Aoyagi Kyota, Rossignol Elsa, Hamdan Fadi F, Mulcahy Ben, Xie Lin, Nagamatsu Shinya, Rouleau Guy A, Zhen Mei, Michaud Jacques L
Department of Biochemistry, Kyorin University School of Medicine, Tokyo, Japan.
CHU Sainte-Justine Research Center, Montreal, Canada.
Hum Mutat. 2015 Aug;36(8):753-7. doi: 10.1002/humu.22797. Epub 2015 Jun 22.
NALCN and its homologues code for the ion channel responsible for half of background Na(+) -leak conductance in vertebrate and invertebrate neurons. Recessive mutations in human NALCN cause intellectual disability (ID) with hypotonia. Here, we report a de novo heterozygous mutation in NALCN affecting a conserved residue (p.R1181Q) in a girl with ID, episodic and persistent ataxia, and arthrogryposis. Interestingly, her episodes of ataxia were abolished by the administration of acetazolamide, similar to the response observed in episodic ataxia associated with other ion channels. Introducing the analogous mutation in the Caenorhabditis elegans homologue nca-1 induced a coiling locomotion phenotype, identical to that obtained with previously characterized C. elegans gain-of-function nca alleles, suggesting that p.R1181Q confers the same property to NALCN. This observation thus suggests that dominant mutations in NALCN can cause a neurodevelopmental phenotype that overlaps with, while being mostly distinct from that associated with recessive mutations in the same gene.
NALCN及其同源物编码负责脊椎动物和无脊椎动物神经元中一半背景钠(Na⁺)渗漏电导的离子通道。人类NALCN中的隐性突变会导致智力障碍(ID)并伴有肌张力减退。在此,我们报告了一名患有ID、发作性和持续性共济失调以及关节挛缩的女孩中,NALCN发生的一个新生杂合突变,该突变影响一个保守残基(p.R1181Q)。有趣的是,给予乙酰唑胺后她的共济失调发作消失了,这与在与其他离子通道相关的发作性共济失调中观察到的反应相似。在秀丽隐杆线虫同源物nca - 1中引入类似突变会诱导卷曲运动表型,这与先前表征的秀丽隐杆线虫功能获得性nca等位基因所产生的表型相同,表明p.R1181Q赋予NALCN相同的特性。因此,这一观察结果表明,NALCN中的显性突变可导致一种神经发育表型,该表型与同一基因隐性突变相关的表型有重叠,但大多不同。
