Your search keyword '"Parent, Philippe"' showing total 11 results

1. A novel mutation in the transmembrane 6 domain of GABBR2 leads to a Rett-like phenotype.

Author

Vuillaume, Marie‐Laure, Jeanne, Médéric, Xue, Li, Blesson, Sophie, Denommé‐Pichon, Anne‐Sophie, Alirol, Servane, Brulard, Céline, Colin, Estelle, Isidor, Bertrand, Gilbert‐Dussardier, Brigitte, Odent, Sylvie, Parent, Philippe, Donnart, Audrey, Redon, Richard, Bézieau, Stéphane, Rondard, Philippe, Laumonnier, Frédéric, Toutain, Annick, Vuillaume, Marie-Laure, and Denommé-Pichon, Anne-Sophie

Subjects

MEMBRANE potential, RETT syndrome, BRAIN diseases, CELL receptors, COMPARATIVE studies, EPILEPSY, RESEARCH methodology, MEDICAL cooperation, GENETIC mutation, PROTEINS, RESEARCH, PHENOTYPES, EVALUATION research

Published

2018

2. Intragenic deletion of the WDR45 gene in a male with encephalopathy, severe psychomotor disability, and epilepsy.

Author

Redon, Sylvia, Benech, Caroline, Schutz, Sacha, Despres, Aurore, Gueguen, Paul, Le Berre, Pauline, Le Marechal, Cédric, Peudenier, Sylviane, Meriot, Philippe, Parent, Philippe, and Ferec, Claude

Published

2017

3. Subtelomeric monosomy 11q and trisomy 16q in siblings and an unrelated child: Molecular characterization of two der(11)t(11;16).

Author

Basinko, Audrey, Audebert-Bellanger, Séverine, Douet-Guilbert, Nathalie, Le Franc, Jérémie, Parent, Philippe, Quemener, Sylvia, La Selve, Philippe, Bovo, Clément, Morel, Frédéric, Le Bris, Marie-Josée, and De Braekeleer, Marc

Abstract

We report here three children with a der(11)t(11;16), two sibs (patients 1 and 2) having inherited a recombinant chromosome from a maternal t(11;16)(q24.3;q23.2) and a third unrelated child with a de novo der(11)t(11;16)(q25;q22.1), leading to partial monosomy 11q and trisomy 16q. Fluorescent in situ hybridization (FISH) using bacterial artificial chromosome (BAC) clones and array-CGH were performed to determine the breakpoints involved in the familial and the de novo rearrangements. The partial 11 monosomy extended from 11q24.3 to 11qter and measured 6.17-6.21 Mb in Patients 1 and 2 while the size of the partial 11q25->qter monosomy was estimated at 1.97-2.11 Mb for Patient 3. The partial 16 trisomy extended from 16q23.2 to 16qter and measured 8.93-8.95 Mb in Patients 1 and 2 while the size of the partial 16q22.1->qter trisomy was 20.82 Mb for Patient 3. Intraventricular hemorrhage and transitional thrombocytopenia were found in both sibs but not in the third patient. The FLI1 gene, which is the most relevant gene for thrombocytopenia in Jacobsen syndrome, was neither deleted in family A nor in Patient 3. We suggest that a positional effect could affect the FLI1 expression for these two sibs. Deafness of our three patients confirmed the association of this anomaly to 11q monosomy and tended to confirm the hypothetic role of DFNB20 in Jacobsen syndrome hearing loss. Both sibs shared most of the features commonly observed in Jacobsen syndrome, but not the third patient. This confirmed that terminal 11q trisomy spanning 1 to 1.97-2.11 Mb is not associated with a typical Jacobsen syndrome. © 2011 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2011

4. Prenatal diagnosis of cystic fibrosis: the 18-year experience of Brittany (western France).

Author

Scotet, Virginie, Duguépéroux, Ingrid, Audrézet, Marie-Pierre, Blayau, Martine, Boisseau, Pierre, Journel, Hubert, Parent, Philippe, and Férec, Claude

