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1. Variants in CUL4B are Associated with Cerebral Malformations

Author

Vulto-van Silfhout, Anneke T, Nakagawa, Tadashi, Bahi-Buisson, Nadia, Haas, Stefan A, Hu, Hao, Bienek, Melanie, Vissers, Lisenka ELM, Gilissen, Christian, Tzschach, Andreas, Busche, Andreas, Müsebeck, Jörg, Rump, Patrick, Mathijssen, Inge B, Avela, Kristiina, Somer, Mirja, Doagu, Fatma, Philips, Anju K, Rauch, Anita, Baumer, Alessandra, Voesenek, Krysta, Poirier, Karine, Vigneron, Jacqueline, Amram, Daniel, Odent, Sylvie, Nawara, Magdalena, Obersztyn, Ewa, Lenart, Jacek, Charzewska, Agnieszka, Lebrun, Nicolas, Fischer, Ute, Nillesen, Willy M, Yntema, Helger G, Järvelä, Irma, Ropers, Hans-Hilger, de Vries, Bert BA, Brunner, Han G, van Bokhoven, Hans, Raymond, F Lucy, Willemsen, Michèl AAP, Chelly, Jamel, Xiong, Yue, Barkovich, A James, Kalscheuer, Vera M, Kleefstra, Tjitske, and de Brouwer, Arjan PM

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Genetics, Clinical Research, Intellectual and Developmental Disabilities (IDD), Brain Disorders, Neurosciences, Pediatric, Rare Diseases, Congenital Structural Anomalies, Aetiology, 2.1 Biological and endogenous factors, Neurological, Adolescent, Adult, Brain, Cell Cycle Proteins, Cells, Cultured, Child, Child, Preschool, Cullin Proteins, Genetic Association Studies, HEK293 Cells, Humans, Infant, Male, Malformations of Cortical Development, Mental Retardation, X-Linked, Middle Aged, Nerve Tissue Proteins, Pedigree, Sequence Analysis, DNA, Young Adult, CUL4B, WDR62, cortical dysplasia, hydrocephalus, intellectual disability, mutation, Clinical Sciences, Genetics & Heredity, Clinical sciences
Abstract

Variants in cullin 4B (CUL4B) are a known cause of syndromic X-linked intellectual disability. Here, we describe an additional 25 patients from 11 families with variants in CUL4B. We identified nine different novel variants in these families and confirmed the pathogenicity of all nontruncating variants. Neuroimaging data, available for 15 patients, showed the presence of cerebral malformations in ten patients. The cerebral anomalies comprised malformations of cortical development (MCD), ventriculomegaly, and diminished white matter volume. The phenotypic heterogeneity of the cerebral malformations might result from the involvement of CUL-4B in various cellular pathways essential for normal brain development. Accordingly, we show that CUL-4B interacts with WDR62, a protein in which variants were previously identified in patients with microcephaly and a wide range of MCD. This interaction might contribute to the development of cerebral malformations in patients with variants in CUL4B.

Published
2015

2. Otopalatodigital spectrum disorders: refinement of the phenotypic and mutational spectrum

Author

Moutton, Sébastien, Fergelot, Patricia, Naudion, Sophie, Cordier, Marie-Pierre, Solé, Guilhem, Guerineau, Elodie, Hubert, Christophe, Rooryck, Caroline, Vuillaume, Marie-Laure, Houcinat, Nada, Deforges, Julie, Bouron, Julie, Devès, Sylvie, Le Merrer, Martine, David, Albert, Geneviève, David, Giuliano, Fabienne, Journel, Hubert, Megarbane, André, Faivre, Laurence, Chassaing, Nicolas, Francannet, Christine, Sarrazin, Elisabeth, Stattin, Eva-Lena, Vigneron, Jacqueline, Leclair, Danielle, Abadie, Caroline, Sarda, Pierre, Baumann, Clarisse, Delrue, Marie-Ange, Arveiler, Benoit, Lacombe, Didier, Goizet, Cyril, and Coupry, Isabelle

Published
2016
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5. Intragenic CAMTA1 rearrangements cause non-progressive congenital ataxia with or without intellectual disability

Author

Thevenon, Julien, Lopez, Estelle, Keren, Boris, Heron, Delphine, Mignot, Cyril, Altuzarra, Cecilia, Béri-Dexheimer, Mylène, Bonnet, Céline, Magnin, Eloi, Burglen, Lydie, Minot, Delphine, Vigneron, Jacqueline, Morle, Sophie, Anheim, Mathieu, Charles, Perrine, Brice, Alexis, Gallagher, Louise, Amiel, Jeanne, Haffen, Emmanuel, Mach, Corinne, Depienne, Christel, Doummar, Diane, Bonnet, Marlène, Duplomb, Laurence, Carmignac, Virginie, Callier, Patrick, Marle, Nathalie, Mosca-Boidron, Anne-Laure, Roze, Virginie, Aral, Bernard, Razavi, Ferechte, Jonveaux, Philippe, Faivre, Laurence, and Thauvin-Robinet, Christel

Published
2012
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7. Search for the best indicators for the presence of a VPS13B gene mutation and confirmation of diagnostic criteria in a series of 34 patients genotyped for suspected Cohen syndrome

Author

El Chehadeh, Salima, Aral, Bernard, Gigot, Nadège, Thauvin-Robinet, Christel, Donzel, Anne, Delrue, Marie-Ange, Lacombe, Didier, David, Albert, Burglen, Lydie, Philip, Nicole, Moncla, Anne, Cormier-Daire, Valérie, Rio, Marlène, Edery, Patrick, Verloes, Alain, Bonneau, Dominique, Afenjar, Alexandra, Jacquette, Aurélia, Heron, Delphine, Sarda, Pierre, Pinson, Lucile, Doray, Bérénice, Vigneron, Jacqueline, Leheup, Bruno, Frances-Guidet, Anne-Marie, Dienne, Gwenaelle, Holder, Muriel, Masurel-Paulet, Alice, Huet, Frédéric, Teyssier, Jean-Raymond, and Faivre, Laurence

Published
2010
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8. GJB2 and GJB6 Mutations: Genotypic and Phenotypic Correlations in a Large Cohort of Hearing-Impaired Patients

Author

Marlin, Sandrine, Feldmann, Delphine, Blons, Hélène, Loundon, Natalie, Rouillon, Isabelle, Albert, Sébastien, Chauvin, Pierre, Garabédian, Eréa-Noël, Couderc, Rémy, Odent, Sylvie, Joannard, Alain, Schmerber, Sébastien, Delobel, Bruno, Leman, Jacques, Journel, Hubert, Catros, Hélène, Lemarechal, Cédric, Dollfus, Hélène, Eliot, Marie-Madeleine, Delaunoy, Jean-Louis, David, Albert, Calais, Catherine, Drouin-Garraud, Valérie, Obstoy, Marie-Françoise, Goizet, Cyril, Duriez, Françoise, Fellmann, Florence, Hélias, Jocelyne, Vigneron, Jacqueline, Montaut, Bettina, Matin-Coignard, Dominique, Faivre, Laurence, Baumann, Clarisse, Lewin, Patricia, Petit, Christine, and Denoyelle, Françoise

