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ARHGEF9的表型谱包括智力残疾、局灶性癫痫和热性惊厥。

The phenotypic spectrum of ARHGEF9 includes intellectual disability, focal epilepsy and febrile seizures.

作者信息

Klein Karl Martin, Pendziwiat Manuela, Eilam Anda, Gilad Ronit, Blatt Ilan, Rosenow Felix, Kanaan Moien, Helbig Ingo, Afawi Zaid

机构信息

Epilepsy Center Frankfurt Rhine-Main, Department of Neurology, Center of Neurology and Neurosurgery, University Hospital, Goethe-University Frankfurt, Frankfurt/Main, Germany.

Epilepsy Center Hessen, Philipps-University Marburg, Marburg, Germany.

出版信息

J Neurol. 2017 Jul;264(7):1421-1425. doi: 10.1007/s00415-017-8539-3. Epub 2017 Jun 15.

DOI:10.1007/s00415-017-8539-3
PMID:28620718
Abstract

Mutations or structural genomic alterations of the X-chromosomal gene ARHGEF9 have been described in male and female patients with intellectual disability. Hyperekplexia and epilepsy were observed to a variable degree, but incompletely described. Here, we expand the phenotypic spectrum of ARHGEF9 by describing a large Ethiopian-Jewish family with epilepsy and intellectual disability. The four affected male siblings, their unaffected parents and two unaffected female siblings were recruited and phenotyped. Parametric linkage analysis was performed using SNP microarrays. Variants from exome sequencing in two affected individuals were confirmed by Sanger sequencing. All affected male siblings had febrile seizures from age 2-3 years and intellectual disability. Three developed afebrile seizures between age 7-17 years. Three showed focal seizure semiology. None had hyperekplexia. A novel ARHGEF9 variant (c.967G>A, p.G323R, NM_015185.2) was hemizygous in all affected male siblings and heterozygous in the mother. This family reveals that the phenotypic spectrum of ARHGEF9 is broader than commonly assumed and includes febrile seizures and focal epilepsy with intellectual disability in the absence of hyperekplexia or other clinically distinguishing features. Our findings suggest that pathogenic variants in ARHGEF9 may be more common than previously assumed in patients with intellectual disability and mild epilepsy.

摘要

患有智力残疾的男性和女性患者中已发现X染色体基因ARHGEF9的突变或结构基因组改变。观察到不同程度的惊吓症和癫痫,但描述并不完整。在此,我们通过描述一个患有癫痫和智力残疾的埃塞俄比亚犹太大家族,扩展了ARHGEF9的表型谱。招募了四名受影响的男性同胞、他们未受影响的父母以及两名未受影响的女性同胞,并对其进行了表型分析。使用SNP微阵列进行参数连锁分析。通过桑格测序确认了两名受影响个体外显子测序中的变异。所有受影响的男性同胞在2至3岁时均出现热性惊厥和智力残疾。三人在7至17岁之间出现无热惊厥。三人表现出局灶性癫痫发作症状学。无人患有惊吓症。一种新的ARHGEF9变异(c.967G>A,p.G323R,NM_015185.2)在所有受影响的男性同胞中为半合子,在母亲中为杂合子。这个家族表明,ARHGEF9的表型谱比通常认为的更广泛,包括在没有惊吓症或其他临床特征的情况下出现热性惊厥和伴有智力残疾的局灶性癫痫。我们的研究结果表明,ARHGEF9中的致病变异在智力残疾和轻度癫痫患者中可能比以前认为的更常见。

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Eur J Med Genet. 2016 Sep;59(9):470-3. doi: 10.1016/j.ejmg.2016.05.014. Epub 2016 May 27.
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Chromodomain-helicase-DNA-binding protein 1-like (CHD1L) silencing inhibits gastric cancer cell proliferation, invasion, and migration.
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A novel hemizygous mutation associated with severe intellectual disability and epilepsy: a case report.一个与严重智力残疾和癫痫相关的新型杂合突变:病例报告。
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Selective Overexpression of Collybistin in Mouse Hippocampal Pyramidal Cells Enhances GABAergic Neurotransmission and Protects against PTZ-Induced Seizures.在小鼠海马锥体神经元中选择性过表达 Collybistin 增强 GABA 能神经传递并预防 PTZ 诱导的癫痫发作。
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The α3 subunit of GABA receptors promotes formation of inhibitory synapses in the absence of collybistin.GABA 受体的 α3 亚基在没有 collybistin 的情况下促进抑制性突触的形成。
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De novo ARHGEF9 missense variants associated with neurodevelopmental disorder in females: expanding the genotypic and phenotypic spectrum of ARHGEF9 disease in females.新发 ARHGEF9 错义变异与女性神经发育障碍相关:扩大女性 ARHGEF9 疾病的基因型和表型谱。
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