Brain expression profiles of two SCN1A antisense RNAs in children and adolescents with epilepsy.

IF 1.8 4区 医学 Q4 NEUROSCIENCES Translational Neuroscience Pub Date : 2024-01-23 eCollection Date: 2024-01-01 DOI:10.1515/tnsci-2022-0330
Marius Frederik Schneider, Miriam Vogt, Johanna Scheuermann, Veronika Müller, Antje H L Fischer-Hentrich, Thomas Kremer, Sebastian Lugert, Friedrich Metzger, Manfred Kudernatsch, Gerhard Kluger, Till Hartlieb, Soheyl Noachtar, Christian Vollmar, Mathias Kunz, Jörg Christian Tonn, Roland Coras, Ingmar Blümcke, Claudia Pace, Florian Heinen, Christoph Klein, Heidrun Potschka, Ingo Borggraefe
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Abstract

Objective: Heterozygous mutations within the voltage-gated sodium channel α subunit (SCN1A) are responsible for the majority of cases of Dravet syndrome (DS), a severe developmental and epileptic encephalopathy. Development of novel therapeutic approaches is mandatory in order to directly target the molecular consequences of the genetic defect. The aim of the present study was to investigate whether cis-acting long non-coding RNAs (lncRNAs) of SCN1A are expressed in brain specimens of children and adolescent with epilepsy as these molecules comprise possible targets for precision-based therapy approaches.

Methods: We investigated SCN1A mRNA expression and expression of two SCN1A related antisense RNAs in brain tissues in different age groups of pediatric non-Dravet patients who underwent surgery for drug resistant epilepsy. The effect of different antisense oligonucleotides (ASOs) directed against SCN1A specific antisense RNAs on SCN1A expression was tested.

Results: The SCN1A related antisense RNAs SCN1A-dsAS (downstream antisense, RefSeq identifier: NR_110598) and SCN1A-usAS (upstream AS, SCN1A-AS, RefSeq identifier: NR_110260) were widely expressed in the brain of pediatric patients. Expression patterns revealed a negative correlation of SCN1A-dsAS and a positive correlation of lncRNA SCN1A-usAS with SCN1A mRNA expression. Transfection of SK-N-AS cells with an ASO targeted against SCN1A-dsAS was associated with a significant enhancement of SCN1A mRNA expression and reduction in SCN1A-dsAS transcripts.

Conclusion: These findings support the role of SCN1A-dsAS in the suppression of SCN1A mRNA generation. Considering the haploinsufficiency in genetic SCN1A related DS, SCN1A-dsAS is an interesting target candidate for the development of ASOs (AntagoNATs) based precision medicine therapeutic approaches aiming to enhance SCN1A expression in DS.

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两种 SCN1A 反义 RNA 在儿童和青少年癫痫患者大脑中的表达谱。
目的:电压门控钠通道α亚基(SCN1A)的杂合子突变是导致严重发育性癫痫性脑病--德雷维特综合征(Dravet Syndrome,DS)大多数病例的原因。为了直接针对遗传缺陷的分子后果,必须开发新型治疗方法。本研究旨在调查 SCN1A 的顺式作用长非编码 RNA(lncRNA)是否在儿童和青少年癫痫患者的脑标本中表达,因为这些分子是精准治疗方法的可能靶点:方法:我们研究了因耐药癫痫接受手术治疗的不同年龄组儿童非特拉维特癫痫患者脑组织中 SCN1A mRNA 的表达情况以及两种 SCN1A 相关反义 RNA 的表达情况。测试了针对SCN1A特异性反义RNA的不同反义寡核苷酸(ASO)对SCN1A表达的影响:结果:SCN1A相关反义RNAs SCN1A-dsAS(下游反义,RefSeq标识符:NR_110598)和SCN1A-usAS(上游AS,SCN1A-AS,RefSeq标识符:NR_110260)在儿科患者脑中广泛表达。表达模式显示 SCN1A-dsAS 与 SCN1A mRNA 表达呈负相关,lncRNA SCN1A-usAS 与 SCN1A mRNA 表达呈正相关。用针对SCN1A-dsAS的ASO转染SK-N-AS细胞可显著提高SCN1A mRNA的表达,减少SCN1A-dsAS转录本:这些发现支持 SCN1A-dsAS 在抑制 SCN1A mRNA 生成中的作用。考虑到遗传性SCN1A相关DS中的单倍体缺陷,SCN1A-dsAS是开发基于ASOs(AntagoNATs)的精准医学治疗方法的一个有趣的候选靶点,旨在增强DS中SCN1A的表达。
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来源期刊
CiteScore
3.00
自引率
4.80%
发文量
45
审稿时长
>12 weeks
期刊介绍: Translational Neuroscience provides a closer interaction between basic and clinical neuroscientists to expand understanding of brain structure, function and disease, and translate this knowledge into clinical applications and novel therapies of nervous system disorders.
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