Your search keyword '"Milà, M."' showing total 17 results

1. Mutations in JMJD1C are involved in Rett syndrome and intellectual disability.

Author

Sáez MA, Fernández-Rodríguez J, Moutinho C, Sanchez-Mut JV, Gomez A, Vidal E, Petazzi P, Szczesna K, Lopez-Serra P, Lucariello M, Lorden P, Delgado-Morales R, de la Caridad OJ, Huertas D, Gelpí JL, Orozco M, López-Doriga A, Milà M, Perez-Jurado LA, Pineda M, Armstrong J, Lázaro C, and Esteller M

Subjects

Adult, Amino Acid Motifs, Amino Acid Sequence, Autism Spectrum Disorder diagnosis, Autism Spectrum Disorder genetics, Brain metabolism, Brain pathology, Conserved Sequence, DNA Mutational Analysis, Female, Gene Expression, Gene Order, Genetic Association Studies, Genetic Loci, Humans, Intellectual Disability diagnosis, Jumonji Domain-Containing Histone Demethylases chemistry, Jumonji Domain-Containing Histone Demethylases metabolism, Male, Middle Aged, Models, Molecular, Neurons metabolism, Oxidoreductases, N-Demethylating chemistry, Oxidoreductases, N-Demethylating metabolism, Position-Specific Scoring Matrices, Protein Conformation, Protein Transport, Rett Syndrome diagnosis, Intellectual Disability genetics, Jumonji Domain-Containing Histone Demethylases genetics, Mutation, Oxidoreductases, N-Demethylating genetics, Rett Syndrome genetics

Abstract

Purpose: Autism spectrum disorders are associated with defects in social response and communication that often occur in the context of intellectual disability. Rett syndrome is one example in which epilepsy, motor impairment, and motor disturbance may co-occur. Mutations in histone demethylases are known to occur in several of these syndromes. Herein, we aimed to identify whether mutations in the candidate histone demethylase JMJD1C (jumonji domain containing 1C) are implicated in these disorders., Methods: We performed the mutational and functional analysis of JMJD1C in 215 cases of autism spectrum disorders, intellectual disability, and Rett syndrome without a known genetic defect., Results: We found seven JMJD1C variants that were not present in any control sample (~ 6,000) and caused an amino acid change involving a different functional group. From these, two de novo JMJD1C germline mutations were identified in a case of Rett syndrome and in a patient with intellectual disability. The functional study of the JMJD1C mutant Rett syndrome patient demonstrated that the altered protein had abnormal subcellular localization, diminished activity to demethylate the DNA damage-response protein MDC1, and reduced binding to MECP2. We confirmed that JMJD1C protein is widely expressed in brain regions and that its depletion compromises dendritic activity., Conclusions: Our findings indicate that mutations in JMJD1C contribute to the development of Rett syndrome and intellectual disability.Genet Med 18 1, 378-385.

Published

2016

2. Contribution of common and rare variants of the PTCHD1 gene to autism spectrum disorders and intellectual disability.

Author

Torrico B, Fernàndez-Castillo N, Hervás A, Milà M, Salgado M, Rueda I, Buitelaar JK, Rommelse N, Oerlemans AM, Bralten J, Freitag CM, Reif A, Battaglia A, Mazzone L, Maestrini E, Cormand B, and Toma C

Subjects

Case-Control Studies, Cell Line, Tumor, Female, Humans, Male, Membrane Proteins metabolism, Mutation, Missense, Promoter Regions, Genetic, Trinucleotide Repeats, Autism Spectrum Disorder genetics, Intellectual Disability genetics, Membrane Proteins genetics, Polymorphism, Single Nucleotide