Abstract

Objective This study reports 18 years of experience in prenatal diagnosis (PD) of cystic fibrosis (CF) in a region where CF is frequent and the uptake of PD is common (Brittany, western France). Method All PDs made over the period 1989-2006 in women living in Brittany were collected. Results We recorded 268 PDs made in 1 in 4 risk couples, plus 22 PDs directly made following the sonographic finding of echogenic bowel. Most of the 268 PDs were done in couples already having CF child(ren) ( n = 195, 72.8%). Close to one-fifth followed cascade screening ( n = 49, 18.3%), which identified 26 new 1 in 4 risk couples among the relatives of CF patients or of carriers identified through newborn screening (NBS). The remaining PDs were mainly made in couples whose 1 in 4 risk was evidenced following the diagnosis of echogenic bowel in a previous pregnancy ( n = 22, 8.2%). Although patients' life expectancy has considerably improved, in our population the great majority of couples chose pregnancy termination when PD indicated that the foetus had CF (95.9%). Conclusion This study describes the distribution of PDs according to the context in which the 1 in 4 risk was discovered and highlights the real decisions of couples as regards pregnancy termination after a positive PD. Copyright © 2008 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2008

5. Phenotype and genotype analysis of a French cohort of 119 patients with CHARGE syndrome.

Author

Legendre M, Abadie V, Attié-Bitach T, Philip N, Busa T, Bonneau D, Colin E, Dollfus H, Lacombe D, Toutain A, Blesson S, Julia S, Martin-Coignard D, Geneviève D, Leheup B, Odent S, Jouk PS, Mercier S, Faivre L, Vincent-Delorme C, Francannet C, Naudion S, Mathieu-Dramard M, Delrue MA, Goldenberg A, Héron D, Parent P, Touraine R, Layet V, Sanlaville D, Quélin C, Moutton S, Fradin M, Jacquette A, Sigaudy S, Pinson L, Sarda P, Guerrot AM, Rossi M, Masurel-Paulet A, El Chehadeh S, Piguel X, Rodriguez-Ballesteros M, Ragot S, Lyonnet S, Bilan F, and Gilbert-Dussardier B

Subjects

Abnormalities, Multiple diagnosis, Abnormalities, Multiple genetics, Adolescent, Adult, Alleles, Amino Acid Substitution, Central Nervous System abnormalities, Child, Child, Preschool, Cohort Studies, Cranial Nerves abnormalities, DNA Helicases genetics, DNA-Binding Proteins genetics, Female, France, Genetic Testing, Humans, Infant, Male, Molecular Diagnostic Techniques, Young Adult, CHARGE Syndrome diagnosis, CHARGE Syndrome genetics, Genetic Association Studies, Genotype, Phenotype

Abstract

CHARGE syndrome (CS) is a genetic disorder whose first description included Coloboma, Heart disease, Atresia of choanae, Retarded growth and development, Genital hypoplasia, and Ear anomalies and deafness, most often caused by a genetic mutation in the CHD7 gene. Two features were then added: semicircular canal anomalies and arhinencephaly/olfactory bulb agenesis, with classification of typical, partial, or atypical forms on the basis of major and minor clinical criteria. The detection rate of a pathogenic variant in the CHD7 gene varies from 67% to 90%. To try to have an overview of this heterogenous clinical condition and specify a genotype-phenotype relation, we conducted a national study of phenotype and genotype in 119 patients with CS. Selected clinical diagnostic criteria were from Verloes (2005), updated by Blake & Prasad (). Besides obtaining a detailed clinical description, when possible, patients underwent a full ophthalmologic examination, audiometry, temporal bone CT scan, gonadotropin analysis, and olfactory-bulb MRI. All patients underwent CHD7 sequencing and MLPA analysis. We found a pathogenic CHD7 variant in 83% of typical CS cases and 58% of atypical cases. Pathogenic variants in the CHD7 gene were classified by the expected impact on the protein. In all, 90% of patients had a typical form of CS and 10% an atypical form. The most frequent features were deafness/semicircular canal hypoplasia (94%), pituitary defect/hypogonadism (89%), external ear anomalies (87%), square-shaped face (81%), and arhinencephaly/anosmia (80%). Coloboma (73%), heart defects (65%), and choanal atresia (43%) were less frequent., (© 2017 Wiley Periodicals, Inc.)

