| Literature DB >> 27541164 |
Reymundo Lozano1, Kristin Herman2, Melanie Rothfuss2, Hillary Rieger1, Pinar Bayrak-Toydemir3, Davide Aprile4, Floriana Fruscione5, Federico Zara5, Anna Fassio4,6.
Abstract
TBC1D24-related disorders include a wide phenotypic ranging from mild to lethal seizure disorders, non-syndromic deafness, and composite syndromes such as DOORS (deafness, onychodystrophy, osteodystrophy, mental retardation, and seizures). The TBC1D24 gene has a role in cerebral cortex development and in presynaptic neurotransmission. Here, we present a familial case of a lethal early-onset epileptic encephalopathy, associated with two novel compound heterozygous missense variants on the TBC1D24 gene, which were detected by exome sequencing. The detailed clinical data of the three siblings is summarized in order to support the variability of the phenotype, severity, and progression of this disorder among these family members. Functional studies demonstrated that the identified novel missense mutations result in a loss of expression of the protein, suggesting a correlation between residual expression, and the disease severity. This indicates that protein expression analysis is important for interpreting genetic results when novel variants are found, as well as for complementing clinical assessment by predicting the functional impact. Further analysis is necessary to delineate the clinical presentation of individuals with TBC1D24 pathogenic variants, as well as to develop markers for diagnosis, prognosis, and potential targeted treatments.Entities:
Keywords: TBC1D24; deafness; lethal seizure disorder; neonatal seizure disorder; non-syndromic deafness; recessive seizures
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Year: 2016 PMID: 27541164 DOI: 10.1002/ajmg.a.37933
Source DB: PubMed Journal: Am J Med Genet A ISSN: 1552-4825 Impact factor: 2.802