Screening for MECP2 mutations in Spanish patients with an unexplained mental retardation

Rett syndrome (RTT) is an X‐linked progressive encephalopathy. Mutations in the MECP2 (methyl‐CpG‐binding protein) gene have been found to cause RTT. In the past few years, the role of MECP2 mutations in patients with mental disorders other than RTT has been studied, finding that mutations in MECP2...

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Bibliographic Details
Published in:Clinical genetics 2006-08, Vol.70 (2), p.140-144
Main Authors: Tejada, M-I, Peñagarikano, O, Rodriguez-Revenga, L, Martinez-Bouzas, C, García, B, Bádenas, C, Guitart, M, Minguez, M, García-Alegría, E, Sanz-Parra, A, Beristain, E, Milá, M
Format: Article
Language:English
Subjects:
Adult and adolescent clinical studies
Angelman Syndrome - genetics
Biological and medical sciences
Degenerative and inherited degenerative diseases of the nervous system. Leukodystrophies. Prion diseases
Female
General aspects. Genetic counseling
Genetic Testing
Humans
Intellectual deficiency
Intellectual Disability - ethnology
Intellectual Disability - genetics
Male
MECP2 gene
Medical genetics
Medical sciences
mental retardation
Methyl-CpG-Binding Protein 2 - genetics
molecular diagnosis
Mutation
mutation screening
Neurology
Polymorphism, Genetic
Prader-Willi Syndrome - genetics
Psychology. Psychoanalysis. Psychiatry
Psychopathology. Psychiatry
Rett syndrome
Rett Syndrome - genetics
Spain
XLMR
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Summary:Rett syndrome (RTT) is an X‐linked progressive encephalopathy. Mutations in the MECP2 (methyl‐CpG‐binding protein) gene have been found to cause RTT. In the past few years, the role of MECP2 mutations in patients with mental disorders other than RTT has been studied, finding that mutations in MECP2 also contribute to non‐syndromic entities. More recently, it has been demonstrated that RTT shares clinical features with those of Angelman syndrome, another neurodevelopmental disorder. These observations must be confirmed in a large series, to better understand the criteria needed for justifying a molecular test. Consequently, we have searched for MECP2 mutations in 294 patients (43 Angelman and Prader–Willi like included) with mental retardation (MR) of unknown aetiology. We found six polymorphisms (three novel, three previously reported) in 10 patients, one novel unclassified silent change (p.V222V) in a man, and one causative mutation in a girl with MR. Once this case was clinically reviewed, the girl presented symptoms of atypical RTT. The mutation (p.Y141C) lies within the methyl‐binding domain, and has only been reported once in another atypical RTT. Our results show that the MECP2 mutations account for a low frequency (1/416 chromosomes = 0.24%) among mentally retarded individuals, which imply that it is necessary to perform an exhaustive clinical examination of patients before determining whether analysis of MECP2 is required or not.
ISSN:0009-9163
1399-0004
DOI:10.1111/j.1399-0004.2006.00647.x