Your search keyword '"Le Merrer, Martine"' showing total 26 results

1. New insights into genotype-phenotype correlation for GLI3 mutations.

Author

Démurger, Florence, Ichkou, Amale, Mougou-Zerelli, Soumaya, Le Merrer, Martine, Goudefroye, Géraldine, Delezoide, Anne-Lise, Quélin, Chloé, Manouvrier, Sylvie, Baujat, Geneviève, Fradin, Mélanie, Pasquier, Laurent, Megarbané, André, Faivre, Laurence, Baumann, Clarisse, Nampoothiri, Sheela, Roume, Joëlle, Isidor, Bertrand, Lacombe, Didier, Delrue, Marie-Ange, and Mercier, Sandra

Subjects

GENOTYPES, PHENOTYPES, GENETIC mutation, ALLELES, GENETICS, GENE expression, SYNDROMES

Abstract

The phenotypic spectrum of GLI3 mutations includes autosomal dominant Greig cephalopolysyndactyly syndrome (GCPS) and Pallister-Hall syndrome (PHS). PHS was first described as a lethal condition associating hypothalamic hamartoma, postaxial or central polydactyly, anal atresia and bifid epiglottis. Typical GCPS combines polysyndactyly of hands and feet and craniofacial features. Genotype-phenotype correlations have been found both for the location and the nature of GLI3 mutations, highlighting the bifunctional nature of GLI3 during development. Here we report on the molecular and clinical study of 76 cases from 55 families with either a GLI3 mutation (49 GCPS and 21 PHS), or a large deletion encompassing the GLI3 gene (6 GCPS cases). Most of mutations are novel and consistent with the previously reported genotype-phenotype correlation. Our results also show a correlation between the location of the mutation and abnormal corpus callosum observed in some patients with GCPS. Fetal PHS observations emphasize on the possible lethality of GLI3 mutations and extend the phenotypic spectrum of malformations such as agnathia and reductional limbs defects. GLI3 expression studied by in situ hybridization during human development confirms its early expression in target tissues. [ABSTRACT FROM AUTHOR]

Published

2015

2. Crouzon syndrome with acanthosis nigricans: a case-based update.

Author

di Rocco, Federico, Collet, Corinne, Legeai-Mallet, Laurence, Arnaud, Eric, Le Merrer, Martine, Hadj-Rabia, Smail, and Renier, Dominique

Subjects

CRANIOFACIAL dysostosis, ACANTHOSIS nigricans, VELOCARDIOFACIAL syndrome, SKIN abnormalities, BONE abnormalities, GENETIC mutation, KIDNEYS, URINARY organs, GENETIC counseling

Abstract

Background: Crouzon syndrome with acanthosis nigricans also named Crouzono-dermo-skeletal is a clinically and genetically distinct entity. It associates a craniofacial phenotype to anomalies of the skin and long bones. This syndrome is due to a specific mutation in FGFR3 gene that can be identified by genetic testing. Illustrative cases: As in our two patients, not all these features might be present and some will be patent only in the infancy or early childhood. Moreover, other organs such as the kidneys might be affected. Discussion: Because several organs might be affected the recognition of such syndrome is important for a correct management of the patient as well as a proper information and genetic counseling of the families. [ABSTRACT FROM AUTHOR]

Published

2011

3. Tartrate-resistant acid phosphatase deficiency causes a bone dysplasia with autoimmunity and a type I interferon expression signature.

