Your search keyword '"T, Bienvenu"' showing total 15 results

1. Further delineation of the MECP2 duplication syndrome phenotype in 59 French male patients, with a particular focus on morphological and neurological features.

Author

Miguet M, Faivre L, Amiel J, Nizon M, Touraine R, Prieur F, Pasquier L, Lefebvre M, Thevenon J, Dubourg C, Julia S, Sarret C, Remerand G, Francannet C, Laffargue F, Boespflug-Tanguy O, David A, Isidor B, Vigneron J, Leheup B, Lambert L, Philippe C, Béri-Dexheimer M, Cuisset JM, Andrieux J, Plessis G, Toutain A, Guibaud L, Cormier-Daire V, Rio M, Bonnefont JP, Echenne B, Journel H, Burglen L, Chantot-Bastaraud S, Bienvenu T, Baumann C, Perrin L, Drunat S, Jouk PS, Dieterich K, Devillard F, Lacombe D, Philip N, Sigaudy S, Moncla A, Missirian C, Badens C, Perreton N, Thauvin-Robinet C, AChro-Puce R, Pedespan JM, Rooryck C, Goizet C, Vincent-Delorme C, Duban-Bedu B, Bahi-Buisson N, Afenjar A, Maincent K, Héron D, Alessandri JL, Martin-Coignard D, Lesca G, Rossi M, Raynaud M, Callier P, Mosca-Boidron AL, Marle N, Coutton C, Satre V, Caignec CL, Malan V, Romana S, Keren B, Tabet AC, Kremer V, Scheidecker S, Vigouroux A, Lackmy-Port-Lis M, Sanlaville D, Till M, Carneiro M, Gilbert-Dussardier B, Willems M, Van Esch H, Portes VD, and El Chehadeh S

Subjects

Adolescent, Adult, Child, Child, Preschool, Chromosomes, Human, X genetics, Developmental Disabilities complications, Developmental Disabilities genetics, Developmental Disabilities physiopathology, Epilepsy complications, Epilepsy genetics, Epilepsy physiopathology, Exotropia complications, Exotropia physiopathology, France epidemiology, Humans, Hyperopia complications, Hyperopia genetics, Hyperopia physiopathology, Hypertension, Pulmonary complications, Hypertension, Pulmonary physiopathology, Infant, Intellectual Disability complications, Intellectual Disability physiopathology, Male, X-Linked Intellectual Disability complications, X-Linked Intellectual Disability physiopathology, Pedigree, Phenotype, Somatosensory Disorders genetics, Somatosensory Disorders physiopathology, Stereotypic Movement Disorder complications, Stereotypic Movement Disorder genetics, Stereotypic Movement Disorder physiopathology, Young Adult, Exotropia genetics, Hypertension, Pulmonary genetics, Intellectual Disability genetics, X-Linked Intellectual Disability genetics, Methyl-CpG-Binding Protein 2 genetics

Abstract

The Xq28 duplication involving the MECP2 gene ( MECP2 duplication) has been mainly described in male patients with severe developmental delay (DD) associated with spasticity, stereotypic movements and recurrent infections. Nevertheless, only a few series have been published. We aimed to better describe the phenotype of this condition, with a focus on morphological and neurological features. Through a national collaborative study, we report a large French series of 59 affected males with interstitial MECP2 duplication. Most of the patients (93%) shared similar facial features, which evolved with age (midface hypoplasia, narrow and prominent nasal bridge, thick lower lip, large prominent ears), thick hair, livedo of the limbs, tapered fingers, small feet and vasomotor troubles. Early hypotonia and global DD were constant, with 21% of patients unable to walk. In patients able to stand, lower limbs weakness and spasticity led to a singular standing habitus: flexion of the knees, broad-based stance with pseudo-ataxic gait. Scoliosis was frequent (53%), such as divergent strabismus (76%) and hypermetropia (54%), stereotypic movements (89%), without obvious social withdrawal and decreased pain sensitivity (78%). Most of the patients did not develop expressive language, 35% saying few words. Epilepsy was frequent (59%), with a mean onset around 7.4 years of age, and often (62%) drug-resistant. Other medical issues were frequent: constipation (78%), and recurrent infections (89%), mainly lung. We delineate the clinical phenotype of MECP2 duplication syndrome in a large series of 59 males. Pulmonary hypertension appeared as a cause of early death in these patients, advocating its screening early in life., Competing Interests: Competing interests: None declared., (© Article author(s) (or their employer(s) unless otherwise stated in the text of the article) 2018. All rights reserved. No commercial use is permitted unless otherwise expressly granted.)

