We hereby extend the recently described spectrum of SCN2A -associated neurologic disorders, emphasizing that SCN2A mutations should also be considered in familial cases of EA. Coincidental imaging findings or other associated events such as immunizations should not protract genetic investigations., Competing Interests: The authors declare that they have no conflict of interest. Written informed consent for research and publication was obtained from the family., (Georg Thieme Verlag KG Stuttgart · New York.)

Published

2018

107. Catatonia Associated With a SCN2A -Related Disorder in a 4-Year-Old Child.

Author

Leroy A, Corfiotti C, Nguyen The Tich S, Ferrafiat V, Amad A, Jardri R, and Medjkane F

Subjects

Catatonia drug therapy, Child, Preschool, Humans, Lorazepam therapeutic use, Mutation, Seizures drug therapy, Seizures etiology, Anticonvulsants therapeutic use, Catatonia genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, Vigabatrin therapeutic use

Abstract

Catatonia is a rare, underdiagnosed syndrome in children. We report the case of a 4-year-old child admitted for recent social withdrawal alternating with psychomotor excitement, verbigeration, and a loss of toilet readiness. He had a history of neonatal seizures, had been stabilized with vigabatrin, and was seizure free without treatment for several months. The pediatric and psychiatric examination revealed motor stereotypes, mannerism, bilateral mydriasis, and visual hallucinations. Laboratory and brain imaging explorations were initially negative. Catatonic symptoms, as measured with the Pediatric Catatonia Rating Scale, significantly decreased after introducing lorazepam, the first-line recommended treatment of this condition. On the basis of the neonatal seizure history, complementary genetic investigations were performed and revealed a mutation in the SCN2A gene, which encodes the voltage-gated sodium channel Nav1.2. Catatonic symptoms progressively disappeared after reintroducing vigabatrin. At the syndromic level, catatonia in young children appears responsive to high-dose lorazepam and is well monitored by using the Pediatric Catatonia Rating Scale. This case reveals the need for wide-ranging explorations in early-onset catatonia because specific targeted treatments might be available., Competing Interests: POTENTIAL CONFLICT OF INTEREST: The authors have indicated they have no potential conflicts of interest to disclose., (Copyright © 2018 by the American Academy of Pediatrics.)

Published

2018

108. Novel mutations and phenotypes of epilepsy-associated genes in epileptic encephalopathies.

Author

Zhou P, He N, Zhang JW, Lin ZJ, Wang J, Yan LM, Meng H, Tang B, Li BM, Liu XR, Shi YW, Zhai QX, Yi YH, and Liao WP

Subjects

Adolescent, Child, Child, Preschool, Chloride Channels genetics, Epilepsies, Myoclonic genetics, Epilepsy genetics, Female, Genetic Association Studies, High-Throughput Nucleotide Sequencing, Humans, Infant, KCNQ2 Potassium Channel genetics, Male, Mutation, NAV1.1 Voltage-Gated Sodium Channel genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, Nerve Tissue Proteins genetics, Phenotype, Potassium Channels genetics, Potassium Channels, Sodium-Activated, Young Adult, Epileptic Syndromes genetics, Spasms, Infantile genetics

Abstract

Epileptic encephalopathies are severe epilepsy disorders with strong genetic bases. We performed targeted next-generation sequencing (NGS) in 70 patients with epileptic encephalopathies. The likely pathogenicity of variants in candidate genes was evaluated by American College of Medical Genetics and Genomics (ACMG) scoring taken together with the accepted clinical presentation. Thirty-three candidate variants were detected after population filtration and computational prediction. According to ACMG, 21 candidate variants, including 18 de novo variants, were assessed to be pathogenic/likely pathogenic with clinical concordance. Twelve variants were initially assessed as uncertain significance by ACMG, among which 3 were considered causative and 3 others were considered possibly causative after analysis of clinical concordance. In total, 24 variants were identified as putatively causative, among which 19 were novel findings. SCN1A mutations were identified in 50% of patients with Dravet syndrome. TSC1/TSC2 mutations were detected in 66.7% of patients with tuberous sclerosis. STXBP1 mutations were the main findings in patients with West syndrome. Mutations in SCN2A, KCNT1, KCNQ2 and CLCN4 were identified in patients with epileptic infantile with migrating focal seizures; among them, KCNQ2 and CLCN4 were first identified as potential causative genes. Only one CHD2 mutation was detected in patients with Lennox-Gastaut syndrome. This study highlighted the utility of targeted NGS in genetic diagnoses of epileptic encephalopathies and a comprehensive evaluation of the pathogenicity of variants based on ACMG scoring and assessment of clinical concordance. Epileptic encephalopathies differ in genetic causes, and the genotype-phenotype correlations would provide insights into the underlying pathogenic mechanisms., (© 2018 John Wiley & Sons Ltd and International Behavioural and Neural Genetics Society.)

Published

2018

109. Whole-Exome Sequencing Implicates SCN2A in Episodic Ataxia, but Multiple Ion Channel Variants May Contribute to Phenotypic Complexity.

Author

Maksemous N, Smith RA, Sutherland HG, Sampaio H, and Griffiths LR

Subjects

Adolescent, Adult, Calcium Channels genetics, DNA Mutational Analysis, Humans, Male, Models, Molecular, Mutation, NAV1.2 Voltage-Gated Sodium Channel chemistry, Pedigree, Protein Conformation, Symptom Assessment, Tomography, X-Ray Computed, Exome Sequencing, Young Adult, Ataxia diagnosis, Ataxia genetics, Genetic Association Studies, Genetic Predisposition to Disease, Genetic Variation, NAV1.2 Voltage-Gated Sodium Channel genetics, Phenotype

Abstract

Although the clinical use of targeted gene sequencing-based diagnostics is valuable, whole-exome sequencing has also emerged as a successful diagnostic tool in molecular genetics laboratories worldwide. Molecular genetic tests for episodic ataxia type 2 (EA2) usually target only the specific calcium channel gene ( CACNA1A ) that is known to cause EA2. In cases where no mutations are identified in the CACNA1A gene, it is important to identify the causal gene so that more effective treatment can be prioritized for patients. Here we present a case of a proband with a complex episodic ataxias (EA)/seizure phenotype with an EA-affected father; and an unaffected mother, all negative for CACNA1A gene mutations. The trio was studied by whole-exome sequencing to identify candidate genes responsible for causing the complex EA/seizure phenotype. Three rare or novel variants in Sodium channel α2-subunit; SCN2A (c.3973G>T: p.Val1325Phe) , Potassium channel, Kv3.2; KCNC2 (c.1006T>C: p.Ser336Pro) and Sodium channel Nav1.6; SCN8A (c.3421C>A: p.Pro1141Thr) genes were found in the proband. While the SCN2A variant is likely to be causal for episodic ataxia, each variant may potentially contribute to the phenotypes observed in this family. This study highlights that a major challenge of using whole-exome/genome sequencing is the identification of the unique causative mutation that is associated with complex disease.

Published

2018

110. Lacosamide for SCN2A-related intractable neonatal and infantile seizures.

Author

Flor-Hirsch H, Heyman E, Livneh A, Reish O, Watemberg N, Litmanovits I, Ben Sason Lilli A, Lev D, Lerman Sagie T, and Bassan H

Subjects

Drug Resistant Epilepsy drug therapy, Drug Resistant Epilepsy genetics, Electroencephalography, Female, Humans, Infant, Newborn, Infant, Newborn, Diseases genetics, Lacosamide administration & dosage, Male, Mutation, Missense, Spasms, Infantile drug therapy, Spasms, Infantile genetics, Voltage-Gated Sodium Channel Blockers administration & dosage, Epilepsy drug therapy, Epilepsy genetics, Infant, Newborn, Diseases drug therapy, Lacosamide pharmacology, NAV1.2 Voltage-Gated Sodium Channel genetics, Voltage-Gated Sodium Channel Blockers pharmacology

Abstract

Voltage-gated sodium channel alpha subunit 2 (SCN2A) gene mutations are associated with neonatal seizures and a wide range of epilepsy syndromes. Previous reports suggest that traditional sodium channel blockers (SCBs) such as phenytoin, carbamazepine, and lamotrigine have a beneficial effect on SCN2A-related neonatal seizures, as they counteract the gain-of-function effect of mutated Nav1.2 channels. Additionally, SCBs are beneficial against other sodium and potassium channel-related neonatal seizures. There are, however, few reports describing the effect of the new SCB lacosamide against neonatal and infantile epileptic seizures. We report herein two neonates with intractable neonatal seizures with SCN2A pathogenic missense variants. Both infants showed temporary seizure relief following IV administrations of phenytoin, but were resistant to a combination of antiepileptic drugs, while complete seizure control was achieved following lacosamide administration. We suggest that SCBs, e.g. phenytoin, should be introduced early for refractory neonatal seizures of non-lesional and presumably genetic origin. If any beneficial response to a SCB is noted, this should prompt an initiation of additional SCBs. New clinical trials will provide data on the efficacy and safety of the new SCB lacosamide for genetic neonatal seizures and perhaps neonatal seizures in general.

Published

2018

111. Successful Adaptation of Targeted Gene Panel Next-Generation Sequencing in Regional Hospital in Hong Kong: Genomic Diagnosis of SCN2A -Related Seizure Disorder.

Author

Lee HH, Lau NK, Yeung CW, Ng SG, Yau KE, and Mak CM

Subjects

Genomics methods, Hong Kong, Hospitals, Humans, Infant, Newborn, Male, Epilepsy diagnosis, Epilepsy genetics, High-Throughput Nucleotide Sequencing methods, NAV1.2 Voltage-Gated Sodium Channel genetics

Abstract

Competing Interests: There are no conflicts of interest

Published

2018

112. Selective ion permeation involves complexation with carboxylates and lysine in a model human sodium channel.

Author

Flood E, Boiteux C, and Allen TW

Subjects

Amines chemistry, Bacterial Proteins chemistry, Humans, Membrane Potentials, Mutation, NAV1.2 Voltage-Gated Sodium Channel genetics, Potassium chemistry, Protein Binding, Protein Domains, Protein Transport, Sodium chemistry, Static Electricity, Thermodynamics, Carboxylic Acids chemistry, Ions, Lysine chemistry, NAV1.2 Voltage-Gated Sodium Channel chemistry

Abstract

Bacterial and human voltage-gated sodium channels (Navs) exhibit similar cation selectivity, despite their distinct EEEE and DEKA selectivity filter signature sequences. Recent high-resolution structures for bacterial Navs have allowed us to learn about ion conduction mechanisms in these simpler homo-tetrameric channels, but our understanding of the function of their mammalian counterparts remains limited. To probe these conduction mechanisms, a model of the human Nav1.2 channel has been constructed by grafting residues of its selectivity filter and external vestibular region onto the bacterial NavRh channel with atomic-resolution structure. Multi-μs fully atomistic simulations capture long time-scale ion and protein movements associated with the permeation of Na+ and K+ ions, and their differences. We observe a Na+ ion knock-on conduction mechanism facilitated by low energy multi-carboxylate/multi-Na+ complexes, akin to the bacterial channels. These complexes involve both the DEKA and vestibular EEDD rings, acting to draw multiple Na+ into the selectivity filter and promote permeation. When the DEKA ring lysine is protonated, we observe that its ammonium group is actively participating in Na+ permeation, presuming the role of another ion. It participates in the formation of a stable complex involving carboxylates that collectively bind both Na+ and the Lys ammonium group in a high-field strength site, permitting pass-by translocation of Na+. In contrast, multiple K+ ion complexes with the DEKA and EEDD rings are disfavored by up to 8.3 kcal/mol, with the K+-lysine-carboxylate complex non-existent. As a result, lysine acts as an electrostatic plug that partially blocks the flow of K+ ions, which must instead wait for isomerization of lysine downward to clear the path for K+ passage. These distinct mechanisms give us insight into the nature of ion conduction and selectivity in human Nav channels, while uncovering high field strength carboxylate binding complexes that define the more general phenomenon of Na+-selective ion transport in nature., Competing Interests: The authors have declared that no competing interests exist.

