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46 results on '"A, Toutain"'

1. A new case of Kaufman Oculocerebrofacial syndrome caused by two splicing variants in UBE3B and review of the literature

Author

Couloigner, Loïc, primary, Planes, Marc, additional, Ka, Chandran, additional, Audebert‐Bellanger, Séverine, additional, Redon, Sylvia, additional, Benech, Caroline, additional, Rouault, Karen, additional, Küry, Sebastien, additional, Peudenier, Sylviane, additional, Autret, Sandrine, additional, Gourlaouen, Isabelle, additional, Bonneau, Dominique, additional, Odent, Sylvie, additional, Bézieau, Stéphane, additional, Gilbert‐Dussardier, Brigitte, additional, Toutain, Annick, additional, Boland, Anne, additional, Deleuze, Jean‐François, additional, Le Marechal, Cédric, additional, Le Gac, Gérald, additional, Ferec, Claude, additional, and Uguen, Kevin, additional

Published
2022
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2. A new case of Kaufman Oculocerebrofacial syndrome caused by two splicing variants in UBE3B and review of the literature

Author

Loïc Couloigner, Marc Planes, Chandran Ka, Séverine Audebert‐Bellanger, Sylvia Redon, Caroline Benech, Karen Rouault, Sebastien Küry, Sylviane Peudenier, Sandrine Autret, Isabelle Gourlaouen, Dominique Bonneau, Sylvie Odent, Stéphane Bézieau, Brigitte Gilbert‐Dussardier, Annick Toutain, Anne Boland, Jean‐François Deleuze, Cédric Le Marechal, Gérald Le Gac, Claude Ferec, Kevin Uguen, Centre Hospitalier Régional Universitaire de Brest (CHRU Brest), Génétique, génomique fonctionnelle et biotechnologies (UMR 1078) (GGB), EFS-Université de Brest (UBO)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Institut Brestois Santé Agro Matière (IBSAM), Université de Brest (UBO), Institut du Thorax [Nantes], Centre hospitalier universitaire de Nantes (CHU Nantes), Centre Hospitalier Universitaire d'Angers (CHU Angers), PRES Université Nantes Angers Le Mans (UNAM), CHU Pontchaillou [Rennes], Institut de Génétique et Développement de Rennes (IGDR), Université de Rennes (UR)-Centre National de la Recherche Scientifique (CNRS)-Structure Fédérative de Recherche en Biologie et Santé de Rennes ( Biosit : Biologie - Santé - Innovation Technologique ), Imagerie et cerveau (iBrain - Inserm U1253 - UNIV Tours ), Université de Tours (UT)-Institut National de la Santé et de la Recherche Médicale (INSERM), Centre National de Recherche en Génomique Humaine (CNRGH), and Commissariat à l'énergie atomique et aux énergies alternatives (CEA)

Subjects
[SDV.GEN.GH]Life Sciences [q-bio]/Genetics/Human genetics, Genetics, Genetics (clinical)
Abstract

International audience

Published
2022
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4. Molecular, clinical and neuropsychological study in 31 patients with Kabuki syndrome and KMT2D mutations

Author

Lehman, N., Mazery, A.C., Visier, A., Baumann, C., Lachesnais, D., Capri, Y., Toutain, A., Odent, S., Mikaty, M., Goizet, C., Taupiac, E., Jacquemont, M.L., Sanchez, E., Schaefer, E., Gatinois, V., Faivre, L., Minot, D., Kayirangwa, H., Sang, K.‐H.L.Q., Boddaert, N., Bayard, S., Lacombe, D., Moutton, S., Touitou, I., Rio, M., Amiel, J., Lyonnet, S., Sanlaville, D., Picot, M.C., and Geneviève, D.

Published
2017
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5. Clinical and neuroimaging findings in 33 patients with <scp>MCAP</scp> syndrome: A survey to evaluate relevant endpoints for future clinical trials

Author

Florence Petit, Fabienne Giuliano, Juliette Mazereeuw-Hautier, Marjolaine Willems, Christel Thauvin-Robinet, Patricia Blanchet, Laurence Faivre, Elodie Gautier, Anne-Claire Bursztejn, Renaud Touraine, Annick Toutain, Frederico Di Rocco, Maxime Luu, Patrick Edery, Arthur Sorlin, Jean-Luc Alessandri, Nicolas Chassaing, Alice Goldenberg, Christine Chiaverini, Fanny Morice-Picard, Aurore Garde, Stéphanie Arpin, Massimiliano Rossi, Marc Bardou, Claire Nicolas, Gilles Morin, Jenny Cornaton, Cyril Mignot, Christophe Philippe, V. Carmignac, Rodolphe Dard, Joelle Roume, Michèle Mathieu-Dramard, Philippe Khau Van Kien, Pierre Vabres, Didier Lacombe, Diane Doummar, Lucile Pinson, Christine Coubes, Laurent Guibaud, Olivia Boccara, Laboratoire Maladies Rares: Génétique et Métabolisme (Bordeaux) (U1211 INSERM/MRGM), and Université de Bordeaux (UB)-Groupe hospitalier Pellegrin-Institut National de la Santé et de la Recherche Médicale (INSERM)

Subjects
Adult, Male, 0301 basic medicine, Pediatrics, medicine.medical_specialty, Cutis marmorata, Adolescent, Class I Phosphatidylinositol 3-Kinases, Neuroimaging, Context (language use), Skin Diseases, Vascular, 030105 genetics & heredity, Cohort Studies, Young Adult, 03 medical and health sciences, Genetics, Polymicrogyria, medicine, Humans, PROS, Abnormalities, Multiple, Telangiectasis, Megalencephaly, Child, MCAP syndrome, Genetics (clinical), Chiari malformation, Clinical Trials as Topic, business.industry, Macrocephaly, PIK3CA, medicine.disease, Magnetic Resonance Imaging, 3. Good health, Clinical trial, 030104 developmental biology, Child, Preschool, Postnatal macrocephaly, Female, medicine.symptom, business, [SDV.MHEP]Life Sciences [q-bio]/Human health and pathology, Forecasting, Ventriculomegaly
Abstract

Megalencephaly-CApillary malformation-Polymicrogyria (MCAP) syndrome results from somatic mosaic gain-of-function variants in PIK3CA. Main features are macrocephaly, somatic overgrowth, cutaneous vascular malformations, connective tissue dysplasia, neurodevelopmental delay, and brain anomalies. The objectives of this study were to describe the clinical and radiological features of MCAP, to suggest relevant clinical endpoints applicable in future trials of targeted drug therapy. Based on a French collaboration, we collected clinical features of 33 patients (21 females, 12 males, median age of 9.9 years) with MCAP carrying mosaic PIK3CA pathogenic variants. MRI images were reviewed for 21 patients. The main clinical features reported were macrocephaly at birth (20/31), postnatal macrocephaly (31/32), body/facial asymmetry (21/33), cutaneous capillary malformations (naevus flammeus 28/33, cutis marmorata 17/33). Intellectual disability was present in 15 patients. Among the MRI images reviewed, the neuroimaging findings were megalencephaly (20/21), thickening of corpus callosum (16/21), Chiari malformation (12/21), ventriculomegaly/hydrocephaly (10/21), cerebral asymmetry (6/21) and polymicrogyria (2/21). This study confirms the main known clinical features that defines MCAP syndrome. Taking into account the phenotypic heterogeneity in MCAP patients, in the context of emerging clinical trials, we suggest that patients should be evaluated based on the main neurocognitive expression on each patient.