Abstract

Recent findings revealed rare copy number variants and missense changes in the X-linked gene PTCHD1 in autism spectrum disorder (ASD) and intellectual disability (ID). Here, we aim to explore the contribution of common PTCHD1 variants in ASD and gain additional evidence for the role of rare variants of this gene in ASD and ID. A two-stage case-control association study investigated 28 tag single nucleotide polymorphisms (SNPs) in 994 ASD cases and 1035 controls from four European populations. Mutation screening was performed in 673 individuals who included 240 ASD cases, 183 ID patients and 250 controls. The case-control association study showed a significant association with rs7052177 (P=6.13E-4) in the ASD discovery sample that was replicated in an independent sample (P=0.03). A Mantel-Haenszel meta-analysis for rs7052177T considering the four European populations showed an odds ratio of 0.58 (P=7E-05). This SNP is predicted to be located in a transcription factor binding site. No rare missense PTCHD1 variants were found in our ASD cohort and only one was identified in the ID sample. A duplication (27 bp) in the promoter region, absent from 590 controls, was found in three ASD patients (Fisher exact test, P=0.024). A gene reporter assay showed a significant decrease in the transcriptional activity (26%) driven by this variant. Moreover, we found that the longest allele of a trinucleotide repeat located upstream from PTCHD1 was associated with ASD (P=0.003, permP=0.0186). Our results further support the involvement of PTCHD1 in ASD, suggesting that both common and rare variants contribute to the disorder.

Published

2015

3. Efficient application of next-generation sequencing for the diagnosis of rare genetic syndromes.

Author

Madrigal I, Alvarez-Mora MI, Karlberg O, Rodríguez-Revenga L, Elurbe DM, Rabionet R, Mur A, Pie J, Ballesta F, Sauer S, Syvänen AC, and Milà M

Subjects

Adult, Exome, Female, Humans, Male, Pedigree, Syndrome, Transcriptome, DNA Mutational Analysis methods, Gene Expression Profiling methods, Intellectual Disability genetics

Abstract

Aims: The causes of intellectual disability, which affects 1%-3% of the general population, are highly heterogeneous and the genetic defect remains unknown in around 40% of patients. The application of next-generation sequencing is changing the nature of biomedical diagnosis. This technology has quickly become the method of choice for searching for pathogenic mutations in rare uncharacterised genetic diseases., Methods: Whole-exome sequencing was applied to a series of families affected with intellectual disability in order to identify variants underlying disease phenotypes., Results: We present data of three families in which we identified the disease-causing mutations and which benefited from receiving a clinical diagnosis: Cornelia de Lange, Cohen syndrome and Dent-2 disease. The genetic heterogeneity and the variability in clinical presentation of these disorders could explain why these patients are difficult to diagnose., Conclusions: The accessibility to next-generation sequencing allows clinicians to save much time and cost in identifying the aetiology of rare diseases. The presented cases are excellent examples that demonstrate the efficacy of next-generation sequencing in rare disease diagnosis., (Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://group.bmj.com/group/rights-licensing/permissions.)

Published

2014

4. Screening individuals with intellectual disability, autism and Tourette's syndrome for KCNK9 mutations and aberrant DNA methylation within the 8q24 imprinted cluster.

Author

Sánchez Delgado M, Camprubí C, Tümer Z, Martínez F, Milà M, and Monk D

Subjects

Epigenesis, Genetic, Gene Frequency genetics, Genetic Predisposition to Disease, Humans, Mutation, Polymorphism, Single Nucleotide genetics, Autistic Disorder genetics, Chromosomes, Human, Pair 8 genetics, DNA Methylation genetics, Genetic Testing, Genomic Imprinting genetics, Intellectual Disability genetics, Potassium Channels, Tandem Pore Domain genetics, Tourette Syndrome genetics

Abstract

The phenotype overlap between autism spectrum disorders (ASD) & intellectual disabilities (ID) is mirrored at the genetic level, with common genes being reported mutated in variety of developmental disabilities. However despite widespread genetic screening for mutations, in approximately 40-60% of childhood developmental disorders the genetic cause remains unknown. Several genome-wide linkage screens in ASD have identified a locus mapping to distal 8q. We have recently identified a novel brain-specific imprinted cluster at this location, which contains the reciprocally expressed maternal KCNK9 and paternally expressed non-coding PEG13 transcripts, the latter located within an intron of TRAPPC9. Interestingly, mutations of KCNK9 and TRAPPC9 have been reported in Birk-Barel mental retardation and non-syndromic familial forms of ID, respectively. Here, we report a genetic screen for KCNK9 coding mutations and potential epigenetic aberrations that could result in deregulated imprinting in a cohort of 120 ID, 86 ASD and 86 Tourette syndrome patients. Fifteen of the ID patients had clinical characteristics overlapping with Birk-Barel syndrome. Sequencing of the two coding exons of KCNK9 failed to identify pathologic mutations, with only one variant, rs2615374, being present with allele frequencies similar to those described in dbSNP database. DNA methylation profiling of the KCNK9 and TRAPPC9 promoters, the maternally methylated PEG13 DMR and a long-range enhancer region were normal in all patients. Our findings suggest that mutations of KCNK9 or epigenetic disturbances within the PEG13 imprinted cluster do not significantly contribute to the cause of the developmental disabilities tested in this study., (© 2014 Wiley Periodicals, Inc.)