Author

Briggs, Tracy A., Rice, Gillian I., Daly, Sarah, Urquhart, Jill, Gornall, Hannah, Bader-Meunier, Brigitte, Baskar, Kannan, Baskar, Shankar, Baudouin, Veronique, Beresford, Michael W., Black, Graeme C. M., Dearman, Rebecca J., de Zegher, Francis, Foster, Emily S., Francès, Camille, Hayman, Alison R., Hilton, Emma, Job-Deslandre, Chantal, Kulkarni, Muralidhar L., and Le Merrer, Martine

Subjects

DYSPLASIA, ACID phosphatase, AUTOIMMUNITY, INTERFERONS, GENE expression, HYPOTHYROIDISM, GENETIC mutation, GENETICS

Abstract

We studied ten individuals from eight families showing features consistent with the immuno-osseous dysplasia spondyloenchondrodysplasia. Of particular note was the diverse spectrum of autoimmune phenotypes observed in these individuals (cases), including systemic lupus erythematosus, Sjögren's syndrome, hemolytic anemia, thrombocytopenia, hypothyroidism, inflammatory myositis, Raynaud's disease and vitiligo. Haplotype data indicated the disease gene to be on chromosome 19p13, and linkage analysis yielded a combined multipoint log10 odds (LOD) score of 3.6. Sequencing of ACP5, encoding tartrate-resistant acid phosphatase, identified biallelic mutations in each of the cases studied, and in vivo testing confirmed a loss of expressed protein. All eight cases assayed showed elevated serum interferon alpha activity, and gene expression profiling in whole blood defined a type I interferon signature. Our findings reveal a previously unrecognized link between tartrate-resistant acid phosphatase activity and interferon metabolism and highlight the importance of type I interferon in the genesis of autoimmunity. [ABSTRACT FROM AUTHOR]

Published

2011

4. A large-scale mutation search reveals genetic heterogeneity in 3M syndrome.

Author

Huber, Céline, Delezoide, Anee-Lise, Guimiot, Fabien, Baumann, Clarisse, Malan, Valérie, Le Merrer, Martine, Da Silva, Daniela Bezerra, Bonneau, Dominique, Chatelain, Pierre, Chu, Carol, Clark, Robin, Cox, Helen, Edery, Patrick, Edouard, Thomas, Fano, Virginia, Gibson, Kate, Gillessen-Kaesbach, Gabriele, Maria-Luisa Giovannucci-Uzielli, Graul-Neumann, Luitgard Margarete, and van Hagen, Johana-Maria

Subjects

GENETIC mutation, INTELLECTUAL disabilities, HUMAN genetics, CONSANGUINITY, CELL nuclei, DEVELOPMENTAL disabilities

Abstract

The 3M syndrome is a rare autosomal recessive disorder recently ascribed to mutations in the CUL7 gene and characterized by severe pre- and postnatal growth retardation. Studying a series of 33 novel cases of 3M syndrome, we have identified deleterious CUL7 mutations in 23/33 patients, including 19 novel mutations and one paternal isodisomy of chromosome 6 encompassing a CUL7 mutation. Lack of mutations in 10/33 cases and exclusion of the CUL7 locus on chromosome 6p21.1 in six consanguineous families strongly support the genetic heterogeneity of the 3M syndrome.European Journal of Human Genetics (2009) 17, 395–400; doi:10.1038/ejhg.2008.200; published online 29 October 2008 [ABSTRACT FROM AUTHOR]

Published

2009

5. ADAMTSL2 mutations in geleophysic dysplasia demonstrate a role for ADAMTS-like proteins in TGF-β bioavailability regulation.

Author

Le Goff, Carine, Morice-Picard, Fanny, Dagoneau, Nathalie, Wang, Lauren W., Perrot, Claire, Crow, Yanick J., Bauer, Florence, Flori, Elisabeth, Prost-Squarcioni, Catherine, Krakow, Deborah, Gaoxiang Ge, Greenspan, Daniel S., Bonnet, Damien, Le Merrer, Martine, Munnich, Arnold, Apte, Suneel S., and Cormier-Daire, Valérie

Subjects

DYSPLASIA, GENETIC mutation, GENETICS, BIOCHEMICAL genetics, PHYSICAL anthropology