Published
2005

11. Complete exon sequencing of all known Usher syndrome genes greatly improves molecular diagnosis

Author

Lacombe Didier, Mom Thierry, Francannet Christine, Duvillard Alain, Thauvin Christel, Dubin Jacques, Bonneau Dominique, Montaut-Verient Bettina, Vigneron Jacqueline, Calais Catherine, David Albert, Eliot Marie-Madeleine, Dollfus Hélène, Vincent Christophe, Delobel Bruno, Weil Dominique, El-Amraoui Aziz, Jonard Laurence, Feldmann Delphine, Zelenika Diana, Délépine Marc, Niasme-Grare Magali, Parodi Marine, Hardelin Jean-Pierre, Levilliers Jacqueline, Marlin Sandrine, Grati M'hamed, Bonnet Crystel, Duriez Françoise, Drouin-Garraud Valérie, Thuillier-Obstoy Marie-Françoise, Sigaudy Sabine, Frances Anne-Marie, Collignon Patrick, Challe Georges, Couderc Rémy, Lathrop Mark, Sahel José-Alain, Weissenbach Jean, Petit Christine, and Denoyelle Françoise

Subjects
Medicine
Abstract

Abstract Background Usher syndrome (USH) combines sensorineural deafness with blindness. It is inherited in an autosomal recessive mode. Early diagnosis is critical for adapted educational and patient management choices, and for genetic counseling. To date, nine causative genes have been identified for the three clinical subtypes (USH1, USH2 and USH3). Current diagnostic strategies make use of a genotyping microarray that is based on the previously reported mutations. The purpose of this study was to design a more accurate molecular diagnosis tool. Methods We sequenced the 366 coding exons and flanking regions of the nine known USH genes, in 54 USH patients (27 USH1, 21 USH2 and 6 USH3). Results Biallelic mutations were detected in 39 patients (72%) and monoallelic mutations in an additional 10 patients (18.5%). In addition to biallelic mutations in one of the USH genes, presumably pathogenic mutations in another USH gene were detected in seven patients (13%), and another patient carried monoallelic mutations in three different USH genes. Notably, none of the USH3 patients carried detectable mutations in the only known USH3 gene, whereas they all carried mutations in USH2 genes. Most importantly, the currently used microarray would have detected only 30 of the 81 different mutations that we found, of which 39 (48%) were novel. Conclusions Based on these results, complete exon sequencing of the currently known USH genes stands as a definite improvement for molecular diagnosis of this disease, which is of utmost importance in the perspective of gene therapy.

Published
2011
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12. Further delineation of theMECP2duplication syndrome phenotype in 59 French male patients, with a particular focus on morphological and neurological features

Author

Miguet, Marguerite, primary, Faivre, Laurence, additional, Amiel, Jeanne, additional, Nizon, Mathilde, additional, Touraine, Renaud, additional, Prieur, Fabienne, additional, Pasquier, Laurent, additional, Lefebvre, Mathilde, additional, Thevenon, Julien, additional, Dubourg, Christèle, additional, Julia, Sophie, additional, Sarret, Catherine, additional, Remerand, Ganaëlle, additional, Francannet, Christine, additional, Laffargue, Fanny, additional, Boespflug-Tanguy, Odile, additional, David, Albert, additional, Isidor, Bertrand, additional, Vigneron, Jacqueline, additional, Leheup, Bruno, additional, Lambert, Laetitia, additional, Philippe, Christophe, additional, Béri-Dexheimer, Mylène, additional, Cuisset, Jean-Marie, additional, Andrieux, Joris, additional, Plessis, Ghislaine, additional, Toutain, Annick, additional, Guibaud, Laurent, additional, Cormier-Daire, Valérie, additional, Rio, Marlene, additional, Bonnefont, Jean-Paul, additional, Echenne, Bernard, additional, Journel, Hubert, additional, Burglen, Lydie, additional, Chantot-Bastaraud, Sandrine, additional, Bienvenu, Thierry, additional, Baumann, Clarisse, additional, Perrin, Laurence, additional, Drunat, Séverine, additional, Jouk, Pierre-Simon, additional, Dieterich, Klaus, additional, Devillard, Françoise, additional, Lacombe, Didier, additional, Philip, Nicole, additional, Sigaudy, Sabine, additional, Moncla, Anne, additional, Missirian, Chantal, additional, Badens, Catherine, additional, Perreton, Nathalie, additional, Thauvin-Robinet, Christel, additional, AChro-Puce, Réseau, additional, Pedespan, Jean-Michel, additional, Rooryck, Caroline, additional, Goizet, Cyril, additional, Vincent-Delorme, Catherine, additional, Duban-Bedu, Bénédicte, additional, Bahi-Buisson, Nadia, additional, Afenjar, Alexandra, additional, Maincent, Kim, additional, Héron, Delphine, additional, Alessandri, Jean-Luc, additional, Martin-Coignard, Dominique, additional, Lesca, Gaëtan, additional, Rossi, Massimiliano, additional, Raynaud, Martine, additional, Callier, Patrick, additional, Mosca-Boidron, Anne-Laure, additional, Marle, Nathalie, additional, Coutton, Charles, additional, Satre, Véronique, additional, Caignec, Cédric Le, additional, Malan, Valérie, additional, Romana, Serge, additional, Keren, Boris, additional, Tabet, Anne-Claude, additional, Kremer, Valérie, additional, Scheidecker, Sophie, additional, Vigouroux, Adeline, additional, Lackmy-Port-Lis, Marilyn, additional, Sanlaville, Damien, additional, Till, Marianne, additional, Carneiro, Maryline, additional, Gilbert-Dussardier, Brigitte, additional, Willems, Marjolaine, additional, Van Esch, Hilde, additional, Portes, Vincent Des, additional, and El Chehadeh, Salima, additional

Published
2018
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13. Variants in CUL4B are Associated with Cerebral Malformations

Author

Philips, Anju K., Voesenek, Krysta, Willemsen, Michèl A.A.P., Obersztyn, Ewa, Xiong, Yue, de Vries, Bert B.A., Odent, Sylvie, Kleefstra, Tjitske, Lebrun, Nicolas, van Bokhoven, Hans, Charzewska, Agnieszka, Chelly, Jamel, Fischer, Ute, Ropers, Hans-Hilger, Nillesen, Willy M., Vigneron, Jacqueline, Baumer, Alessandra, Lenart, Jacek, Barkovich, A. James, Brunner, Han G., Rauch, Anita, Kalscheuer, Vera M., Poirier, Karine, Yntema, Helger G., Amram, Daniel, de Brouwer, Arjan P.M., Nawara, Magdalena, Raymond, F. Lucy, and Järvelä, Irma

Abstract

Variants in cullin 4B (CUL4B) are a known cause of syndromic X-linked intellectual disability. Here, we describe an additional 25 patients from 11 families with variants in CUL4B. We identified nine different novel variants in these families and confirmed the pathogenicity of all nontruncating variants. Neuroimaging data, available for 15 patients, showed the presence of cerebral malformations in ten patients. The cerebral anomalies comprised malformations of cortical development (MCD), ventriculomegaly, and diminished white matter volume. The phenotypic heterogeneity of the cerebral malformations might result from the involvement of CUL-4B in various cellular pathways essential for normal brain development. Accordingly, we show that CUL-4B interacts with WDR62, a protein in which variants were previously identified in patients with microcephaly and a wide range of MCD. This interaction might contribute to the development of cerebral malformations in patients with variants in CUL4B.