Published

2017

6. Phenotype and genotype in 52 patients with Rubinstein-Taybi syndrome caused by EP300 mutations.

Author

Fergelot P, Van Belzen M, Van Gils J, Afenjar A, Armour CM, Arveiler B, Beets L, Burglen L, Busa T, Collet M, Deforges J, de Vries BB, Dominguez Garrido E, Dorison N, Dupont J, Francannet C, Garciá-Minaúr S, Gabau Vila E, Gebre-Medhin S, Gener Querol B, Geneviève D, Gérard M, Gervasini CG, Goldenberg A, Josifova D, Lachlan K, Maas S, Maranda B, Moilanen JS, Nordgren A, Parent P, Rankin J, Reardon W, Rio M, Roume J, Shaw A, Smigiel R, Sojo A, Solomon B, Stembalska A, Stumpel C, Suarez F, Terhal P, Thomas S, Touraine R, Verloes A, Vincent-Delorme C, Wincent J, Peters DJ, Bartsch O, Larizza L, Lacombe D, and Hennekam RC

Subjects

Adult, Chromatin Assembly and Disassembly genetics, Female, Genetic Association Studies, Genetic Predisposition to Disease, Genotype, Humans, Male, Middle Aged, Mutation, Missense genetics, Pre-Eclampsia physiopathology, Pregnancy, Rubinstein-Taybi Syndrome pathology, Sequence Deletion, CREB-Binding Protein genetics, E1A-Associated p300 Protein genetics, Pre-Eclampsia genetics, Rubinstein-Taybi Syndrome genetics

Abstract

Rubinstein-Taybi syndrome (RSTS) is a developmental disorder characterized by a typical face and distal limbs abnormalities, intellectual disability, and a vast number of other features. Two genes are known to cause RSTS, CREBBP in 60% and EP300 in 8-10% of clinically diagnosed cases. Both paralogs act in chromatin remodeling and encode for transcriptional co-activators interacting with >400 proteins. Up to now 26 individuals with an EP300 mutation have been published. Here, we describe the phenotype and genotype of 42 unpublished RSTS patients carrying EP300 mutations and intragenic deletions and offer an update on another 10 patients. We compare the data to 308 individuals with CREBBP mutations. We demonstrate that EP300 mutations cause a phenotype that typically resembles the classical RSTS phenotype due to CREBBP mutations to a great extent, although most facial signs are less marked with the exception of a low-hanging columella. The limb anomalies are more similar to those in CREBBP mutated individuals except for angulation of thumbs and halluces which is very uncommon in EP300 mutated individuals. The intellectual disability is variable but typically less marked whereas the microcephaly is more common. All types of mutations occur but truncating mutations and small rearrangements are most common (86%). Missense mutations in the HAT domain are associated with a classical RSTS phenotype but otherwise no genotype-phenotype correlation is detected. Pre-eclampsia occurs in 12/52 mothers of EP300 mutated individuals versus in 2/59 mothers of CREBBP mutated individuals, making pregnancy with an EP300 mutated fetus the strongest known predictor for pre-eclampsia. © 2016 Wiley Periodicals, Inc., (© 2016 Wiley Periodicals, Inc.)