Abstract

Geleophysic dysplasia is an autosomal recessive disorder characterized by short stature, brachydactyly, thick skin and cardiac valvular anomalies often responsible for an early death. Studying six geleophysic dysplasia families, we first mapped the underlying gene to chromosome 9q34.2 and identified five distinct nonsense and missense mutations in ADAMTSL2 (a disintegrin and metalloproteinase with thrombospondin repeats–like 2), which encodes a secreted glycoprotein of unknown function. Functional studies in HEK293 cells showed that ADAMTSL2 mutations lead to reduced secretion of the mutated proteins, possibly owing to the misfolding of ADAMTSL2. A yeast two-hybrid screen showed that ADAMTSL2 interacts with latent TGF-β–binding protein 1. In addition, we observed a significant increase in total and active TGF-β in the culture medium as well as nuclear localization of phosphorylated SMAD2 in fibroblasts from individuals with geleophysic dysplasia. These data suggest that ADAMTSL2 mutations may lead to a dysregulation of TGF-β signaling and may be the underlying mechanism of geleophysic dysplasia. [ABSTRACT FROM AUTHOR]

Published

2008

6. Czech dysplasia metatarsal type: another type II collagen disorder.

Author

Hoornaert, Kristien P., Marik, Ivo, Kozlowski, Kazimierz, Cole, Trevor, Le Merrer, Martine, Leroy, Jules G., Coucke, Paul J., Sillence, David, and Mortier, Geert R.

Subjects

DYSPLASIA, COLLAGEN, CONNECTIVE tissues, EXTRACELLULAR matrix proteins, GENOTYPE-environment interaction, GENETICS

Abstract

Czech dysplasia metatarsal type is an autosomal-dominant disorder characterized by an early-onset, progressive spondyloarthropathy with normal stature. Shortness of third and/or fourth toes is a frequently observed clinical feature. Similarities between individuals with this dysplasia and patients with an R275C mutation in the COL2A1 gene, prompted us to analyze the COL2A1 gene in the original families reported with Czech dysplasia. Targeted sequencing of exon 13 of the COL2A1 gene was performed, followed by sequencing of the remaining exons in case the R275C mutation was not identified. We identified the R275C substitution in two of the original patients reported with Czech dysplasia and three additional patients. All affected individuals had a similar phenotype characterized by normal height, spondyloarthropathy, short postaxial toes and absence of ocular and orofacial anomalies. The R275C mutation was excluded in a third patient reported with Czech dysplasia. However, the identification of the Y1391C mutation in this patient with disproportionate short stature made the diagnosis of spondyloperipheral dysplasia (SPD) more probable. The Y1391C mutation is located in the C-propeptide of the procollagen chain and has been reported before in a patient with the Torrance type of lethal platyspondylic skeletal dysplasia (PLSD-T). Our observation of the same Y1391C mutation in an additional unrelated patient with SPD further supports the evidence that PLSD-T and SPD represent a phenotypic continuum. The R275C mutation in the COL2A1 gene causes a specific type II collagen disorder that was recently delineated as Czech dysplasia.European Journal of Human Genetics (2007) 15, 1269–1275; doi:10.1038/sj.ejhg.5201913; published online 29 August 2007 [ABSTRACT FROM AUTHOR]

Published

2007

7. Novel FGFR3 mutations creating cysteine residues in the extracellular domain of the receptor cause achondroplasia or severe forms of hypochondroplasia.

Author

Heuertz, Solange, Le Merrer, Martine, Zabel, Bernhard, Wright, Michael, Legeai-Mallet, Laurence, Cormier-Daire, Valérie, Gibbs, Linda, and Bonaventure, Jacky

Subjects

*ACHONDROPLASIA, *BONE diseases, *GENETIC mutation, *PROTEIN-tyrosine kinases, *GROWTH disorders, *HUMAN genetics