Published
2015
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14. Increased dosage of RAB39B affects neuronal development and could explain the cognitive impairment in male patients with distal Xq28 copy number gains

Author

Katrin Õunap, Maila Giannandrea, Vigneron Jacqueline, Martine Raynaud, Nathalie Fieremans, Patrizia D'Adamo, Jelle Verbeeck, Hilde Van Esch, Guy Froyen, Lieselot Vanmarsenille, Annick Vogels, Stefanie Belet, Katrin Männik, Sylvain Briault, Clinical sciences, and Medical Genetics

Subjects
Estonia, Male, mice, DNA Copy Number Variations, Methyl-CpG-Binding Protein 2, European Continental Ancestry Group, Non-allelic homologous recombination, Methyl-CpG-Binding Protein 2/genetics, Biology, Hippocampal formation, Bioinformatics, White People, X-inactivation, MECP2, Neurons/cytology, Chromosomes, Human, X/genetics, Belgium, Intellectual Disability, Gene Duplication, rab GTP-Binding Proteins/genetics, Gene duplication, Genetics, Animals, Humans, Child, Gene, Genetics (clinical), Neurons, Regulation of gene expression, Chromosomes, Human, X, Chromosome Mapping, Cell Differentiation, Intellectual Disability/genetics, Xq28, Gene Expression Regulation, rab GTP-Binding Proteins, X chromosome inactivation
Abstract

Copy number gains at Xq28 are a frequent cause of X-linked intellectual disability (XLID). Here, we report on a recurrent 0.5 Mb tandem copy number gain at distal Xq28 not including MECP2, in four male patients with nonsyndromic mild ID and behavioral problems. The genomic region is duplicated in two families and triplicated in a third reflected by more distinctive clinical features. The X-inactivation patterns in carrier females correspond well with their clinical symptoms. Our mapping data confirm that this recurrent gain is likely mediated by nonallelic homologous recombination between two directly oriented Int22h repeats. The affected region harbors eight genes of which RAB39B encoding a small GTPase, was the prime candidate since loss-of-function mutations had been linked to ID. RAB39B is expressed at stable levels in lymphocytes from control individuals, suggesting a tight regulation. mRNA levels in our patients were almost two-fold increased. Overexpression of Rab39b in mouse primary hippocampal neurons demonstrated a significant decrease in neuronal branching as well as in the number of synapses when compared with the control neurons. Taken together, we provide evidence that the increased dosage of RAB39B causes a disturbed neuronal development leading to cognitive impairment in patients with this recurrent copy number gain.

Published
2014

16. Treacher Collins syndrome: a clinical and molecular study based on a large series of patients

Author

Vincent, Marie, primary, Geneviève, David, additional, Ostertag, Agnès, additional, Marlin, Sandrine, additional, Lacombe, Didier, additional, Martin-Coignard, Dominique, additional, Coubes, Christine, additional, David, Albert, additional, Lyonnet, Stanislas, additional, Vilain, Catheline, additional, Dieux-Coeslier, Anne, additional, Manouvrier, Sylvie, additional, Isidor, Bertrand, additional, Jacquemont, Marie-Line, additional, Julia, Sophie, additional, Layet, Valérie, additional, Naudion, Sophie, additional, Odent, Sylvie, additional, Pasquier, Laurent, additional, Pelras, Sybille, additional, Philip, Nicole, additional, Pierquin, Geneviève, additional, Prieur, Fabienne, additional, Aboussair, Nisrine, additional, Attie-Bitach, Tania, additional, Baujat, Geneviève, additional, Blanchet, Patricia, additional, Blanchet, Catherine, additional, Dollfus, Hélène, additional, Doray, Bérénice, additional, Schaefer, Elise, additional, Edery, Patrick, additional, Giuliano, Fabienne, additional, Goldenberg, Alice, additional, Goizet, Cyril, additional, Guichet, Agnès, additional, Herlin, Christian, additional, Lambert, Laetitia, additional, Leheup, Bruno, additional, Martinovic, Jelena, additional, Mercier, Sandra, additional, Mignot, Cyril, additional, Moutard, Marie-Laure, additional, Perez, Marie-José, additional, Pinson, Lucile, additional, Puechberty, Jacques, additional, Willems, Marjolaine, additional, Randrianaivo, Hanitra, additional, Szaskon, Kateline, additional, Toutain, Annick, additional, Verloes, Alain, additional, Vigneron, Jacqueline, additional, Sanchez, Elodie, additional, Sarda, Pierre, additional, Laplanche, Jean-Louis, additional, and Collet, Corinne, additional

Published
2016
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17. The expanding spectrum of COL2A1 gene variants IN 136 patients with a skeletal dysplasia phenotype

Author

Barat-Houari, Mouna, primary, Dumont, Bruno, additional, Fabre, Aurélie, additional, Them, Frédéric TM, additional, Alembik, Yves, additional, Alessandri, Jean-Luc, additional, Amiel, Jeanne, additional, Audebert, Séverine, additional, Baumann-Morel, Clarisse, additional, Blanchet, Patricia, additional, Bieth, Eric, additional, Brechard, Marie, additional, Busa, Tiffany, additional, Calvas, Patrick, additional, Capri, Yline, additional, Cartault, François, additional, Chassaing, Nicolas, additional, Ciorca, Vidrica, additional, Coubes, Christine, additional, David, Albert, additional, Delezoide, Anne-Lise, additional, Dupin-Deguine, Delphine, additional, El Chehadeh, Salima, additional, Faivre, Laurence, additional, Giuliano, Fabienne, additional, Goldenberg, Alice, additional, Isidor, Bertrand, additional, Jacquemont, Marie-Line, additional, Julia, Sophie, additional, Kaplan, Josseline, additional, Lacombe, Didier, additional, Lebrun, Marine, additional, Marlin, Sandrine, additional, Martin-Coignard, Dominique, additional, Martinovic, Jelena, additional, Masurel, Alice, additional, Melki, Judith, additional, Mozelle-Nivoix, Monique, additional, Nguyen, Karine, additional, Odent, Sylvie, additional, Philip, Nicole, additional, Pinson, Lucile, additional, Plessis, Ghislaine, additional, Quélin, Chloé, additional, Shaeffer, Elise, additional, Sigaudy, Sabine, additional, Thauvin, Christel, additional, Till, Marianne, additional, Touraine, Renaud, additional, Vigneron, Jacqueline, additional, Baujat, Geneviève, additional, Cormier-Daire, Valérie, additional, Le Merrer, Martine, additional, Geneviève, David, additional, and Touitou, Isabelle, additional

Published
2015
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18. Further delineation of the MECP2 duplication syndrome phenotype in 59 French male patients, with a particular focus on morphological and neurological features.