Published
2021
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6. Genetic counselling difficulties and ethical implications of incidental findings from array-CGH: a 7-year national survey

Author

Lefebvre, M., Sanlaville, D., Marle, N., Thauvin-Robinet, C., Gautier, E., Chehadeh, S. E., Mosca-Boidron, A.-L., Thevenon, J., Edery, P., Alex-Cordier, M.-P., Till, M., Lyonnet, S., Cormier-Daire, V., Amiel, J., Philippe, A., Romana, S., Malan, V., Afenjar, A., Marlin, S., Chantot-Bastaraud, S., Bitoun, P., Heron, B., Piparas, E., Morice-Picard, F., Moutton, S., Chassaing, N., Vigouroux-Castera, A., Lespinasse, J., Manouvrier-Hanu, S., Boute-Benejean, O., Vincent-Delorme, C., Petit, F., Meur, N. L., Marti-Dramard, M., Guerrot, A.-M., Goldenberg, A., Redon, S., Ferrec, C., Odent, S., Caignec, C. L., Mercier, S., Gilbert-Dussardier, B., Toutain, A., Arpin, S., Blesson, S., Mortemousque, I., Schaefer, E., Martin, D., Philip, N., Sigaudy, S., Busa, T., Missirian, C., Giuliano, F., Benailly, H. K., Kien, P. K.V., Leheup, B., Benneteau, C., Lambert, L., Caumes, R., Kuentz, P., François, I., Heron, D., Keren, B., Cretin, E., Callier, P., Julia, S., and Faivre, L.

Published
2016
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7. Phenotypic spectrum associated with PTCHD1 deletions and truncating mutations includes intellectual disability and autism spectrum disorder

Author

Chaudhry, A., Noor, A., Degagne, B., Baker, K., Bok, L. A., Brady, A. F., Chitayat, D., Chung, B. H., Cytrynbaum, C., Dyment, D., Filges, I., Helm, B., Hutchison, H. T., Jeng, L. J. B., Laumonnier, F., Marshall, C. R., Menzel, M., Parkash, S., Parker, M. J., Raymond, L. F., Rideout, A. L., Roberts, W., Rupps, R., Schanze, I., Schrander-Stumpel, C. T. R. M., Speevak, M. D., Stavropoulos, D. J., Stevens, S. J. C., Thomas, E. R. A., Toutain, A., Vergano, S., Weksberg, R., Scherer, S. W., Vincent, J. B., and Carter, M. T.

Published
2015
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8. Search for ReCQL4 mutations in 39 patients genotyped for suspected Rothmund–Thomson/Baller-Gerold syndromes

Author

Piard, J., Aral, B., Vabres, P., Holder-Espinasse, M., Mégarbané, A., Gauthier, S., Capra, V., Pierquin, G., Callier, P., Baumann, C., Pasquier, L., Baujat, G., Martorell, L., Rodriguez, A., Brady, A. F., Boralevi, F., González-Enseñat, M. A., Rio, M., Bodemer, C., Philip, N., Cordier, M.-P., Goldenberg, A., Demeer, B., Wright, M., Blair, E., Puzenat, E., Parent, P., Sznajer, Y., Francannet, C., DiDonato, N., Boute, O., Barlogis, V., Moldovan, O., Bessis, D., Coubes, C., Tardieu, M., Cormier-Daire, V., Sousa, A. B., Franques, J., Toutain, A., Tajir, M., Elalaoui, S. C., Geneviève, D., Thevenon, J., Courcet, J.-B., Rivière, J.-B., Collet, C., Gigot, N., Faivre, L., and Thauvin-Robinet, C.

Published
2015
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9. Molecular findings and clinical data in a cohort of 150 patients with anophthalmia/microphthalmia

Author

Chassaing, N., Causse, A., Vigouroux, A., Delahaye, A., Alessandri, J.-L., Boespflug-Tanguy, O., Boute-Benejean, O., Dollfus, H., Duban-Bedu, B., Gilbert-Dussardier, B., Giuliano, F., Gonzales, M., Holder-Espinasse, M., Isidor, B., Jacquemont, M.-L., Lacombe, D., Martin-Coignard, D., Mathieu-Dramard, M., Odent, S., Picone, O., Pinson, L., Quelin, C., Sigaudy, S., Toutain, A., Thauvin-Robinet, C., Kaplan, Josseline, and Calvas, Patrick

Published
2014
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10. Heterozygous HMGB1 loss‐of‐function variants are associated with developmental delay and microcephaly

Author

Uguen, Kévin, primary, Krysiak, Kilannin, additional, Audebert‐Bellanger, Séverine, additional, Redon, Sylvia, additional, Benech, Caroline, additional, Viora‐Dupont, Eléonore, additional, Tran Mau‐Them, Frederic, additional, Rondeau, Sophie, additional, Elsharkawi, Ibrahim, additional, Granadillo, Jorge L., additional, Neidich, Julie, additional, Soares, Celia Azevedo, additional, Tkachenko, Natáliya, additional, M. Amudhavalli, Shivarajan, additional, Engleman, Kendra, additional, Boland, Anne, additional, Deleuze, Jean‐François, additional, Bezieau, Stéphane, additional, Odent, Sylvie, additional, Toutain, Annick, additional, Bonneau, Dominique, additional, Gilbert‐Dussardier, Brigitte, additional, Faivre, Laurence, additional, Rio, Marlène, additional, Le Marechal, Cedric, additional, Ferec, Claude, additional, Repnikova, Elena, additional, and Cao, Yang, additional

Published
2021
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11. Systematic molecular and cytogenetic screening of 100 patients with marfanoid syndromes and intellectual disability

Author

Callier, P, Aral, B, Hanna, N, Lambert, S, Dindy, H, Ragon, C, Payet, M, Collod-Beroud, G, Carmignac, V, Delrue, M A, Goizet, C, Philip, N, Busa, T, Dulac, Y, Missotte, I, Sznajer, Y, Toutain, A, Francannet, C, Megarbane, A, Julia, S, Edouard, T, Sarda, P, Amiel, J, Lyonnet, S, Cormier-Daire, V, Gilbert, B, Jacquette, A, Heron, D, Collignon, P, Lacombe, D, Morice-Picard, F, Jouk, P S, Cusin, V, Willems, M, Sarrazin, E, Amarof, K, Coubes, C, Addor, M C, Journel, H, Colin, E, Van Kien, Khau P, Baumann, C, Leheup, B, Coignard, Martin- D, Doco-Fenzy, M, Goldenberg, A, Plessis, G, Thevenon, J, Pasquier, L, Odent, S, Vabres, P, Huet, F, Marle, N, Boidron, Mosca- AL, Mugneret, F, Gauthier, S, Binquet, C, Thauvin-Robinet, C, Jondeau, G, Boileau, C, and Faivre, L

Published
2013
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12. Clinical and neuroimaging findings in 33 patients with MCAP syndrome: A survey to evaluate relevant endpoints for future clinical trials