Abstract

Achondroplasia (ACH) and hypochondroplasia (HCH) are two autosomal-dominant skeletal disorders caused by recurrent missense FGFR3 mutations in the transmembrane (TM) and tyrosine kinase 1 (TK1) domains of the receptor. Although 98% of ACH cases are accounted for by a single G380R substitution in the TM, a common mutation (N540K) in the TK1 region is detected in only 60–65% of HCH cases. The aim of this study was to determine whether the frequency of mutations in patients with HCH was the result of incomplete mutation screening or genetic heterogeneity. Eighteen exons of the FGFR3 gene were entirely sequenced in a cohort of 25 HCH and one ACH patients in whom common mutations had been excluded. Seven novel missense FGFR3 mutations were identified, one causing ACH and six resulting in HCH. Six of these substitutions were located in the extracellular region and four of them creating additional cysteine residues, were associated with severe phenotypes. No mutations were detected in 19 clinically diagnosed HCH patients. Our results demonstrate that the spectrum of FGFR3 mutations causing short-limb dwarfism is wider than originally recognised and emphasise the requirement for complete screening of the FGFR3 gene if appropriate genetic counselling is to be offered to patients with HCH or ACH lacking the most common mutations and their families.European Journal of Human Genetics (2006) 14, 1240–1247. doi:10.1038/sj.ejhg.5201700; published online 16 August 2006 [ABSTRACT FROM AUTHOR]

Published

2006

8. Interstitial 9q22.3 microdeletion: clinical and molecular characterisation of a newly recognised overgrowth syndrome.

Author

Redon, Richard, Baujat, Geneviève, Sanlaville, Damien, Le Merrer, Martine, Vekemans, Michel, Munnich, Arnold, Carter, Nigel P., Cormier-Daire, Valérie, and Colleaux, Laurence

Subjects

DEVELOPMENTAL disabilities, INTELLECTUAL disabilities, HUMAN genetics, PHENOTYPES, GENOTYPE-environment interaction, PEOPLE with intellectual disabilities

Abstract

In the course of a systematic whole genome screening of patients with unexplained overgrowth syndrome by microarray-based comparative genomic hybridisation (array-CGH), we have identified two children with nearly identical 6.5 Mb-long de novo interstitial deletions at 9q22.32–q22.33. The clinical phenotype includes macrocephaly, overgrowth and trigonocephaly. In addition, both children present with psychomotor delay, hyperactivity and distinctive facial features. Further analysis with a high-resolution custom microarray covering the whole breakpoint intervals with fosmids mapped the deletion breakpoints within 100-kb intervals: although the deletion boundaries are different for the two patients, nearly the same genes are deleted in both cases. We suggest therefore that microdeletion of 9q22.32–q22.33 is a novel cause of overgrowth and mental retardation. Its association with distinctive facial features should help in recognising this novel phenotype.European Journal of Human Genetics (2006) 14, 759–767. doi:10.1038/sj.ejhg.5201613; published online 29 March 2006 [ABSTRACT FROM AUTHOR]

Published

2006

9. Mutation screening in patients with syndromic craniosynostoses indicates that a limited number of recurrent FGFR2 mutations accounts for severe forms of Pfeiffer syndrome.

Author

Lajeunie, Elisabeth, Heuertz, Solange, El Ghouzzi, Vincent, Martinovic, Jelena, Renier, Dominique, Le Merrer, Martine, and Bonaventure, Jacky

Subjects

MONONUCLEOSIS, BLOOD diseases, CRANIOFACIAL dysostosis, CRANIOSYNOSTOSES, SKULL abnormalities, GENETIC mutation, GENETICS, GENOMES