Published

2018

113. SCN2A mutation in an infant presenting with migrating focal seizures and infantile spasm responsive to a ketogenic diet.

Author

Su DJ, Lu JF, Lin LJ, Liang JS, and Hung KL

Subjects

Brain physiopathology, Drug Resistant Epilepsy genetics, Drug Resistant Epilepsy physiopathology, Humans, Infant, Male, Mutation, Seizures genetics, Seizures physiopathology, Spasms, Infantile genetics, Spasms, Infantile physiopathology, Diet, Ketogenic, Drug Resistant Epilepsy diet therapy, NAV1.2 Voltage-Gated Sodium Channel genetics, Seizures diet therapy, Spasms, Infantile diet therapy

Abstract

SCN2A mutations have been identified in various encephalopathy phenotypes, ranging from benign familial neonatal-infantile seizure (BFNIS) to more severe forms of epileptic encephalopathy such as Ohtahara syndrome or epilepsy of infancy with migrating focal seizure (EIMFS). Thus far, no particularly effective treatment is available for severe epileptic encephalopathy caused by SCN2A mutations in children. We present the case of a boy who developed seizures on the third day of life and received a diagnosis of EIMFS based on his clinical presentations and electroencephalography reports. Antiepileptic drugs, namely oxcarbazepine, phenytoin, valproate, levetiracetam, and clonazepam, as well as adrenocorticotropic hormone therapy failed to reduce the severity of the seizures. Seizure pattern changed to infantile spasm with extensor thrust since 5 months of age. A ketogenic diet consisting of a medium-chain triglyceride recipe was introduced at 8 months of age and the seizures were resolved in the following 10 months. A de novo mutation in SCN2A (c.573G > T; p.W191C) was proven through next-generation sequencing., (Copyright © 2018 The Japanese Society of Child Neurology. Published by Elsevier B.V. All rights reserved.)

Published

2018

114. Axonal sodium channel NaV1.2 drives granule cell dendritic GABA release and rapid odor discrimination.

Author

Nunes D and Kuner T

Subjects

Action Potentials physiology, Animals, Axons ultrastructure, Dendrites ultrastructure, Discrimination Learning physiology, Gene Expression, Mice, Mice, Inbred C57BL, Microtomy, NAV1.2 Voltage-Gated Sodium Channel metabolism, Neurotransmitter Agents metabolism, Olfactory Bulb cytology, RNA, Small Interfering genetics, RNA, Small Interfering metabolism, Sensory Receptor Cells physiology, Sensory Receptor Cells ultrastructure, Synapses physiology, Synaptic Transmission physiology, Tissue Culture Techniques, gamma-Aminobutyric Acid metabolism, Axons physiology, Dendrites physiology, NAV1.2 Voltage-Gated Sodium Channel genetics, Odorants analysis, Olfactory Bulb physiology, Olfactory Perception physiology

Abstract

Dendrodendritic synaptic interactions between olfactory bulb mitral and granule cells represent a key neuronal mechanism of odor discrimination. Dendritic release of gamma-aminobutyric acid (GABA) from granule cells contributes to stimulus-dependent, rapid, and accurate odor discrimination, yet the physiological mechanisms governing this release and its behavioral relevance are unknown. Here, we show that granule cells express the voltage-gated sodium channel α-subunit NaV1.2 in clusters distributed throughout the cell surface including dendritic spines. Deletion of NaV1.2 in granule cells abolished spiking and GABA release as well as inhibition of synaptically connected mitral cells (MCs). As a consequence, mice required more time to discriminate highly similar odorant mixtures, while odor discrimination learning remained unaffected. In conclusion, we show that expression of NaV1.2 in granule cells is crucial for physiological dendritic GABA release and rapid discrimination of similar odorants with high accuracy. Hence, our data indicate that neurotransmitter-releasing dendritic spines function just like axon terminals., Competing Interests: The authors have declared that no competing interests exist.

Published

2018

115. Heterozygous deletion of SCN2A and SCN3A in a patient with autism spectrum disorder and Tourette syndrome: a case report.

Author

Nickel K, Tebartz van Elst L, Domschke K, Gläser B, Stock F, Endres D, Maier S, and Riedel A

Subjects

Adaptor Proteins, Signal Transducing genetics, Adult, Chromosome Deletion, Humans, Male, NAV1.1 Voltage-Gated Sodium Channel genetics, Phenotype, Transcription Factors genetics, Autism Spectrum Disorder genetics, Developmental Disabilities genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, NAV1.3 Voltage-Gated Sodium Channel genetics, Sodium Channels genetics, Tourette Syndrome genetics

Abstract

Background: Mutations in voltage-gated sodium channel (SCN) genes are supposed to be of importance in the etiology of psychiatric and neurological diseases, in particular in the etiology of seizures. Previous studies report a potential susceptibility region at the chromosomal locus 2q including SCN1A, SCN2A and SCN3A genes for autism spectrum disorder (ASD). To date, there is no previous description of a patient with comorbid ASD and Tourette syndrome showing a deletion containing SCN2A and SCN3A., Case Presentation: We present the unique complex case of a 28-year-old male patient suffering from developmental retardation and exhibiting a range of behavioral traits since birth. He received the diagnoses of ASD (in early childhood) and of Tourette syndrome (in adulthood) according to ICD-10 and DSM-5 criteria. Investigations of underlying genetic factors yielded a heterozygous microdeletion of approximately 719 kb at 2q24.3 leading to a deletion encompassing the five genes SCN2A (exon 1 to intron 14-15), SCN3A, GRB14 (exon 1 to intron 2-3), COBLL1 and SCL38A11., Conclusions: We discuss the association of SCN2A, SCN3A, GRB14, COBLL1 and SCL38A11 deletions with ASD and Tourette syndrome and possible implications for treatment.

Published

2018

116. Deletions of SCN2A and SCN3A genes in a patient with West syndrome and autistic spectrum disorder.

Author

Chong PF, Saitsu H, Sakai Y, Imagi T, Nakamura R, Matsukura M, Matsumoto N, and Kira R

Subjects

Autism Spectrum Disorder complications, Autism Spectrum Disorder diagnostic imaging, Autism Spectrum Disorder physiopathology, Brain diagnostic imaging, Brain physiopathology, Diagnosis, Differential, Humans, Infant, Male, Spasms, Infantile complications, Spasms, Infantile diagnostic imaging, Spasms, Infantile physiopathology, Autism Spectrum Disorder genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, NAV1.3 Voltage-Gated Sodium Channel genetics, Sequence Deletion, Sodium Channels genetics, Spasms, Infantile genetics

Abstract

SCN2A encodes the alpha-subunit of voltage-gated sodium channel, Nav1.2, which is highly expressed at an early stage of the postnatal brain. Genetic studies revealed that de novo heterozygous mutations of SCN2A caused severe developmental disorders in childhood, such as autism and epileptic encephalopathy. However, few reports have demonstrated the cases carrying segmental deletions at the SCN2A locus for those with epileptic disorders. In this study, we report a 1.8-year-old boy, who presented with West syndrome in infancy and developed the sequelae of psychomotor delay and autism. Since whole-exome sequencing did not detect pathogenic mutations, we extensively searched for microdeletions and duplications by applying the eXome Hidden Markov Model (XHMM) for read depths of sequenced intervals. Using this approach, we identified a de novo deletion spanning the 1.1-Mb region of chromosome 2q24.3. We found that the deleted interval included the SCN2A and SCN3A loci. These data validate the utility of XHMM and support that SCN2A is involved in the pathogenic processes underlying epileptic encephalopathy in childhood., (Copyright © 2018 British Epilepsy Association. Published by Elsevier Ltd. All rights reserved.)

Published

2018

117. Insight into tetrodotoxin blockade and resistance mechanisms of Na v 1.2 sodium channel by theoretical approaches.

Author

Xu L, Li D, Ding J, Pan L, and Ding X

Subjects

Binding Sites, Humans, Hydrogen Bonding, Mutagenesis, Site-Directed, NAV1.2 Voltage-Gated Sodium Channel chemistry, NAV1.2 Voltage-Gated Sodium Channel genetics, Protein Binding, Tetrodotoxin analogs & derivatives, Thermodynamics, Molecular Docking Simulation, Molecular Dynamics Simulation, NAV1.2 Voltage-Gated Sodium Channel metabolism, Tetrodotoxin metabolism

Abstract

Na v 1.2, a member of voltage-gated sodium channels (Na v s) that are responsible for the generation and propagation of action potentials along the cell membrane, and play a vital role in the process of information transmission within the nervous system and muscle contraction, is preferentially expressed in the central nervous system. As a potent and selective blocker of Na v s, tetrodotoxin (TTX) has been extensively studied in biological and chemical sciences, whereas the detailed mechanism by which it blocks nine Na v 1 channel subtypes remain elusive. Despite the high structural similarity, the TTX metabolite 4,9-anhydro-TTX is 161 times less effective toward the mammalian Na v 1.2, which puzzled us to ask a question why such a subtle structural variation results in the largely binding affinity difference. In the current work, an integrated computational strategy, including homology modeling, induced fit docking, explicit-solvent MD simulations, and free energy calculations, was employed to investigate the binding mechanism and conformational determinants of TTX analogs. Based on the computational results, the H-bond interactions between C4-OH and C9-OH of TTX and the outer ring carboxylates of the selectivity-filter residues, and the cation-π interaction between the primary amine of guanidinium of TTX and Phe385 determine the difference of their binding affinities. Moreover, the computationally simulations were carried out for the D384N and E945K mutants of hNa v 1.2-TTX, and the rank of the predicted binding free energies is in accordance with the experimental data. These observations provide a valuable model to design potent and selective neurotoxins of Na v 1.2 and shed light on the blocking mechanism of TTX to sodium channels., (© 2018 John Wiley & Sons A/S.)

Published

2018

118. Association between SCN1A and SCN2A mutations and clinical/EEG features in Chinese patients from epilepsy or severe seizures.