Author

Miguet, Marguerite, Faivre, Laurence, Amiel, Jeanne, Nizon, Mathilde, Touraine, Renaud, Prieur, Fabienne, Pasquier, Laurent, Lefebvre, Mathilde, Thevenon, Julien, Dubourg, Christèle, Julia, Sophie, Sarret, Catherine, Remerand, Ganaëlle, Francannet, Christine, Laffargue, Fanny, Boespflug-Tanguy, Odile, David, Albert, Isidor, Bertrand, Vigneron, Jacqueline, and Leheup, Bruno

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, broadbased 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. [ABSTRACT FROM AUTHOR]

Published
2018
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19. Large national series of patients with Xq28 duplication involving MECP2: Delineation of brain MRI abnormalities in 30 affected patients

Author

El Chehadeh, Salima, primary, Faivre, Laurence, additional, Mosca‐Boidron, Anne‐Laure, additional, Malan, Valérie, additional, Amiel, Jeanne, additional, Nizon, Mathilde, additional, Touraine, Renaud, additional, Prieur, Fabienne, additional, Pasquier, Laurent, additional, Callier, Patrick, additional, Lefebvre, Mathilde, additional, Marle, Nathalie, additional, Dubourg, Christèle, additional, Julia, Sophie, additional, Sarret, Catherine, additional, Francannet, Christine, additional, Laffargue, Fanny, additional, Boespflug‐Tanguy, Odile, additional, David, Albert, additional, Isidor, Bertrand, additional, Le Caignec, Cédric, additional, Vigneron, Jacqueline, additional, Leheup, Bruno, additional, Lambert, Laetitia, additional, Philippe, Christophe, additional, Cuisset, Jean‐Marie, additional, Andrieux, Joris, additional, Plessis, Ghislaine, additional, Toutain, Annick, additional, Goldenberg, Alice, additional, Cormier‐Daire, Valérie, additional, Rio, Marlène, additional, Bonnefont, Jean‐Paul, additional, Thevenon, Julien, additional, Echenne, Bernard, additional, Journel, Hubert, additional, Afenjar, Alexandra, additional, Burglen, Lydie, additional, Bienvenu, Thierry, additional, Addor, Marie‐Claude, additional, Lebon, Sébastien, additional, Martinet, Danièle, additional, Baumann, Clarisse, additional, Perrin, Laurence, additional, Drunat, Séverine, additional, Jouk, Pierre‐Simon, additional, Devillard, Françoise, additional, Coutton, Charles, additional, Lacombe, Didier, additional, Delrue, Marie‐Ange, additional, Philip, Nicole, additional, Moncla, Anne, additional, Badens, Catherine, additional, Perreton, Nathalie, additional, Masurel, Alice, additional, Thauvin‐Robinet, Christel, additional, Portes, Vincent Des, additional, and Guibaud, Laurent, additional

Published
2015
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20. A systematic variant screening in familial cases of congenital heart defects demonstrates the usefulness of molecular genetics in this field

Author

El Malti, Rajae, primary, Liu, Hui, additional, Doray, Bérénice, additional, Thauvin, Christel, additional, Maltret, Alice, additional, Dauphin, Claire, additional, Gonçalves-Rocha, Miguel, additional, Teboul, Michel, additional, Blanchet, Patricia, additional, Roume, Joëlle, additional, Gronier, Céline, additional, Ducreux, Corinne, additional, Veyrier, Magali, additional, Marçon, François, additional, Acar, Philippe, additional, Lusson, Jean-René, additional, Levy, Marilyne, additional, Beyler, Constance, additional, Vigneron, Jacqueline, additional, Cordier-Alex, Marie-Pierre, additional, Heitz, François, additional, Sanlaville, Damien, additional, Bonnet, Damien, additional, and Bouvagnet, Patrice, additional

Published
2015
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22. Variants inCUL4Bare Associated with Cerebral Malformations

Author

Vulto-van Silfhout, Anneke T., primary, Nakagawa, Tadashi, additional, Bahi-Buisson, Nadia, additional, Haas, Stefan A., additional, Hu, Hao, additional, Bienek, Melanie, additional, Vissers, Lisenka E.L.M., additional, Gilissen, Christian, additional, Tzschach, Andreas, additional, Busche, Andreas, additional, Müsebeck, Jörg, additional, Rump, Patrick, additional, Mathijssen, Inge B., additional, Avela, Kristiina, additional, Somer, Mirja, additional, Doagu, Fatma, additional, Philips, Anju K., additional, Rauch, Anita, additional, Baumer, Alessandra, additional, Voesenek, Krysta, additional, Poirier, Karine, additional, Vigneron, Jacqueline, additional, Amram, Daniel, additional, Odent, Sylvie, additional, Nawara, Magdalena, additional, Obersztyn, Ewa, additional, Lenart, Jacek, additional, Charzewska, Agnieszka, additional, Lebrun, Nicolas, additional, Fischer, Ute, additional, Nillesen, Willy M., additional, Yntema, Helger G., additional, Järvelä, Irma, additional, Ropers, Hans-Hilger, additional, de Vries, Bert B.A., additional, Brunner, Han G., additional, van Bokhoven, Hans, additional, Raymond, F. Lucy, additional, Willemsen, Michèl A.A.P., additional, Chelly, Jamel, additional, Xiong, Yue, additional, Barkovich, A. James, additional, Kalscheuer, Vera M., additional, Kleefstra, Tjitske, additional, and de Brouwer, Arjan P.M., additional

Published
2014
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23. Further delineation of the MECP2duplication syndrome phenotype in 59 French male patients, with a particular focus on morphological and neurological features

