SNP array-based homozygosity mapping reveals MCPH1 deletion in family with autosomal recessive mental retardation and mild microcephaly |
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Authors: | Masoud Garshasbi Mohammad Mahdi Motazacker Kimia Kahrizi Farkhondeh Behjati Seyedeh Sedigheh Abedini Sahar Esmaeeli Nieh Saghar Ghasemi Firouzabadi Christian Becker Franz Rüschendorf Peter Nürnberg Andreas Tzschach Reza Vazifehmand Fikret Erdogan Reinhard Ullmann Steffen Lenzner Andreas W. Kuss H. Hilger Ropers Hossein Najmabadi |
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Affiliation: | (1) Max Planck Institute for Molecular Genetics, Ihnestr. 63–73, 14195 Berlin, Germany;(2) Genetics Research Center, University of Social Welfare and Rehabilitation Sciences, Teheran, Iran;(3) Gene Mapping Center, Max Delbrück Center for Molecular Medicine, Berlin, Germany;(4) Present address: Cologne Center for Genomics and Institute for Genetics, University of Cologne, Cologne, Germany |
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Abstract: | Very little is known about the molecular basis of autosomal recessive MR (ARMR) because in developed countries, small family sizes preclude mapping and identification of the relevant gene defects. We therefore chose to investigate genetic causes of ARMR in large consanguineous Iranian families. This study reports on a family with six mentally retarded members. Array-based homozygosity mapping and high-resolution microarray-based comparative genomic hybridization (array CGH) revealed a deletion of approximately 150–200 kb, encompassing the promoter and the first six exons of the MCPH1 gene, one out of four genes that have been previously implicated in ARMR with microcephaly. Reexamination of affected individuals revealed a high proportion of prematurely condensed chromosomes, which is a hallmark of this condition, but in spite of the severity of the mutation, all patients showed only borderline to mild microcephaly. Therefore the phenotypic spectrum of MCPH1 mutations may be wider than previously assumed, with ARMR being the only consistent clinical finding. |
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