The Role of the Reanalysis of Genetic Test Results in the Diagnosis of Dysmorphic Syndrome Caused by Inherited xq24 Deletion including the UBE2A and CXorf56 Genes.
Ewelina WolańskaAgnieszka PollakMalgorzata RydzaniczKarolina PeszKlaniewska MagdalenaAnna RozensztrauchPaweł SkibaPiotr StawińskiPloski RafalRobert ŚmigielPublished in: Genes (2021)
Psychomotor delay, hypotonia, and intellectual disability, as well as heart defects, urogenital malformations, and characteristic cranio-facial dysmorphism are the main symptoms of dysmorphic syndrome associated with intergenic deletion in the Xq24 chromosome region including the UBE2A and CXorf56 genes. To date, there is limited information in the literature about the symptoms and clinical course of the Xq24 deletion. Here, we present a case of Xq24 deletion including the UBE2A and CXorf56 genes in a nine-year-old boy, in whom the array comparative genomic hybridization (array-CGH) and whole exome sequencing (WES) tests were performed in 2015 with normal results. The WES results were reanalyzed in 2019. Intergenic, hemizygous deletion in the Xq24 chromosome region including the UBE2A and CXorf56 genes was revealed and subsequently confirmed in the array-CGH study as the deletion of 35kb in the Xq24 region. Additionally, the carriership of deletion in the mother of the child was confirmed.
Keyphrases
- genome wide
- intellectual disability
- copy number
- autism spectrum disorder
- high resolution
- bioinformatics analysis
- high throughput
- heart failure
- genome wide identification
- dna methylation
- case report
- healthcare
- gene expression
- high density
- physical activity
- social media
- single molecule
- sleep quality
- soft tissue
- label free