Author

Miguet, Marguerite, Faivre, Laurence, Amiel, Jeanne, Nizon, Mathilde, Touraine, Renaud, Prieur, Fabienne, Pasquier, Laurent, Lefebvre, Mathilde, Thevenon, Julien, Dubourg, Christèle, Julia, Sophie, Sarret, Catherine, Remerand, Ganaelle, Francannet, Christine, Laffargue, Fanny, Boespflug-Tanguy, Odile, David, Albert, Isidor, Bertrand, Vigneron, Jacqueline, Leheup, Bruno, Lambert, Laetitia, Philippe, Christophe, Bèèéri-Dexheimer, Mylèène, Cuisset, Jean-Marie, Andrieux, Joris, Plessis, Ghislaine, Toutain, Annick, Guibaud, Laurent, Cormier-Daire, Valèèéérie, Rio, Marlene, Bonnefont, Jean-Paul, Echenne, Bernard, Journel, Hubert, Burglen, Lydie, Chantot-Bastaraud, Sandrine, Bienvenu, Thierry, Baumann, Clarisse, Perrin, Laurence, Drunat, Sèèéééverine, Jouk, Pierre-Simon, Dieterich, Klaus, Devillard, Francoise, Lacombe, Didier, Philip, Nicole, Sigaudy, Sabine, Moncla, Anne, Missirian, Chantal, Badens, Catherine, Perreton, Nathalie, Thauvin-Robinet, Christel, AChro-Puce, Rèèééééseau, Pedespan, Jean-Michel, Rooryck, Caroline, Goizet, Cyril, Vincent-Delorme, Catherine, Duban-Bedu, Bèèééééénèèéééééédicte, Bahi-Buisson, Nadia, Afenjar, Alexandra, Maincent, Kim, Hèèéééééééron, Delphine, Alessandri, Jean-Luc, Martin-Coignard, Dominique, Lesca, Gaetan, Rossi, Massimiliano, Raynaud, Martine, Callier, Patrick, Mosca-Boidron, Anne-Laure, Marle, Nathalie, Coutton, Charles, Satre, Vèèééééééééronique, Caignec, Cèèééééééééédric Le, Malan, Valèèéééééééééérie, Romana, Serge, Keren, Boris, Tabet, Anne-Claude, Kremer, Valèèééééééééééérie, Scheidecker, Sophie, Vigouroux, Adeline, Lackmy-Port-Lis, Marilyn, Sanlaville, Damien, Till, Marianne, Carneiro, Maryline, Gilbert-Dussardier, Brigitte, Willems, Marjolaine, Van Esch, Hilde, Portes, Vincent Des, and El Chehadeh, Salima

Abstract

The Xq28 duplication involving the MECP2gene (MECP2duplication) 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 MECP2duplication. 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 MECP2duplication 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.

Published
2018
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24. Cobblestone-like brain dysgenesis and altered glycosylation in congenital cutis laxa, Debré type

Author

Van Maldergem, Lionel, Yuksel-Apak, Memnune, Kayserili, Hulya, Seemanova, Eva, Giurgea, Sanda, Basel-Vanagaite, Lina, Leao-Teles, Elisa, Vigneron, Jacqueline, Foulon, Martine, Greally, Marie, Jaeken, Jaak, Mundlos, Stefan, Dobyns, William Bill, Van Maldergem, Lionel, Yuksel-Apak, Memnune, Kayserili, Hulya, Seemanova, Eva, Giurgea, Sanda, Basel-Vanagaite, Lina, Leao-Teles, Elisa, Vigneron, Jacqueline, Foulon, Martine, Greally, Marie, Jaeken, Jaak, Mundlos, Stefan, and Dobyns, William Bill

Abstract

Objective: To delineate a new syndrome of brain dysgenesis and cutis laxa based on the description of 11 patients belonging to nine unrelated families recruited through an international collaboration effort. Methods: Careful clinical assessment of patients from birth to the age of 23 years with follow-up studies ranging from 3 to 20 years. Biochemical studies of serum proteins glycosylation by isoelectric focusing and capillary zone electrophoresis were performed in 10 patients. Brain MRI studies using conventional methods were analyzed in eight patients. Results: An expanded clinical spectrum of a syndrome comprising facial dysmorphia (enlarged anterior fontanelles, downward slant of palpebral fissures, prominent root of the nose), a connective tissue disorder (inguinal hernia, hip dislocation, high myopia), and neurologic impairment was defined. Early developmental delay was followed by onset of generalized seizures by the end of the first decade and a subsequent neurodegenerative course. A defect of N- or N- plus O-glycosylation of serum transferrins and ApoCIII was observed in 10 patients. An unusual cobblestone-like cortical malformation over the frontal and parietal regions was seen in eight patients and cerebellar abnormalities, including two patients with Dandy-Walker malformation, were observed in three patients. Conclusions: Our results suggest that autosomal recessive cutis laxa, Debré type, initially considered a dermatologic syndrome, is a multisystemic disorder with cobblestone-like brain dysgenesis manifesting as developmental delay and an epileptic neurodegenerative syndrome. It might represent a metabolic cause of Dandy-Walker malformation. It is associated with a deficient N- and-O glycosylation of proteins and shares many similarities with muscle-eye-brain syndromes. © 2008 by AAN Enterprises, Inc., SCOPUS: ar.j, info:eu-repo/semantics/published

Published
2008

25. Large deletions encompassing the TCOF1 and CAMK2A genes are responsible for Treacher Collins syndrome with intellectual disability

Author

Vincent, Marie, primary, Collet, Corinne, additional, Verloes, Alain, additional, Lambert, Laetitia, additional, Herlin, Christian, additional, Blanchet, Catherine, additional, Sanchez, Elodie, additional, Drunat, Séverine, additional, Vigneron, Jacqueline, additional, Laplanche, Jean-Louis, additional, Puechberty, Jacques, additional, Sarda, Pierre, additional, and Geneviève, David, additional

Published
2013
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27. IntragenicCAMTA1rearrangements cause non-progressive congenital ataxia with or without intellectual disability

Author

Thevenon, Julien, primary, Lopez, Estelle, additional, Keren, Boris, additional, Heron, Delphine, additional, Mignot, Cyril, additional, Altuzarra, Cecilia, additional, Béri-Dexheimer, Mylène, additional, Bonnet, Céline, additional, Magnin, Eloi, additional, Burglen, Lydie, additional, Minot, Delphine, additional, Vigneron, Jacqueline, additional, Morle, Sophie, additional, Anheim, Mathieu, additional, Charles, Perrine, additional, Brice, Alexis, additional, Gallagher, Louise, additional, Amiel, Jeanne, additional, Haffen, Emmanuel, additional, Mach, Corinne, additional, Depienne, Christel, additional, Doummar, Diane, additional, Bonnet, Marlène, additional, Duplomb, Laurence, additional, Carmignac, Virginie, additional, Callier, Patrick, additional, Marle, Nathalie, additional, Mosca-Boidron, Anne-Laure, additional, Roze, Virginie, additional, Aral, Bernard, additional, Razavi, Ferechte, additional, Jonveaux, Philippe, additional, Faivre, Laurence, additional, and Thauvin-Robinet, Christel, additional

Published
2012
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29. Complete exon sequencing of all known Usher syndrome genes greatly improves molecular diagnosis