Published

2018

2. WWOX-related encephalopathies: delineation of the phenotypical spectrum and emerging genotype-phenotype correlation.

Author

Mignot C, Lambert L, Pasquier L, Bienvenu T, Delahaye-Duriez A, Keren B, Lefranc J, Saunier A, Allou L, Roth V, Valduga M, Moustaïne A, Auvin S, Barrey C, Chantot-Bastaraud S, Lebrun N, Moutard ML, Nougues MC, Vermersch AI, Héron B, Pipiras E, Héron D, Olivier-Faivre L, Guéant JL, Jonveaux P, and Philippe C

Subjects

Codon, Nonsense genetics, Comparative Genomic Hybridization, High-Throughput Nucleotide Sequencing, Humans, Mutation, Missense genetics, Spasms, Infantile pathology, Spinocerebellar Ataxias pathology, WW Domain-Containing Oxidoreductase, Oxidoreductases genetics, Phenotype, Spasms, Infantile genetics, Spinocerebellar Ataxias genetics, Tumor Suppressor Proteins genetics

Abstract

Background: Homozygous mutations in WWOX were reported in eight individuals of two families with autosomal recessive spinocerebellar ataxia type 12 and in two siblings with infantile epileptic encephalopathy (IEE), including one who deceased prior to DNA sampling., Methods: By combining array comparative genomic hybridisation, targeted Sanger sequencing and next generation sequencing, we identified five further patients from four families with IEE due to biallelic alterations of WWOX., Results: We identified eight deleterious WWOX alleles consisting in four deletions, a four base-pair frameshifting deletion, one missense and two nonsense mutations. Genotype-phenotype correlation emerges from the seven reported families. The phenotype in four patients carrying two predicted null alleles was characterised by (1) little if any psychomotor acquisitions, poor spontaneous motility and absent eye contact from birth, (2) pharmacoresistant epilepsy starting in the 1st weeks of life, (3) possible retinal degeneration, acquired microcephaly and premature death. This contrasted with the less severe autosomal recessive spinocerebellar ataxia type 12 phenotype due to hypomorphic alleles. In line with this correlation, the phenotype in two siblings carrying a null allele and a missense mutation was intermediate., Conclusions: Our results obtained by a combination of different molecular techniques undoubtedly incriminate WWOX as a gene for recessive IEE and illustrate the usefulness of high throughput data mining for the identification of genes for rare autosomal recessive disorders. The structure of the WWOX locus encompassing the FRA16D fragile site might explain why constitutive deletions are recurrently reported in genetic databases, suggesting that WWOX-related encephalopathies, although likely rare, may not be exceptional., (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

2015

3. CFTR p.Arg117His associated with CBAVD and other CFTR-related disorders.

Author

Thauvin-Robinet C, Munck A, Huet F, de Becdelièvre A, Jimenez C, Lalau G, Gautier E, Rollet J, Flori J, Nové-Josserand R, Soufir JC, Haloun A, Hubert D, Houssin E, Bellis G, Rault G, David A, Janny L, Chiron R, Rives N, Hairion D, Collignon P, Valeri A, Karsenty G, Rossi A, Audrézet MP, Férec C, Leclerc J, Georges Md, Claustres M, Bienvenu T, Gérard B, Boisseau P, Cabet-Bey F, Cheillan D, Feldmann D, Clavel C, Bieth E, Iron A, Simon-Bouy B, Izard V, Steffann J, Viville S, Costa C, Drouineaud V, Fauque P, Binquet C, Bonithon-Kopp C, Morris MA, Faivre L, Goossens M, Roussey M, and Girodon E