Author

Kong Y, Yan K, Hu L, Wang M, Dong X, Lu Y, Wu B, Wang H, Yang L, and Zhou W

Subjects

Brain diagnostic imaging, Cohort Studies, Epilepsy diagnosis, Epilepsy therapy, Female, Humans, Infant, Infant, Newborn, Magnetic Resonance Imaging, Phenotype, Prognosis, Seizures diagnosis, Seizures therapy, Asian People genetics, Electroencephalography, Epilepsy genetics, Mutation, NAV1.1 Voltage-Gated Sodium Channel genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, Seizures genetics

Abstract

Background: We investigated the association between SCN1A and SCN2A mutations and clinical phenotype and electroencephalography (EEG) features., Methods: In this study, 48 patients suffered from epilepsy or severe seizures with SCN1A and SCN2A mutations were recruited. Medical data and molecular diagnosis were analyzed., Results: A total of 47 mutations were identified, including 33 novel mutations. The onset of most epilepsy caused by SCN1A mutations (1-6 m) was later than that of SCN2A mutations (neonatal). SCN1A mutations included truncating mutations and missense mutations occurred in the crucial region were associated with more severe phenotypes and developmental delay (85.7%, P = 0.020). De novo mutations or truncating mutations of SCN2A mutations are mainly associated with severe phenotypes. The proportion of initial abnormal EEG of SCN2A mutation was higher than that of SCN1A mutation (54.2%, 100%). Patients with SCN1A mutations showed more focal epileptiform discharges (69.2%), while patients with SCN2A mutations had more multifocal epileptiform discharges (53.8%). Sodium channel blockers were less effective for patients with SCN1A mutations and SCN2A mutations with early seizures onset., Conclusions: Our study expanded the mutation spectrum of the SCN1A and SCN2A, and led to a better understanding of the similarities and difference in the genetic and clinical features between the two genes., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

119. Role of sodium channel subtype in action potential generation by neocortical pyramidal neurons.

Author

Katz E, Stoler O, Scheller A, Khrapunsky Y, Goebbels S, Kirchhoff F, Gutnick MJ, Wolf F, and Fleidervish IA

Subjects

Animals, Gene Deletion, Mice, Mice, Transgenic, NAV1.2 Voltage-Gated Sodium Channel genetics, NAV1.6 Voltage-Gated Sodium Channel genetics, Neocortex cytology, Pyramidal Cells cytology, Action Potentials physiology, Axons metabolism, NAV1.2 Voltage-Gated Sodium Channel metabolism, NAV1.6 Voltage-Gated Sodium Channel metabolism, Neocortex metabolism, Pyramidal Cells metabolism

Abstract

Neocortical pyramidal neurons express several distinct subtypes of voltage-gated Na + channels. In mature cells, Na v 1.6 is the dominant channel subtype in the axon initial segment (AIS) as well as in the nodes of Ranvier. Action potentials (APs) are initiated in the AIS, and it has been proposed that the high excitability of this region is related to the unique characteristics of the Na v 1.6 channel. Knockout or loss-of-function mutation of the Scn8a gene is generally lethal early in life because of the importance of this subtype in noncortical regions of the nervous system. Using the Cre/loxP system, we selectively deleted Na v 1.6 in excitatory neurons of the forebrain and characterized the excitability of Na v 1.6-deficient layer 5 pyramidal neurons by patch-clamp and Na + and Ca 2+ imaging recordings. We now report that, in the absence of Na v 1.6 expression, the AIS is occupied by Na v 1.2 channels. However, APs are generated in the AIS, and differences in AP propagation to soma and dendrites are minimal. Moreover, the channels that are expressed in the AIS still show a clear hyperpolarizing shift in voltage dependence of activation, compared with somatic channels. The only major difference between Na v 1.6-null and wild-type neurons was a strong reduction in persistent sodium current. We propose that the molecular environment of the AIS confers properties on whatever Na channel subtype is present and that some other benefit must be conferred by the selective axonal presence of the Na v 1.6 channel., Competing Interests: The authors declare no conflict of interest.

Published

2018

120. [Phenotype study of SCN2A gene related epilepsy].

Author

Zeng Q, Zhang YH, Yang XL, Zhang J, Liu AJ, Liu XY, Jiang YW, and Wu XR

Subjects

Brain pathology, Child, Developmental Disabilities etiology, Electroencephalography, Female, Humans, Infant, Infant, Newborn, Male, Mutation, Phenotype, Retrospective Studies, Epilepsy genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, Spasms, Infantile genetics

Abstract

Objective: To summarize the phenotype of epileptic children with SCN2A mutations. Methods: Epileptic patients who were treated in the Pediatric Department of Peking University First Hospital from September 2006 to October 2017 and detected with SCN2A mutations by targeted next-generation sequencing were enrolled. Clinical manifestations of all patients were analyzed retrospectively. Results: A total of 21 patients (16 boys and 5 girls) with SCN2A mutations were collected. Twenty-one SCN2A mutations were identified. Ten patients had mutations inherited from one of their parents and 11 patients had de novo mutations. The age of epilepsy onset was from 2 days to 2 years and 6 months: six patients with seizure onset in neonates (29%) , six patients with seizure onset between 1 month and 3 months of age (29%), three patients with seizure onset between 4 months and 6 months of age, two patients with seizure onset between 7 months and one year of age, and four patients with seizure onset beyond one year of age. Multiple seizure types were observed. The focal seizure was the most common seizure type which was observed in 18 patients (86%) . Spasm seizure was observed in 6 patients (29%) . Other seizure types were rare. In 19 patients, seizures manifested in clusters (90%) . In 3 patients, seizures manifested fever-sensitive. Nine of ten patients with inherited SCN2A mutations had normal development. However, all patients with de novo SCN2A mutations had mild or severer development delay. In 21 patients with SCN2A mutations, five were diagnosed with benign familial infantile epilepsy, 3 with benign familial neonatal-infantile epilepsy, 3 with Ohtahara syndrome, 3 with West syndrome, 2 with encephalopathy with early infantile onset epilepsy, one with febrile seizures plus, one with Dravet syndrome, one with encephalopathy with childhood-onset epilepsy, one with autism with epilepsy and one with intellectual disability with epilepsy. Conclusions: The clinical features of patients with SCN2A mutations include that main seizure onset is the neonate and early infancy, and the main seizure type is the focal seizure, manifested in clusters. The large spectrum of SCN2A-related epilepsy, which not only includes epilepsy with a comparatively favorable prognosis, but also epileptic encephalopathy. De novo mutations often lead to severe phenotype with development delay.

Published

2018

121. Progress in Understanding and Treating SCN2A-Mediated Disorders.

Author

Sanders SJ, Campbell AJ, Cottrell JR, Moller RS, Wagner FF, Auldridge AL, Bernier RA, Catterall WA, Chung WK, Empfield JR, George AL Jr, Hipp JF, Khwaja O, Kiskinis E, Lal D, Malhotra D, Millichap JJ, Otis TS, Petrou S, Pitt G, Schust LF, Taylor CM, Tjernagel J, Spiro JE, and Bender KJ

Subjects

Animals, Humans, Neurodevelopmental Disorders drug therapy, NAV1.2 Voltage-Gated Sodium Channel genetics, NAV1.2 Voltage-Gated Sodium Channel metabolism, Neurodevelopmental Disorders genetics, Neurodevelopmental Disorders metabolism

Abstract

Advances in gene discovery for neurodevelopmental disorders have identified SCN2A dysfunction as a leading cause of infantile seizures, autism spectrum disorder, and intellectual disability. SCN2A encodes the neuronal sodium channel Na V 1.2. Functional assays demonstrate strong correlation between genotype and phenotype. This insight can help guide therapeutic decisions and raises the possibility that ligands that selectively enhance or diminish channel function may improve symptoms. The well-defined function of sodium channels makes SCN2A an important test case for investigating the neurobiology of neurodevelopmental disorders more generally. Here, we discuss the progress made, through the concerted efforts of a diverse group of academic and industry scientists as well as policy advocates, in understanding and treating SCN2A-related disorders., (Copyright © 2018 Elsevier Ltd. All rights reserved.)

Published

2018

122. Altered hippocampal replay is associated with memory impairment in mice heterozygous for the Scn2a gene.

Author

Middleton SJ, Kneller EM, Chen S, Ogiwara I, Montal M, Yamakawa K, and McHugh TJ

Subjects

Action Potentials physiology, Animals, Behavior, Animal physiology, Heterozygote, Male, Memory Disorders physiopathology, Mice, Mice, Knockout, Neural Pathways physiopathology, Neurons physiology, Sleep physiology, Hippocampus physiopathology, Memory Disorders genetics, Memory, Short-Term physiology, NAV1.2 Voltage-Gated Sodium Channel genetics, Spatial Memory physiology

Abstract

An accumulating body of experimental evidence has implicated hippocampal replay occurring within sharp wave ripples (SPW-Rs) as crucial for learning and memory in healthy subjects. This raises speculation that neurological disorders impairing memory disrupt either SPW-Rs or their underlying neuronal activity. We report that mice heterozygous for the gene Scn2a, a site of frequent de novo mutations in humans with intellectual disability, displayed impaired spatial memory. While we observed no changes during encoding, to either single place cells or cell assemblies, we identified abnormalities restricted to SPW-R episodes that manifest as decreased cell assembly reactivation strengths and truncated hippocampal replay sequences. Our results suggest that alterations to hippocampal replay content may underlie disease-associated memory deficits.

Published

2018

123. Dynamic action potential clamp predicts functional separation in mild familial and severe de novo forms of SCN2A epilepsy.

Author

Berecki G, Howell KB, Deerasooriya YH, Cilio MR, Oliva MK, Kaplan D, Scheffer IE, Berkovic SF, and Petrou S

Subjects

Adolescent, Adult, Brain Diseases genetics, Child, Child, Preschool, Female, Genetic Association Studies methods, Genetic Variation genetics, Genotype, Humans, Infant, Infant, Newborn, Male, Phenotype, Seizures genetics, Spasms, Infantile genetics, Young Adult, Action Potentials genetics, Epilepsy genetics, NAV1.2 Voltage-Gated Sodium Channel genetics

Abstract

De novo variants in SCN2A developmental and epileptic encephalopathy (DEE) show distinctive genotype-phenotype correlations. The two most recurrent SCN2A variants in DEE, R1882Q and R853Q, are associated with different ages and seizure types at onset. R1882Q presents on day 1 of life with focal seizures, while infantile spasms is the dominant seizure type seen in R853Q cases, presenting at a median age of 8 months. Voltage clamp, which characterizes the functional properties of ion channels, predicted gain-of-function for R1882Q and loss-of-function for R853Q. Dynamic action potential clamp, that we implement here as a method for modeling neurophysiological consequences of a given epilepsy variant, predicted that the R1882Q variant would cause a dramatic increase in firing, whereas the R853Q variant would cause a marked reduction in action potential firing. Dynamic clamp was also able to functionally separate the L1563V variant, seen in benign familial neonatal-infantile seizures from R1882Q, seen in DEE, suggesting a diagnostic potential for this type of analysis. Overall, the study shows a strong correlation between clinical phenotype, SCN2A genotype, and functional modeling. Dynamic clamp is well positioned to impact our understanding of pathomechanisms and for development of disease mechanism-targeted therapies in genetic epilepsy., Competing Interests: Conflict of interest statement: G.B. is funded by RogCon, Inc., Miami, Florida, a biotechnology company focused on drug research, discovery, and development for select ion channelopathies, including SCN2A. I.E.S. has served on scientific advisory boards for UCB, Eisai, GlaxoSmithKline, Biomarin, and Nutricia; editorial boards of the Annals of Neurology, Neurology and Epileptic Disorders; may accrue future revenue on pending patent WO61/010176 (filed: 2008): Therapeutic Compound; has received speaker honoraria from GlaxoSmithKline, Athena Diagnostics, UCB, Eisai, and Transgenomics; has received funding for travel from Athena Diagnostics, UCB, Biocodex, GlaxoSmithKline, Biomarin, and Eisai; and receives/has received research support from the National Health and Medical Research Council of Australia, National Institutes of Health, Australian Research Council, Health Research Council of New Zealand, CURE, The American Epilepsy Society, the US Department of Defense Autism Spectrum Disorder Research Program, March of Dimes, and Perpetual Charitable Trustees. S.P. is cofounder, Chief Scientific Officer, and equity holder of RogCon, Inc., Miami, Florida, a biotech company focused on the delivery of novel therapeutics for SCN2A disorders. RogCon, Inc. provided funding for this project. S.P. is also cofounder and equity holder in Praxis Precision Medicines, Inc., Cambridge, Massachusetts, which develops precision medicines for neurogenetic disorders, including those caused by SCN2A mutations. S.P. is a Scientific Advisor and equity holder in Pairnomix, Inc., Minneaopolis, Minnisota, which is undertaking precision medicine development in epilepsy and related disorders.