Author

Garde, Aurore, primary, Guibaud, Laurent, additional, Goldenberg, Alice, additional, Petit, Florence, additional, Dard, Rodolphe, additional, Roume, Joelle, additional, Mazereeuw‐Hautier, Juliette, additional, Chassaing, Nicolas, additional, Lacombe, Didier, additional, Morice‐Picard, Fanny, additional, Toutain, Annick, additional, Arpin, Stéphanie, additional, Boccara, Olivia, additional, Touraine, Renaud, additional, Blanchet, Patricia, additional, Coubes, Christine, additional, Willems, Marjolaine, additional, Pinson, Lucile, additional, Van Kien, Philippe Khau, additional, Chiaverini, Christine, additional, Giuliano, Fabienne, additional, Alessandri, Jean‐Luc, additional, Mathieu‐Dramard, Michèle, additional, Morin, Gilles, additional, Bursztejn, Anne‐Claire, additional, Mignot, Cyril, additional, Doummar, Diane, additional, Di Rocco, Frederico, additional, Cornaton, Jenny, additional, Nicolas, Claire, additional, Gautier, Elodie, additional, Luu, Maxime, additional, Bardou, Marc, additional, Sorlin, Arthur, additional, Philippe, Christophe, additional, Edery, Patrick, additional, Rossi, Massimiliano, additional, Carmignac, Virginie, additional, Thauvin‐Robinet, Christel, additional, Vabres, Pierre, additional, and Faivre, Laurence, additional

Published
2021
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14. Neuropsychological study in 19 French patients with White‐Sutton syndrome and POGZ mutations

Author

Garde, Aurore, primary, Cornaton, Jenny, additional, Sorlin, Arthur, additional, Moutton, Sébastien, additional, Nicolas, Claire, additional, Juif, Christine, additional, Geneviève, David, additional, Perrin, Laurence, additional, Khau‐Van‐Kien, Philippe, additional, Smol, Thomas, additional, Vincent‐Delorme, Catherine, additional, Isidor, Bertrand, additional, Cogné, Benjamin, additional, Afenjar, Alexandra, additional, Keren, Boris, additional, Coubes, Christine, additional, Prieur, Fabienne, additional, Toutain, Annick, additional, Trousselet, Yann, additional, Bourgouin, Solène, additional, Gonin‐Olympiade, Coralie, additional, Giraudat, Kim, additional, Piton, Amélie, additional, Gérard, Bénédicte, additional, Odent, Sylvie, additional, Tessier, Fanny, additional, Lemasson, Lola, additional, Heide, Solveig, additional, Gelineau, Anne‐Claire, additional, Sarret, Catherine, additional, Miret, Anne, additional, Schaefer, Elise, additional, Piard, Juliette, additional, Mathevet, Rémi, additional, Boucon, Marion, additional, Bruel, Ange‐Line, additional, Mau‐Them, Frederic Tran, additional, Chevarin, Martin, additional, Vitobello, Antonio, additional, Philippe, Christophe, additional, Thauvin‐Robinet, Christel, additional, and Faivre, Laurence, additional

Published
2020
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15. A new case of Kaufman Oculocerebrofacial syndrome caused by two splicing variants in UBE3B and review of the literature.

Author

Couloigner, Loïc, Planes, Marc, Ka, Chandran, Audebert‐Bellanger, Séverine, Redon, Sylvia, Benech, Caroline, Rouault, Karen, Küry, Sebastien, Peudenier, Sylviane, Autret, Sandrine, Gourlaouen, Isabelle, Bonneau, Dominique, Odent, Sylvie, Bézieau, Stéphane, Gilbert‐Dussardier, Brigitte, Toutain, Annick, Boland, Anne, Deleuze, Jean‐François, Le Marechal, Cédric, and Le Gac, Gérald

Subjects
LITERATURE reviews, MEDICAL genetics, SYNDROMES, STOP codons
Published
2023
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19. RELNandVLDLRmutations underlie two distinguishable clinico-radiological phenotypes

Author

Marie-Anne Barthez, Magalie Barth, Diana Rodriguez, Caroline Paris, Catherine Garel, Michèle Mayer, Lydie Burglen, Annick Toutain, Stéphanie Valence, and Daniel Amsallem

Subjects
0301 basic medicine, Cerebellum, Pathology, medicine.medical_specialty, Pontocerebellar hypoplasia, Lissencephaly, 03 medical and health sciences, 0302 clinical medicine, Genetics, Medicine, Reelin, Cerebellar hypoplasia, Genetics (clinical), Cerebellar ataxia, biology, business.industry, Neurodegeneration, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, nervous system, Cerebellar vermis, biology.protein, medicine.symptom, business, 030217 neurology & neurosurgery
Abstract

Pontocerebellar hypoplasias (PCH) are characterized by lack of development and/or early neurodegeneration of cerebellum and brainstem. We report five patients referred for PCH, showing atypical clinical and magnetic resonance imaging (MRI) features suggestive of defects in the Reelin pathway. We screened for mutations in RELN or VLDLR and compared the phenotype of these patients with that of previously reported patients. All patients had profound cerebellar hypoplasia on MRI with peculiar cerebellar morphology, associated with flattened pons and neocortical abnormalities. Patient 1 had profound motor and intellectual disability with moderate lissencephaly suggestive of RELN mutations and was shown to harbor a splicing homozygous RELN mutation. The four other patients had a milder phenotype consistent with CARMQ1 (cerebellar ataxia and mental retardation with or without quadrupedal locomotion). These patients showed mild simplification or thickening of cortical gyration and had VLDLR mutations. Reelin signaling regulates neuronal migration in the developing mammalian brain. VLDLR is a key component of the Reelin pathway. Our patients had a very small and dysplatic cerebellar vermis that should suggest the involvement of these genes. Moreover, differences in clinical severity, involvement of the cerebellar hemispheres, together with the severity of the neocortical defect, enables RELN-mutated patients to be distinguished from VLDLR-mutated patients.

Published
2016
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20. Are all Xq26.2 duplications overlapping GPC3 on array-CGH a cause of Simpson-Golabi-Behmel syndrome? When do we need transcript analysis?

Author

E. Hammouche, Marie-Laure Vuillaume, Marie Ange Delrue, C. Dupont, Clarisse Baumann, Edouard Cottereau, Séverine Drunat, Annick Toutain, C. Maftei, Marie-Pierre Moizard, and Laurence Perrin

Subjects
0301 basic medicine, 03 medical and health sciences, 030104 developmental biology, Cardiac pathology, Genetics, medicine, Transcript analysis, Computational biology, Simpson–Golabi–Behmel syndrome, Biology, medicine.disease, Genetics (clinical), Comparative genomic hybridization
Published
2018
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21. Small patella syndrome: New clinical and molecular insights into a consistent phenotype

Author

Jamal Ghoumid, Bert Callewaert, Anne Dieux, Sylvie Manouvrier-Hanu, Michael Wright, Sophie Dupuis-Girod, Sheila Unger, Clémence Vanlerberghe, A-S Jourdain, Bertrand Isidor, Florence Petit, Fabienne Escande, Annick Toutain, and N. Boutry

Subjects
0301 basic medicine, 03 medical and health sciences, 030104 developmental biology, Small patella syndrome, Developmental genetics, Evolutionary biology, Developmental epidemiology, Genetics, Patella, Anatomy, Biology, Phenotype, Genetics (clinical)
Published
2017
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22. Fetal phenotype of Rubinstein-Taybi syndrome caused by CREBBP mutations

Author

Julien Van-Gils, Jérôme Toutain, Marie Gonzales, Laurence Taine, Sophie Blesson, Sophie Naudion, Benoit Arveiler, Tania Attié-Bitach, Jelena Martinovic, Didier Lacombe, Gwenaelle Lancelot, Bérénice Doray, Bénédicte Demeer, Sandra Whalen, and Patricia Fergelot

