Myoclonic-atonic epilepsy caused by a novel de novo heterozygous missense variant in the SLC6A1 gene: Brief discussion of the literature and detailed case description of a severely intellectually disabled adult male patient
Publication year
2022Author(s)
Number of pages
7 p.
Source
International Medical Case Reports Journal, 15, (2022), pp. 753-759ISSN
Publication type
Article / Letter to editor
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Organization
Human Genetics
SW OZ DCC NRP
Journal title
International Medical Case Reports Journal
Volume
vol. 15
Languages used
English (eng)
Page start
p. 753
Page end
p. 759
Subject
Neuropsychology and rehabilitation psychology; Radboudumc 7: Neurodevelopmental disorders DCMN: Donders Center for Medical Neuroscience; Neuro- en revalidatiepsychologie; Radboud University Medical CenterAbstract
Introduction: Diagnostic exome sequencing has yielded over the past decades a great number of molecular diagnoses for genetic disorders in which both intellectual disability and epilepsy are present. One of these syndromes is myoclonic-atonic epilepsy (MAE) that is caused by pathogenic variants in the SLC6A1 gene located at 3p25.3. The most relevant clinical characteristics are intellectual disability, several forms of mostly treatment-resistant epilepsy starting at young age, serious disinhibitory behavioural problems, language impairment, higher pain tolerance, and symptoms from the autism spectrum, all in the absence of any consistent dysmorphism or malformation. Methods: After an overview of the literature, here, the developmental trajectory of a 55-year-old severely intellectually disabled male with therapy-resistant epilepsy and aggressive outburst is reported in detail, in whom no etiological diagnosis had been performed. Next to genetic, neurological, and neuropsychiatric examination, psychological assessment with validated instruments was performed. Results: Exome sequencing and targeted analysis of the patient and both his parents demonstrated a de novo missense variant in the SLC6A1 gene which was never before described in the literature nor in control databases. The phenotypical presentation of the patient with treatment-resistant epilepsy, especially absences and myoclonic seizures, as well as sleep disturbances and autism, corresponds with a diagnosis of MAE. Discussion: This case stresses that exome sequencing should be the first-tier diagnostic test for patients with unexplained neurodevelopmental disorders, regardless of their age, and that as yet the most suitable approach is the formation of an interdisciplinary team for treatment design and clinical management.
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