Published

2018

124. The finding of a new heterozygous mutation site of the SCN2A gene in a monozygotic twin family carrying and exhibiting genetic epilepsy with febrile seizures plus (GEFS+) using targeted next-generation sequencing.

Author

Liu XW, Li W, Han T, Wei K, Qiao S, Su L, and Chi Z

Subjects

Amino Acid Sequence, Child, Preschool, Epilepsy, Generalized diagnosis, Heterozygote, Humans, Male, Seizures, Febrile diagnosis, Epilepsy, Generalized genetics, Mutation genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, Seizures, Febrile genetics, Twins, Monozygotic genetics, Exome Sequencing methods

Abstract

Objectives: Generalized epilepsy with febrile seizures plus (GEFS+) is a new epilepsy syndrome named by the International League Against Epilepsy (ILAE) in 2001. The SCN2A gene encoding α2 subunit of the neuronal sodium channel has been reported to be associated with BFNIS, GFES+, Dravet syndrome and some intractable childhood epilepsies. This study aimed to develop an approach based on next-generation sequencing to determine the genetic defects in a monozygotic twin family with GEFS+., Patients and Methods: We collected a twin family with GEFS+. The DNA of the twin patients was extracted from their peripheral venous whole blood. A total of 308 known genes related to epilepsies were selected for deep exon resequencing. The patients family's DNA was sequenced through Sanger's sequencing for expanded validation. Through systematic data analysis using established bioinformatics pipeline and segregation analysis techniques, a number of genetic variants were released., Results: Through detailed data analysis, we found a new heterozygous mutation c.1399G > A on exon11 of SCN2A (Nav1.2) which has not been reported in the HGMD (Human Gene Mutation Database), in the twin patients. Then we tested and verified the presence of the same mutation site in all individuals of the family. Asymptomatic individuals of this family didn't show this mutation., Conclusion: The methodology provides a reliable strategy for routine gene diagnosis of GEFS+. This observation of a potentially pathogenic mutation of SCN2A (Nav1.2) indicates that this gene should be further evaluated in order to determine possible routes of causation of GEFS+., (Copyright © 2017. Published by Elsevier B.V.)

Published

2018

125. Integration of biological/pathophysiological contexts to help clarify genotype-phenotype mismatches in monogenetic diseases. Childhood epilepsies associated with SCN2A as a case study.

Author

Winquist RJ and Cohen CJ

Subjects

Genetic Association Studies, Genotype, Humans, Mutation, Missense, Phenotype, Spasms, Infantile etiology, Mutation, NAV1.2 Voltage-Gated Sodium Channel genetics, Severity of Illness Index, Spasms, Infantile genetics

Abstract

Monogenetic diseases offer clear human validation for launching drug discovery programs in Pharma designed to develop important new medicines for unmet medical needs. However, mismatches in the genotype-phenotype of presenting patients complicate both the preclinical 'research target profile' and the clinical development strategy. Additional biological and pathophysiological data associated with the identified mutations are necessary for more optimal prosecution of these drug discovery programs. This added contextual setting goes beyond identification of modifier genes and needs to encompass microenvironmental factors which can differentially affect the phenotype of patients harboring the same mutation. The Early Infantile Epileptic Encephalopathies (EIEEs) associated with de novo mutations in voltage gated sodium channels are interesting case studies that include examples of genotype-phenotype mismatches. With EIEE11, associated with mutations in SCN2A, incorporation of biological/pathophysiological contexts are helpful in clarifying the apparent genotype-phenotype mismatches which are captured with more reductionist approaches., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

126. FOXD3 inhibits SCN2A gene transcription in intractable epilepsy cell models.

Author

Xiang J, Wen F, Zhang L, and Zhou Y

Subjects

Analysis of Variance, Animals, Animals, Newborn, Cells, Cultured, Chromatin Immunoprecipitation, Forkhead Transcription Factors genetics, Gene Deletion, Gene Expression Regulation drug effects, Hippocampus cytology, NAV1.2 Voltage-Gated Sodium Channel metabolism, Neurons drug effects, Oxidoreductases metabolism, RNA, Messenger metabolism, RNA, Small Interfering genetics, RNA, Small Interfering metabolism, Rats, Rats, Sprague-Dawley, Repressor Proteins genetics, Transcription Factors metabolism, Transfection, Forkhead Transcription Factors metabolism, Gene Expression Regulation genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, Neurons metabolism, Repressor Proteins metabolism

Abstract

The expression of sodium voltage-gated channel alpha subunit 2 (SCN2A) is closely related to the development of epilepsy. This study investigated regulatory element of the SCN2A gene involved in epilepsy. An intractable epilepsy cell model was constructed using hippocampal primary neurons and the SH-SY5Y cell line. SCN2A protein and gene expression in cells as well as the level of lactic acid dehydrogenase (LDH) in the cell culture supernatants was detected. Potential regulatory factors of SCN2A and its upstream regulatory elements were identified using the dual-luciferase reporter assay. Finally, the role of the hypothetical transcription factor in epilepsy was examined by using its small interfering RNA (siRNA). Results found that levels of LDH and expression of the hypothetical transcription factor, Forkhead box D3 (FOXD3), was both increased in the model cells, whereas that of SCN2A was decreased. The results of dual-luciferase reporter assays revealed that an upstream region of SCN2A gene spanning from nucleotides -1617 to -1470 was a transcription factor binding region and a trans-acting factor role of FOXD3 was identified in the core region (GGCAAAATTAT). Then the FOXD3 binding site was further verified by the chromatin immunoprecipitation (ChIP) assay and electrophoretic mobility shift assay (EMSA). After SH-SY5Y cells were transfected with FOXD3 siRNA, the release of LDH into culture supernatants and the LDH expression levels in cells were significantly decreased. SCN2A expression in model cells was increased by knockdown of FOXD3. Therefore, this study demonstrated that FOXD3 is a trans-acting factor of SCN2A, and this mechanism may play a role in cell injury after epilepsy., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2018

127. Genetic analysis of benign familial epilepsies in the first year of life in a Chinese cohort.

Author

Zeng Q, Yang X, Zhang J, Liu A, Yang Z, Liu X, Wu Y, Wu X, Wei L, and Zhang Y

Subjects

Asian People, China, Female, Humans, Infant, Infant, Newborn, Male, Epilepsy, Benign Neonatal genetics, Genetic Testing, KCNQ2 Potassium Channel genetics, Membrane Proteins genetics, Mutation, NAV1.2 Voltage-Gated Sodium Channel genetics, Nerve Tissue Proteins genetics, Receptors, GABA-A genetics

Abstract

Benign familial epilepsies that present themselves in the first year of life include benign familial neonatal epilepsy (BFNE), benign familial neonatal-infantile epilepsy (BFNIE) and benign familial infantile epilepsy (BFIE). We used Sanger sequencing and targeted next-generation sequencing to detect gene mutations in a Chinese cohort of patients with these three disorders. A total of 79 families were collected, including 4 BFNE, 7 BFNIE, and 68 BFIE. Genetic testing led to the identification of gene mutations in 60 families (60 out of 79, 75.9%). A total of 42 families had PRRT2 mutations, 9 had KCNQ2 mutations, 8 had SCN2A mutations, and 1 had a GABRA6 mutation. In total three of four BFNE families were detected with KCNQ2 mutations. Mutations were detected in all BFNIE families, including 3 KCNQ2 mutations, 3 SCN2A mutations, and 1 PRRT2 mutation. Gene mutations were identified in 50 out of 68 BFIE families (73.5%), including 41 PRRT2 mutations (41 out of 68, 60.3%), 5 SCN2A mutations, 3 KCNQ2 mutations, and 1 GABRA6 mutation. Our results confirmed that mutations in KCNQ2, SCN2A, and PRRT2 are major genetic causes of benign familial epilepsy in the first year of life in the Chinese population. KCNQ2 is the major gene related to BFNE. PRRT2 is the main gene responsible for BFIE.

Published

2018

128. In utero seizures revealing dentato-olivary dysplasia caused by SCN2A mutation.

Author

Sauvestre F, Moutton S, Badens C, Broussin B, Carles D, Houcinat N, Lacoste C, Marguet F, Pecheux C, Villard L, Pelluard F, Laquerrière A, and André G

Subjects

Adult, Female, Humans, Seizures pathology, Genetic Predisposition to Disease, Mutation genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, Seizures genetics

Published

2017

129. A case-control collapsing analysis identifies epilepsy genes implicated in trio sequencing studies focused on de novo mutations.

Author

Zhu X, Padmanabhan R, Copeland B, Bridgers J, Ren Z, Kamalakaran S, O'Driscoll-Collins A, Berkovic SF, Scheffer IE, Poduri A, Mei D, Guerrini R, Lowenstein DH, Allen AS, Heinzen EL, and Goldstein DB

Subjects

Case-Control Studies, DNA Mutational Analysis, Female, Genes, Dominant, Genome-Wide Association Study, Humans, Male, Munc18 Proteins genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, Nerve Tissue Proteins genetics, Potassium Channels genetics, Potassium Channels, Sodium-Activated, Exome Sequencing, Epilepsy genetics, Mutation

Abstract

Trio exome sequencing has been successful in identifying genes with de novo mutations (DNMs) causing epileptic encephalopathy (EE) and other neurodevelopmental disorders. Here, we evaluate how well a case-control collapsing analysis recovers genes causing dominant forms of EE originally implicated by DNM analysis. We performed a genome-wide search for an enrichment of "qualifying variants" in protein-coding genes in 488 unrelated cases compared to 12,151 unrelated controls. These "qualifying variants" were selected to be extremely rare variants predicted to functionally impact the protein to enrich for likely pathogenic variants. Despite modest sample size, three known EE genes (KCNT1, SCN2A, and STXBP1) achieved genome-wide significance (p<2.68×10-6). In addition, six of the 10 most significantly associated genes are known EE genes, and the majority of the known EE genes (17 out of 25) originally implicated in trio sequencing are nominally significant (p<0.05), a proportion significantly higher than the expected (Fisher's exact p = 2.33×10-17). Our results indicate that a case-control collapsing analysis can identify several of the EE genes originally implicated in trio sequencing studies, and clearly show that additional genes would be implicated with larger sample sizes. The case-control analysis not only makes discovery easier and more economical in early onset disorders, particularly when large cohorts are available, but also supports the use of this approach to identify genes in diseases that present later in life when parents are not readily available.

