Your search keyword '"Bénédicte Demeer"' showing total 5 results

1. Prenatal diagnosis of femoral facial syndrome: Three case reports and literature review

Author

Céline Klein, Catherine Gondry-Jouet, J. Gondry, Gilles Morin, Philippe Naepels, Bénédicte Demeer, Guillaume Jedraszak, Marion Luisin, J. Chevreau, Anne Dieux-Coeslier, and Michèle Mathieu-Dramard

Subjects

Adult, Male, 0301 basic medicine, Pediatrics, medicine.medical_specialty, Cleft Lip, Prenatal diagnosis, 030105 genetics & heredity, Ultrasonography, Prenatal, 03 medical and health sciences, Fetus, 0302 clinical medicine, Pregnancy, Prenatal Diagnosis, Retrognathia, Genetics, medicine, Humans, Abnormalities, Multiple, Femur, Exome, Genetics (clinical), Comparative Genomic Hybridization, 030219 obstetrics & reproductive medicine, Pierre Robin Syndrome, business.industry, Infant, Newborn, Karyotype, Anatomy, Middle Aged, medicine.disease, Hypoplasia, Diabetes, Gestational, Agenesis, Female, Abnormality, business, Comparative genomic hybridization

Abstract

Facial femoral syndrome (FFS) is a rare congenital abnormality, also known as femoral hypoplasia-unusual facies syndrome, characterized by variable degrees of femoral hypoplasia, associated with specific facial features. Other organ malformations are sometimes present. Most cases are sporadic, but rare family observations suggest genetic origin. However, no chromosomal or genetic abnormalities have ever been incriminated. We conducted a comprehensive literature review and added three new unreported observations. Through these 92 cases, authors aimed to determine sonographic signs that should direct towards diagnosis, and discuss potential genetic etiology. Diagnosis was suspected prenatally in 27.2% of cases, and maternal diabetes was found in 42.4% of patients. When fetal karyotype was available, it was normal in 97.1% of cases, but genomic variations of unknown significance were discovered in all three cases in which array comparative genomic hybridization (CGH) techniques were applied. Femoral affection defining FFS was hypoplasia in 78.3% of cases, agenesis in 12%, and both in 9.8%. Affection was bilateral in 84.8% of cases. Retrognathia was present in 65.2% of cases, cleft lip and/or palate in 63%, and other organ malformations in 53.3%. Intellectual development was normal in 79.2% of cases. Better prenatal recognition of this pathology, notably frequently associated malformations, should lead to a more precise estimation of functional prognosis. It seems likely that today's tendency to systematically employ array-CGH and exome/genome sequencing methods to investigate malformative sequences will allow the identification of a causal genetic abnormality in the near future.

Published

2017

2. Author response for 'Fetal phenotype of Rubinstein-Taybi syndrome caused by CREBBP mutations'

Author

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

Subjects

Genetics, Fetus, Rubinstein–Taybi syndrome, business.industry, medicine, medicine.disease, business, Phenotype

Published

2018

3. A patient with Simpson-Golabi-Behmel syndrome, biliary cirrhosis and successful liver transplantation

Author

Christophe Chardot, Antonio Mellos, Djamal-Dine Djeddi, Bénédicte Demeer, Muriel Girard, Jean Gondry, Marie-Pierre Moizard, Michèle Mathieu-Dramard, Florence Lacaille, Henri Sevestre, Audrey Vanrenterghem, and Guillaume Jedraszak

Subjects

Heart Defects, Congenital, Male, medicine.medical_specialty, Biopsy, Biliary cirrhosis, medicine.medical_treatment, Liver transplantation, Gastroenterology, Gigantism, Organomegaly, Biliary disease, Liver disease, Glypicans, Intellectual Disability, Internal medicine, Genetics, Humans, Medicine, Genetics (clinical), Liver Cirrhosis, Biliary, business.industry, Infant, Arrhythmias, Cardiac, Genetic Diseases, X-Linked, Simpson–Golabi–Behmel syndrome, medicine.disease, Liver regeneration, Liver Transplantation, Phenotype, Treatment Outcome, Endocrinology, Liver, Overgrowth syndrome, Mutation, medicine.symptom, business

Abstract

Simpson–Golabi–Behmel syndrome type 1 (SGBS1) -OMIM 312870- is a rare X-linked inherited overgrowth syndrome caused by a loss of function mutation in the GPC3 gene. Affected patients present a variable phenotype with pre- and post-natal macrosomia, distinctive facial dysmophism, organomegaly, and multiple congenital anomalies. Intellectual disability is not constant. About 10% of patients have an increased risk of developing embryonic tumors in early childhood. Only one case of biliary disease has been described so far. GPC3 is localized on Xq26. It encodes for glypican 3, a heparan sulfate proteoglycan, which among its different known roles, negatively regulates liver regeneration and hepatocyte proliferation. This report concerns a male with a SGBS1, carrier of a GPC3 pathogenic mutation, and neonatal liver disease, who developed an early biliary cirrhosis. Together with the associated risk of cancer and developmental delay, liver transplantation was discussed and then successfully performed at the age of 19 months. A hypothesis on the role of GPC3 in the patient's liver disease is also proposed. © 2013 Wiley Periodicals, Inc.