Author

Bonnet, Crystel, primary, Grati, M'hamed, additional, Marlin, Sandrine, additional, Levilliers, Jacqueline, additional, Hardelin, Jean-Pierre, additional, Parodi, Marine, additional, Niasme-Grare, Magali, additional, Zelenika, Diana, additional, Délépine, Marc, additional, Feldmann, Delphine, additional, Jonard, Laurence, additional, El-Amraoui, Aziz, additional, Weil, Dominique, additional, Delobel, Bruno, additional, Vincent, Christophe, additional, Dollfus, Hélène, additional, Eliot, Marie-Madeleine, additional, David, Albert, additional, Calais, Catherine, additional, Vigneron, Jacqueline, additional, Montaut-Verient, Bettina, additional, Bonneau, Dominique, additional, Dubin, Jacques, additional, Thauvin, Christel, additional, Duvillard, Alain, additional, Francannet, Christine, additional, Mom, Thierry, additional, Lacombe, Didier, additional, Duriez, Françoise, additional, Drouin-Garraud, Valérie, additional, Thuillier-Obstoy, Marie-Françoise, additional, Sigaudy, Sabine, additional, Frances, Anne-Marie, additional, Collignon, Patrick, additional, Challe, Georges, additional, Couderc, Rémy, additional, Lathrop, Mark, additional, Sahel, José-Alain, additional, Weissenbach, Jean, additional, Petit, Christine, additional, and Denoyelle, Françoise, additional

Published
2011
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30. Notable contribution of large CFTR gene rearrangements to the diagnosis of cystic fibrosis in fetuses with bowel anomalies

Author

de Becdelièvre, Alix, primary, Costa, Catherine, additional, LeFloch, Annick, additional, Legendre, Marie, additional, Jouannic, Jean-Marie, additional, Vigneron, Jacqueline, additional, Bresson, Jean-Luc, additional, Gobin, Stéphanie, additional, Martin, Josiane, additional, Goossens, Michel, additional, and Girodon, Emmanuelle, additional

Published
2010
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31. Large deletion of theGJB6gene in deaf patients heterozygous for theGJB2gene mutation: Genotypic and phenotypic analysis

Author

Feldmann, Delphine, primary, Denoyelle, Françoise, additional, Chauvin, Pierre, additional, Garabédian, Eréa-Noël, additional, Couderc, Rémy, additional, Odent, Sylvie, additional, Joannard, Alain, additional, Schmerber, Sébastien, additional, Delobel, Bruno, additional, Leman, Jacques, additional, Journel, Hubert, additional, Catros, Hélène, additional, Maréchal, Cédric Le, additional, Dollfus, Hélène, additional, Eliot, Marie-Madeleine, additional, Delaunoy, Jean-Pierre, additional, David, Albert, additional, Calais, Catherine, additional, Drouin-Garraud, Valérie, additional, Obstoy, Marie-Françoise, additional, Bouccara, Didier, additional, Sterkers, Olivier, additional, Huy, Patrice Tran Ba, additional, Goizet, Cyril, additional, Duriez, Françoise, additional, Fellmann, Florence, additional, Hélias, Jocelyne, additional, Vigneron, Jacqueline, additional, Montaut, Bétina, additional, Lewin, Patricia, additional, Petit, Christine, additional, and Marlin, Sandrine, additional

Published
2004
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32. The expanding spectrum of COL2A1 gene variants IN 136 patients with a skeletal dysplasia phenotype

Author

Barat-Houari, Mouna, Dumont, Bruno, Fabre, Aurélie, Them, Frédéric TM, Alembik, Yves, Alessandri, Jean-Luc, Amiel, Jeanne, Audebert, Séverine, Baumann-Morel, Clarisse, Blanchet, Patricia, Bieth, Eric, Brechard, Marie, Busa, Tiffany, Calvas, Patrick, Capri, Yline, Cartault, François, Chassaing, Nicolas, Ciorca, Vidrica, Coubes, Christine, David, Albert, Delezoide, Anne-Lise, Dupin-Deguine, Delphine, El Chehadeh, Salima, Faivre, Laurence, Giuliano, Fabienne, Goldenberg, Alice, Isidor, Bertrand, Jacquemont, Marie-Line, Julia, Sophie, Kaplan, Josseline, Lacombe, Didier, Lebrun, Marine, Marlin, Sandrine, Martin-Coignard, Dominique, Martinovic, Jelena, Masurel, Alice, Melki, Judith, Mozelle-Nivoix, Monique, Nguyen, Karine, Odent, Sylvie, Philip, Nicole, Pinson, Lucile, Plessis, Ghislaine, Quélin, Chloé, Shaeffer, Elise, Sigaudy, Sabine, Thauvin, Christel, Till, Marianne, Touraine, Renaud, Vigneron, Jacqueline, Baujat, Geneviève, Cormier-Daire, Valérie, Le Merrer, Martine, Geneviève, David, and Touitou, Isabelle

Abstract

Heterozygous COL2A1 variants cause a wide spectrum of skeletal dysplasia termed type II collagenopathies. We assessed the impact of this gene in our French series. A decision tree was applied to select 136 probands (71 Stickler cases, 21 Spondyloepiphyseal dysplasia congenita cases, 11 Kniest dysplasia cases, and 34 other dysplasia cases) before molecular diagnosis by Sanger sequencing. We identified 66 different variants among the 71 positive patients. Among those patients, 18 belonged to multiplex families and 53 were sporadic. Most variants (38/44, 86%) were located in the triple helical domain of the collagen chain and glycine substitutions were mainly observed in severe phenotypes, whereas arginine to cysteine changes were more often encountered in moderate phenotypes. This series of skeletal dysplasia is one of the largest reported so far, adding 44 novel variants (15%) to published data. We have confirmed that about half of our Stickler patients (46%) carried a COL2A1 variant, and that the molecular spectrum was different across the phenotypes. To further address the question of genotype–phenotype correlation, we plan to screen our patients for other candidate genes using a targeted next-generation sequencing approach.

Published
2016
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33. A systematic variant screening in familial cases of congenital heart defects demonstrates the usefulness of molecular genetics in this field

Author

El Malti, Rajae, Liu, Hui, Doray, Bérénice, Thauvin, Christel, Maltret, Alice, Dauphin, Claire, Gonçalves-Rocha, Miguel, Teboul, Michel, Blanchet, Patricia, Roume, Joëlle, Gronier, Céline, Ducreux, Corinne, Veyrier, Magali, Marçon, François, Acar, Philippe, Lusson, Jean-René, Levy, Marilyne, Beyler, Constance, Vigneron, Jacqueline, Cordier-Alex, Marie-Pierre, Heitz, François, Sanlaville, Damien, Bonnet, Damien, and Bouvagnet, Patrice

Abstract

The etiology of congenital heart defect (CHD) combines environmental and genetic factors. So far, there were studies reporting on the screening of a single gene on unselected CHD or on familial cases selected for specific CHD types. Our goal was to systematically screen a proband of familial cases of CHD on a set of genetic tests to evaluate the prevalence of disease-causing variant identification. A systematic screening of GATA4, NKX2-5, ZIC3 and Multiplex ligation-dependent probe amplification (MLPA) P311 Kit was setup on the proband of 154 families with at least two cases of non-syndromic CHD. Additionally, ELN screening was performed on families with supravalvular arterial stenosis. Twenty-two variants were found, but segregation analysis confirmed unambiguously the causality of 16 variants: GATA4 (1 ×), NKX2-5 (6 ×), ZIC3 (3 ×), MLPA (2 ×) and ELN (4 ×). Therefore, this approach was able to identify the causal variant in 10.4% of familial CHD cases. This study demonstrated the existence of a de novo variant even in familial CHD cases and the impact of CHD variants on adult cardiac condition even in the absence of CHD. This study showed that the systematic screening of genetic factors is useful in familial CHD cases with up to 10.4% elucidated cases. When successful, it drastically improved genetic counseling by discovering unaffected variant carriers who are at risk of transmitting their variant and are also exposed to develop cardiac complications during adulthood thus prompting long-term cardiac follow-up. This study provides an important baseline at dawning of the next-generation sequencing era.