Subjects
0301 basic medicine, Male, Pediatrics, medicine.medical_specialty, Genotype, Genetic counseling, Gene Dosage, Prenatal diagnosis, Autopsy, 030105 genetics & heredity, 03 medical and health sciences, Exome Sequencing, Genetics, medicine, Humans, Genetic Predisposition to Disease, Cerebellar hypoplasia, Fetal Death, Genetics (clinical), Genetic Association Studies, Rubinstein-Taybi Syndrome, Fetus, Pregnancy, Rubinstein–Taybi syndrome, business.industry, medicine.disease, CREB-Binding Protein, Developmental disorder, 030104 developmental biology, Phenotype, Mutation, Female, business
Abstract

Rubinstein-Taybi syndrome (RSTS; OMIM 180849) is an autosomal dominant developmental disorder characterized by facial dysmorphism, broad thumbs and halluces associated with intellectual disability. RSTS is caused by alterations in CREBBP (about 60%) and EP300 genes (8%). RSTS is often diagnosed at birth or during early childhood but generally not suspected during antenatal period. We report nine cases of well-documented fetal RSTS. Two cases were examined after death in utero at 18 and 35 weeks of gestation and seven cases after identification of ultrasound abnormalities and termination of pregnancy. On prenatal sonography, a large gallbladder was detected in two cases, and brain malformations were noted in four cases, especially cerebellar hypoplasia. However, the diagnosis of RSTS has not been suggested during pregnancy. Fetal autopsy showed that all fetuses had large thumbs and/or suggestive facial dysmorphism. A CREBBP gene anomaly was identified in all cases. Alterations were similar to those found in typical RSTS children. This report will contribute to a better knowledge of the fetal phenotype to consider the hypothesis of RSTS during pregnancy. Genotyping allows reassuring genetic counseling.

Published
2018

23. Genetic counselling difficulties and ethical implications of incidental findings from array-CGH: a 7-year national survey

Author

Jeanne Amiel, Sophie Julia, Catherine Vincent-Delorme, Christel Thauvin-Robinet, Paul Kuentz, Salima El Chehadeh, Stanislas Lyonnet, Bruno Leheup, Elodie Gautier, Odile Boute-Benejean, Nathalie Le Meur, Sandrine Marlin, Irène François, Delphine Héron, Marianne Till, Patrick Edery, Houda Karmous Benailly, Serge Romana, Nicole Philip, Patrick Callier, Valérie Cormier-Daire, Bénédicte Héron, Adeline Vigouroux-Castera, Mathilde Lefebvre, Chantal Missirian, Sylvie Odent, Fanny Morice-Picard, Roseline Caumes, Dominique Martin, Cédric Le Caignec, Nicolas Chassaing, Claire Benneteau, Anne-Laure Mosca-Boidron, Claude Ferrec, Anne-Marie Guerrot, Sylvie Manouvrier-Hanu, Eva Piparas, Damien Sanlaville, Florence Petit, Stéphanie Arpin, Sébastien Moutton, Marie-Pierre Alex-Cordier, Elodie Cretin, Laurence Faivre, Sabine Sigaudy, Tiffany Busa, Brigitte Gilbert-Dussardier, Sandra Chantot-Bastaraud, Julien Thevenon, Alexandra Afenjar, Annick Toutain, Boris Keren, Anne Philippe, Valérie Malan, Laetitia Lambert, Sandra Mercier, Elise Schaefer, James Lespinasse, Nathalie Marle, Sylvia Redon, Fabienne Giuliano, Isabelle Mortemousque, Philippe Khau Van Kien, Pierre Bitoun, Alice Goldenberg, Sophie Blesson, and Michèle Marti-Dramard

Subjects
0301 basic medicine, Genetics, medicine.medical_specialty, education.field_of_study, Ethical issues, business.industry, Genetic counseling, Population, Retrospective cohort study, 030105 genetics & heredity, medicine.disease, Penetrance, 3. Good health, 03 medical and health sciences, Generalization (learning), Family medicine, Intellectual disability, Medicine, business, education, Genetics (clinical), Comparative genomic hybridization
Abstract

Microarray-based comparative genomic hybridization (aCGH) is commonly used in diagnosing patients with intellectual disability (ID) with or without congenital malformation. Because aCGH interrogates with the whole genome, there is a risk of being confronted with incidental findings (IF). In order to anticipate the ethical issues of IF with the generalization of new genome-wide analysis technologies, we questioned French clinicians and cytogeneticists about the situations they have faced regarding IF from aCGH. Sixty-five IF were reported. Forty corresponded to autosomal dominant diseases with incomplete penetrance, 7 to autosomal dominant diseases with complete penetrance, 14 to X-linked diseases, and 4 were heterozygotes for autosomal recessive diseases with a high prevalence of heterozygotes in the population. Therapeutic/preventive measures or genetic counselling could be argued for all cases except four. These four IF were intentionally not returned to the patients. Clinicians reported difficulties in returning the results in 29% of the cases, mainly when the question of IF had not been anticipated. Indeed, at the time of the investigation, only 48% of the clinicians used consents mentioning the risk of IF. With the emergence of new technologies, there is a need to report such national experiences; they show the importance of pre-test information on IF.

Published
2016
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24. Neuropsychological study in 19 French patients with White‐Sutton syndrome and POGZ mutations.

Author

Garde, Aurore, Cornaton, Jenny, Sorlin, Arthur, Moutton, Sébastien, Nicolas, Claire, Juif, Christine, Geneviève, David, Perrin, Laurence, Khau‐Van‐Kien, Philippe, Smol, Thomas, Vincent‐Delorme, Catherine, Isidor, Bertrand, Cogné, Benjamin, Afenjar, Alexandra, Keren, Boris, Coubes, Christine, Prieur, Fabienne, Toutain, Annick, Trousselet, Yann, and Bourgouin, Solène

Subjects
CHILDREN with learning disabilities, WHITE spot syndrome virus, ZINC-finger proteins, LEARNING disabilities, AUTISM spectrum disorders, INTELLECTUAL disabilities
Abstract

White‐Sutton syndrome is a rare developmental disorder characterized by global developmental delay, intellectual disabilities (ID), and neurobehavioral abnormalities secondary to pathogenic pogo transposable element‐derived protein with zinc finger domain (POGZ) variants. The purpose of our study was to describe the neurocognitive phenotype of an unbiased national cohort of patients with identified POGZ pathogenic variants. This study is based on a French collaboration through the AnDDI‐Rares network, and includes 19 patients from 18 families with POGZ pathogenic variants. All clinical data and neuropsychological tests were collected from medical files. Among the 19 patients, 14 patients exhibited ID (six mild, five moderate and three severe). The five remaining patients had learning disabilities and shared a similar neurocognitive profile, including language difficulties, dysexecutive syndrome, attention disorders, slowness, and social difficulties. One patient evaluated for autism was found to have moderate autism spectrum disorder. This study reveals that the cognitive phenotype of patients with POGZ pathogenic variants can range from learning disabilities to severe ID. It highlights that pathogenic variations in the same genes can be reported in a large spectrum of neurocognitive profiles, and that children with learning disabilities could benefit from next generation sequencing techniques. [ABSTRACT FROM AUTHOR]

Published
2021
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25. Small patella syndrome: New clinical and molecular insights into a consistent phenotype

Author

C, Vanlerberghe, A-S, Jourdain, A, Dieux, A, Toutain, B, Callewaert, S, Dupuis-Girod, S, Unger, M, Wright, B, Isidor, J, Ghoumid, F, Petit, N, Boutry, F, Escande, and S, Manouvrier-Hanu