Published

2014

5. 15q11.2 microdeletion and FMR1 premutation in a family with intellectual disabilities and autism.

Author

Madrigal I, Rodríguez-Revenga L, Xunclà M, and Milà M

Subjects

Child, Comparative Genomic Hybridization, Family, Female, Humans, Male, RNA, Messenger genetics, Real-Time Polymerase Chain Reaction, Autistic Disorder genetics, Chromosome Aberrations, Chromosomes, Human, Pair 15 genetics, Fragile X Mental Retardation Protein genetics, Intellectual Disability genetics, Mutation genetics

Abstract

Genomic rearrangements of chromosome 15q11-q13 are responsible for diverse phenotypes including intellectual disabilities and autism. 15q11.2 deletion, implicating common PWS/AS breakpoints BP1-BP2, has been described in patients with delayed motor and speech development and behavioural problems. Here we report the clinical and molecular characterisation of a maternally inherited BP1-BP2 deletion in two siblings with intellectual, motor and speech delay, autistic syndrome disorder and several dysmorphic features. One of the patients was also a carrier of an FMR1 allele in the low premutation range. The four genes within the deletion were under-expressed in all deletion carriers but FMR1 mRNA levels remained normal. Our results suggest that BP1-BP2 deletion could be considered as a risk factor for neuropsychological phenotypes and that it presents with variable clinical expressivity., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2012

6. A170P mutation in SHOX gene in a patient not presenting with Madelung deformity.

Author

Alvarez-Mora MI, Madrigal I, Rodriguez-Revenga L, Mur A, Calvo D, Pascual I Bardají J, and Milà M

Subjects

Adult, Comparative Genomic Hybridization, DNA Mutational Analysis, Female, Genetic Predisposition to Disease, Heterozygote, Humans, Phenotype, Polymerase Chain Reaction, Short Stature Homeobox Protein, Growth Disorders genetics, Homeodomain Proteins genetics, Intellectual Disability genetics, Mutation, Osteochondrodysplasias genetics

Abstract

Idiopathic short stature is a multifactorial disease caused by defects in several genes. Among them, short stature homeobox-containing gene (SHOX) mutations have an incidence of 2%-15% within the idiopathic short population. The authors report a patient with moderate intellectual disability, short stature and no other radiological traits referred for subtelomeric screening. MLPA and sequencing results showed a heterozygous mutation in SHOX gene (A170P). This mutation has been described to fully cosegregate with Madelung deformity in patients affected with Léri-Weill dyschondrosteosis and Langer mesomelic dysplasia. The authors report the first case of idiopathic short stature due to the A170P mutation in a patient without any radiological trait. The A170P mutation is the most prevalent mutation in the Spanish gypsy population affected with short stature disorders. The authors strongly recommend SHOX screening for deletions, duplications and point mutations in patients affected with short stature although they do not present any radiological traits.

Published

2012

7. 12p13 rearrangements: 6 Mb deletion responsible for ID/MCA and reciprocal duplication without clinical responsibility.

Author

Madrigal I, Martinez M, Rodriguez-Revenga L, Carrió A, and Milà M

Subjects

Family, Humans, Segmental Duplications, Genomic, Translocation, Genetic, Chromosomes, Human, Pair 12 genetics, Gene Rearrangement, Intellectual Disability genetics, Sequence Deletion

