Mutation in an alternative transcript of CDKL5 in a boy with early-onset seizures

Infantile-onset epilepsies are a set of severe, heterogeneous disorders for which clinical genetic testing yields causative mutations in ∼20%–50% of affected individuals. We report the case of a boy presenting with intractable seizures at 2 wk of age, for whom gene panel testing was unrevealing. Res...

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Bibliographic Details
Published inCold Spring Harbor molecular case studies Vol. 4; no. 3; p. a002360
Main Authors Bodian, Dale L., Schreiber, John M., Vilboux, Thierry, Khromykh, Alina, Hauser, Natalie S.
Format Journal Article
LanguageEnglish
Published United States Cold Spring Harbor Laboratory Press 01.06.2018
Subjects
Age
Age of Onset
Alleles
Alternative Splicing
Biomarkers
Brain
Chromosome Mapping
Convulsions & seizures
Diagnostic systems
DNA Mutational Analysis
Electroencephalography
Encephalopathy
Epilepsy
Epileptic Syndromes - diagnosis
Epileptic Syndromes - genetics
Exons
Gene Frequency
Gene sequencing
Genetic screening
Genomes
Humans
Infant, Newborn
Male
Mutation
Pedigree
Phenotype
Protein-Serine-Threonine Kinases - genetics
Research Reports
Seizures
Seizures - diagnosis
Seizures - genetics
Sequence Deletion
Spasms, Infantile - diagnosis
Spasms, Infantile - genetics
Transcription
Whole Genome Sequencing
infantile spasms
generalized tonic seizures
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ISSN2373-2865
2373-2873
2373-2873
DOI10.1101/mcs.a002360

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Summary:Infantile-onset epilepsies are a set of severe, heterogeneous disorders for which clinical genetic testing yields causative mutations in ∼20%–50% of affected individuals. We report the case of a boy presenting with intractable seizures at 2 wk of age, for whom gene panel testing was unrevealing. Research-based whole-genome sequencing of the proband and four unaffected family members identified a de novo mutation, NM_001323289.1:c.2828_2829delGA in CDKL5, a gene associated with X-linked early infantile epileptic encephalopathy 2. CDKL5 has multiple alternative transcripts, and the mutation lies in an exon in the brain-expressed forms. The mutation was undetected by gene panel sequencing because of its intronic location in the CDKL5 transcript typically used to define the exons of this gene for clinical exon-based tests (NM_003159). This is the first report of a patient with a mutation in an alternative transcript of CDKL5 . This finding suggests that incorporating alternative transcripts into the design and variant interpretation of exon-based tests, including gene panel and exome sequencing, could improve the diagnostic yield.
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ISSN:2373-2865
2373-2873
2373-2873
DOI:10.1101/mcs.a002360