Subjects

Child, Child, Preschool, Cystic Fibrosis complications, Cystic Fibrosis pathology, Female, Heterozygote, Humans, Infant, Infant, Newborn, Infertility, Male complications, Infertility, Male genetics, Male, Male Urogenital Diseases complications, Male Urogenital Diseases pathology, Mutation, Mutation Rate, Phenotype, Sweat chemistry, Vas Deferens abnormalities, Vas Deferens pathology, Cystic Fibrosis genetics, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Male Urogenital Diseases genetics, Prenatal Diagnosis

Abstract

Background: The high frequency of the cystic fibrosis (CF) transmembrane conductance regulator (CFTR) gene mutation p.Arg117His in patients with congenital bilateral absence of the vas deferens (CBAVD) and in newborns screened for CF has created a dilemma., Methods: Phenotypic and genotypic data were retrospectively collected in 179 non-newborn French individuals carrying p.Arg117His and a second CFTR mutation referred for symptoms or family history, by all French molecular genetics laboratories, referring physicians, CF care centres and infertility clinics., Results: 97% of the patients had the intronic T7 normal variant in cis with p.Arg117His. 89% patients were male, with CBAVD being the reason for referral in 76%. In 166/179 patients with available detailed clinical features, final diagnoses were: four late-onset marked pulmonary disease, 83 isolated CBAVD, 67 other CFTR-related phenotypes, including 44 CBAVD with pulmonary and/or pancreatic symptoms and 12 asymptomatic cases. Respiratory symptoms were observed in 30% of the patients, but the overall phenotype was mild. No correlation was observed between sweat chloride concentrations and disease severity. Five couples at risk of CF offspring were identified and four benefited from prenatal or preimplantation genetic diagnoses (PND or PGD). Eight children were born, including four who were compound heterozygous for p.Arg117His and one with a severe CF mutation., Conclusions: Patients with CBAVD carrying p.Arg117His and a severe CF mutation should benefit from a clinical evaluation and follow-up. Depending on the CBAVD patients' genotype, a CFTR analysis should be considered in their partners in order to identify CF carrier couples and offer PND or PGD.

Published

2013

4. Novel FOXG1 mutations associated with the congenital variant of Rett syndrome.

Author

Mencarelli MA, Spanhol-Rosseto A, Artuso R, Rondinella D, De Filippis R, Bahi-Buisson N, Nectoux J, Rubinsztajn R, Bienvenu T, Moncla A, Chabrol B, Villard L, Krumina Z, Armstrong J, Roche A, Pineda M, Gak E, Mari F, Ariani F, and Renieri A

Subjects

Child, Preschool, Female, Humans, Mutation, Forkhead Transcription Factors genetics, Methyl-CpG-Binding Protein 2 genetics, Nerve Tissue Proteins genetics, Rett Syndrome genetics

Abstract

Background: Rett syndrome is a severe neurodevelopmental disorder representing one of the most common genetic causes of mental retardation in girls. The classic form is caused by MECP2 mutations. In two patients affected by the congenital variant of Rett we have recently identified mutations in the FOXG1 gene encoding a brain specific transcriptional repressor, essential for early development of the telencephalon., Methods: 60 MECP2/CDKL5 mutation negative European Rett patients (classic and variants), 43 patients with encephalopathy with early onset seizures, and four atypical Rett patients were analysed for mutations in FOXG1., Results and Conclusions: Mutations have been identified in four patients, independently classified as congenital Rett variants from France, Spain and Latvia. Clinical data have been compared with the two previously reported patients with mutations in FOXG1. In all cases hypotonia, irresponsiveness and irritability were present in the neonatal period. At birth, head circumference was normal while a deceleration of growth was recognised soon afterwards, leading to severe microcephaly. Motor development was severely impaired and voluntary hand use was absent. In contrast with classic Rett, patients showed poor eye contact. Typical stereotypic hand movements with hand washing and hand mouthing activities were present continuously. Some patients showed abnormal movements of the tongue and jerky movements of the limbs. Brain magnetic resonance imaging showed corpus callosum hypoplasia in most cases, while epilepsy was a variable sign. Scoliosis was present and severe in the older patients. Neurovegetative symptoms typical of Rett were frequently present.

