De novo and inherited mutations in the X-linked gene CLCN4 are associated with syndromic intellectual disability and behavior and seizure disorders in males and females

Palmer, Elizabeth E.; Stuhlmann, Till; Weinert, Stefanie; Haan, Eric; Esch, Hilde Van; Holvoet, Maureen; Boyle, J.; Leffler, Melanie; Raynaud, Martine; Moraine, Claude; Bokhoven, Hans van; Kleefstra, Tjitske; Kahrizi, Kimia; Najmabadi, Hossein; Ropers, Hans‐Hilger; Delgado, Mauricio R.; Sirsi, Deepa; Golla, Sailaja; Sommer, Annemarie; Pietryga, Marguerite; Chung, Wendy K.; Wynn, Julia; Rohena, Luis; Bernardo, Eduardo Roberto de Almeida; Hamlin, Damara; Faux, Brian M.; Grange, Dorothy K.; Manwaring, Linda; Tolmie, John; Joss, Shelagh; Cobben, Jan Maarten; Duijkers, Floor A.M.; Goehringer, Jessica; Challman, Thomas D.; Hennig, Friederike; Fischer, Ute; Grimme, Astrid; Suckow, Vanessa; Musante, Luciana; Nicholl, Jillian; Shaw, Marie; Lodh, Suhrid; Niu, Zhiyv; Rosenfeld, Jill A.; Stankiewicz, Paweł; Jentsch, Thomas J.; Gécz, Jozef; Field, Michael; Kalscheuer, Vera M.

doi:10.1038/mp.2016.135

Cited by 48 publications

(104 citation statements)

References 39 publications

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“…In the present study, the patient with a de novo KCNQ2 missense mutation displayed a very early‐onset age (2 days), similar to that of BFNS; but the patient also presented features of EIMFS, such as intellectual disability and multiple focal discharges on EEG. Similarly, mutations in CLCN4 have been reported to cause X‐linked intellectual disability and epilepsies, in which focal seizures were prominent in some cases . We identified a de novo CLCN4 mutation in a boy with EIMFS featuring frequent complex partial seizures and multiple focal discharges.…”

Section: Discussionmentioning

confidence: 69%

“…In contrast, KCNQ2 mutations were mainly associated with benign familial neonatal epilepsy (BFNS) and severe neonatal onset epileptic encephalopathies, such as Ohtahara syndrome . CLCN4 mutations were mainly identified in patients with intellectual disabilities with only a few associated with epileptic encephalopathies . Three of the 4 mutations in EIMFS were novel findings.…”

Section: Resultsmentioning

confidence: 99%

“…25 CLCN4 mutations were mainly identified in patients with intellectual disabilities with only a few associated with epileptic encephalopathies. 26,27 Three of the 4 mutations in EIMFS were novel findings.…”

Section: Resultsmentioning

confidence: 99%

“…Similarly, mutations in CLCN4 have been reported to cause X-linked intellectual disability and epilepsies, in which focal seizures were prominent in some cases. 26,27 We identified a de novo CLCN4 mutation in a boy with EIMFS featuring frequent complex partial seizures and multiple focal discharges. Until now, distinct association between gene and phenotype of epileptic encephalopathy has been found in only a few genes, such as SLC6A1 mutations in EMAS 37 and SLC35A2 mutations in infantile spasms with hypsarrhythmia on EEGs.…”

Section: Discussionmentioning

confidence: 99%

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Novel mutations and phenotypes of epilepsy‐associated genes in epileptic encephalopathies

Zhou

Zhang

et al. 2018

Genes Brain and Behavior

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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.

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Section: Discussionmentioning

confidence: 69%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Novel mutations and phenotypes of epilepsy‐associated genes in epileptic encephalopathies

Zhou

Zhang

et al. 2018

Genes Brain and Behavior

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“…The physiological importance of vesicular CLCs is highlighted by mouse models and patients carrying CLCN mutations. Their pathologies range from impaired renal endocytosis and kidney stones (ClC‐5) (Lloyd et al , ; Piwon et al , ; Wang et al , ) to severe neurodegeneration (ClC‐3) (Stobrawa et al , ), intellectual disability and epilepsy (ClC‐4) (Veeramah et al , ; Hu et al , ; Palmer et al , ), to lysosomal storage disease (ClC‐6) (Poët et al , ) or osteopetrosis associated with lysosomal storage and neurodegeneration (ClC‐7) (Kornak et al , ; Kasper et al , ). A gain‐of‐function mutation in CLCN7 causes lysosomal storage disease and hypopigmentation without osteopetrosis (Nicoli et al , ).…”

Section: Introductionmentioning

confidence: 99%

Uncoupling endosomal CLC chloride/proton exchange causes severe neurodegeneration

et al. 2020

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CLC chloride/proton exchangers may support acidification of endolysosomes and raise their luminal Cl À concentration. Disruption of endosomal ClC-3 causes severe neurodegeneration. To assess the importance of ClC-3 Cl À /H + exchange, we now generate Clcn3 unc/unc mice in which ClC-3 is converted into a Cl À channel. Unlike Clcn3 À/À mice, Clcn3 unc/unc mice appear normal owing to compensation by ClC-4 with which ClC-3 forms heteromers. ClC-4 protein levels are strongly reduced in Clcn3 À/À , but not in Clcn3 unc/unc mice because ClC-3 unc binds and stabilizes ClC-4 like wild-type ClC-3. Although mice lacking ClC-4 appear healthy, its absence in Clcn3 unc/unc /Clcn4 À/À mice entails even stronger neurodegeneration than observed in Clcn3 À/À mice. A fraction of ClC-3 is found on synaptic vesicles, but miniature postsynaptic currents and synaptic vesicle acidification are not affected in Clcn3 unc/unc or Clcn3 À/À mice before neurodegeneration sets in. Both, Cl À /H + -exchange activity and the stabilizing effect on ClC-4, are central to the biological function of ClC-3.

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Genome Sequencing as a Diagnostic Test in Children With Unexplained Medical Complexity

et al. 2020

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Key Points Question What is the diagnostic yield of genome sequencing in children with unexplained medical complexity and prior negative results of genetic testing? Findings In this cohort study that included 138 individuals from 49 families, genome sequencing detected all genomic variation previously identified by conventional genetic testing and resulted in a new diagnosis for 31% of patients. Meaning This study suggests that, because of its high yield, comprehensive nature, and increasingly competitive costs, genome sequencing is a potentially first-tier genetic test for children with unexplained medical complexity.

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De novo and inherited mutations in the X-linked gene CLCN4 are associated with syndromic intellectual disability and behavior and seizure disorders in males and females

Cited by 48 publications

References 39 publications

Novel mutations and phenotypes of epilepsy‐associated genes in epileptic encephalopathies

Novel mutations and phenotypes of epilepsy‐associated genes in epileptic encephalopathies

Uncoupling endosomal CLC chloride/proton exchange causes severe neurodegeneration

Genome Sequencing as a Diagnostic Test in Children With Unexplained Medical Complexity

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