Published

2017

130. Dravet syndrome and its mimics: Beyond SCN1A.

Author

Steel D, Symonds JD, Zuberi SM, and Brunklaus A

Subjects

Humans, NAV1.2 Voltage-Gated Sodium Channel genetics, NAV1.6 Voltage-Gated Sodium Channel genetics, Phenotype, Receptors, GABA-A genetics, Epilepsies, Myoclonic diagnosis, Epilepsies, Myoclonic genetics, Mutation genetics, NAV1.1 Voltage-Gated Sodium Channel genetics

Abstract

Objective: Dravet syndrome (DS) is a severe developmental and epileptic encephalopathy characterized by the onset of prolonged febrile and afebrile seizures in infancy, and evolving to drug-resistant epilepsy with accompanying cognitive, behavioral, and motor impairment. Most cases are now known to be caused by pathogenic variants in the sodium channel gene SCN1A, but several other genes have also been implicated. This review examines current understanding of the role of non-SCN1A genes in DS, and what is known about phenotypic similarities and differences. We discuss whether these are best thought of as minority causes of DS, or as similar but distinct conditions., Methods: Based on a review of literature, a list of genes linked to DS was compiled and PubMed was searched for reports of DS-like phenotypes arising from variants in each. Online Mendelian Inheritance in Man (OMIM) was used to identify further reports relevant to each gene., Results: Genes that have been reported to cause DS-like phenotypes include SCN2A, SCN8A, SCN9A, SCN1B, PCDH19, GABRA1, GABRG2, STXBP1, HCN1, CHD2, and KCNA2. Many of these genes, however, appear to be associated with their own, different, clinical picture. Other candidate genes for DS have been reported, but there is currently an insufficient body of literature to support their causative role., Significance: Although most cases of DS arise from SCN1A variants, numerous other genes cause encephalopathies that are clinically similar. Increasingly, a tendency is noted to define newly described epileptic disorders primarily in genetic terms, with clinical features being linked to genotypes. As genetic diagnosis becomes more readily available, its potential to guide pathophysiologic understanding and therapeutic strategy cannot be ignored. Clinical assessment remains essential; the challenge now is to develop a gene-based taxonomy that complements traditional syndromic classifications, allowing elements of both to inform new approaches to treatment., (Wiley Periodicals, Inc. © 2017 International League Against Epilepsy.)

Published

2017

131. Identification of crucial miRNAs and the targets in renal cortex of hypertensive patients by expression profiles.

Author

Wang G, Wu L, Chen Z, and Sun J

Subjects

Down-Regulation, Gene Expression Profiling, Humans, Male, Microarray Analysis, Up-Regulation, Collagen Type XII genetics, Extracellular Matrix Proteins genetics, Hypertension genetics, Kidney Cortex metabolism, MicroRNAs genetics, NAV1.2 Voltage-Gated Sodium Channel genetics

Abstract

Backgrounds: Defect in kidney is one major reason of hypertension. The study aimed ao uncovering the regulatory mechanisms of miRNAs and the targets in hypertensive kidney., Methods: Gene expression profile of GSE28345 and miRNA expression profile of GSE28283 were downloaded from GEO database. After data preprocessing, differently expressed genes (DEGs) and miRNAs (DE-miRs) were identified using limma package. Then targets of miRNAs were predicted according to information in relevant databases. Function and pathway enrichment analyses were performed for DEGs using DAVID software. Furthermore, protein-protein interaction (PPI) networks were constructed for up- and down-regulated genes, respectively, using the Cytoscape. Additionally, for down-regulated DEGs, the integrated regulatory network was established combining PPI network with the miRNA-mRNA interactions., Results: As a result, 285 DEGs were identified, including 177 up-regulated and 108 down-regulated genes. Combined with the predicted targets of miRNAs, 22 up-regulated DE-miRs were identified. In the integrated network for down-regulated DEGs, three crucial nodes were identified as ASPN, COL12A1, and SCN2A. ASPN was predicted as target of miR-21 and miR-374b, and COL12A1 was the target of miR-30e, miR-21, and miR-195, while SCN2A was the target of miR-30e, miR-374b, and miR-195. Notably, COL12A1 and ASPN were linked with each other in the network., Conclusion: Three crucial genes were identified in hypertensive kidney, such as COL12A1, ASPN, and SCN2A. ASPN might co-function with COL12A1, and they both might be the targets of miR-21. SCN2A might be a novel target of miR-30e and miR-374b. However, more experiments are needed to validate these results.

Published

2017

132. The therapeutic implication of a novel SCN2A mutation associated early-onset epileptic encephalopathy with Rett-like features.

Author

Liang JS, Lin LJ, Yang MT, Wang JS, and Lu JF

Subjects

Child, Epilepsy physiopathology, Female, High-Throughput Nucleotide Sequencing, Humans, Intellectual Disability drug therapy, Mutation, Mutation, Missense genetics, Phenotype, Rett Syndrome genetics, Rett Syndrome metabolism, Seizures drug therapy, Seizures, Febrile drug therapy, Spasms, Infantile metabolism, NAV1.2 Voltage-Gated Sodium Channel genetics, NAV1.2 Voltage-Gated Sodium Channel metabolism, Spasms, Infantile genetics

Abstract

Epileptic encephalopathies are highly heterogeneous and phenotypical disorders with different underlying genetic defects. Mutations in the SCN2A gene cause different epilepsy syndromes, including epilepsy of infancy with migrating focal seizures, Ohtahara syndrome, and West syndrome. We utilized a targeted next generation sequencing (NGS) approach on a girl with early-onset seizures and Rett-like features, including autistic behavior, limited hand function with chorea, and profound intellectual disability, to identify novel missense mutation (c.1270G>A; p.V424M) in the SCN2A gene, which encodes the αII-subunit of the voltage-gated Na + channel (Na v 1.2). The identified SCN2A mutation responsible for the development of the disease is confirmed to be de novo for the proband. Our findings broaden the clinical spectrum of SCN2A mutations, which resembles clinical phenotypes of SCN1A mutations by manifesting as fever sensitive seizures, and highlights that SCN2A mutations are an important cause of early-onset epileptic encephalopathies with movement disorders. In addition, the use of levetiracetam to treat SCN2A epileptic encephalopathy, when Na + channel-blocking anticonvulsants are ineffective, is also recommended., (Copyright © 2017 The Japanese Society of Child Neurology. Published by Elsevier B.V. All rights reserved.)

Published

2017

133. Characterization of the axon initial segment of mice substantia nigra dopaminergic neurons.

Author

González-Cabrera C, Meza R, Ulloa L, Merino-Sepúlveda P, Luco V, Sanhueza A, Oñate-Ponce A, Bolam JP, and Henny P

Subjects

Action Potentials physiology, Animals, Ankyrins metabolism, Ankyrins ultrastructure, Axon Initial Segment ultrastructure, Gene Expression physiology, Imaging, Three-Dimensional, Male, Mice, Mice, Inbred C57BL, Microscopy, Electron, Transmission, Microscopy, Immunoelectron, NAV1.2 Voltage-Gated Sodium Channel genetics, NAV1.2 Voltage-Gated Sodium Channel metabolism, NAV1.2 Voltage-Gated Sodium Channel ultrastructure, NAV1.6 Voltage-Gated Sodium Channel genetics, NAV1.6 Voltage-Gated Sodium Channel metabolism, NAV1.6 Voltage-Gated Sodium Channel ultrastructure, Neuroimaging, RNA, Messenger metabolism, Tyrosine 3-Monooxygenase metabolism, Tyrosine 3-Monooxygenase ultrastructure, Axon Initial Segment physiology, Dopaminergic Neurons cytology, Substantia Nigra cytology

Abstract

The axon initial segment (AIS) is the site of initiation of action potentials and influences action potential waveform, firing pattern, and rate. In view of the fundamental aspects of motor function and behavior that depend on the firing of substantia nigra pars compacta (SNc) dopaminergic neurons, we identified and characterized their AIS in the mouse. Immunostaining for tyrosine hydroxylase (TH), sodium channels (Na v ) and ankyrin-G (Ank-G) was used to visualize the AIS of dopaminergic neurons. Reconstructions of sampled AIS of dopaminergic neurons revealed variable lengths (12-60 μm) and diameters (0.2-0.8 μm), and an average of 50% reduction in diameter between their widest and thinnest parts. Ultrastructural analysis revealed submembranous localization of Ank-G at nodes of Ranvier and AIS. Serial ultrathin section analysis and 3D reconstructions revealed that Ank-G colocalized with TH only at the AIS. Few cases of synaptic innervation of the AIS of dopaminergic neurons were observed. mRNA in situ hybridization of brain-specific Na v subunits revealed the expression of Na v 1.2 by most SNc neurons and a small proportion expressing Na v 1.6. The presence of sodium channels, along with the submembranous location of Ank-G is consistent with the role of AIS in action potential generation. Differences in the size of the AIS likely underlie differences in firing pattern, while the tapering diameter of AIS may define a trigger zone for action potentials. Finally, the conspicuous expression of Na v 1.2 by the majority of dopaminergic neurons may explain their high threshold for firing and their low discharge rate., (© 2017 Wiley Periodicals, Inc.)

Published

2017

134. Oligodendroglial excitability mediated by glutamatergic inputs and Nav1.2 activation.

Author

Berret E, Barron T, Xu J, Debner E, Kim EJ, and Kim JH

Subjects

Action Potentials, Animals, Axons metabolism, Myelin Sheath genetics, Myelin Sheath metabolism, NAV1.2 Voltage-Gated Sodium Channel genetics, Neurons metabolism, Rats, Rats, Sprague-Dawley, Glutamic Acid metabolism, NAV1.2 Voltage-Gated Sodium Channel metabolism, Oligodendroglia metabolism

Abstract

Oligodendrocyte (OL) maturation and axon-glial communication are required for proper myelination in the developing brain. However, physiological properties of OLs remain largely uncharacterized in different brain regions. The roles of oligodendroglial voltage-activated Na + channels (Na v ) and electrical excitability in relation to maturation to the myelinating stage are controversial, although oligodendroglial excitability is potentially important for promoting axon myelination. Here we show spiking properties of OLs and their role in axon-glial communication in the auditory brainstem. A subpopulation of pre-myelinating OLs (pre-OLs) can generate Na v 1.2-driven action potentials throughout postnatal development to early adulthood. In addition, excitable pre-OLs receive glutamatergic inputs from neighboring neurons that trigger pre-OL spikes. Knockdown of Na v 1.2 channels in pre-OLs alters their morphology, reduces axon-OL interactions and impairs myelination. Our results suggest that Na v 1.2-driven spiking of pre-OLs is an integral component of axon-glial communication and is required for the function and maturation of OLs to promote myelination.Axon-glial communication is important for myelination. Here the authors show that during postnatal development in rats, a subpopulation of pre-myelinating oligodendrocytes in the auditory brainstem receive excitatory inputs and can generate Na v 1.2-driven action potentials, and that such process promotes myelination.

Published

2017

135. Opposing Effects on Na V 1.2 Function Underlie Differences Between SCN2A Variants Observed in Individuals With Autism Spectrum Disorder or Infantile Seizures.

