dc.contributor.author
He, Hailan
dc.contributor.author
Guzman, Raul E.
dc.contributor.author
Cao, Dezhi
dc.contributor.author
Sierra-Marquez, Juan
dc.contributor.author
Yin, Fei
dc.contributor.author
Fahlke, Christoph
dc.contributor.author
Peng, Jing
dc.contributor.author
Stauber, Tobias
dc.date.accessioned
2021-06-02T07:02:46Z
dc.date.available
2021-06-02T07:02:46Z
dc.identifier.uri
https://refubium.fu-berlin.de/handle/fub188/30903
dc.identifier.uri
http://dx.doi.org/10.17169/refubium-30642
dc.description.abstract
Objective
This study was undertaken to expand the phenotypic and genetic spectrum of CLCN4-related epilepsy and to investigate genotype–phenotype correlations.
Methods
We systematically reviewed the phenotypic and genetic spectrum of newly diagnosed and previously reported patients with CLCN4-related epilepsy. Three novel variants identified in four patients reported in this study were evaluated through in silico prediction and functional analysis by Western blot, immunofluorescence, and electrophysiological measurements.
Results
Epilepsy was diagnosed in 54.55% (24/44) of individuals with CLCN4-related disorders and was drug-resistant in most cases. Of 24 patients, 15 had epileptic encephalopathy and four died at an early age; 69.57% of patients had seizure onset within the first year of life. Myoclonic seizures are the most common seizure type, and 56.25% of patients presented multiple seizure types. Notably, seizure outcome was favorable in individuals with only one seizure type. All patients showed intellectual disability, which was severe in 65.22% of patients. Additional common features included language delay, behavioral disorders, and dysmorphic features. Five patients benefitted from treatment with lamotrigine. Most variants, which were mainly missense (79.17%), were inherited (70.83%). Whereas frameshift, intragenic deletion, or inherited variants were associated with milder phenotypes, missense or de novo variants led to more severe phenotypes. All evaluated CLCN4 variants resulted in loss of function with reduced ClC-4 currents. Nonetheless, genotype–phenotype relationships for CLCN4-related epilepsy are not straightforward, as phenotypic variability was observed in recurrent variants and within single families.
Significance
Pathogenic CLCN4 variants contribute significantly to the genetic etiology of epilepsy. The phenotypic spectrum of CLCN4-related epilepsy includes drug-resistant seizures, cognitive and language impairment, behavioral disorders, and congenital anomalies. Notably, the mutation type and the number of seizure types correlate with the severity of the phenotype, suggesting its use for clinical prognosis. Lamotrigine can be considered a therapeutic option.
en
dc.format.extent
15 Seiten
dc.rights.uri
https://creativecommons.org/licenses/by-nc/4.0/
dc.subject
behavior disorders
en
dc.subject
Cl-/H+ exchanger
en
dc.subject
intellectual disability
en
dc.subject.ddc
500 Naturwissenschaften und Mathematik::570 Biowissenschaften; Biologie::570 Biowissenschaften; Biologie
dc.title
The molecular and phenotypic spectrum of CLCN4-related epilepsy
dc.type
Wissenschaftlicher Artikel
dcterms.bibliographicCitation.doi
10.1111/epi.16906
dcterms.bibliographicCitation.journaltitle
Epilepsia
dcterms.bibliographicCitation.number
6
dcterms.bibliographicCitation.pagestart
1401
dcterms.bibliographicCitation.pageend
1415
dcterms.bibliographicCitation.volume
62
dcterms.bibliographicCitation.url
https://doi.org/10.1111/epi.16906
refubium.affiliation
Biologie, Chemie, Pharmazie
refubium.affiliation.other
Institut für Chemie und Biochemie
refubium.funding
DEAL Wiley
refubium.note.author
Die Publikation wurde aus Open Access Publikationsgeldern der Freien Universität Berlin gefördert.
refubium.resourceType.isindependentpub
no
dcterms.accessRights.openaire
open access
dcterms.isPartOf.eissn
1528-1167
refubium.resourceType.provider
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