Subjects
Adult, Male, Bone Diseases, Developmental, Hip, Adolescent, Patella, Middle Aged, Pedigree, Young Adult, Phenotype, Ischium, Child, Preschool, Mutation, Humans, Female, Child, T-Box Domain Proteins, Hip Dislocation, Congenital
Published
2017

26. Phenotypic spectrum associated withPTCHD1deletions and truncating mutations includes intellectual disability and autism spectrum disorder

Author

Michael Parker, Ellen R A Thomas, Angela F. Brady, Isabel Filges, Christian R. Marshall, Kate Baker, Marsha Speevak, Levinus A. Bok, David A. Dyment, Laure Raymond, Sandhya Parkash, A. L. Rideout, Dimitri J. Stavropoulos, L. J. B. Jeng, W. Roberts, John B. Vincent, Ammar Chaudhry, Servi J. C. Stevens, S. Vergano, Stephen W. Scherer, Rosemarie Rupps, B. Helm, David Chitayat, Cheryl Cytrynbaum, Rosanna Weksberg, Abdul Noor, Frédéric Laumonnier, H. T. Hutchison, Melissa T. Carter, Brian Hy Chung, I. Schanze, Bryan Degagne, C. T. R. M. Schrander-Stumpel, M. Menzel, and Annick Toutain

Subjects
Genetics, medicine.medical_specialty, business.industry, Neuropsychology, Cognition, Audiology, medicine.disease, 3. Good health, Neurodevelopmental disorder, Autism spectrum disorder, Intellectual disability, Medicine, Global developmental delay, Copy-number variation, 10. No inequality, business, Genetics (clinical), Loss function
Abstract

Studies of genomic copy number variants (CNVs) have identified genes associated with autism spectrum disorder (ASD) and intellectual disability (ID) such as NRXN1, SHANK2, SHANK3 and PTCHD1. Deletions have been reported in PTCHD1 however there has been little information available regarding the clinical presentation of these individuals. Herein we present 23 individuals with PTCHD1 deletions or truncating mutations with detailed phenotypic descriptions. The results suggest that individuals with disruption of the PTCHD1 coding region may have subtle dysmorphic features including a long face, prominent forehead, puffy eyelids and a thin upper lip. They do not have a consistent pattern of associated congenital anomalies or growth abnormalities. They have mild to moderate global developmental delay, variable degrees of ID, and many have prominent behavioral issues. Over 40% of subjects have ASD or ASD-like behaviors. The only consistent neurological findings in our cohort are orofacial hypotonia and mild motor incoordination. Our findings suggest that hemizygous PTCHD1 loss of function causes an X-linked neurodevelopmental disorder with a strong propensity to autistic behaviors. Detailed neuropsychological studies are required to better define the cognitive and behavioral phenotype.

Published
2014
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27. Search forReCQL4mutations in 39 patients genotyped for suspected Rothmund-Thomson/Baller-Gerold syndromes

Author

Nadège Gigot, Valeria Capra, Annick Toutain, Alice Goldenberg, Geneviève Pierquin, Nicole Philip, Odile Boute, S. Gauthier, Mariam Tajir, Yves Sznajer, Muriel Holder-Espinasse, Loreto Martorell, Laurence Faivre, J. Piard, Jean-Benoît Courcet, Christine Francannet, Cédric Baumann, Philippe Parent, Valérie Cormier-Daire, Michael Wright, N. Didonato, Marie-Pierre Cordier, David Geneviève, Didier Bessis, Ana Berta Sousa, Laurent Pasquier, Angela F. Brady, F. Boralevi, Siham Chafai Elalaoui, André Mégarbané, Bernard Aral, Edward Blair, Christine Bodemer, Eve Puzenat, B. Demeer, M. Tardieu, Corinne Collet, V. Barlogis, C. Thauvin-Robinet, Marlène Rio, Christine Coubes, Pierre Vabres, Geneviève Baujat, J. Franques, Patrick Callier, Jean-Baptiste Rivière, María Antonia González-Enseñat, Julien Thevenon, Olga Domnica Moldovan, and A. Rodríguez

Subjects
Genetics, medicine.medical_specialty, business.industry, Poikiloderma, Consanguinity, Baller–Gerold syndrome, medicine.disease, Dermatology, 3. Good health, Hereditary sclerosing poikiloderma, Genotype, medicine, business, Rothmund–Thomson syndrome, Genetics (clinical), Comparative genomic hybridization, Porokeratosis
Abstract

Three overlapping conditions, namely Rothmund-Thomson (RTS), Baller-Gerold (BGS) and RAPADILINO syndromes, have been attributed to RECQL4 mutations. Differential diagnoses depend on the clinical presentation, but the numbers of known genes remain low, leading to the widespread prescription of RECQL4 sequencing. The aim of our study was therefore to determine the best clinical indicators for the presence of RECQL4 mutations in a series of 39 patients referred for RECQL4 molecular analysis and belonging to the RTS (27 cases) and BGS (12 cases) spectrum. One or two deleterious RECQL4 mutations were found in 10/27 patients referred for RTS diagnosis. Clinical and molecular reevaluation led to a different diagnosis in 7/17 negative cases, including Clericuzio-type poikiloderma with neutropenia, hereditary sclerosing poikiloderma, and craniosynostosis/anal anomalies/porokeratosis. No RECQL4 mutations were found in the BGS group without poikiloderma, confirming that RECQL4 sequencing was not indicated in this phenotype. One chromosomal abnormality and one TWIST mutation was found in this cohort. This study highlights the search for differential diagnoses before the prescription of RECQL4 sequencing in this clinically heterogeneous group. The combination of clinically defined subgroups and next-generation sequencing will hopefully bring to light new molecular bases of syndromes with poikiloderma, as well as BGS without poikiloderma.

Published
2014
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28. Fetal phenotype of Rubinstein‐Taybi syndrome caused by CREBBP mutations

Author

Van‐Gils, Julien, primary, Naudion, Sophie, additional, Toutain, Jérôme, additional, Lancelot, Gwenaelle, additional, Attié‐Bitach, Tania, additional, Blesson, Sophie, additional, Demeer, Bénédicte, additional, Doray, Bérénice, additional, Gonzales, Marie, additional, Martinovic, Jelena, additional, Whalen, Sandra, additional, Taine, Laurence, additional, Arveiler, Benoit, additional, Lacombe, Didier, additional, and Fergelot, Patricia, additional

Published
2019
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29. Molecular findings and clinical data in a cohort of 150 patients with anophthalmia/microphthalmia

Author

Marie-Line Jacquemont, Christel Thauvin-Robinet, Didier Lacombe, Josseline Kaplan, Odile Boute-Benejean, Bertrand Isidor, Dominique Martin-Coignard, Fabienne Giuliano, Chloé Quélin, J.-L. Alessandri, Lucile Pinson, Sabine Sigaudy, H. Dollfus, Adeline Vigouroux, Michèle Mathieu-Dramard, Odile Boespflug-Tanguy, Brigitte Gilbert-Dussardier, Alexandre Causse, Marie Gonzales, Sylvie Odent, Andrée Delahaye, Nicolas Chassaing, Muriel Holder-Espinasse, P Calvas, Bénédicte Duban-Bedu, Annick Toutain, and Olivier Picone

Subjects
Genetics, Anophthalmia, Genetic heterogeneity, Genetic counseling, Biology, medicine.disease, Microphthalmia, eye diseases, 3. Good health, Testis determining factor, Multiplex polymerase chain reaction, medicine, Homeobox, sense organs, Gene, Genetics (clinical)
Abstract