Published

2010

5. The very low penetrance of cystic fibrosis for the R117H mutation: a reappraisal for genetic counselling and newborn screening.

Author

Thauvin-Robinet C, Munck A, Huet F, Génin E, Bellis G, Gautier E, Audrézet MP, Férec C, Lalau G, Georges MD, Claustres M, Bienvenu T, Gérard B, Boisseau P, Cabet-Bey F, Feldmann D, Clavel C, Bieth E, Iron A, Simon-Bouy B, Costa C, Medina R, Leclerc J, Hubert D, Nové-Josserand R, Sermet-Gaudelus I, Rault G, Flori J, Leroy S, Wizla N, Bellon G, Haloun A, Perez-Martin S, d'Acremont G, Corvol H, Clément A, Houssin E, Binquet C, Bonithon-Kopp C, Alberti-Boulmé C, Morris MA, Faivre L, Goossens M, Roussey M, and Girodon E

Subjects

Cross-Sectional Studies, Cystic Fibrosis diagnosis, Cystic Fibrosis epidemiology, Humans, Infant, Newborn, Kaplan-Meier Estimate, Mutation, Phenotype, Cystic Fibrosis genetics, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Genetic Counseling, Heterozygote, Neonatal Screening, Penetrance

Abstract

Background: Cystic fibrosis (CF) is caused by compound heterozygosity or homozygosity of CF transmembrane conductance regulator gene (CFTR) mutations. Phenotypic variability associated with certain mutations makes genetic counselling difficult, notably for R117H, whose disease phenotype varies from asymptomatic to classical CF. The high frequency of R117H observed in CF newborn screening has also introduced diagnostic dilemmas. The aim of this study was to evaluate the disease penetrance for R117H in order to improve clinical practice., Methods: The phenotypes in all individuals identified in France as compound heterozygous for R117H and F508del, the most frequent CF mutation, were described. The allelic prevalences of R117H (p(R117H)), on either intron 8 T5 or T7 background, and F508del (p(F508del)) were determined in the French population, to permit an evaluation of the penetrance of CF for the [R117H]+[F508del] genotype., Results: Clinical details were documented for 184 [R117H]+[F508del] individuals, including 72 newborns. The disease phenotype was predominantly mild; one child had classical CF, and three adults' severe pulmonary symptoms. In 5245 healthy adults, p(F508del) was 1.06%, p(R117H;T7) 0.27% and p(R117H;T5)<0.01%. The theoretical number of [R117H;T7]+[F508del] individuals in the French population was estimated at 3650, whereas only 112 were known with CF related symptoms (3.1%). The penetrance of classical CF for [R117H;T7]+[F508del] was estimated at 0.03% and that of severe CF in adulthood at 0.06%., Conclusions: These results suggest that R117H should be withdrawn from CF mutation panels used for screening programmes. The real impact of so-called disease mutations should be assessed before including them in newborn or preconceptional carrier screening programmes.

Published

2009

6. Impairment of CDKL5 nuclear localisation as a cause for severe infantile encephalopathy.

Author

Rosas-Vargas H, Bahi-Buisson N, Philippe C, Nectoux J, Girard B, N'Guyen Morel MA, Gitiaux C, Lazaro L, Odent S, Jonveaux P, Chelly J, and Bienvenu T

Subjects

Amino Acid Sequence, Amino Acid Substitution, Animals, Base Sequence, Brain Diseases, Metabolic, Inborn pathology, Brain Diseases, Metabolic, Inborn physiopathology, COS Cells, Child, Preschool, Chlorocebus aethiops, DNA Mutational Analysis, Electroencephalography, Female, Humans, Infant, Magnetic Resonance Imaging, Phenotype, Plasmids genetics, RNA, Messenger genetics, Sequence Homology, Amino Acid, Transfection, X Chromosome Inactivation, Brain Diseases, Metabolic, Inborn enzymology, Brain Diseases, Metabolic, Inborn genetics, Cell Nucleus enzymology, Mutation, Missense, Protein Serine-Threonine Kinases genetics, Protein Serine-Threonine Kinases metabolism