Published

2013

4. Phenotypic Spectrum of Simpson-Golabi-Behmel Syndrome in a Series of 42 Cases With a Mutation in GPC 3 and Review of the Literature

Author

Laurence Faivre, Valérie Cormier-Daire, Fabiana Viana Ramos, Delphine Héron, Bénédicte Demeer, Dominique Gaillard, Edouard Cottereau, Sylvie Odent, Lydie Burglen, Jenneke van den Ende, Sylvie Rossignol, Odile Boute, Nicole Philip, Albert David, Marylin Lackmy‐Port Lis, Jeanne Amiel, Eric Bieth, Adeline Jacquinet, Marie-Françoise Frouté, Dominique Bonneau, Robert Robertson, Alice Goldenberg, Pierre Sarda, Isabelle Mortemousque, Annick Toutain, Alain Verloes, Marie-Pierre Moizard, Patricia Blanchet, Michèle Mathieu, Geneviève Baujat, Lucile Pinson, Sabine Sigaudy, Isabelle Maystadt, Ilham Ratbi, Didier Lacombe, Brigitte Gilbert-Dussardier, Lionel Van Maldergem, and Marjolaine Willems

Subjects

Genetics, 0303 health sciences, Pediatrics, medicine.medical_specialty, Genetic heterogeneity, Point mutation, 030305 genetics & heredity, Macrocephaly, Simpson–Golabi–Behmel syndrome, Biology, medicine.disease, Organomegaly, 3. Good health, Gigantism, 03 medical and health sciences, Gene duplication, Intellectual disability, medicine, medicine.symptom, Genetics (clinical), 030304 developmental biology

Abstract

Simpson-Golabi-Behmel syndrome (SGBS) is a rare X-linked multiple congenital abnormality/intellectual disability syndrome characterized by pre- and post-natal overgrowth, distinctive craniofacial features, macrocephaly, variable congenital malformations, organomegaly, increased risk of tumor and mild/moderate intellectual deficiency. In 1996, Glypican 3 (GPC3) was identified as the major gene causing SGBS but the mutation detection rate was only 28-70%, suggesting either genetic heterogeneity or that some patients could have alternative diagnoses. This was particularly suggested by some reports of atypical cases with more severe prognoses. In the family reported by Golabi and Rosen, a duplication of GPC4 was recently identified, suggesting that GPC4 could be the second gene for SGBS but no point mutations within GPC4 have yet been reported. In the genetics laboratory in Tours Hospital, GPC3 molecular testing over more than a decade has detected pathogenic mutations in only 8.7% of individuals with SGBS. In addition, GPC4 mutations have not been identified thus raising the question of frequent misdiagnosis. In order to better delineate the phenotypic spectrum of SGBS caused by GPC3 mutations, and to try to define specific clinical criteria for GPC3 molecular testing, we reviewed the clinical features of all male cases with a GPC3 mutation identified in the two molecular laboratories providing this test in France (Tours and Paris). We present here the results of the analysis of 42 patients belonging to 31 families and including five fetuses and three deceased neonates.

Published

2013

5. Mutations inWNT10Aare frequently involved in oligodontia associated with minor signs of ectodermal dysplasia

Author

Encarna Guillén-Navarro, Sabine Sigaudy, Christine Coubes, Ghislaine Plessis, Dominique Martin-Coignard, Marc Abramowicz, Philippe Jonveaux, Catherine Vincent-Delorme, Frédéric Vaysse, Isabelle Bailleul-Forestier, Estelle Colin, V. Gaston, Nicolas Chassaing, Didier Lacombe, Bénédicte Demeer, Muriel Holder-Espinasse, Patrick Calvas, Julie Plaisancié, Hélène Dollfus, Eric Bieth, Alain Verloes, and Laurence Faivre

Subjects

Male, Ectodermal dysplasia, Genotype, Molecular Sequence Data, medicine.disease_cause, Compound heterozygosity, Ectodermal Dysplasia, Genetics, medicine, Humans, Amino Acid Sequence, Hypohidrotic ectodermal dysplasia, Genetic Association Studies, Genetics (clinical), Anodontia, Mutation, EDARADD, Edar Receptor, Genetic heterogeneity, business.industry, medicine.disease, Wnt Proteins, Hypodontia, Phenotype, Female, Ectodysplasin A, business, Sequence Alignment

Abstract

Ectodermal dysplasias (ED) are a clinically and genetically heterogeneous group of hereditary disorders that have in common abnormal development of ectodermal derivatives. Hypohidrotic ectodermal dysplasia (HED) is characterized by abnormal development of eccrine sweat glands, hair, and teeth. The X-linked form of the disease, caused by mutations in the EDA gene, represents the majority of patients with the hypohidrotic form. Autosomal dominant and autosomal recessive forms are occasionally seen, and result from mutations in at least three genes (WNT10A, EDAR, or more rarely EDARADD). We have screened for mutations in EDAR (commonly involved in the hypohidrotic form) and WNT10A (involved in a wide spectrum of ED and in isolated hypodontia) in a cohort of 36 patients referred for EDA molecular screening, which failed to identify any mutation. We identified eight EDAR mutations in five patients (two with homozygous mutations, one with compound heterozygous mutations, and two with heterozygous mutation), four of which were novel variants. We identified 28 WNT10A mutations in 16 patients (5 with homozygous mutations, 7 with compound heterozygous mutations, and 4 with heterozygous mutations), seven of which were novel variants. Our study allows a more precise definition of the phenotypic spectrum associated with EDAR and WNT10A mutations and underlines the importance of the implication of WNT10A among patients with ED. © 2013 Wiley Periodicals, Inc.

Published

2013