Bi-Allelic c.1746G>T; p.Leu582= Variants in TUBGCP4 in a Boy with Autism: Clinical Data and Literature Review

Fernández Mayoralas, Daniel Martín; Albert, Jacobo; López Martín, Sara; Jiménez de la Peña, Mar; Fernández Perrone, Ana Laura; Jiménez de Domingo, Ana; Calleja Pérez, Beatriz; Martínez García, Mónica; Álvarez de Andrés, Sara; Fernández Jaén, Alberto

doi:10.1159/000519365

Inicio

Bi-Allelic c.1746G>T; p.Leu582= Variants in TUBGCP4 in a Boy with Autism: Clinical Data and Literature Review

Fernández Mayoralas, Daniel Martín; Albert, Jacobo; López Martín, Sara; Jiménez de la Peña, Mar; Fernández Perrone, Ana Laura; Jiménez de Domingo, Ana; Calleja Pérez, Beatriz; Martínez García, Mónica; Álvarez de Andrés, Sara; Fernández Jaén, Alberto

Use este identificador para citar o enlazar este ítem: http://hdl.handle.net/11268/11363

Fecha: 2021

Materia UNESCO: Deficiencia mental
Materia UNESCO: Genética humana
Materia UNESCO: Mutación

Tipo: article

Versión del editor: https://doi.org/10.1159/000519365

Exportar a:

Resumen:

Bi-allelic mutations in the TUBGCP4 gene have been recently associated with autosomal recessive microcephaly with chorioretinopathy. However, little is known about the genotype-phenotype characteristics of this disorder. Here, we describe a 5-year-old male patient with autism and a normal occipitofrontal circumference. No retinal abnormalities were observed. Brain MRI revealed the presence of enlarged sheaths of both tortuous optic nerves; both eyes had shorter axial lengths. Whole-exome sequencing in trio revealed synonymous TUBGCP4 variants in homozygous state: c.1746G>T; p.Leu582=. This synonymous variant has been previously described and probably leads to skipping of exon 16 of TUBGCP4. These results broaden the clinical spectrum of this new syndrome and suggest that TUBGCP4 bi-allelic mutations may underlie complex neurodevelopmental disorders.

Mostrar el registro completo del ítem