Abstract

Congenital balanced reciprocal translocations are one of the most frequent structural chromosomal aberrations in the population. We report a familial translocation t(12;22)(p13.3;pter) responsible for intellectual disabilities and congenital anomalies characterized by FISH and array CGH. Two patients carried a der(12)t(12;22)(p13.3;pter), resulting in a 6 Mb 12pter deletion. Patients presented with intellectual disabilities, pre- and post-natal growth retardation, ponderal development delay, global hypotonia, feeding problems and dysmorphic features. Two relatives presented with the reciprocal 12pter duplication, which had no clinical manifestations associated. For this translocation, we propose a mechanism based on a non-allelic recombination model, in which recombination of direct oriented segmental duplications between non-homologous chromatids leads to the reciprocal translocation. The characterization of this translocation has been critical for the family. Translocation carriers have a risk of 40% of having offspring carrying unbalanced products. 12p13.3 deletion carriers present with a recognizable syndrome and on the contrary, 12p13.3 duplication carriers present without clinical manifestations. Other published cases of 12p13.3 duplication show that this syndrome has a variable phenotype. It is advisable to delineate the duplication size and to discard other genetic aberrations, in order to give an accurate genetic counseling in patients carrying 12pter duplications., (Copyright © 2012 Wiley Periodicals, Inc.)

Published

2012

8. [A study of subtelomeric rearrangements in 300 patients with mental retardation and multiple congenital anomalies: their clinical and molecular characterisation].

Author

Madrigal I, Rodríguez-Revenga L, Costa L, Xunclà M, Sánchez A, and Milà M

Subjects

Comparative Genomic Hybridization, Genetic Counseling, Genetic Predisposition to Disease, Humans, In Situ Hybridization, Fluorescence, Mass Screening, Abnormalities, Multiple genetics, Chromosome Aberrations, DNA Mutational Analysis methods, Gene Rearrangement, Intellectual Disability genetics

Abstract

Introduction: The study of mental retardation is one of the most complex fields in human genetics due to its high degree of clinical and genetic heterogeneity. About 50% of cases of mental retardation remain undiagnosed. It is known that about 6-10% of cases are due to subtelomeric rearrangements. Some of these are responsible for a clinically recognized phenotype, i.e. 1p36 or 22q13.33 microdeletion syndromes, but others affect few patients and are not well characterized., Patients and Methods: We have analyzed 300 consecutive mentally retarded patients for subtelomeric rearrangements by MLPA., Results: About 5.3% of patients presented subtelomeric rearrangements; from these, 75% contained de novo rearrangements and 18.7% included inherited aberrations from a healthy parent. In 14 cases, aberrations were likely related to disease and in two cases were putative polymorphisms., Conclusions: This study confirms the high frequency of subtelomeric rearrangements in mental retardation and reinforces the idea of a routine subtelomeric screening in these patients in order to get a correct diagnosis, establish genotype-phenotype correlations and offer an accurate genetic counseling.

Published

2010

9. Deletion of the OPHN1 gene detected by aCGH.

Author

Madrigal I, Rodríguez-Revenga L, Badenas C, Sánchez A, and Milà M

Subjects

Base Sequence genetics, Humans, Male, Nucleic Acid Hybridization methods, Polymerase Chain Reaction, Sequence Deletion genetics, Cytoskeletal Proteins genetics, GTPase-Activating Proteins genetics, Intellectual Disability genetics, Nuclear Proteins genetics

Abstract

Background: The oligophrenin 1 gene (OPHN1) is an Rho-GTPase-activating protein involved in the regulation of the G-protein cycle required for dendritic spine morphogenesis. Mutations in this gene are implicated in X-linked mental retardation (XLMR)., Methods: We report a deletion spanning exons 21 and 22 of the OPHN1 gene identified by a tiling path X-chromosome array comparative genomic hybridization (CGH) and multiplex ligation-dependent probe amplification, confirmed by polymerase chain reaction (PCR), in a family with four males with intellectual disabilities., Results: Patients harbouring mutations in this gene share the same clinical manifestations reinforcing the idea of a syndromic XLMR. The most important neurological findings are cerebellar hypoplasia and ventriculomegaly., Conclusions: We recommend screening of the OPHN1 gene in male patients with XLMR and cerebellar anomalies. This case highlights the value of high-resolution techniques as Multiplex Ligation Probe Amplification (MLPA) and CGH array for a better characterization of copy number changes and suggests that MLPA technology may be very useful for an initial screening of small deletions and duplications in XLMR patients.