Author

Ben-Shalom R, Keeshen CM, Berrios KN, An JY, Sanders SJ, and Bender KJ

Subjects

Cerebral Cortex metabolism, Computer Simulation, Genetic Predisposition to Disease, HEK293 Cells, Humans, Immunohistochemistry, Infant, Membrane Potentials physiology, Models, Neurological, Mutation, NAV1.2 Voltage-Gated Sodium Channel metabolism, Patch-Clamp Techniques, Pyramidal Cells cytology, Pyramidal Cells metabolism, Seizures genetics, Seizures metabolism, Autism Spectrum Disorder genetics, Autism Spectrum Disorder metabolism, Epilepsy, Benign Neonatal genetics, Epilepsy, Benign Neonatal metabolism, NAV1.2 Voltage-Gated Sodium Channel genetics, Spasms, Infantile genetics, Spasms, Infantile metabolism

Abstract

Background: Variants in the SCN2A gene that disrupt the encoded neuronal sodium channel Na V 1.2 are important risk factors for autism spectrum disorder (ASD), developmental delay, and infantile seizures. Variants observed in infantile seizures are predominantly missense, leading to a gain of function and increased neuronal excitability. How variants associated with ASD affect Na V 1.2 function and neuronal excitability are unclear., Methods: We examined the properties of 11 ASD-associated SCN2A variants in heterologous expression systems using whole-cell voltage-clamp electrophysiology and immunohistochemistry. Resultant data were incorporated into computational models of developing and mature cortical pyramidal cells that express Na V 1.2., Results: In contrast to gain of function variants that contribute to seizure, we found that all ASD-associated variants dampened or eliminated channel function. Incorporating these electrophysiological results into a compartmental model of developing excitatory neurons demonstrated that all ASD variants, regardless of their mechanism of action, resulted in deficits in neuronal excitability. Corresponding analysis of mature neurons predicted minimal change in neuronal excitability., Conclusions: This functional characterization thus identifies SCN2A mutation and Na V 1.2 dysfunction as the most frequently observed ASD risk factor detectable by exome sequencing and suggests that associated changes in neuronal excitability, particularly in developing neurons, may contribute to ASD etiology., (Copyright © 2017 Society of Biological Psychiatry. Published by Elsevier Inc. All rights reserved.)

Published

2017

136. High-throughput electrophysiological assays for voltage gated ion channels using SyncroPatch 768PE.

Author

Li T, Lu G, Chiang EY, Chernov-Rogan T, Grogan JL, and Chen J

Subjects

Animals, CHO Cells, Cricetulus, Drug Evaluation, Preclinical, Gene Expression, High-Throughput Screening Assays instrumentation, Kv1.3 Potassium Channel deficiency, Kv1.3 Potassium Channel genetics, NAV1.1 Voltage-Gated Sodium Channel genetics, NAV1.1 Voltage-Gated Sodium Channel metabolism, NAV1.2 Voltage-Gated Sodium Channel genetics, NAV1.2 Voltage-Gated Sodium Channel metabolism, NAV1.3 Voltage-Gated Sodium Channel genetics, NAV1.3 Voltage-Gated Sodium Channel metabolism, NAV1.4 Voltage-Gated Sodium Channel genetics, NAV1.4 Voltage-Gated Sodium Channel metabolism, NAV1.5 Voltage-Gated Sodium Channel genetics, NAV1.5 Voltage-Gated Sodium Channel metabolism, NAV1.6 Voltage-Gated Sodium Channel genetics, NAV1.6 Voltage-Gated Sodium Channel metabolism, NAV1.7 Voltage-Gated Sodium Channel genetics, Patch-Clamp Techniques instrumentation, Primary Cell Culture, Rats, Sodium Channels genetics, Sodium Channels metabolism, T-Lymphocytes cytology, T-Lymphocytes drug effects, T-Lymphocytes metabolism, Transgenes, High-Throughput Screening Assays methods, Membrane Potentials physiology, NAV1.7 Voltage-Gated Sodium Channel metabolism, Patch-Clamp Techniques methods, Potassium Channel Blockers pharmacology, Sodium Channel Blockers pharmacology

Abstract

Ion channels regulate a variety of physiological processes and represent an important class of drug target. Among the many methods of studying ion channel function, patch clamp electrophysiology is considered the gold standard by providing the ultimate precision and flexibility. However, its utility in ion channel drug discovery is impeded by low throughput. Additionally, characterization of endogenous ion channels in primary cells remains technical challenging. In recent years, many automated patch clamp (APC) platforms have been developed to overcome these challenges, albeit with varying throughput, data quality and success rate. In this study, we utilized SyncroPatch 768PE, one of the latest generation APC platforms which conducts parallel recording from two-384 modules with giga-seal data quality, to push these 2 boundaries. By optimizing various cell patching parameters and a two-step voltage protocol, we developed a high throughput APC assay for the voltage-gated sodium channel Nav1.7. By testing a group of Nav1.7 reference compounds' IC50, this assay was proved to be highly consistent with manual patch clamp (R > 0.9). In a pilot screening of 10,000 compounds, the success rate, defined by > 500 MΩ seal resistance and >500 pA peak current, was 79%. The assay was robust with daily throughput ~ 6,000 data points and Z' factor 0.72. Using the same platform, we also successfully recorded endogenous voltage-gated potassium channel Kv1.3 in primary T cells. Together, our data suggest that SyncroPatch 768PE provides a powerful platform for ion channel research and drug discovery.

Published

2017

137. Comparison and optimization of in silico algorithms for predicting the pathogenicity of sodium channel variants in epilepsy.

Author

Holland KD, Bouley TM, and Horn PS

Subjects

DNA Mutational Analysis, Databases, Genetic, Genetic Predisposition to Disease genetics, Humans, Infant, Phenotype, Predictive Value of Tests, Algorithms, Computer Simulation, Epilepsy genetics, Epilepsy physiopathology, Genetic Variation genetics, Mutation, Missense genetics, NAV1.1 Voltage-Gated Sodium Channel genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, NAV1.6 Voltage-Gated Sodium Channel genetics, Sodium Channels genetics

Abstract

Objective: Variants in neuronal voltage-gated sodium channel α-subunits genes SCN1A, SCN2A, and SCN8A are common in early onset epileptic encephalopathies and other autosomal dominant childhood epilepsy syndromes. However, in clinical practice, missense variants are often classified as variants of uncertain significance when missense variants are identified but heritability cannot be determined. Genetic testing reports often include results of computational tests to estimate pathogenicity and the frequency of that variant in population-based databases. The objective of this work was to enhance clinicians' understanding of results by (1) determining how effectively computational algorithms predict epileptogenicity of sodium channel (SCN) missense variants; (2) optimizing their predictive capabilities; and (3) determining if epilepsy-associated SCN variants are present in population-based databases. This will help clinicians better understand the results of indeterminate SCN test results in people with epilepsy., Methods: Pathogenic, likely pathogenic, and benign variants in SCNs were identified using databases of sodium channel variants. Benign variants were also identified from population-based databases. Eight algorithms commonly used to predict pathogenicity were compared. In addition, logistic regression was used to determine if a combination of algorithms could better predict pathogenicity., Results: Based on American College of Medical Genetic Criteria, 440 variants were classified as pathogenic or likely pathogenic and 84 were classified as benign or likely benign. Twenty-eight variants previously associated with epilepsy were present in population-based gene databases. The output provided by most computational algorithms had a high sensitivity but low specificity with an accuracy of 0.52-0.77. Accuracy could be improved by adjusting the threshold for pathogenicity. Using this adjustment, the Mendelian Clinically Applicable Pathogenicity (M-CAP) algorithm had an accuracy of 0.90 and a combination of algorithms increased the accuracy to 0.92., Significance: Potentially pathogenic variants are present in population-based sources. Most computational algorithms overestimate pathogenicity; however, a weighted combination of several algorithms increased classification accuracy to >0.90., (Wiley Periodicals, Inc. © 2017 International League Against Epilepsy.)

Published

2017

138. Scn2a deletion improves survival and brain-heart dynamics in the Kcna1-null mouse model of sudden unexpected death in epilepsy (SUDEP).

Author

Mishra V, Karumuri BK, Gautier NM, Liu R, Hutson TN, Vanhoof-Villalba SL, Vlachos I, Iasemidis L, and Glasscock E

Subjects

Animals, Biomarkers, Brain physiopathology, Death, Sudden, Disease Models, Animal, Electrocardiography, Electroencephalography, Epilepsy complications, Genotype, Heart physiopathology, Heart Rate, Kv1.1 Potassium Channel genetics, Kv1.1 Potassium Channel metabolism, Mice, Mice, Knockout, Seizures genetics, Epilepsy genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, NAV1.2 Voltage-Gated Sodium Channel metabolism

Abstract

People with epilepsy have greatly increased probability of premature mortality due to sudden unexpected death in epilepsy (SUDEP). Identifying which patients are most at risk of SUDEP is hindered by a complex genetic etiology, incomplete understanding of the underlying pathophysiology and lack of prognostic biomarkers. Here we evaluated heterozygous Scn2a gene deletion (Scn2a+/-) as a protective genetic modifier in the Kcna1 knockout mouse (Kcna1-/-) model of SUDEP, while searching for biomarkers of SUDEP risk embedded in electroencephalography (EEG) and electrocardiography (ECG) recordings. The human epilepsy gene Kcna1 encodes voltage-gated Kv1.1 potassium channels that act to dampen neuronal excitability whereas Scn2a encodes voltage-gated Nav1.2 sodium channels important for action potential initiation and conduction. SUDEP-prone Kcna1-/- mice with partial genetic ablation of Nav1.2 channels (i.e. Scn2a+/-; Kcna1-/-) exhibited a two-fold increase in survival. Classical analysis of EEG and ECG recordings separately showed significantly decreased seizure durations in Scn2a+/-; Kcna1-/- mice compared with Kcna1-/- mice, without substantial modification of cardiac abnormalities. Novel analysis of the EEG and ECG together revealed a significant reduction in EEG-ECG association in Kcna1-/- mice compared with wild types, which was partially restored in Scn2a+/-; Kcna1-/- mice. The degree of EEG-ECG association was also proportional to the survival rate of mice across genotypes. These results show that Scn2a gene deletion acts as protective genetic modifier of SUDEP and suggest measures of brain-heart association as potential indices of SUDEP susceptibility., (© The Author 2017. Published by Oxford University Press. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2017

139. Unusual association of SCN2A epileptic encephalopathy with severe cortical dysplasia detected by prenatal MRI.

Author

Bernardo S, Marchionni E, Prudente S, De Liso P, Spalice A, Giancotti A, Manganaro L, and Pizzuti A

Subjects

Adult, Brain Diseases complications, Carbamazepine therapeutic use, Female, Humans, Infant, Newborn, Infant, Premature, Magnetic Resonance Imaging, Male, Malformations of Cortical Development complications, Malformations of Cortical Development drug therapy, Malformations of Cortical Development genetics, Mutation, Neuroimaging, Phenotype, Seizures complications, Brain Diseases drug therapy, Brain Diseases genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, Seizures drug therapy, Seizures genetics

Abstract

We present an atypical association of SCN2A epileptic encephalopathy with severe cortical dysplasia. SCN2A mutations are associated with epileptic syndromes from benign to extremely severe in absence of such macroscopic brain findings. Prenatal MRI (Magnetic Resonance Imaging) in a 32 weeks fetus, with US (Ultrasonography) diagnosis of isolated ventriculomegaly showed CNS (Central Nervous System) dysplasia characterized by lack of differentiation between cortical and subcortical layers, pachygyria and corpus callosum dysgenesis. Postnatal MRI confirmed the prenatal findings. On day 6 the baby presented a focal status epilepticus, partially controlled by phenobarbital, phenytoin, and levetiracetam. After three weeks a moderate improvement in seizure control has been achieved with carbamazepine. Exome sequencing detected a de novo heterozygous mutation in the SCN2A gene, encoding the α II -subunit of a sodium channel. The patient findings expand the phenotype spectrum of SCN2A mutations to epileptic encephalopathies with macroscopic brain developmental features., (Copyright © 2017 European Paediatric Neurology Society. Published by Elsevier Ltd. All rights reserved.)