Anophthalmia and microphthalmia (AM) are the most severe malformations of the eye, corresponding respectively to reduced size or absent ocular globe. Wide genetic heterogeneity has been reported and different genes have been demonstrated to be causative of syndromic and non-syndromic forms of AM. We screened seven AM genes [GDF6 (growth differentiation factor 6), FOXE3 (forkhead box E3), OTX2 (orthodenticle protein homolog 2), PAX6 (paired box 6), RAX (retina and anterior neural fold homeobox), SOX2 (SRY sex determining region Y-box 2), and VSX2 (visual system homeobox 2 gene)] in a cohort of 150 patients with isolated or syndromic AM. The causative genetic defect was identified in 21% of the patients (32/150). Point mutations were identified by direct sequencing of these genes in 25 patients (13 in SOX2, 4 in RAX, 3 in OTX2, 2 in FOXE3, 1 in VSX2, 1 in PAX6, and 1 in GDF6). In addition eight gene deletions (five SOX2, two OTX2 and one RAX) were identified using a semi-quantitative multiplex polymerase chain reaction (PCR) [quantitative multiplex PCR amplification of short fluorescent fragments (QMPSF)]. The causative genetic defect was identified in 21% of the patients. This result contributes to our knowledge of the molecular basis of AM, and will facilitate accurate genetic counselling.

Published
2013
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30. Phenotype and genotype in females withPOU3F4mutations

Author

Sandrine Marlin, Albert David, N Chaissang, Marie-Pierre Moizard, Natalie Loundon, Martine Raynaud, Laurence Jonard, Annick Toutain, Françoise Denoyelle, and Delphine Feldmann

Subjects
Adult, Heterozygote, Genotype, Hearing loss, Genetic counseling, Physiology, Biology, medicine.disease_cause, Inner ear malformation, otorhinolaryngologic diseases, Genetics, medicine, Humans, Gene, Genetics (clinical), Mutation, Middle Aged, Phenotype, Stapes surgery, POU Domain Factors, Audiometry, Pure-Tone, Female, medicine.symptom, Tomography, X-Ray Computed
Abstract

X-linked deafness is a rare cause of hereditary isolated hearing impairment estimated as at least 1% or 2% of the non-syndromic hearing loss. To date, four loci for DFN have been identified and only one gene, POU3F4 responsible for DFN3, has been cloned. In males, DFN3 is characterized by a progressive deafness associated with perilymphatic gusher at stapes surgery and with a characteristic inner ear malformation. The phenotype of eight independent females carrying POU3F4 anomalies is defined, and a late-onset hearing loss is found in three patients. Only one has an inner ear malformation. No genotype/phenotype correlation is identified.

Published
2009
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32. X-linked mental retardation exhibiting linkage to DXS255 and PGKP1: a new MRX family (MRX14) with localization in the pericentromeric region

Author

Martine Raynaud, Marie-Pierre Moizard, J. P. Muh, Nathalie Ronce, Sylvain Briault, Chantal Gendrot, Juliette Dourlens, Claude Moraine, and Annick Toutain

Subjects
Adult, Male, Microcephaly, X Chromosome, Genetic Linkage, Centromere, Biology, Gene mapping, Genetic linkage, Intellectual Disability, Genetics, medicine, Humans, Child, Gene, Sex Chromosome Aberrations, Genetics (clinical), X chromosome, Linkage (software), Macroorchidism, Chromosome Mapping, Sequence Analysis, DNA, medicine.disease, Pedigree, body regions, Phenotype, Female, Lod Score, Recombination
Abstract

Gene localization was determined by linkage analysis in a large French family with X-linked mental retardation (MRX). Seven living affected males were clinically studied and the clinical picture was characterized by moderate to severe mental handicap with poor secondary speech acquisition. Seizures, slight microcephaly, simian crease, anteverted pinnae, and macroorchidism were observed in some patients only. Linkage analysis revealed no recombination between the MRX gene and two loci: DXS255 at Xp11.22 (Zmax = 3.31 at theta = 0.00) and PGKP1 at Xq11.2-q12 (Zmax = 3.08 at theta = 0.00). One recombination was observed between the gene and the two loci DXS164 at Xp21.2 and DXS441 at Xq13.3, respectively. These results suggested gene localization in the pericentromeric region of the X chromosome, and the LOD scores justified assignment of the symbol MRX14 to this family.

Published
2008
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33. RELN and VLDLR mutations underlie two distinguishable clinico-radiological phenotypes

Author

S, Valence, C, Garel, M, Barth, A, Toutain, C, Paris, D, Amsallem, M-A, Barthez, M, Mayer, D, Rodriguez, and L, Burglen

Subjects
Adult, Male, Extracellular Matrix Proteins, Adolescent, Cell Adhesion Molecules, Neuronal, Developmental Disabilities, Homozygote, Serine Endopeptidases, Nerve Tissue Proteins, Nervous System Malformations, Magnetic Resonance Imaging, Reelin Protein, Phenotype, Receptors, LDL, Cerebellum, Child, Preschool, Intellectual Disability, Mutation, Humans, Female, Child
Abstract

Pontocerebellar hypoplasias (PCH) are characterized by lack of development and/or early neurodegeneration of cerebellum and brainstem. We report five patients referred for PCH, showing atypical clinical and magnetic resonance imaging (MRI) features suggestive of defects in the Reelin pathway. We screened for mutations in RELN or VLDLR and compared the phenotype of these patients with that of previously reported patients. All patients had profound cerebellar hypoplasia on MRI with peculiar cerebellar morphology, associated with flattened pons and neocortical abnormalities. Patient 1 had profound motor and intellectual disability with moderate lissencephaly suggestive of RELN mutations and was shown to harbor a splicing homozygous RELN mutation. The four other patients had a milder phenotype consistent with CARMQ1 (cerebellar ataxia and mental retardation with or without quadrupedal locomotion). These patients showed mild simplification or thickening of cortical gyration and had VLDLR mutations. Reelin signaling regulates neuronal migration in the developing mammalian brain. VLDLR is a key component of the Reelin pathway. Our patients had a very small and dysplatic cerebellar vermis that should suggest the involvement of these genes. Moreover, differences in clinical severity, involvement of the cerebellar hemispheres, together with the severity of the neocortical defect, enables RELN-mutated patients to be distinguished from VLDLR-mutated patients.

Published
2016

34. Screening of SLC26A4 (PDS) gene in Pendred's syndrome: a large spectrum of mutations in France and phenotypic heterogeneity

Author

Oden S, Leman J, Christine Petit, Duval, Houang M, Messaz O, Annick Toutain, Blons H, Hubert Journel, Sandrine Marlin, Delphine Feldmann, Natalie Loundon, Toublanc Je, Rémy Couderc, Catros H, Sergout-Allaoui A, Françoise Denoyelle, Bruno Delobel, Duriez F, Drouin-Garraud, Erea-Noel Garabedian, Didier Lacombe, and Obstoy Mf

Subjects
Genetics, medicine.medical_specialty, Goiter, business.industry, Hearing loss, Genetic heterogeneity, Thyroid disease, medicine.disease, Endocrinology, Internal medicine, Genotype, otorhinolaryngologic diseases, Medicine, Allele, medicine.symptom, business, Genetics (clinical), Pendred syndrome, Enlarged vestibular aqueduct
Abstract

Sensorineural hearing defect and goiter are common features of Pendred's syndrome. The clinical diagnosis of Pendred's syndrome remains difficult because of the lack of sensitivity and specificity of the thyroid signs. The identification of PDS as the causative gene allowed molecular screening and enabled a re-evaluation of the syndrome to identify potential diagnostic characteristics. This report presents the clinical and genotypic findings of 30 French families, for whom a diagnosis of Pendred's syndrome had been made. Twenty-seven families had at least one mutated allele. Twenty-eight different mutations were identified, 11 of which had never been previously reported. The main clinical characteristics were: early hearing loss, fluctuation in terms of during deafness evolution, and the presence of an enlarged vestibular aqueduct.