Published

2008

10. A novel mutation in JARID1C gene associated with mental retardation.

Author

Santos C, Rodriguez-Revenga L, Madrigal I, Badenas C, Pineda M, and Milà M

Subjects

Amino Acid Sequence, Base Sequence, Chromosomes, Human, X, DNA Mutational Analysis, Exons, Genetic Linkage, Histone Demethylases, Humans, Male, Molecular Sequence Data, Oxidoreductases, N-Demethylating, Pedigree, Phenotype, Protein Structure, Tertiary, Intellectual Disability genetics, Mutation, Proteins genetics

Abstract

X-linked mental retardation (XLMR) is an extremely heterogeneous condition that account for 15-25% of all mentally retarded patients. The number of genes newly reported in relation with this condition has been rapidly increased in the past years. One of the latest is called Jumonji AT-rich interactive domain 1C (JARID1C). This gene encodes for a member of a recently discovered protein family that harbours DNA-binding motifs, suggesting a possible role in transcriptional regulation and in the modification of chromatin structure. In this work we describe the results obtained by screening JARID1C gene in 24 mentally retarded males with history of at least two affected males. Remarkably, we have found a novel missense mutation in exon 10 of the gene that results in a Serine-to-arginine change at amino-acid 451 (S451R). This nucleotide change appears to be restricted to mentally retarded patients, since it has not been detected in control samples. Familial analysis has confirmed the segregation of this mutation with mental retardation. Furthermore, sequence alignment analysis with the different members of the human JARID1 family and with homologous proteins of mouse and fruit fly has revealed that the affected amino acid is conserved. Our data highlights the importance of reporting mutations in this gene since it might support the recent findings that implicates JARID1C with XLMR.

Published

2006

11. Cryptic chromosomal rearrangement screening in 30 patients with mental retardation and dysmorphic features.

Author

Rodriguez-Revenga L, Badenas C, Sánchez A, Mallolas J, Carrió A, Pedrinaci S, Barrionuevo JL, and Milà M

Subjects

Adolescent, Adult, Child, Child, Preschool, Face abnormalities, Female, Gene Rearrangement, Humans, Intellectual Disability complications, Male, Syndrome, Telomere genetics, Chromosomes, Human, Pair 1 genetics, Chromosomes, Human, Pair 13 genetics, Genetic Testing, In Situ Hybridization, Fluorescence methods, Intellectual Disability genetics, Translocation, Genetic genetics

Abstract

Mental retardation affects 1-3% of the general population, and the genetic causes in many cases are unknown. Cytogenetically undetected chromosomal imbalances have been indicated as an explanation. Nowadays, due to the development of molecular cytogenetic techniques, it is possible to identify cryptic rearrangements involving the ends of chromosomes. We report a screening using chromosome-specific telomere fluorescence in-situ hybridization (FISH) probes, in a group of 30 patients with a well-characterized phenotype including mental retardation, dysmorphic features, and a normal karyotype. Among them, two subtelomeric rearrangements have been detected and characterized. One of them is a de novo deletion of 1p36, which has been previously described as a new contiguous gene syndrome. The second is an unbalanced product of a cryptic translocation involving chromosomes 1 and 13, which results in a partial 1q trisomy and partial 13q monosomy. These findings highlight, the importance of searching for cryptic subtelomeric rearrangements in non-syndromic mentally retarded patients.

Published

2004

12. Linkage analysis in Spanish families with nonspecific X-linked mental retardation: Significant linkage at Xq13-q21.

Author

Badenas C, Castellví-Bel S, Volpini V, Jiménez D, Sánchez A, Estivill X, and Milà M

Subjects

DNA genetics, Family Health, Female, Genetic Linkage, Humans, Male, Microsatellite Repeats, Pedigree, Software, Spain, Intellectual Disability genetics, X Chromosome genetics

Abstract

Mental retardation (MR) is a genetically heterogeneous, clinically variable condition. Many cases of MR are linked to the X chromosome. The aim of this study was to identify candidate loci for nonspecific MR in Spanish samples. We selected seven families with nonspecific MR and a pattern of inheritance compatible with an X-linked disorder and a group of 26 sib pairs of mentally retarded individuals. We performed linkage analysis with a panel of 15 markers evenly distributed along the X chromosome. The study showed linkage to marker DXS8076, located in Xq21.1, by the lod score method (z = 2.11 at straight theta = 0.155) and the nonparametric extended relative pair analysis method (chi(2) = 5.32; P < 0.03). Genetic heterogeneity was found, with an estimated 75% of the families linked at recombination fraction straight theta = 0.10 to the DXS8076 locus (chi(2) = 9.51; P < 0.009). Xq13-q21 is one of the critical regions for X-linked MR previously reported, and our study supports the idea that this region may contain a locus for MR in Spanish patients., (Copyright 2001 Wiley-Liss, Inc.)