Published

2017

140. Genetic and phenotypic heterogeneity suggest therapeutic implications in SCN2A-related disorders.

Author

Wolff M, Johannesen KM, Hedrich UBS, Masnada S, Rubboli G, Gardella E, Lesca G, Ville D, Milh M, Villard L, Afenjar A, Chantot-Bastaraud S, Mignot C, Lardennois C, Nava C, Schwarz N, Gérard M, Perrin L, Doummar D, Auvin S, Miranda MJ, Hempel M, Brilstra E, Knoers N, Verbeek N, van Kempen M, Braun KP, Mancini G, Biskup S, Hörtnagel K, Döcker M, Bast T, Loddenkemper T, Wong-Kisiel L, Baumeister FM, Fazeli W, Striano P, Dilena R, Fontana E, Zara F, Kurlemann G, Klepper J, Thoene JG, Arndt DH, Deconinck N, Schmitt-Mechelke T, Maier O, Muhle H, Wical B, Finetti C, Brückner R, Pietz J, Golla G, Jillella D, Linnet KM, Charles P, Moog U, Õiglane-Shlik E, Mantovani JF, Park K, Deprez M, Lederer D, Mary S, Scalais E, Selim L, Van Coster R, Lagae L, Nikanorova M, Hjalgrim H, Korenke GC, Trivisano M, Specchio N, Ceulemans B, Dorn T, Helbig KL, Hardies K, Stamberger H, de Jonghe P, Weckhuysen S, Lemke JR, Krägeloh-Mann I, Helbig I, Kluger G, Lerche H, and Møller RS

Subjects

Adolescent, Adult, Age of Onset, Child, Child, Preschool, Denmark epidemiology, Epilepsy epidemiology, Female, Humans, Infant, Male, Mutation, Phenotype, Young Adult, Epilepsy drug therapy, Epilepsy genetics, Epilepsy physiopathology, NAV1.2 Voltage-Gated Sodium Channel genetics, NAV1.2 Voltage-Gated Sodium Channel physiology, Neurodevelopmental Disorders genetics, Sodium Channel Blockers therapeutic use

Abstract

Mutations in SCN2A, a gene encoding the voltage-gated sodium channel Nav1.2, have been associated with a spectrum of epilepsies and neurodevelopmental disorders. Here, we report the phenotypes of 71 patients and review 130 previously reported patients. We found that (i) encephalopathies with infantile/childhood onset epilepsies (≥3 months of age) occur almost as often as those with an early infantile onset (<3 months), and are thus more frequent than previously reported; (ii) distinct phenotypes can be seen within the late onset group, including myoclonic-atonic epilepsy (two patients), Lennox-Gastaut not emerging from West syndrome (two patients), and focal epilepsies with an electrical status epilepticus during slow sleep-like EEG pattern (six patients); and (iii) West syndrome constitutes a common phenotype with a major recurring mutation (p.Arg853Gln: two new and four previously reported children). Other known phenotypes include Ohtahara syndrome, epilepsy of infancy with migrating focal seizures, and intellectual disability or autism without epilepsy. To assess the response to antiepileptic therapy, we retrospectively reviewed the treatment regimen and the course of the epilepsy in 66 patients for which well-documented medical information was available. We find that the use of sodium channel blockers was often associated with clinically relevant seizure reduction or seizure freedom in children with early infantile epilepsies (<3 months), whereas other antiepileptic drugs were less effective. In contrast, sodium channel blockers were rarely effective in epilepsies with later onset (≥3 months) and sometimes induced seizure worsening. Regarding the genetic findings, truncating mutations were exclusively seen in patients with late onset epilepsies and lack of response to sodium channel blockers. Functional characterization of four selected missense mutations using whole cell patch-clamping in tsA201 cells-together with data from the literature-suggest that mutations associated with early infantile epilepsy result in increased sodium channel activity with gain-of-function, characterized by slowing of fast inactivation, acceleration of its recovery or increased persistent sodium current. Further, a good response to sodium channel blockers clinically was found to be associated with a relatively small gain-of-function. In contrast, mutations in patients with late-onset forms and an insufficient response to sodium channel blockers were associated with loss-of-function effects, including a depolarizing shift of voltage-dependent activation or a hyperpolarizing shift of channel availability (steady-state inactivation). Our clinical and experimental data suggest a correlation between age at disease onset, response to sodium channel blockers and the functional properties of mutations in children with SCN2A-related epilepsy., (© The Author (2017). Published by Oxford University Press on behalf of the Guarantors of Brain. All rights reserved. For Permissions, please email: journals.permissions@oup.com.)

Published

2017

141. Efficacy of sodium channel blockers in SCN2A early infantile epileptic encephalopathy.

Author

Dilena R, Striano P, Gennaro E, Bassi L, Olivotto S, Tadini L, Mosca F, Barbieri S, Zara F, and Fumagalli M

Subjects

Anticonvulsants therapeutic use, Brain diagnostic imaging, Brain drug effects, Brain physiopathology, Dose-Response Relationship, Drug, Humans, Infant, Newborn, Male, Spasms, Infantile diagnostic imaging, Spasms, Infantile physiopathology, Treatment Outcome, Carbamazepine therapeutic use, NAV1.2 Voltage-Gated Sodium Channel genetics, Phenytoin therapeutic use, Sodium Channel Blockers therapeutic use, Spasms, Infantile drug therapy, Spasms, Infantile genetics

Abstract

Background: Recent clinical evidence supports a targeted therapeutic approach for genetic epileptic encephalopathies based on the molecular dysfunction., Patient Description: A 2-day-old male infant presented with epileptic encephalopathy characterized by burst-suppression EEG background and tonic-clonic migrating partial seizures. The condition was refractory to phenobarbital, pyridoxine, pyridoxal phosphate and levetiracetam, but a dramatic response to an intravenous loading dose of phenytoin was documented by video-EEG monitoring. Over weeks phenytoin was successfully switched to carbamazepine to prevent seizure relapses associated with difficulty in maintaining proper blood levels of phenytoin. Genetic analysis identified a novel de novo heterozygous mutation (c.[4633A>G]p.[Met1545Val]) in SCN2A. At two years and three months of age the patient is still seizure-free on carbamazepine, although a developmental delay is evident., Conclusions: Sodium channel blockers represent the first-line treatment for confirmed or suspected SCN2A-related epileptic encephalopathies. In severe cases with compatible electro-clinical features we propose a treatment algorithm based on a test trial with high dose intravenous phenytoin followed in case of a positive response by carbamazepine, more suitable for long-term maintenance treatment. Because of their rarity, collaborative studies are needed to delineate shared therapeutic protocols for EIEE based on the electro-clinical features and the presumed underlying genetic substrate., (Copyright © 2016 The Japanese Society of Child Neurology. Published by Elsevier B.V. All rights reserved.)

Published

2017

142. CaMKII modulates sodium current in neurons from epileptic Scn2a mutant mice.

Author

Thompson CH, Hawkins NA, Kearney JA, and George AL Jr

Subjects

Animals, Epilepsy genetics, HEK293 Cells, Hippocampus metabolism, Humans, Membrane Potentials, Mice, Inbred C57BL, Mice, Inbred Strains, Mice, Transgenic, Mutation, NAV1.2 Voltage-Gated Sodium Channel genetics, Neurons metabolism, Patch-Clamp Techniques, Sodium metabolism, Calcium-Calmodulin-Dependent Protein Kinase Type 2 metabolism, Epilepsy metabolism, NAV1.2 Voltage-Gated Sodium Channel metabolism, Neurons physiology

Abstract

Monogenic epilepsies with wide-ranging clinical severity have been associated with mutations in voltage-gated sodium channel genes. In the Scn2a Q54 mouse model of epilepsy, a focal epilepsy phenotype is caused by transgenic expression of an engineered Na V 1.2 mutation displaying enhanced persistent sodium current. Seizure frequency and other phenotypic features in Scn2a Q54 mice depend on genetic background. We investigated the neurophysiological and molecular correlates of strain-dependent epilepsy severity in this model. Scn2a Q54 mice on the C57BL/6J background (B6.Q54) exhibit a mild disorder, whereas animals intercrossed with SJL/J mice (F1.Q54) have a severe phenotype. Whole-cell recording revealed that hippocampal pyramidal neurons from B6.Q54 and F1.Q54 animals exhibit spontaneous action potentials, but F1.Q54 neurons exhibited higher firing frequency and greater evoked activity compared with B6.Q54 neurons. These findings correlated with larger persistent sodium current and depolarized inactivation in neurons from F1.Q54 animals. Because calcium/calmodulin protein kinase II (CaMKII) is known to modify persistent current and channel inactivation in the heart, we investigated CaMKII as a plausible modulator of neuronal sodium channels. CaMKII activity in hippocampal protein lysates exhibited a strain-dependence in Scn2a Q54 mice with higher activity in F1.Q54 animals. Heterologously expressed Na V 1.2 channels exposed to activated CaMKII had enhanced persistent current and depolarized channel inactivation resembling the properties of F1.Q54 neuronal sodium channels. By contrast, inhibition of CaMKII attenuated persistent current, evoked a hyperpolarized channel inactivation, and suppressed neuronal excitability. We conclude that CaMKII-mediated modulation of neuronal sodium current impacts neuronal excitability in Scn2a Q54 mice and may represent a therapeutic target for the treatment of epilepsy.

Published

2017

143. SCN2A p.Ala263Val Variant a Phenotype of Neonatal Seizures Followed by Paroxysmal Ataxia in Toddlers.

Author

Gorman KM and King MD

Subjects

Child, Preschool, Disease Progression, Humans, Male, Ataxia genetics, Epilepsy, Benign Neonatal genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, Seizures genetics

Published

2017

144. Activated ClC-2 Inhibits p-Akt to Repress Myelination in GDM Newborn Rats.

Author

He F, Peng Y, Yang Z, Ge Z, Tian Y, Ma T, and Li H

Subjects

Animals, Animals, Newborn, Apoptosis genetics, Apoptosis physiology, Blotting, Western, Caspase 3 genetics, Caspase 3 metabolism, Corpus Callosum metabolism, Diabetes, Gestational genetics, Female, Gyrus Cinguli metabolism, Immunohistochemistry, In Situ Nick-End Labeling, Male, Mice, Myelin Sheath genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, Nitric Oxide Synthase Type II genetics, Nitric Oxide Synthase Type II metabolism, Phosphatidylinositol 3-Kinases genetics, Pregnancy, Proto-Oncogene Proteins c-akt genetics, Proto-Oncogene Proteins c-akt metabolism, Rats, Rats, Sprague-Dawley, Reactive Oxygen Species metabolism, Reverse Transcriptase Polymerase Chain Reaction, Tumor Necrosis Factor-alpha genetics, Tumor Necrosis Factor-alpha metabolism, Diabetes, Gestational metabolism, Myelin Sheath metabolism, NAV1.2 Voltage-Gated Sodium Channel metabolism, Phosphatidylinositol 3-Kinases metabolism

Abstract

This study aims to investigate the effect and mechanism of type 2 voltage-gated chloride channel (ClC-2) on myelin development of newborn rats' cerebral white matter with gestational diabetes mellitus (GDM). In this study, GDM model was induced in late pregnant rat model. The alteration of ClC-2 expression in various developmental stages of cerebral white matter with/without being exposed to high glucose was analyzed using RT-PCR, active oxygen detection, TUNEL staining, Western Blot as well as immuno-histochemical staining. Our results showed that ClC-2 mRNA and protein expressions in GDM group were significantly increased in white matter of fetal rats after E18 stage, and elevated the level of TNF-α and iNOS in white matter at P0 and P3 stage of newborn rats. Meanwhile, In GDM group, reactive oxygen species (ROS) levels of the white matter at E18, P0, and P3 stage were significantly higher than control group. Furthermore, the expression level of myelin transcription factor Olig2 at P0 stage and CNPase at P3 stage were strikingly lower than that of the control group. In GDM group, ClC-2 expression in the corpus callosum (CC) and cingulate gyrus (CG) regains, and TUNEL positive cell number were increased at P0 and P3 stage. However, PDGFα positive cell number at P0 stage and CNPase expression at P3 stage were significantly decreased. Caspase-3 was also increased in those white matter regions in GDM group, but p-Akt expression was inhibited. While DIDS (a chloride channel blocker) can reverse these changes. In conclusion, ClC-2 and caspase-3 were induced by GDM, which resulted in apoptosis and myelination inhibition. The effect was caused by repressing PI3K-Akt signaling pathway. Application of ClC-2 inhibitor DIDS showed protective effects on cerebral white matter damage stimulated by high glucose concentration., Competing Interests: Competing Interests: The authors have declared that no competing interest exists.