Abstract

Mutations in the human X-linked cyclin-dependent kinase-like 5 (CDKL5) gene have been shown to cause infantile spasms as well as Rett syndrome-like phenotype. To date, fewer than 20 different mutations have been reported. So far, no clear genotype-phenotype correlation has been established. We screened the entire coding region of CDKL5 in 151 affected girls with a clinically heterogeneous phenotype ranging from encephalopathy with epilepsy to atypical Rett syndrome by denaturing high liquid performance chromatography and direct sequencing, and we identified three novel missense mutations located in catalytic domain (p.Ala40Val, p.Arg65Gln, p.Leu220Pro). Segregation analysis showed that p.Arg65Gln was inherited from the healthy father, which rules out the involvement of CDKL5 in the aetiology of the phenotype in this patient. However, the de novo occurrence was shown for p.Ala40Val and p.Leu220Pro. The p.Ala40Val mutation was observed in two unrelated patients and represented the first recurrent mutation in the CDKL5 gene. For the two de novo mutations, we analysed the cellular localisation of the wild-type and CDKL5 mutants by transfection experiments. We showed that the two CDKL5 mutations cause mislocalisation of the mutant CDKL5 proteins in the cytoplasm. Interestingly these missense mutations that result in a mislocalisation of the CDKL5 protein are associated with severe developmental delay which was apparent within the first months of life characterised by early and generalised hypotonia, and autistic features, and as well as early infantile spasms.

Published

2008

7. Mutations in the AP1S2 gene encoding the sigma 2 subunit of the adaptor protein 1 complex are associated with syndromic X-linked mental retardation with hydrocephalus and calcifications in basal ganglia.

Author

Saillour Y, Zanni G, Des Portes V, Heron D, Guibaud L, Iba-Zizen MT, Pedespan JL, Poirier K, Castelnau L, Julien C, Franconnet C, Bonthron D, Porteous ME, Chelly J, and Bienvenu T

Subjects

Adaptor Protein Complex sigma Subunits chemistry, Adaptor Protein Complex sigma Subunits deficiency, Basal Ganglia Diseases epidemiology, Brain embryology, Brain pathology, Calcinosis epidemiology, Cerebellar Nuclei pathology, Codon, Nonsense, Face abnormalities, France epidemiology, Humans, Hydrocephalus epidemiology, Infant, Newborn, Male, X-Linked Intellectual Disability epidemiology, Optic Atrophies, Hereditary genetics, Pedigree, Protein Transport genetics, RNA Splice Sites genetics, Scotland epidemiology, Syndrome, Adaptor Protein Complex sigma Subunits genetics, Basal Ganglia Diseases genetics, Calcinosis genetics, Exons genetics, Hydrocephalus genetics, X-Linked Intellectual Disability genetics

Abstract

Fried syndrome, first described in 1972, is a rare X-linked mental retardation that has been mapped by linkage to Xp22. Clinical characteristics include mental retardation, mild facial dysmorphism, calcifications of basal ganglia and hydrocephalus. A large four-generation family in which the affected males have striking clinical features of Fried syndrome were investigated for linkage to X-chromosome markers; the results showed that the gene for this condition lies within the interval DXS7109-DXS7593 in Xp22.2. In total, 60 candidate genes located in this region, including AP1S2, which was recently shown to be involved in mental retardation, were screened for mutations. A mutation in the third intron of AP1S2 was found in all affected male subjects in this large French family. The mutation resulted in skipping of exon 3, predicting a protein with three novel amino-acids and with termination at codon 64. In addition, the first known large Scottish family affected by Fried syndrome was reinvestigated, and a new nonsense mutation, p.Gln66X, was found in exon 3. Using CT, both affected patients from the French family who were analysed had marked calcifications of the basal ganglia, as previously observed in the first Scottish family, suggesting that the presence of distinctive basal ganglia calcification is an essential parameter to recognise this syndromic disorder. It may be possible to use this feature to identify families with X-linked mental retardation that should be screened for mutations in AP1S2.

