1. A rare cause of epileptic encephalopathy: case report of a novel patient with PEHO-like phenotype and CCDC88A gene pathogenic variants.
- Author
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Papuc, Sorina-Mihaela, Glangher, Adelina, Erbescu, Alina, Arsene, Oana Tarta, Arghir, Aurora, and Budisteanu, Magdalena
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BRAIN abnormalities , *GENETICS of epilepsy , *GENETIC disorder diagnosis , *MICROCEPHALY , *OPTIC nerve diseases , *DIFFERENTIAL diagnosis , *BRAIN , *MICROFILAMENT proteins , *MAGNETIC resonance imaging , *BRAIN diseases , *NEURODEGENERATION , *GENES , *MUSCLE hypotonia , *EPILEPSY , *CHILD development deviations , *SEIZURES (Medicine) , *GENETIC mutation , *GENETIC testing , *PHENOTYPES , *SEQUENCE analysis , *DISEASE progression , *MEMBRANE proteins , *CEREBRAL edema , *SYMPTOMS , *CHILDREN - Abstract
Background: The Coiled-Coil Domain-Containing Protein 88 A (CCDC88A) gene encodes the actin-binding protein Girdin, which plays important roles in maintaining the actin cytoskeleton and in cell migration and was recently associated with a specific form of epileptic encephalopathy. Biallelic protein-truncating variants of CCDC88A have been considered responsible for progressive encephalopathy with edema, hypsarrhythmia, and optic atrophy (PEHO)-like syndrome. To date, only three consanguineous families with loss-of-function homozygous variants in the CCDC88A gene have been reported. The described patients share many clinical features, such as microcephaly, neonatal hypotonia, seizures, profound developmental delay, face and limb edema, and dysmorphic features, with a similar appearance of the eyes, nose, mouth, and fingers. Case presentation: We report on a child from a nonconsanguineous family who presented with profound global developmental delay, severe epilepsy, and brain malformations, including subcortical band heterotopia. The patient harbored two heterozygous pathogenic variants in the trans configuration in the CCDC88A gene, which affected the coiled-coil and C-terminal domains. Conclusions: We detail the clinical and cerebral imaging data of our patient in the context of previously reported patients with disease-causing variants in the CCDC88A gene, emphasizing the common phenotypes, including cortical malformations, that warrant screening for sequence variants in this gene. [ABSTRACT FROM AUTHOR]
- Published
- 2024
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