Published

2001

13. Genes responsible for nonspecific mental retardation.

Author

Castellví-Bel S and Milà M

Subjects

Cloning, Molecular, Exons, Female, Fragile X Syndrome genetics, Humans, Male, Models, Genetic, X Chromosome, Intellectual Disability genetics

Abstract

Mental retardation (MR) is a group of heterogeneous clinical conditions. There are more than 900 genetic disorders associated with MR and it affects around 3% of the general population. MR can be subdivided into syndromic, if it is characterized by consistent and distinctive clinical findings, and nonspecific, if mental retardation is the only primary symptom among affected individuals. Many MR conditions described are syndromic, fragile X syndrome being the most common clinical entity among them. In the past years, knowledge of the molecular basis of mental retardation has increased remarkably. Eight genes involved in nonspecific X-linked MR have been identified so far, including FMR2, OPHN1, GDI1, PAK3, IL1RAPL, TM4SF2, VCX-A, and ARHGEF6. Two other genes also located on the X chromosome have been involved both in syndromic and in MRX forms (RSK2 and XNP/ATR-X). New insights into the pathogenesis of mental retardation are being provided by the discovery of these genes involved in different cellular signaling pathways in the central nervous system although many others remain to be identified., (Copyright 2001 Academic Press.)

Published

2001

14. Molecular study of the PAK3 and GDI1 genes in nonsyndromic X-linked mental retardation spanish patients.

Author

Rifé M, Mallolas J, Castellví-Bel S, Badenas C, Jiménez D, and Milà M

Subjects

Base Sequence, DNA chemistry, DNA genetics, DNA Mutational Analysis, Family Health, Genetic Linkage, Humans, Polymorphism, Genetic, Polymorphism, Single-Stranded Conformational, Spain, p21-Activated Kinases, Guanine Nucleotide Dissociation Inhibitors genetics, Intellectual Disability genetics, Protein Serine-Threonine Kinases genetics, X Chromosome genetics

Published

2000

15. Detection of the fragile X syndrome protein for the evaluation of FMR1 intermediate alleles.

Author

Castellví-Bel S, Fernández-Burriel M, Rifé M, Jiménez D, Mallolas J, Sánchez A, Ramos F, and Milà M

Subjects

Alleles, Child, Child, Preschool, Fragile X Mental Retardation Protein, Genetic Testing, Humans, Nerve Tissue Proteins metabolism, Fragile X Syndrome metabolism, Intellectual Disability genetics, Nerve Tissue Proteins genetics, RNA-Binding Proteins, Trinucleotide Repeat Expansion genetics

Abstract

Molecular screening programs in mentally retarded individuals have been performed in several populations worldwide. One finding has been an excess of FMR1 intermediate alleles in a population with learning difficulties. However, other published reports with similar characteristics did not corroborate those previous results. In order to contribute additional data from our population, we studied 563 patients affected with nonspecific mental retardation (MRX) that did not present a CGG expansion in the FMR1 gene and 208 individuals as a control population. Forty MRX patients presented alleles within the intermediate range. Among them, one case showed a pattern of expression of the FMR1 protein (FMRP) concordant with a fragile X syndrome case with an intermediate allele/full mutation mosaicism, although it was not detected by Southern blot analysis. Statistical analysis was performed again showing no statistically significant difference regarding the intermediate allele frequency in the MRX and control populations. This finding is in agreement with the hypothesis that the incidence of intermediate FMR1 alleles in MRX populations does not seem to be higher than in control populations, and it emphasizes the importance of FMRP detection as a diagnostic tool for fragile X syndrome.