Abstract

Crouzon Syndrome (CS), Pfeiffer syndrome (PS) and the phenotypically related Jackson-Weiss (JW) variant are three craniosynostotic conditions caused by heterozygous mutations in Fibroblast Growth Factor Receptor (FGFR) genes. Screening a large cohort of 84 patients with clinical features of CS, PS or JW by direct sequencing of genomic DNA, enabled FGFR1, 2 or 3 mutation detection in 79 cases. Mutations preferentially occurred in exons 8 and 10 of FGFR2 encoding the third Ig loop of the receptor. Among the 74 FGFR2 mutations that we identified, four were novel including three missense substitutions causing CS and a 2 bp deletion creating a premature stop codon and producing JW phenotype. Five FGFR2 mutations were found in one of the two tyrosine kinase subdomains and one in the Ig I loop. Interestingly, two FGFR2 mutations creating cysteine residues (W290C and Y340C) caused severe forms of PS while conversion of the same residues into another amino-acid (W290G/R, Y340H) resulted in Crouzon phenotype exclusively. Our data provide conclusive evidence that the mutational spectrum of FGFR2 mutations in CS and PS is wider than originally thought. Genotype-phenotype analyses based on our cohort and previous studies further indicate that in spite of some overlap, PS and CS are preferentially accounted for by two distinct sets of FGFR2 mutations. A limited number of recurrent amino-acid changes (W290C, Y340C, C342R and S351C) is commonly associated with the most severe Pfeiffer phenotypes of poor prognosis.European Journal of Human Genetics (2006) 14, 289–298. doi:10.1038/sj.ejhg.5201558; published online 18 January 2006 [ABSTRACT FROM AUTHOR]

Published

2006

10. Exclusion of the dymeclin and PAPSS2 genes in a novel form of spondyloepimetaphyseal dysplasia and mental retardation.

Author

Geneviève, David, Héron, Delphine, El Ghouzzi, Vincent, Prost-Squarcioni, Catherine, Le Merrer, Martine, Jacquette, Aurélia, Sanlaville, Damien, Pinton, Florence, Villeneuve, Nathalie, Kalifa, Gabriel, Munnich, Arnold, and Cormier-Daire, Valérie

Subjects

DYSPLASIA, CELL transformation, CELLULAR pathology, INTELLECTUAL disabilities, LYSOSOMAL storage diseases, GENES

Abstract

Spondyloepimetaphyseal dysplasias (SEMD) represent a heterogeneous group of conditions composed of at least 15 well-defined entities. The classification is based on clinical, radiological and molecular findings. Among them, several conditions also include a mental retardation (MR) syndrome, namely Wolcott-Rallison syndrome, Dyggve-Melchior-Clausen syndrome (DMC) and lysosomal storage disorders. Here, we report on a novel form of SEMD with MR in two Pakistani sisters born to first-cousin parents. SEMD, MR, microcephaly, ataxia, facial dysmorphism and hirsutism of back and legs were noted in the two children. Skeletal findings included flat vertebral bodies with irregular vertebral plates, irregular and flared metaphyses with vertical striations, small and irregular epiphyses, small carpal bones and narrow iliac wings without lacy pelvis iliac crest. Similarities with DMC prompted us to test and eventually exclude the DMC gene, dymeclin, by direct sequencing. Similarly, we excluded the PAPSS2 gene (3'-alpha phosphoadenosine 5'-phosphosulphate synthase 2) responsible for SEMD Pakistani type. The combination of features observed in the two sisters does not fit with any previously reported SEMD and represents therefore a novel form of autosomal recessive SEMD with MR.European Journal of Human Genetics (2005) 13, 541-546. doi:10.1038/sj.ejhg.5201339 Published online 23 February 2005 [ABSTRACT FROM AUTHOR]

Published

2005

11. Failure to detect an 8p22-8p23.1 duplication in patients with Kabuki (Niikawa-Kuroki) syndrome.

Author

Sanlaville, Damien, Genevieve, David, Bernardin, Céline, Amiel, Jeanne, Baumann, Clarisse, de Blois, Marie-Christine, Cormier-Daire, Valérie, Gerard, Bénédicte, Gerard, Marion, Le Merrer, Martine, Parent, Philippe, Prieur, Fabienne, Prieur, Marguerite, Raoul, Odile, Toutain, Annick, Verloes, Alain, Viot, Géraldine, Romana, Serge, Munnich, Arnold, and Lyonnet, Stanislas

Subjects

CHROMOSOME abnormalities, CHROMOSOME replication, GENETIC mutation, DYSPLASIA, DWARFISM, INTELLECTUAL disabilities, HUMAN abnormalities, SYNDROMES

