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No mental retardation in a man with 40% abnormal methylation at the FMR-1 locus and transmission of sperm cell mutations as premutations

We report the case of a mentally normal male carrier of a fragile X full mutation with a ‘methylation mosaic’ hybridization pattern, who carried premutation-size mutations in his sperm cells and transmitted one of them to a daughter. Clinical evaluation of the father revealed a phenotype resembling...

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Published in:	Human molecular genetics 1994-06, Vol.3 (6), p.927-930
Main Authors:	Rousseau, François, Robb, Laura J., Rouillard, Patricia, Kaloustian, Vazken M. Der
Format:	Article
Language:	English
Subjects:	Adult Biological and medical sciences Child Chromosome fragility (bloom syndrome, ataxia telangiectasia, fanconi anemia, x-linked mental retardation...) DNA - genetics DNA - metabolism Female FMR-1 gene Fragile X Mental Retardation Protein fragile X syndrome Fragile X Syndrome - genetics genes Genetic Carrier Screening genotypes Humans Intellectual Disability - genetics Leukocytes - metabolism Male man Medical genetics Medical sciences mental retardation Methylation mutation Nerve Tissue Proteins - genetics Pedigree Phenotype RNA-Binding Proteins - genetics Spermatozoa - physiology transmission
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container_title	Human molecular genetics
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creator	Rousseau, François Robb, Laura J. Rouillard, Patricia Kaloustian, Vazken M. Der
description	We report the case of a mentally normal male carrier of a fragile X full mutation with a ‘methylation mosaic’ hybridization pattern, who carried premutation-size mutations in his sperm cells and transmitted one of them to a daughter. Clinical evaluation of the father revealed a phenotype resembling that of the fragile X syndrome but without mental impairment and 4% fragile sites on cytogenetic analysis. Direct FRAXA genotyping revealed 40% abnormal methylation at the classical Eagl FMR-1 restriction site, a Δ of 400 bp to 1400 bp associated, in the non-methylated region, to a widely spread smear. This is thus a rare occurrence of a male carrier of a fragile X full mutation with significant methylation of the Eagl site and no mental impairment. A permutation of 400 bp was detected in his daughter's leukocytes and analysis of sperm cells from the father revealed a normal spermogram and only 400 bp permutations. This is the first documented case of transmission (with analysis of sperm DNA) of a fragile X mutation from a male carrier of a full fragile X mutation to a girl. This may be due to the early setting apart of progenitor germ cells in males having inherited a permutation from their mother. It is more likely that there could be a strong selection process favouring those cells with a reverted full mutation which produced a small and unmethylated FMR-1 CpG island allowing for re-expression of the FMR-1 gene, especially in male germ cells.
doi_str_mv	10.1093/hmg/3.6.927
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A permutation of 400 bp was detected in his daughter's leukocytes and analysis of sperm cells from the father revealed a normal spermogram and only 400 bp permutations. This is the first documented case of transmission (with analysis of sperm DNA) of a fragile X mutation from a male carrier of a full fragile X mutation to a girl. This may be due to the early setting apart of progenitor germ cells in males having inherited a permutation from their mother. 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Der</creatorcontrib><title>No mental retardation in a man with 40% abnormal methylation at the FMR-1 locus and transmission of sperm cell mutations as premutations</title><title>Human molecular genetics</title><addtitle>Hum Mol Genet</addtitle><description>We report the case of a mentally normal male carrier of a fragile X full mutation with a ‘methylation mosaic’ hybridization pattern, who carried premutation-size mutations in his sperm cells and transmitted one of them to a daughter. Clinical evaluation of the father revealed a phenotype resembling that of the fragile X syndrome but without mental impairment and 4% fragile sites on cytogenetic analysis. Direct FRAXA genotyping revealed 40% abnormal methylation at the classical Eagl FMR-1 restriction site, a Δ of 400 bp to 1400 bp associated, in the non-methylated region, to a widely spread smear. This is thus a rare occurrence of a male