Published

2000

16. A female compound heterozygote (pre- and full mutation) for the CGG FMR1 expansion.

Author

Milà M, Castellví-Bel S, Giné R, Vazquez C, Badenas C, Sánchez A, and Estivill X

Subjects

Adult, Atlantic Islands, Chromosome Mapping, Female, Fragile X Mental Retardation Protein, Humans, Male, Methylation, Pedigree, RNA-Binding Proteins genetics, Reference Values, X Chromosome, Fragile X Syndrome genetics, Genetic Carrier Screening, Intellectual Disability genetics, Mutation, Nerve Tissue Proteins genetics, Trinucleotide Repeats

Abstract

Fragile X syndrome is the most common cause of inherited mental retardation. The incidence has been estimated to be 1 in 1250 males and 1 in 2000 females. Molecular studies have shown that 95% of fragile X syndrome cases are caused by the expansion of a CGG triplet in the FMR1 gene with hypermethylation of the adjacent CpG island. In spite of the high incidence of this syndrome, a female with both FMR1 genes in the expanded form has never been reported. We presenting mental retardation and attention problems. Molecular analysis has revealed that both of her FMR1 genes have the CGG expansion, one with a premutation and the other with a full mutation. We have studied the CGG repeat in the FMR1 gene in 64 members of her family and detected 33 normal individuals, 14 carriers with the premutation (1 male and 13 females), and 18 individuals with full mutations (8 males and 10 females). The index case illustrates that the possibility of both parents being carriers of the fragile X syndrome premutation should be considered in consanguineous families or in small communities.

Published

1996

17. Molecular testing for fragile X: Analysis of 5062 tests from 1105 fragile X families - Performed in 12 clinical laboratories in Spain

Author

María-Teresa Calvo, Elizabet Pintado, Yolanda de Diego-Otero, Jordi Rosell, G. Glover, Francisco Martínez, María-Antonia Ramos-Arroyo, Montserrat Milà, Carmen Ayuso, Isabel Fernandez-Carvajal, Miriam Guitart, Concepción Hernández-Chico, Maria-Isabel Tejada, Feliciano J. Ramos, Hiart Maortua, Ministerio de Sanidad, Servicios Sociales e Igualdad (España), Asociación Girmogen (España), [Tejada,MI, and Maortua,H] Laboratorio de Genetica Molecular, Servicio de Genética, Hospital Universitario Cruces, BioCruces Health Research Institute, GCV-CIBER de Enfermedades Raras (CIBERER-ISCIII), Barakaldo, Bizkaia, Spain. [Glover,G] Unidad de Genetica Molecular, Centro de Bioquímica y Genetica Clínica, Hospital Clínico Universitario Virgen de la Arrixaca, El Palmar, Murcia, Spain. [Martínez,F] Unidad de Genetica, Hospital Universitario La Fe, Valencia, Spain. [Guitart,M] Laboratorio de Genetica, UDIAT-Centre Diagnóstic, Corporaciò Sanitária Parc Taulí, Institut Universitari UAB, Sabadell, Barcelona, Spain. [Diego-Otero,Y de] Unidad de Gestion Clínica de Salud Mental, Hospital Regional Universitario de Malaga, Instituto de Investigacion Biomédica de Málaga (IBIMA), Málaga, Spain. [Fernández-Carvajal] Instituto de Biología y Genetica Molecular (IBGM), Universidad de Valladolid, CSIC, Valladolid, Spain. [Ramos,FJ] Consulta de Genetica Clínica, Servicio de Pediatría, Hospital Clínico Universitario Lozano Blesa, Facultad de Medicina, Universidad de Zaragoza, GCV-CIBER de Enfermedades Raras (CIBERER-ISCIII), Zaragoza, Spain. [Hernández-Chico,C] Servicio de Genetica, Hospital Ramón y Cajal, Madrid, Spain. [Pintado,E] Servicio de Biología Molecular, Hospital Virgen Macarena y Universidad de Sevilla, Sevilla, Spain. [Rosell,J] Servicio de Genetica, Hospital Universitari Son Espases, GCV-CIBER de Enfermedades Raras (CIBERER-ISCIII), Palma de Mallorca, Illes Balears, Spain. [Calvo,MT] Unidad de Genetica Médica, Hospital Universitario Miguel Servet, Zaragoza, Spain. [Ayuso,C] Servicio de Genetica, IIS-Hospital Universitario Fundacion Jiménez Díaz (IIS-FJD, UAM), CIBER de Enfermedades Raras (CIBERER-ISCIII), Madrid, Spain. [Ramos-Arroyo,MA] Servicio de Genetica, Complejo Hospitalario de Navarra, Pamplona, Spain. [Milà,M] Servicio de Bioquímica y Genetica Molecular, Hospital Clinic, IDIBAPS, CIBER de Enfermedades Raras (CIBERER-ISCIII), Barcelona, Spain.