Published
2016
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34. Large deletions encompassing the TCOF1 and CAMK2A genes are responsible for Treacher Collins syndrome with intellectual disability.

Author

Vincent, Marie, Collet, Corinne, Verloes, Alain, Lambert, Laetitia, Herlin, Christian, Blanchet, Catherine, Sanchez, Elodie, Drunat, Séverine, Vigneron, Jacqueline, Laplanche, Jean-Louis, Puechberty, Jacques, Sarda, Pierre, and Geneviève, David

Subjects
MANDIBULOFACIAL dysostosis, ESOPHAGEAL atresia, COGNITIVE development, TRANSCRIPTION factors, ARYLSULFATASES
Abstract

Mandibulofacial dysostosis is part of a clinically and genetically heterogeneous group of disorders of craniofacial development, which lead to malar and mandibular hypoplasia. Treacher Collins syndrome is the major cause of mandibulofacial dysostosis and is due to mutations in the TCOF1 gene. Usually patients with Treacher Collins syndrome do not present with intellectual disability. Recently, the EFTUD2 gene was identified in patients with mandibulofacial dysostosis associated with microcephaly, intellectual disability and esophageal atresia. We report on two patients presenting with mandibulofacial dysostosis characteristic of Treacher Collins syndrome, but associated with unexpected intellectual disability, due to a large deletion encompassing several genes including the TCOF1 gene. We discuss the involvement of the other deleted genes such as CAMK2A or SLC6A7 in the cognitive development delay of the patients reported, and we propose the systematic investigation for 5q32 deletion when intellectual disability is associated with Treacher Collins syndrome. [ABSTRACT FROM AUTHOR]

Published
2014
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36. A human homologue of the Drosophila eyes absent gene underlies Branchio-Oto-Renal (BOR) syndrome and identifies a novel gene family

Author

Abdelhak, Sonia, primary, Kalatzis, Vasiliki, additional, Heilig, Roland, additional, Compain, Sylvie, additional, Samson, Delphine, additional, Vincent, Christophe, additional, Weil, Dominique, additional, Cruaud, Corinne, additional, Sahly, Iman, additional, Leibovici, Michel, additional, Bitner-Glindzicz, Maria, additional, Francis, Mary, additional, Lacombe, Didier, additional, Vigneron, Jacqueline, additional, Charachon, Robert, additional, Boven, Katia, additional, Bedbeder, Philippe, additional, Regemorter, Nicole Van, additional, Weissenbach, Jean, additional, and Petit, Christine, additional

Published
1997
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37. A proposed new contiguous gene syndrome on 8q consists of Branchio-Oto-Renal (BOR) syndrome, Duane syndrome, a dominant form of hydrocephalus and trapeze aplasia; implications for the mapping of the BOR gene

Author

Vincent, Christophe, primary, Kalatzis, Vasiliki, additional, Compain, Sylvie, additional, Levilliers, Jacqueline, additional, Slim, Rima, additional, Graia, Fatima, additional, Pereira, Maria de Lurdes, additional, Nivelon, Annie, additional, Croquette, Marie-France, additional, Lacombe, Didier, additional, Vigneron, Jacqueline, additional, Helias, Jocelyne, additional, Broyer, Michel, additional, Callen, David F., additional, Haan, Eric A., additional, Weissenbach, Jean, additional, Lacroix, Bruno, additional, Bellané-Chantelot, Christine, additional, Paslier, Denis Le, additional, Cohen, Daniel, additional, and Petit, Christine, additional

Published
1994
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38. A novel TFAP2A mutation in familial Branchio-Oculo-Facial Syndrome with predominant ocular phenotype.

Author

Aliferis, Konstantinos, Stoetzel, Corinne, Pelletier, Valérie, Hellé, Sophie, Angioï-Duprez, Karine, Vigneron, Jacqueline, Leheup, Bruno, Marion, Vincent, and Dollfus, Hélène

Subjects
GENETIC mutation, PHENOTYPES, VELOCARDIOFACIAL syndrome, GENE expression, CLEFT lip
Abstract

Introduction: Branchio-Oculo-Facial Syndrome (BOFS) is a rare autosomal dominant congenital disorder defined by branchial defects, ocular anomalies and craniofacial malformations, including variable degrees of cleft lip with or without cleft palate. In addition, temporal bone anomalies, renal and ectodermal manifestations can be present. Mutations in the TFAP2A gene have been reported in patients with BOFS, prompting phenotype-genotype studies because of the variable clinical spectrum. Materials and Methods: We report on a family (a mother, her daughter and son) with BOFS and significant variability in clinical expression. The daughter presents predominantly with an ocular phenotype of unilateral microphthalmia and bilateral chorioretinal colobomas, whereas her brother is more severely affected contrasting with the paucisymptomatic mother. TFAP2A molecular analysis revealed a novel frameshift mutation. Discussion: We confirm the wide clinical spectrum of BOFS. The importance of upper lip examination in mild and paucisymptomatic cases is underlined. TFAP2A mutation spectrum is discussed and broadened by the report of the second frameshift mutation in this gene. Conclusion: Patients with BOFS and predominant ocular phenotypes can be underdiagnosed. In such cases, upper lip examination can be of important diagnostic value. TFAP2A analysis provides diagnostic confirmation and improves genetic counselling. [ABSTRACT FROM AUTHOR]

Published
2011
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40. Distal trisomy 14q.

Author

Gilgenkrantz, Simone, Vigneron, Jacqueline, Peter, Marie-Odile, Dufier, J., Teboul, M., Chery, Michèle, Keyeux, Genoveva, and Lefranc, Marie-Paule

Abstract

Two cases of de novo duplication of the distal part of the long arm of chromosome 14 are reported. In one case, the partial trisomy of 14q is due to translocation of a segment (14q24 to 14qter) at the end of the satellite stalk of chromosome 14. The clinical picture is very severe. In the second case, a tandem duplication in 14 (q23→q32) is present with only minor malformations and mild mental retardation. [ABSTRACT FROM AUTHOR]

Published
1990
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41. Large national series of patients with Xq28 duplication involving MECP2: Delineation of brain MRI abnormalities in 30 affected patients.