Published

2007

8. Rare polymorphic variants of the AGTR2 gene in boys with non-specific mental retardation.

Author

Bienvenu T, Poirier K, Van Esch H, Hamel B, Moraine C, Fryns JP, Ropers HH, Beldjord C, Yntema HG, and Chelly J

Subjects

Base Sequence, Chromosomes, Human, X genetics, DNA Mutational Analysis, Exons genetics, Genetic Linkage, Humans, Male, Receptor, Angiotensin, Type 2, Genetic Variation genetics, Intellectual Disability genetics, Polymorphism, Genetic genetics, Receptors, Angiotensin genetics

Published

2003

9. Evidence of somatic mosaicism for a MECP2 mutation in females with Rett syndrome: diagnostic implications.

Author

Bourdon V, Philippe C, Bienvenu T, Koenig B, Tardieu M, Chelly J, and Jonveaux P

Subjects

Adolescent, Child, Preschool, DNA-Binding Proteins chemistry, Exons genetics, Female, Heteroduplex Analysis, Humans, Infant, Infant, Newborn, Methyl-CpG-Binding Protein 2, Polymerase Chain Reaction, Rett Syndrome pathology, Chromosomal Proteins, Non-Histone, DNA-Binding Proteins genetics, Mosaicism genetics, Mutation genetics, Repressor Proteins, Rett Syndrome diagnosis, Rett Syndrome genetics

Published

2001

10. Cystic fibrosis patients with the 3272-26A>G splicing mutation have milder disease than F508del homozygotes: a large European study.

Author

Amaral MD, Pacheco P, Beck S, Farinha CM, Penque D, Nogueira P, Barreto C, Lopes B, Casals T, Dapena J, Gartner S, Vásquez C, Pérez-Frías J, Olveira C, Cabanas R, Estivill X, Tzetis M, Kanavakis E, Doudounakis S, Dörk T, Tümmler B, Girodon-Boulandet E, Cazeneuve C, Goossens M, Blayau M, Verlingue C, Vieira I, Féréc C, Claustres M, des Georges M, Clavel C, Birembaut P, Hubert D, Bienvenu T, Adoun M, Chomel JC, De Boeck K, Cuppens H, and Lavinha J

Subjects

Alleles, Cystic Fibrosis pathology, DNA chemistry, DNA genetics, DNA Mutational Analysis, Europe, Female, Genotype, Haplotypes, Homozygote, Humans, Male, Phenotype, Point Mutation, Severity of Illness Index, Alternative Splicing genetics, Cystic Fibrosis genetics, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Sequence Deletion genetics

Published

2001

11. Cystic fibrosis screening: a fetus with hyperechogenic bowel may be the index case.

Author

Muller F, Dommergues M, Simon-Bouy B, Ferec C, Oury JF, Aubry MC, Bessis R, Vuillard E, Denamur E, Bienvenu T, and Serre JL

Subjects

Cystic Fibrosis epidemiology, Female, Follow-Up Studies, Genetic Testing, Humans, Incidence, Intestines embryology, Predictive Value of Tests, Pregnancy, Pregnancy Outcome, Prospective Studies, Cystic Fibrosis genetics, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Intestines diagnostic imaging, Ultrasonography, Prenatal

Abstract

Background: The potential of hyperechogenic fetal bowel to act as a hallmark for prenatal cystic fibrosis screening in the general population is controversial., Methods: Our goal was to evaluate the incidence of cystic fibrosis in 209 fetuses with hyperechogenic bowel diagnosed at routine ultrasonography and with no family history of cystic fibrosis. The diagnosis of cystic fibrosis was based on prenatal screening for the eight mutations most frequently observed in France (deltaF508, deltaI507, 1717-1G-->A, G542X, G551D, R553X, W1282X, N1303K) and at postnatal follow up., Results: The overall incidence of cystic fibrosis was 7/209 (3.3%) which is 84 times the estimated risk of CF in the general population (112500). Of these seven cases, six were diagnosed prenatally based on DNA analysis (deltaF508/deltaF508, n=5; deltaF508/G542X, n=1). One case in which only one mutation had been recognised was diagnosed clinically after birth (deltaF508/unidentified mutation). Of the seven cases, none was diagnosed at 16-19 weeks, four at 16-24 weeks, and three after this. The incidence of heterozygous fetuses (15/209, 7%) was not significantly higher than the 5% expected in the general population. The mutations involved in these heterozygous cases were deltaF508 (n=13), G542X (n=1), and G551D (n=1)., Conclusions: Screening for cystic fibrosis should be offered to families in which fetal hyperechogenic bowel is diagnosed at routine ultrasonography. This underlines the need to review genetic counselling in this situation where the fetus is the index case for a genetic disease.