Subjects

Male, alelos, Síndrome del cromosoma X frágil, Fragile x, sistema de registros, humanos, España, adolescente, lcsh:Medicine, ComputingMilieux_LEGALASPECTSOFCOMPUTING, frecuencia génica, Named Groups::Persons::Age Groups::Adult::Middle Aged [Medical Subject Headings], Organisms::Eukaryota::Animals::Chordata::Vertebrates::Mammals::Primates::Haplorhini::Catarrhini::Hominidae::Humans [Medical Subject Headings], Gene Frequency, Intellectual disability, Registries, Child, Full mutation, mediana edad, síndrome del cromosoma X frágil, Geographicals::Geographic Locations::Europe::Spain [Medical Subject Headings], Genetics, Named Groups::Persons::Age Groups::Child::Child, Preschool [Medical Subject Headings], Analytical, Diagnostic and Therapeutic Techniques and Equipment::Investigative Techniques::Genetic Techniques::Genetic Testing [Medical Subject Headings], General Medicine, adulto, Middle Aged, Fragile X syndrome, Child, Preschool, Named Groups::Persons::Age Groups::Adolescent [Medical Subject Headings], Female, Sistema de registros, Named Groups::Persons::Age Groups::Infant [Medical Subject Headings], Alelos, Pruebas genéticas, Research Article, Adult, Adolescent, Article Subject, Offspring, Genetic counseling, Check Tags::Male [Medical Subject Headings], Biology, Named Groups::Persons::Age Groups::Infant::Infant, Newborn [Medical Subject Headings], General Biochemistry, Genetics and Molecular Biology, Named Groups::Persons::Age Groups::Adult [Medical Subject Headings], medicine, Humans, Diseases::Congenital, Hereditary, and Neonatal Diseases and Abnormalities::Congenital Abnormalities::Chromosome Disorders::Sex Chromosome Disorders::Fragile X Syndrome [Medical Subject Headings], pruebas genéticas, Genetic Testing, Allele, Alleles, Phenomena and Processes::Genetic Phenomena::Genetic Structures::Genome::Genome Components::Genes::Alleles [Medical Subject Headings], Named Groups::Persons::Age Groups::Child [Medical Subject Headings], lactante, General Immunology and Microbiology, lcsh:R, Infant, Newborn, Infant, medicine.disease, Frecuencia génica, Check Tags::Female [Medical Subject Headings], Spain, Fragile X Syndrome, Data_GENERAL, Analytical, Diagnostic and Therapeutic Techniques and Equipment::Investigative Techniques::Epidemiologic Methods::Data Collection::Registries [Medical Subject Headings], Klinefelter syndrome, Phenomena and Processes::Genetic Phenomena::Gene Frequency [Medical Subject Headings]

Abstract

This is an open access article distributed under the Creative Commons Attribution License.-- et al., Fragile X syndrome is the most common inherited form of intellectual disability. Here we report on a study based on a collaborative registry, involving 12 Spanish centres, of molecular diagnostic tests in 1105 fragile X families comprising 5062 individuals, of whom, 1655 carried a full mutation or were mosaic, three cases had deletions, 1840 had a premutation, and 102 had intermediate alleles. Two patients with the full mutation also had Klinefelter syndrome. We have used this registry to assess the risk of expansion from parents to children. From mothers with premutation, the overall rate of allele expansion to full mutation is 52.5%, and we found that this rate is higher for male than female offspring (63.6% versus 45.6%; P < 0.001). Furthermore, in mothers with intermediate alleles (45-54 repeats), there were 10 cases of expansion to a premutation allele, and for the smallest premutation alleles (55-59 repeats), there was a 6.4% risk of expansion to a full mutation, with 56 repeats being the smallest allele that expanded to a full mutation allele in a single meiosis. Hence, in our series the risk for alleles of < 59 repeats is somewhat higher than in other published series. These findings are important for genetic counselling. © 2014 María-Isabel Tejada et al., Thanks are due to the agreements between GIRMOGEN and the Real Patronato sobre Discapacidad of the Spain’s Ministry for Health, Social Services and Equality (Spain) to carry out this study.

Published

2014