Published

2017

145. Infantile Epileptic Encephalopathy Associated With SCN2A Mutation Responsive to Oral Mexiletine.

Author

Foster LA, Johnson MR, MacDonald JT, Karachunski PI, Henry TR, Nascene DR, Moran BP, and Raymond GV

Subjects

Administration, Oral, Anti-Arrhythmia Agents administration & dosage, Epilepsy physiopathology, Humans, Infant, Infant, Newborn, Mutation, Anticonvulsants administration & dosage, Epilepsy drug therapy, Epilepsy genetics, Mexiletine administration & dosage, NAV1.2 Voltage-Gated Sodium Channel genetics, Voltage-Gated Sodium Channel Blockers administration & dosage

Abstract

Background: Genetic alterations are significant causes of epilepsy syndromes; especially early-onset epileptic encephalopathies and voltage-gated sodium channelopathies are among the best described. Mutations in the SCN2A subunit of voltage-gated sodium channels have been associated with benign familial neonatal-infantile seizures, generalized epilepsy febrile seizures plus, and an early-onset infantile epileptic encephalopathy., Method: We describe two infants with medically refractory seizures due to a de novo SCN2A mutation., Results: The first child responded to intravenous lidocaine with significant reduction in seizure frequency and was successfully transitioned to enteral mexiletine. Mexiletine was subsequently used in a second infant with reduction in seizure frequency., Conclusion: Class 1b antiarrhythmic agents, lidocaine and mexiletine, may be useful in infants with medically refractory early infantile epileptic encephalopathy secondary to mutations in SCN2A., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2017

146. Whole gene duplication of SCN2A and SCN3A is associated with neonatal seizures and a normal intellectual development.

Author

Thuresson AC, Van Buggenhout G, Sheth F, Kamate M, Andrieux J, Clayton Smith J, and Soussi Zander C

Subjects

Adolescent, Age of Onset, Child, Child Development, Child, Preschool, Chromosomes, Human, Pair 2 genetics, Female, Humans, In Situ Hybridization, Fluorescence, Infant, Newborn, Intelligence, Male, Seizures psychology, Gene Duplication, Genetic Predisposition to Disease genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, NAV1.3 Voltage-Gated Sodium Channel genetics, Seizures genetics, Sodium Channels genetics

Abstract

Duplications at 2q24.3 encompassing the voltage-gated sodium channel gene cluster are associated with early onset epilepsy. All cases described in the literature have presented in addition with different degrees of intellectual disability, and have involved neighbouring genes in addition to the sodium channel gene cluster. Here, we report eight new cases with overlapping duplications at 2q24 ranging from 0.05 to 7.63 Mb in size. Taken together with the previously reported cases, our study suggests that having an extra copy of SCN2A has an effect on epilepsy pathogenesis, causing benign familial infantile seizures which eventually disappear at the age of 1-2 years. However, the number of copies of SCN2A does not appear to have an effect on cognitive outcome., (© 2016 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published

2017

147. Rapid and safe response to low-dose carbamazepine in neonatal epilepsy.

Author

Sands TT, Balestri M, Bellini G, Mulkey SB, Danhaive O, Bakken EH, Taglialatela M, Oldham MS, Vigevano F, Holmes GL, and Cilio MR

Subjects

Child, Preschool, Electroencephalography, Epilepsy, Benign Neonatal diagnostic imaging, Epilepsy, Benign Neonatal genetics, Family Health, Female, Follow-Up Studies, Gestational Age, Humans, Infant, Magnetic Resonance Imaging, Male, Mutation genetics, NAV1.2 Voltage-Gated Sodium Channel genetics, Potassium Channels genetics, Anticonvulsants therapeutic use, Carbamazepine pharmacology, Epilepsy, Benign Neonatal drug therapy

Abstract

Objective: To evaluate treatment responses in benign familial neonatal epilepsy (BFNE)., Methods: We recruited patients with BFNE through a multicenter international collaboration and reviewed electroclinical and genetic details, and treatment response. All patients were tested at minimum for mutations/deletions in the KCNQ2, KCNQ3, and SCN2A genes., Results: Nineteen patients were included in this study. A family history of neonatal seizures was positive in 16 patients, and one additional patient had a family history of infantile seizures. Mutations or deletions of KCNQ2 were found in 14, and of KCNQ3 in 2, of the 19 patients. In all patients, seizures began at 2-5 days of life and occurred multiple times per day. Four patients developed status epilepticus. Seizures were focal, alternating between hemispheres, and characterized by asymmetric tonic posturing associated with apnea and desaturation, followed by unilateral or bilateral asynchronous clonic jerking. Twelve of 19 patients were treated with multiple medications prior to seizure cessation. Seventeen of (88%) 19 patients were seizure-free within hours of receiving oral carbamazepine (CBZ) or oxcarbazepine (OXC). Earlier initiation of CBZ was associated with shorter hospitalization (p < 0.01). No side effects of CBZ were reported. All patients had normal development and remain seizure-free at a mean follow-up period of 7.8 years (6 months-16 years)., Significance: This study provides evidence that CBZ is safe and rapidly effective in neonates with BFNE, even in status epilepticus. We propose that CBZ should be the drug of choice in benign familial neonatal seizures., (Wiley Periodicals, Inc. © 2016 International League Against Epilepsy.)

Published

2016

148. Polymorphisms of ABAT, SCN2A and ALDH5A1 may affect valproic acid responses in the treatment of epilepsy in Chinese.

Author

Li X, Zhang J, Wu X, Yan H, Zhang Y, He RH, Tang YJ, He YJ, Tan D, Mao XY, Yin JY, Liu ZQ, Zhou HH, and Liu J

Subjects

Adolescent, Child, Child, Preschool, Epilepsy genetics, Female, Humans, Male, Young Adult, 4-Aminobutyrate Transaminase genetics, Anticonvulsants therapeutic use, Epilepsy drug therapy, NAV1.2 Voltage-Gated Sodium Channel genetics, Polymorphism, Single Nucleotide, Succinate-Semialdehyde Dehydrogenase genetics, Valproic Acid therapeutic use

Abstract

Aim: The clinical efficacy of valproic acid (VPA) varies greatly among epileptic patients. To find the potential genetic factors related to VPA responses, the pharmacogenetics study was conducted., Methods: Two hundred and one Chinese Han epileptic patients who were treated by VPA for at least 1 year were recruited. Up to 24 SNPs in 11 candidate genes that correlate with the metabolism, transport or target of VPA were genotyped., Results: Three SNPs, rs1731017 (ABAT), rs2304016 (SCN2A) and rs1054899 (ALDH5A1) were found associated with VPA responses with the p-values of 0.003, 0.007 and 0.048, respectively. Further interaction analysis showed that the interaction between rs17183814 (ABAT) and rs1641022 (SCN2A) was also correlated with the response of VPA (p = 0.006)., Conclusion: This study found three SNPs and one interaction among ABAT, SCN2A and ALDH5A1 were significantly associated with VPA response, which indicated that these genes may play important roles in the pharmacological mechanism of VPA.

Published

2016

149. Activity of Na V 1.2 promotes neurodegeneration in an animal model of multiple sclerosis.

Author

Schattling B, Fazeli W, Engeland B, Liu Y, Lerche H, Isbrandt D, and Friese MA

Subjects

Animals, Encephalomyelitis, Autoimmune, Experimental genetics, Gene Knock-In Techniques, Humans, Mice, Mice, Inbred C57BL, Multiple Sclerosis, Axons pathology, Encephalomyelitis, Autoimmune, Experimental pathology, Gain of Function Mutation, NAV1.2 Voltage-Gated Sodium Channel genetics, Nerve Degeneration pathology

Abstract

Counteracting the progressive neurological disability caused by neuronal and axonal loss is the major unmet clinical need in multiple sclerosis therapy. However, the mechanisms underlying irreversible neuroaxonal degeneration in multiple sclerosis and its animal model experimental autoimmune encephalomyelitis (EAE) are not well understood. A long-standing hypothesis holds that the distribution of voltage-gated sodium channels along demyelinated axons contributes to neurodegeneration by increasing neuroaxonal sodium influx and energy demand during CNS inflammation. Here, we tested this hypothesis in vivo by inserting a human gain-of-function mutation in the mouse Na V 1.2-encoding gene Scn2a that is known to increase Na V 1.2-mediated persistent sodium currents. In mutant mice, CNS inflammation during EAE leads to elevated neuroaxonal degeneration and increased disability and lethality compared with wild-type littermate controls. Importantly, immune cell infiltrates were not different between mutant EAE mice and wild-type EAE mice. Thus, this study shows that increased neuronal Na V 1.2 activity exacerbates inflammation-induced neurodegeneration irrespective of immune cell alterations and identifies Na V 1.2 as a promising neuroprotective drug target in multiple sclerosis., Competing Interests: The authors have declared that no conflict of interest exists.

Published

2016

150. Episodic ataxia associated with a de novo SCN2A mutation.

Author

Leach EL, van Karnebeek CD, Townsend KN, Tarailo-Graovac M, Hukin J, and Gibson WT

Subjects

Acetazolamide therapeutic use, Adolescent, Anticonvulsants therapeutic use, Ataxia drug therapy, Humans, Male, Ataxia genetics, Mutation, NAV1.2 Voltage-Gated Sodium Channel genetics

Abstract

Introduction: Episodic ataxia (EA) is characterized by paroxysmal attacks of ataxia interspersed by asymptomatic periods. Dominant mutations or copy number variants in CACNA1A are a well-known cause of EA., Clinical Presentation: This boy presented with clinical features of episodic ataxia, and also showed cerebellar atrophy, hypotonia, autism and global developmental delay at age 4 years. Acetazolamide prevented further episodes of ataxia, dystonia and encephalopathy. Extensive biochemical and genetic tests were unrevealing; whole exome sequencing found a previously unreported variant in SCN2A, proven to be de novo and predicted to be protein-damaging., Conclusion: Considered alongside previous reports of episodic ataxia in SCN2A mutation-positive patients, our case further illustrates the genetic heterogeneity of episodic ataxia. In addition, this case suggests that acetazolamide may be an effective treatment for some aspects of the phenotype in a broader range of channelopathy-related conditions., (Copyright © 2016 European Paediatric Neurology Society. Published by Elsevier Ltd. All rights reserved.)

Published

2016