Published
2004
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36. Phenotypic spectrum associated with PTCHD1 deletions and truncating mutations includes intellectual disability and autism spectrum disorder

Author

Chaudhry, A., Noor, A., Degagne, B., Baker, K., Bok, L. A., Brady, A. F., Chitayat, D., Chung, B. H., Cytrynbaum, C., Dyment, D., Filges, I., Helm, B., Hutchison, H. T., Jeng, L. J. B., Laumonnier, F., Marshall, C. R., Menzel, M., Parkash, S., Parker, M. J., Raymond, L. F., Rideout, A. L., Roberts, W., Rupps, R., Schanze, I., Schrander-Stumpel, C. T. R. M., Speevak, M. D., Stavropoulos, D. J., Stevens, S. J. C., Thomas, E. R. A., Toutain, A., Vergano, S., Weksberg, R., Scherer, S. W., Vincent, J. B., Carter, M. T., RS: GROW - Developmental Biology, RS: GROW - R4 - Reproductive and Perinatal Medicine, Afdeling Onderwijs FHML, and MUMC+: DA Pat Cytologie (9)

Subjects
X-linked, Adult, Male, Adolescent, Autism Spectrum Disorder, PTCHD1, Facies, Infant, Membrane Proteins, Exons, Young Adult, Phenotype, Child, Preschool, Intellectual Disability, Mutation, Humans, Female, Child, Sequence Deletion
Abstract

Studies of genomic copy number variants (CNVs) have identified genes associated with autism spectrum disorder (ASD) and intellectual disability (ID) such as NRXN1, SHANK2, SHANK3 and PTCHD1. Deletions have been reported in PTCHD1 however there has been little information available regarding the clinical presentation of these individuals. Herein we present 23 individuals with PTCHD1 deletions or truncating mutations with detailed phenotypic descriptions. The results suggest that individuals with disruption of the PTCHD1 coding region may have subtle dysmorphic features including a long face, prominent forehead, puffy eyelids and a thin upper lip. They do not have a consistent pattern of associated congenital anomalies or growth abnormalities. They have mild to moderate global developmental delay, variable degrees of ID, and many have prominent behavioral issues. Over 40% of subjects have ASD or ASD-like behaviors. The only consistent neurological findings in our cohort are orofacial hypotonia and mild motor incoordination. Our findings suggest that hemizygous PTCHD1 loss of function causes an X-linked neurodevelopmental disorder with a strong propensity to autistic behaviors. Detailed neuropsychological studies are required to better define the cognitive and behavioral phenotype.

Published
2014

37. Are all Xq26.2 duplications overlapping <italic>GPC3</italic> on array‐CGH a cause of Simpson‐Golabi‐Behmel syndrome? When do we need transcript analysis?

Author

Hammouche, E., Cottereau, E., Vuillaume, M.‐L., Moizard, M.‐P., Toutain, A., Delrue, M.‐A., Maftei, C., Perrin, L., Baumann, C., Dupont, C., and Drunat, S.

Subjects
X-linked genetic disorders, CHROMOSOME duplication, CONGENITAL disorders, COMPARATIVE genomic hybridization, GENETIC transcription
Abstract

The article presents a case study of two patients with Simpson-Golabi-Behmel syndrome (SGBS) caused by the loss of-function of the glypican-3 gene (GPC3) and which showed Xq26.2 duplication. It informs about the tandem duplication of GPC3 identified by array comparative genomic hybridization (array-CGH). It also recommends a molecular transcription analysis to assess a possible gene disruption.

Published
2018
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38. Twenty-five novel mutations including duplications in the ATP7A gene

Author

Claude Moraine, Benoît Dessay, Sophie Blesson, Marie-Pierre Moizard, Martine Raynaud, Nathalie Ronce, Cyril Mignot, Isabelle Mortemousque, Pierre Castelnau, Nadine Marmin, Eric Bieth, Lydie Burglen, Cesare Danesino, François Feillet, and Annick Toutain

Subjects
Male, Mutation rate, Nonsense mutation, Occipital horn syndrome, Mutation, Missense, Biology, medicine.disease_cause, Cutis Laxa, Gene Duplication, Gene duplication, Genetics, medicine, Missense mutation, Humans, Point Mutation, Menkes Kinky Hair Syndrome, Cation Transport Proteins, Genetics (clinical), Sequence Deletion, Adenosine Triphosphatases, Gene Rearrangement, Mutation, Point mutation, Gene Expression Profiling, Exons, medicine.disease, Copper-Transporting ATPases, Menkes disease, Ehlers-Danlos Syndrome, Female, RNA Splice Sites, Multiplex Polymerase Chain Reaction
Abstract

Moizard M-P, Ronce N, Blesson S, Bieth E, Burglen L, Mignot C, Mortemousque I, Marmin N, Dessay B, Danesino C, Feillet F, Castelnau P, Toutain A, Moraine C, Raynaud M. Twenty-five novel mutations including duplications in the ATP7A gene. Menkes disease (MD) and occipital horn syndrome (OHS) are allelic X-linked recessive copper deficiency disorders resulting from ATP7A gene mutations. MD is a severe condition leading to progressive neurological degeneration and death in early childhood, whereas OHS has a milder phenotype with mainly connective tissue abnormalities. Until now, molecular analyses have revealed only deletions and point mutations in both diseases. This study reports new molecular data in a series of 40 patients referred for either MD or OHS. We describe 23 point mutations (9 missense mutations, 7 splice site variants, 4 nonsense mutations, and 3 small insertions or deletions) and 7 intragenic deletions. Of these, 18 point mutations and 3 deletions are novel. Furthermore, our finding of four whole exon duplications enlarges the mutation spectrum in the ATP7A gene. ATP7A alterations were found in 85% of cases. Of these alterations, two thirds were point mutations and the remaining one third consisted of large rearrangements. We found that 66.6% of point mutations resulted in impaired ATP7A transcript splicing, a phenomenon more frequent than expected. This finding enabled us to confirm the pathogenic role of ATP7A mutations, particularly in missense and splice site variants.