carrier of a fragile X full mutation with significant methylation of the Eagl site and no mental impairment. A permutation of 400 bp was detected in his daughter's leukocytes and analysis of sperm cells from the father revealed a normal spermogram and only 400 bp permutations. This is the first documented case of transmission (with analysis of sperm DNA) of a fragile X mutation from a male carrier of a full fragile X mutation to a girl. This may be due to the early setting apart of progenitor germ cells in males having inherited a permutation from their mother. It is more likely that there could be a strong selection process favouring those cells with a reverted full mutation which produced a small and unmethylated FMR-1 CpG island allowing for re-expression of the FMR-1 gene, especially in male germ cells.</description><subject>Adult</subject><subject>Biological and medical sciences</subject><subject>Child</subject><subject>Chromosome fragility (bloom syndrome, ataxia telangiectasia, fanconi anemia, x-linked mental retardation...)</subject><subject>DNA - genetics</subject><subject>DNA - metabolism</subject><subject>Female</subject><subject>FMR-1 gene</subject><subject>Fragile X Mental Retardation Protein</subject><subject>fragile X syndrome</subject><subject>Fragile X Syndrome - genetics</subject><subject>genes</subject><subject>Genetic Carrier Screening</subject><subject>genotypes</subject><subject>Humans</subject><subject>Intellectual Disability - genetics</subject><subject>Leukocytes - metabolism</subject><subject>Male</subject><subject>man</subject><subject>Medical genetics</subject><subject>Medical sciences</subject><subject>mental retardation</subject><subject>Methylation</subject><subject>mutation</subject><subject>Nerve Tissue Proteins - genetics</subject><subject>Pedigree</subject><subject>Phenotype</subject><subject>RNA-Binding Proteins - genetics</subject><subject>Spermatozoa - physiology</subject><subject>transmission</subject><issn>0964-6906</issn><issn>1460-2083</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>1994</creationdate><recordtype>article</recordtype><recordid>eNqFkUFv1DAQhS0EKtvCiTOSD8AFZWvHsR0fq4q2iAVEAWnVizVxJmwgThbbEfQf8LPxsqu9chqN3jejefMIecbZkjMjzjf-27lYqqUp9QOy4JViRclq8ZAsmFFVoQxTj8lpjN8Z46oS-oScaCN5KcyC_PkwUY9jgoEGTBBaSP000n6kQD2M9FefNrRiLyk04xR8xjymzf2wxyDRtEF69f624HSY3BwpjC1NAcbo-xh3zNTRuMXgqcMhT8_p32gGI90GPPZPyKMOhohPD_WMfL168-Xyplh9vH57ebEqXGl0KjrkwlVtJduu7rQ22rQCygayU4OccyydkQ5ZpSWiZLrRXHYaGuQKDHAhzsir_d5tmH7OGJPNh-5OgxGnOVqt8m-Yrv8LcmW4lHWVwdd70IUpxoCd3YbeQ7i3nNldQDYHZIVVNgeU6eeHtXPjsT2yh0Sy_uKgQ3QwdPmVro9HrOKlFHJno9hjfUz4-yhD-GGVFlram_WdrdefP929u13ZtfgLR-WpSA</recordid><startdate>199406</startdate><enddate>199406</enddate><creator>Rousseau, François</creator><creator>Robb, Laura J.</creator><creator>Rouillard, Patricia</creator><creator>Kaloustian, Vazken M. 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Direct FRAXA genotyping revealed 40% abnormal methylation at the classical Eagl FMR-1 restriction site, a Δ of 400 bp to 1400 bp associated, in the non-methylated region, to a widely spread smear. This is thus a rare occurrence of a male carrier of a fragile X full mutation with significant methylation of the Eagl site and no mental impairment. A permutation of 400 bp was detected in his daughter's leukocytes and analysis of sperm cells from the father revealed a normal spermogram and only 400 bp permutations. This is the first documented case of transmission (with analysis of sperm DNA) of a fragile X mutation from a male carrier of a full fragile X mutation to a girl. This may be due to the early setting apart of progenitor germ cells in males having inherited a permutation from their mother. 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subjects	Adult Biological and medical sciences Child Chromosome fragility (bloom syndrome, ataxia telangiectasia, fanconi anemia, x-linked mental retardation...) DNA - genetics DNA - metabolism Female FMR-1 gene Fragile X Mental Retardation Protein fragile X syndrome Fragile X Syndrome - genetics genes Genetic Carrier Screening genotypes Humans Intellectual Disability - genetics Leukocytes - metabolism Male man Medical genetics Medical sciences mental retardation Methylation mutation Nerve Tissue Proteins - genetics Pedigree Phenotype RNA-Binding Proteins - genetics Spermatozoa - physiology transmission
title	No mental retardation in a man with 40% abnormal methylation at the FMR-1 locus and transmission of sperm cell mutations as premutations
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