Published

1998

12. Dominant X linked subcortical laminar heterotopia and lissencephaly syndrome (XSCLH/LIS): evidence for the occurrence of mutation in males and mapping of a potential locus in Xq22.

Author

des Portes V, Pinard JM, Smadja D, Motte J, Boespflüg-Tanguy O, Moutard ML, Desguerre I, Billuart P, Carrie A, Bienvenu T, Vinet MC, Bachner L, Beldjord C, Dulac O, Kahn A, Ponsot G, and Chelly J

Subjects

Adult, Child, Child, Preschool, Chromosome Mapping, Female, Genes, Dominant, Genetic Linkage, Haplotypes, Humans, Male, Microsatellite Repeats, Mutation, Pedigree, Syndrome, Cerebral Cortex abnormalities, Epilepsy genetics, Intellectual Disability genetics, Sex Chromosome Aberrations genetics, X Chromosome genetics

Abstract

X linked subcortical laminar heterotopia and lissencephaly syndrome (XSCLH/ LIS) is an intriguing disorder of cortical development, which causes classical lissencephaly with severe mental retardation and epilepsy in hemizygous males, and subcortical laminar heterotopia (SCLH) associated with milder mental retardation and epilepsy in heterozygous females. Here we report an exclusion mapping study carried out in three unrelated previously described families in which males are affected with lissencephaly and females with SCLH, using 38 microsatellite markers evenly distributed on the X chromosome. Most of the X chromosome was excluded and potential intervals of assignment in Xq22.3-q23 or in Xq27 are reported. Although the number of informative meioses did not allow a decision between these two loci, it is worth noting that the former interval is compatible with the mapping of a breakpoint involved in a de novo X;autosomal balanced translocation 46,XX,t(X;2)(q22;p25) previously described in a female with classical lissencephaly. In addition, haplotype inheritance in two families showed a grandpaternal origin of the mutation and suggested in one family the presence of mosaicism in germline cells of normal transmitting males.

Published

1997

13. Severe cystic fibrosis phenotype in a delta F508/3272-26A-->G compound heterozygote.

Author

Bienvenu T, Beldjord C, Kaplan JC, Hubert D, and Dusser D

Subjects

Child, Fatal Outcome, Heterozygote, Humans, Male, Phenotype, Cystic Fibrosis genetics, Cystic Fibrosis Transmembrane Conductance Regulator genetics, Point Mutation, Sequence Deletion

Published

1995

14. Male infertility as the only presenting sign of cystic fibrosis when homozygous for the mild mutation R117H.

Author

Bienvenu T, Beldjord C, Adjiman M, and Kaplan JC

Subjects

Adult, Arginine genetics, Cystic Fibrosis complications, Cystic Fibrosis Transmembrane Conductance Regulator, Homozygote, Humans, Male, Membrane Proteins genetics, Point Mutation, Cystic Fibrosis genetics, Cystic Fibrosis pathology, Infertility, Male etiology, Infertility, Male genetics, Vas Deferens abnormalities

Published

1993

15. Severe cystic fibrosis in a child homozygous for the G542 nonsense mutation in the CFTR gene.

Author

Bienvenu T, Beldjord C, Fonknechten N, Kaplan JC, and Lenoir G

Subjects

Celiac Disease etiology, Cystic Fibrosis complications, Cystic Fibrosis Transmembrane Conductance Regulator, Exocrine Pancreatic Insufficiency complications, Humans, Infant, Newborn, Intestinal Obstruction etiology, Lung microbiology, Lung physiology, Male, Meconium, Phenotype, Cystic Fibrosis genetics, Exocrine Pancreatic Insufficiency etiology, Membrane Proteins genetics, Point Mutation

Published

1993