Published
2011

39. Screening of SLC26A4 (PDS) gene in Pendred's syndrome: a large spectrum of mutations in France and phenotypic heterogeneity

Author

H, Blons, D, Feldmann, V, Duval, O, Messaz, F, Denoyelle, N, Loundon, A, Sergout-Allaoui, M, Houang, F, Duriez, D, Lacombe, B, Delobel, J, Leman, H, Catros, H, Journel, V, Drouin-Garraud, M-F, Obstoy, A, Toutain, S, Oden, J E, Toublanc, R, Couderc, C, Petit, E-N, Garabédian, and S, Marlin

Subjects
Adult, Male, Adolescent, Goiter, Membrane Transport Proteins, Biological Transport, Syndrome, Middle Aged, Vestibular Aqueduct, Genetic Heterogeneity, Phenotype, Sulfate Transporters, Child, Preschool, Mutation, Humans, Mass Screening, Female, France, Child, Hearing Loss
Abstract

Sensorineural hearing defect and goiter are common features of Pendred's syndrome. The clinical diagnosis of Pendred's syndrome remains difficult because of the lack of sensitivity and specificity of the thyroid signs. The identification of PDS as the causative gene allowed molecular screening and enabled a re-evaluation of the syndrome to identify potential diagnostic characteristics. This report presents the clinical and genotypic findings of 30 French families, for whom a diagnosis of Pendred's syndrome had been made. Twenty-seven families had at least one mutated allele. Twenty-eight different mutations were identified, 11 of which had never been previously reported. The main clinical characteristics were: early hearing loss, fluctuation in terms of during deafness evolution, and the presence of an enlarged vestibular aqueduct.

Published
2004

40. Search forReCQL4mutations in 39 patients genotyped for suspected Rothmund-Thomson/Baller-Gerold syndromes

Author

Piard, J., primary, Aral, B., additional, Vabres, P., additional, Holder‐Espinasse, M., additional, Mégarbané, A., additional, Gauthier, S., additional, Capra, V., additional, Pierquin, G., additional, Callier, P., additional, Baumann, C., additional, Pasquier, L., additional, Baujat, G., additional, Martorell, L., additional, Rodriguez, A., additional, Brady, A. F., additional, Boralevi, F., additional, González‐Enseñat, M. A., additional, Rio, M., additional, Bodemer, C., additional, Philip, N., additional, Cordier, M.‐P., additional, Goldenberg, A., additional, Demeer, B., additional, Wright, M., additional, Blair, E., additional, Puzenat, E., additional, Parent, P., additional, Sznajer, Y., additional, Francannet, C., additional, DiDonato, N., additional, Boute, O., additional, Barlogis, V., additional, Moldovan, O., additional, Bessis, D., additional, Coubes, C., additional, Tardieu, M., additional, Cormier‐Daire, V., additional, Sousa, A. B., additional, Franques, J., additional, Toutain, A., additional, Tajir, M., additional, Elalaoui, S. C., additional, Geneviève, D., additional, Thevenon, J., additional, Courcet, J.‐B., additional, Rivière, J.‐B., additional, Collet, C., additional, Gigot, N., additional, Faivre, L., additional, and Thauvin‐Robinet, C., additional

Published
2014
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41. Molecular findings and clinical data in a cohort of 150 patients with anophthalmia/microphthalmia

Author

Chassaing, N., primary, Causse, A., additional, Vigouroux, A., additional, Delahaye, A., additional, Alessandri, J.‐L., additional, Boespflug‐Tanguy, O., additional, Boute‐Benejean, O., additional, Dollfus, H., additional, Duban‐Bedu, B., additional, Gilbert‐Dussardier, B., additional, Giuliano, F., additional, Gonzales, M., additional, Holder‐Espinasse, M., additional, Isidor, B., additional, Jacquemont, M.‐L., additional, Lacombe, D., additional, Martin‐Coignard, D., additional, Mathieu‐Dramard, M., additional, Odent, S., additional, Picone, O., additional, Pinson, L., additional, Quelin, C., additional, Sigaudy, S., additional, Toutain, A., additional, Thauvin‐Robinet, C., additional, Kaplan, Josseline, additional, and Calvas, Patrick, additional

Published
2013
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42. Monosomy 6q: report on four new cases

Author

R Mettey, D Galliano, C Valtat, Annick Toutain, and Claude Moraine

Subjects
Adult, Male, Monosomy, Pathology, medicine.medical_specialty, Chromosome Breakpoints, Aneuploidy, Biology, Long arm, Genetics, medicine, Humans, Dysmorphic facial features, Child, Genetics (clinical), Infant, Newborn, Chromosome, Karyotype, medicine.disease, Infant newborn, Child, Preschool, Karyotyping, Chromosomes, Human, Pair 6, Female, Chromosome Deletion
Abstract

We report on four patients with partial monosomy of the long arm of chromosome 6: two children presenting with an interstitial deletion del(6)(q14q16), the two others presenting with a terminal deletion del(6)(q25qter). These patients are compared with previous reports in the literature: 16 cases of terminal deletion and 17 cases of interstitial deletion. The deletions most often occur de novo. Mental retardation is always described. Dysmorphic facial features range between minor and major. There may be associated visceral abnormalities. After comparing the size and the localisation of the deletions with clinical data, we are now able to suggest a clinical localisation on chromosome 6.

Published
1992

45. Screening ofSLC26A4(PDS) gene in Pendred's syndrome: a large spectrum of mutations in France and phenotypic heterogeneity.

Author

Blons, H., Feldmann, D., Duval, V., Messaz, O., Denoyell, F., Loundon, N., Sergout-Allaoui, A., Houang, M., Duriez, F., Lacombe, D., Delobel, B., Leman, J., Catros, H., Journel, H., Drouin-Garraud, V., Obstoy, M.-F., Toutain, A., Oden, S., Toublanc, J. E., and Couderc, R.

Subjects
GENETIC testing, PHENOTYPES, HEARING disorders, GOITER, GENETIC mutation, MEDICAL genetics
Abstract

Blons H, Feldmann D, Duval V, Messaz O, Denoyelle F, Loundon N, Sergout-Allaoui A, Houang M, Duriez F, Lacombe D, Delobel B, Leman J, Catros H, Journel H, Drouin-Garraud V, Obstoy M-F, Toutain A, Odent S, Toublanc JE, Couderc R, Petit C, Garabédian E-N, Marlin S. Screening ofSLC26A4(PDS) gene in Pendred's syndrome: a large spectrum of mutations in France and phenotypic heterogeneity.Sensorineural hearing defect and goiter are common features of Pendred's syndrome. The clinical diagnosis of Pendred's syndrome remains difficult because of the lack of sensitivity and specificity of the thyroid signs. The identification ofPDSas the causative gene allowed molecular screening and enabled a re-evaluation of the syndrome to identify potential diagnostic characteristics. This report presents the clinical and genotypic findings of 30 French families, for whom a diagnosis of Pendred's syndrome had been made. Twenty-seven families had at least one mutated allele. Twenty-eight different mutations were identified, 11 of which had never been previously reported. The main clinical characteristics were: early hearing loss, fluctuation in terms of during deafness evolution, and the presence of an enlarged vestibular aqueduct. [ABSTRACT FROM AUTHOR]

Published
2004
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46. Identification of a Rare Branch Point Variant in the SMS Gene in a Large Family With a Severe Form of Snyder–Robinson Syndrome.

Author

Civit, Antoine, Ronce, Nathalie, Cogné, Benjamin, Besnard, Thomas, Laurenceau, David, Hubert, Catherine, Moizard, Marie‐Pierre, Gueguen, Paul, Toutain, Annick, and Vuillaume, Marie‐Laure

Subjects
*MEDICAL genetics, *HUMAN genetics, *GENETIC engineering, *GENETIC variation, *LEARNING disabilities
Abstract

The article in Clinical Genetics discusses the identification of a rare branch point variant in the SMS gene in a large family with a severe form of Snyder-Robinson Syndrome. The study highlights the impact of this variant on splicing and gene expression, leading to disease consequences. The findings emphasize the importance of focusing on noncoding regions to improve molecular diagnosis and provide insights into the genetic basis of Snyder-Robinson Syndrome. [Extracted from the article]

Published
2024
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