Xp22.33p22.12 Duplication in a Patient with Intellectual Disability and Dysmorphic Facial Features | Zendy

Carla Lintas | Zendy; Chiara Picinelli | Zendy; Ignazio S. Piras | Zendy; Roberto Sacco | Zendy; Stefano Gabriele | Zendy; Magda Verdecchia | Zendy; Antonio M. Persico | Zendy

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Xp22.33p22.12 Duplication in a Patient with Intellectual Disability and Dysmorphic Facial Features

Author(s) -

Carla Lintas,

Chiara Picinelli,

Ignazio S. Piras,

Roberto Sacco,

Stefano Gabriele,

Magda Verdecchia,

Antonio M. Persico

Publication year - 2015

Publication title -

molecular syndromology

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.609

H-Index - 36

eISSN - 1661-8777

pISSN - 1661-8769

DOI - 10.1159/000443232

Subject(s) - gene duplication , intellectual disability , genetics , phenotype , hypotonia , neuroligin , gene , medicine , copy number variation , biology , bioinformatics , genome , receptor , excitatory postsynaptic potential

A novel 19.98-Mb duplication in chromosome Xp22.33p22.12 was detected by array CGH in a 30-year-old man affected by intellectual disability, congenital hypotonia and dysmorphic features. The duplication encompasses more than 100 known genes. Many of these genes (such as neuroligin 4, cyclin-dependent kinase like 5, and others) have already correlated with X-linked intellectual disability and/or neurodevelopmental disorders. Due to the high number of potentially pathogenic genes involved in the reported duplication, we cannot correlate the clinical phenotype to a single gene. Indeed, we suggest that the resulting clinical phenotype may have arisen from the overexpression and consequent perturbation of fine gene dosage.

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