Published

2016

7. Clinical and molecular findings in 39 patients with KBG syndrome caused by deletion or mutation of ANKRD11.

Author

Goldenberg A, Riccardi F, Tessier A, Pfundt R, Busa T, Cacciagli P, Capri Y, Coutton C, Delahaye-Duriez A, Frebourg T, Gatinois V, Guerrot AM, Genevieve D, Lecoquierre F, Jacquette A, Khau Van Kien P, Leheup B, Marlin S, Verloes A, Michaud V, Nadeau G, Mignot C, Parent P, Rossi M, Toutain A, Schaefer E, Thauvin-Robinet C, Van Maldergem L, Thevenon J, Satre V, Perrin L, Vincent-Delorme C, Sorlin A, Missirian C, Villard L, Mancini J, Saugier-Veber P, and Philip N

Subjects

Adolescent, Adult, Aged, Alleles, Amino Acid Substitution, Child, Child, Preschool, Chromosome Deletion, Chromosomes, Human, Pair 16, Comparative Genomic Hybridization, Facies, Female, Humans, Infant, Male, Middle Aged, Phenotype, Retrospective Studies, Young Adult, Abnormalities, Multiple diagnosis, Abnormalities, Multiple genetics, Bone Diseases, Developmental diagnosis, Bone Diseases, Developmental genetics, Genetic Association Studies, Intellectual Disability diagnosis, Intellectual Disability genetics, Mutation, Repressor Proteins genetics, Tooth Abnormalities diagnosis, Tooth Abnormalities genetics

Abstract

KBG syndrome, due to ANKRD11 alteration is characterized by developmental delay, short stature, dysmorphic facial features, and skeletal anomalies. We report a clinical and molecular study of 39 patients affected by KBG syndrome. Among them, 19 were diagnosed after the detection of a 16q24.3 deletion encompassing the ANKRD11 gene by array CGH. In the 20 remaining patients, the clinical suspicion was confirmed by the identification of an ANKRD11 mutation by direct sequencing. We present arguments to modulate the previously reported diagnostic criteria. Macrodontia should no longer be considered a mandatory feature. KBG syndrome is compatible with autonomous life in adulthood. Autism is less frequent than previously reported. We also describe new clinical findings with a potential impact on the follow-up of patients, such as precocious puberty and a case of malignancy. Most deletions remove the 5'end or the entire coding region but never extend toward 16q telomere suggesting that distal 16q deletion could be lethal. Although ANKRD11 appears to be a major gene associated with intellectual disability, KBG syndrome remains under-diagnosed. NGS-based approaches for sequencing will improve the detection of point mutations in this gene. Broad knowledge of the clinical phenotype is essential for a correct interpretation of the molecular results. © 2016 Wiley Periodicals, Inc., (© 2016 Wiley Periodicals, Inc.)

Published

2016

8. Balanced transmission of a paternal complex chromosomal rearrangement involving chromosomes 2, 3, and 18.

Author

Basinko A, Perrin A, Nguyen HA, Morel F, Le Bris MJ, Saliou AH, Collet M, Parent P, Benech C, Quemener S, Ferec C, Douet-Guilbert N, and De Braekeleer M

Subjects

Adult, Amniotic Fluid cytology, Crossing Over, Genetic, Female, Humans, Karyotyping, Lymphocytes physiology, Male, Pregnancy, Recombination, Genetic, Translocation, Genetic, Chromosomes, Human, Pair 18 genetics, Chromosomes, Human, Pair 2 genetics, Chromosomes, Human, Pair 3 genetics, Gene Rearrangement

Published

2010

9. Molecular cytogenetic characterization of an 8p22-8p23.2 duplication derived from a maternal intrachromosomal insertion in a child with congenital heart malformation, delayed puberty, and learning disabilities.

Author

Basinko A, Douet-Guilbert N, Le Bris MJ, Parent P, Ansquer H, Morel F, and De Braekeleer M

Subjects

Child, Chromosomes, Artificial, Bacterial genetics, Female, Humans, In Situ Hybridization, Fluorescence, Young Adult, Chromosome Aberrations, Chromosomes, Human, Pair 8 genetics, Heart Defects, Congenital genetics, Learning Disabilities genetics, Puberty, Delayed genetics

Published

2008

10. Familial interstitial deletion of the short arm of chromosome 4 (p15.33-p16.3) characterized by molecular cytogenetic analysis.