Author

El Chehadeh S, Faivre L, Mosca-Boidron AL, Malan V, Amiel J, Nizon M, Touraine R, Prieur F, Pasquier L, Callier P, Lefebvre M, Marle N, Dubourg C, Julia S, Sarret C, Francannet C, Laffargue F, Boespflug-Tanguy O, David A, Isidor B, Le Caignec C, Vigneron J, Leheup B, Lambert L, Philippe C, Cuisset JM, Andrieux J, Plessis G, Toutain A, Goldenberg A, Cormier-Daire V, Rio M, Bonnefont JP, Thevenon J, Echenne B, Journel H, Afenjar A, Burglen L, Bienvenu T, Addor MC, Lebon S, Martinet D, Baumann C, Perrin L, Drunat S, Jouk PS, Devillard F, Coutton C, Lacombe D, Delrue MA, Philip N, Moncla A, Badens C, Perreton N, Masurel A, Thauvin-Robinet C, Des Portes V, and Guibaud L

Subjects
Adolescent, Adult, Brain Diseases pathology, Child, Child, Preschool, Female, Genetic Association Studies, Genotype, Humans, Infant, Infant, Newborn, Male, Mental Retardation, X-Linked pathology, Middle Aged, Pedigree, Phenotype, Prognosis, Young Adult, Brain Diseases genetics, Chromosomes, Human, X genetics, Gene Duplication, Magnetic Resonance Imaging methods, Mental Retardation, X-Linked genetics, Methyl-CpG-Binding Protein 2 genetics
Abstract

Xq28 duplications encompassing MECP2 have been described in male patients with a severe neurodevelopmental disorder associated with hypotonia and spasticity, severe learning disability, stereotyped movements, and recurrent pulmonary infections. We report on standardized brain magnetic resonance imaging (MRI) data of 30 affected patients carrying an Xq28 duplication involving MECP2 of various sizes (228 kb to 11.7 Mb). The aim of this study was to seek recurrent malformations and attempt to determine whether variations in imaging features could be explained by differences in the size of the duplications. We showed that 93% of patients had brain MRI abnormalities such as corpus callosum abnormalities (n = 20), reduced volume of the white matter (WM) (n = 12), ventricular dilatation (n = 9), abnormal increased hyperintensities on T2-weighted images involving posterior periventricular WM (n = 6), and vermis hypoplasia (n = 5). The occipitofrontal circumference varied considerably between >+2SD in five patients and <-2SD in four patients. Among the nine patients with dilatation of the lateral ventricles, six had a duplication involving L1CAM. The only patient harboring bilateral posterior subependymal nodular heterotopia also carried an FLNA gene duplication. We could not demonstrate a correlation between periventricular WM hyperintensities/delayed myelination and duplication of the IKBKG gene. We thus conclude that patients with an Xq28 duplication involving MECP2 share some similar but non-specific brain abnormalities. These imaging features, therefore, could not constitute a diagnostic clue. The genotype-phenotype correlation failed to demonstrate a relationship between the presence of nodular heterotopia, ventricular dilatation, WM abnormalities, and the presence of FLNA, L1CAM, or IKBKG, respectively, in the duplicated segment., (© 2015 Wiley Periodicals, Inc.)

Published
2016
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42. GJB2 and GJB6 mutations: genotypic and phenotypic correlations in a large cohort of hearing-impaired patients.

Author

Marlin S, Feldmann D, Blons H, Loundon N, Rouillon I, Albert S, Chauvin P, Garabédian EN, Couderc R, Odent S, Joannard A, Schmerber S, Delobel B, Leman J, Journel H, Catros H, Lemarechal C, Dollfus H, Eliot MM, Delaunoy JL, David A, Calais C, Drouin-Garraud V, Obstoy MF, Goizet C, Duriez F, Fellmann F, Hélias J, Vigneron J, Montaut B, Matin-Coignard D, Faivre L, Baumann C, Lewin P, Petit C, and Denoyelle F

Subjects
Chromosome Deletion, Connexin 26, Connexin 30, DNA Mutational Analysis, Genotype, Hearing Disorders physiopathology, Humans, Mutation, Phenotype, Prospective Studies, Connexins genetics, Hearing Disorders genetics
Abstract

Objectives: To analyze the clinical features of hearing impairment and to search for correlations with the genotype in patients with DFNB1., Design: Case series., Setting: Collaborative study in referral centers, institutional practice. Patients A total of 256 hearing-impaired patients selected on the basis of the presence of biallelic mutations in GJB2 or the association of 1 GJB2 mutation with the GJB6 deletion (GJB6-D13S1830)del., Main Outcome Measures: The prevalence of GJB2 mutations and the GJB6 deletion and audiometric phenotypes related to the most frequent genotypes., Results: Twenty-nine different GJB2 mutations were identified. Allelic frequency of 35delG was 69%, and the other common mutations, 313del14, E47X, Q57X, and L90P, accounted for 2.6% to 2.9% of the variants. Concerning GJB6, (GJB6-D13S1830)del accounted for 5% of all mutated alleles and was observed in 25 of 93 compound heterozygous patients. Three novel GJB2 mutations, 355del9, V95M, and 573delCA, were identified. Hearing impairment was frequently less severe in compound heterozygotes 35delG/L90P and 35delG/N206S than in 35delG homozygotes. Moderate or mild hearing impairment was more frequent in patients with 1 or 2 noninactivating mutations than in patients with 2 inactivating mutations. Of 93 patients, hearing loss was stable in 73, progressive in 21, and fluctuant in 2. Progressive hearing loss was more frequent in patients with 1 or 2 noninactivating mutations than in those with 2 inactivating mutations. In 49 families, hearing loss was compared between siblings with similar genotypes, and variability in terms of severity was found in 18 families (37%)., Conclusion: Genotype may affect deafness severity, but environmental and other genetic factors may also modulate the severity and evolution of GJB2-GJB6 deafness.

Published
2005
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43. Large deletion of the GJB6 gene in deaf patients heterozygous for the GJB2 gene mutation: genotypic and phenotypic analysis.

Author

Feldmann D, Denoyelle F, Chauvin P, Garabédian EN, Couderc R, Odent S, Joannard A, Schmerber S, Delobel B, Leman J, Journel H, Catros H, Le Maréchal C, Dollfus H, Eliot MM, Delaunoy JP, David A, Calais C, Drouin-Garraud V, Obstoy MF, Bouccara D, Sterkers O, Huy PT, Goizet C, Duriez F, Fellmann F, Hélias J, Vigneron J, Montaut B, Lewin P, Petit C, and Marlin S

Subjects
Connexin 26, Connexin 30, Humans, Phenotype, Connexins genetics, Deafness genetics, Gene Deletion, Heterozygote, Mutation
Abstract

Recent investigations identified a large deletion of the GJB6 gene in trans to a mutation of GJB2 in deaf patients. We looked for GJB2 mutations and GJB6 deletions in 255 French patients presenting with a phenotype compatible with DFNB1. 32% of the patients had biallelic GJB2 mutations and 6% were a heterozygous for a GJB2 mutation and a GJB6 deletion. Biallelic GJB2 mutations and combined GJB2/GJB6 anomalies were more frequent in profoundly deaf children. Based on these results, we are now assessing GJB6 deletion status in cases of prelingual hearing loss., (Copyright 2004 Wiley-Liss, Inc.)

Published
2004
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