1. Cytogenetic and molecular characterization of a recombinant X chromosome in a family with a severe neurologic phenotype and macular degeneration
- Author
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Manuela Vargiolu, Claudio Graziano, Duccio Maria Cordelli, Simona Ferrari, Anita Wischmeijer, Giovanni Romeo, Marco Seri, Pamela Magini, Monica Poscente, Emilio Franzoni, Elena Bacchelli, Daniela Turchetti, Valentina Marchiani, Elisabetta Malaspina, Magini, Pamela, Poscente, Monica, Ferrari, Simona, Vargiolu, Manuela, Bacchelli, Elena, Graziano, Claudio, Wischmeijer, Anita, Turchetti, Daniela, Malaspina, Elisabetta, Marchiani, Valentina, Cordelli, Duccio Maria, Franzoni, Emilio, Romeo, Giovanni, and Seri, Marco
- Subjects
medicine.medical_specialty ,congenital, hereditary, and neonatal diseases and abnormalities ,Xq28 disomy ,Case Report ,Biology ,Bioinformatics ,Biochemistry ,MECP2 ,03 medical and health sciences ,MECP2 duplication ,Genetic ,Gene duplication ,medicine ,Genetics ,Genetics(clinical) ,Recombinant X chromosome ,Molecular Biology ,X chromosome ,Genetics (clinical) ,030304 developmental biology ,Biochemistry, medical ,0303 health sciences ,Macular degeneration ,030305 genetics & heredity ,Biochemistry (medical) ,Cytogenetics ,Chromosome ,Phenotype ,Human genetics ,3. Good health ,Xq28 ,nervous system diseases ,Molecular Medicine - Abstract
BACKGROUND: Duplications of MECP2 gene in males cause a syndrome characterized by distinctive clinical features, including severe to profound mental retardation, infantile hypotonia, mild dysmorphic features, poor speech development, autistic features, seizures, progressive spasticity and recurrent infections. Patients with complex chromosome rearrangements, leading to Xq28 duplication, share most of the clinical features of individuals with tandem duplications, in particular neurologic problems, suggesting a major pathogenetic role of MECP2 overexpression. RESULTS: We performed cytogenetic and molecular cytogenetic studies in a previously described family with affected males showing congenital ataxia, late-onset progressive myoclonic encephalopathy and selective macular degeneration. Microsatellite, FISH and array-CGH analyses identified a recombinant X chromosome with a deletion of the PAR1 region, encompassing SHOX, replaced by a duplicated segment of the Xq28 terminal portion, including MECP2. CONCLUSIONS: Our report describes the identification of the actual genetic cause underlying a severe syndrome that previous preliminary analyses erroneously associated to a terminal Xp22.33 region. In the present family as well as in previously reported patients with similar rearrangements, the observed neurologic phenotype is ascribable to MECP2 duplication, with an undefined contribution of the other involved genes. Maculopathy, presented by affected males reported here, could be a novel clinical feature associated to Xq28 disomy due to recombinant X chromosomes, but at present the underlying pathogenetic mechanism is unknown and this potential clinical correlation should be confirmed through the collection of additional patients.
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