Author

Basinko A, Douet-Guilbert N, Parent P, Blondin G, Mingam M, Monot F, Morel F, Le Bris MJ, and De Braekeleer M

Subjects

Chromosomes, Artificial, Bacterial, Humans, In Situ Hybridization, Fluorescence, Infant, Karyotyping, Male, Chromosome Deletion, Chromosomes, Human, Pair 4

Abstract

This 15-month boy was expressed at the cytogenetic laboratory because of psychomotor development delay. He was tall and had plagiocephaly, micrognathia, high nasal bridge, anteverted nostrils and pectus excavatum. A 46,XY,del(4)(p16.1p16.3) karyotype was found using high-resolution R-banding technique. FISH studies using the LSI Wolf-Hirschhorn dual color 4p16.3 and the TelVysion 4p probes showed no deletion. Using BACs, the distal breakpoint was located in 4p16.3, between RP11-165K4 and RP11-717M10 and the proximal breakpoint in 4p15.33, between RP11-74M11 and RP11-1J7; therefore, approximately 7.96 Mb of the short arm were deleted. The maternal karyotype showed the same deletion, but in a mosaic status. Two distinct phenotypes have been recognized on the basis of the chromosomal bands involved in 4p deletion: the Wolf-Hirschhorn syndrome (WHS) and a proximal 4p deletion syndrome (4p15.2-p15.32). Our observation confirms that the basic WHS phenotype maps distally to this region., (Copyright 2008 Wiley-Liss, Inc.)

Published

2008

11. Prenatal diagnosis of mosaic tetrasomy 8p.

Author

Le Bris MJ, Marcorelles P, Audrézet MP, Parent P, Heren P, Le Guern H, Herry A, Morel F, Collet M, Férec C, and De Braekeleer M

Subjects

Amniocentesis, Chromosome Aberrations, Chromosome Banding, Chromosome Disorders, Chromosomes ultrastructure, Female, Humans, In Situ Hybridization, Fluorescence, Isochromosomes, Karyotyping, Lymphocytes metabolism, Male, Maternal Age, Middle Aged, Phenotype, Placenta metabolism, Pregnancy, Aneuploidy, Chromosomes, Human, Pair 8, Mosaicism, Prenatal Diagnosis

Abstract

Tetrasomy 8p is a rare chromosomal disorder that has only been detected in a mosaic form. At the present time, 11 cases have been reported; their phenotype included agenesis of the corpus callosum, enlarged ventricles, minor facial dysmorphism, rib and vertebral anomalies, and mild to moderate developmental delay. To the best of our knowledge, tetrasomy 8p has never been prenatally diagnosed. This 43-year-old woman was referred for amniocentesis at 20 weeks' gestation because of advanced maternal age. Amniotic fluid cells were cultured according to standard techniques by the in situ method. A supernumerary chromosomal marker was detected in a single clone of cultured amniotic cells and interpreted by RHG banding as an isochromosome of the short arm of chromosome 8 (i(8p)). The ultrasound investigation at 27 weeks gestation revealed enlarged ventricles and agenesis of the corpus callosum, which were confirmed at fetal autopsy after medical termination of the pregnancy. Chromosomal analyses, including RHG banding and FISH, of several tissues showed different levels of i(8p) mosaicism. Whereas no i(8p) was detected on cytotrophoblast nor additional amniotic fluid cells, 97% and 30% of cells from long-term cultures of placenta and lymphocytes, respectively, had the i(8p). Using DNA markers, the isochromosome 8p was interpreted as the result of a prezygotic event during maternal meiosis. Our findings suggest that the i(8p) is the subject of tissue selection. Tetrasomy 8p might be underdiagnosed during pregnancy; therefore, karyotyping on a fetal blood sample following detection of agenesis of the corpus callosum when no chromosomal abnormality has been found on the amniotic fluid cell cultures should be discussed with the parents., (Copyright 2003 Wiley-Liss, Inc.)

Published

2003