Abstract

Kabuki syndrome (KS) is a rare MCA/MR syndrome with an estimated frequency of 1/32?000 in Japan. This syndrome is characterized by postnatal growth retardation, distinctive facial features, dermatoglyphic anomalies, skeletal dysplasia, and mental retardation. The molecular basis of KS remains unknown. Recently, Milunsky and Huang reported on six unrelated patients with a clinical diagnosis of KS and an 8p22-8p23.1 duplication using comparative genomic hybridization and BAC-FISH studies. Also, they suggested that a paracentric inversion may contribute to the occurrence of KS. In the present study, 24 patients with a clinical diagnosis of KS based on Niikawa-Kuroki criteria have been collected. They were tested for the presence of an 8p duplication using the same clones as described by Milunsky and Huang. Our results do not confirm the previously described association between KS and an 8p22-8p23.1 duplication.European Journal of Human Genetics (2005) 13, 690-693. doi:10.1038/sj.ejhg.5201383 Published online 16 March 2005 [ABSTRACT FROM AUTHOR]

Published

2005

12. Early diagnosis of Maroteaux-Lamy syndrome in two patients with accelerated growth and advanced bone maturation.

Author

Heron, Delphine, Baumann, Clarisse, Jacques, Jean, Jean, Benichou, Harpey, Paul, Merrer, Martine Le, Benichou, Jean Jacques, Harpey, Jean Paul, and Le Merrer, Martine

Subjects

MUCOPOLYSACCHARIDOSIS, INTELLECTUAL disabilities, SKELETAL maturity, LYSOSOMAL storage diseases, DERMATAN sulfate, ARYLSULFATASES

Abstract

Unlabelled: The diagnosis of mucopolysaccharidosis (MPS) VI is usually not made before the age of 2 or 3 years when the main clinical signs of dwarfed stature, skeletal deformities, coarsening facies, stiff joints and hepatosplenomegaly described in textbooks are recognisable. Conversely, accelerated growth with advanced bone age, a precocious feature of this condition although not suggestive of a storage disorder, is usually neither recognised, nor adequately interpreted. We report on two infants with MPS VI who presented with these two "unexpected" features within the 1st year of life.Conclusion: Recognition of precocious excessive growth in a mucopolysaccharidosis enables an early diagnosis, the prime responsibility of the clinician, in order to propose early treatment like bone marrow transplantation or active recombinant sulphatase therapy, and appropriate genetic counselling. [ABSTRACT FROM AUTHOR]

Published

2004

13. Phenotypic variability at the TGF-β1 locus in Camurati-Engelmann disease.

Author

Campos-Xavier, Ana, Saraiva, Jorge M., Savarirayan, Ravi, Verloes, Alain, Feingold, Josué, Faivre, Laurence, Munnich, Arnold, Le Merrer, Martine, and Cormier-Daire, Valérie

Subjects

PHENOTYPES, BIOLOGICAL variation, TRANSFORMING growth factors-beta, GENETIC mutation, CHROMOSOME polymorphism, BONE diseases, FAMILIAL diseases, MEDICAL genetics

Abstract

Camurati-Engelmann disease (CED) [OMIM 131300] is an autosomal dominant sclerosing bone dysplasia recently ascribed to mutations of the transforming growth factor (TGF-β1) gene on chromosome 19q13.1-q13.3. Five mutations consistently located in the TGF-β1 propeptide have been hitherto identified in 21 families. Here, we report on TGF-β1 mutations in one Australian and six European families. Three distinct mutations were identified among seven families: namely, R218H (family 1), R218C (families 2, 6, 7) and C225R (families 3, 4, 5). The three mutations identified in our pedigrees have been previously observed in families of Japanese and Israeli origin and the R218C appears to be the most prevalent mutation worldwide (17/28 reported families). No obvious correlation between the nature of the mutations and the severity of the clinical manifestations could be established, but a marked intrafamilial clinical variability was observed, supporting incomplete penetrance of CED. Interestingly, the polymorphisms in the TGF-β1 gene showed no correlation with the severity of the disease. We conclude that CED is a clinically variable condition and that this clinical variability is not accounted for by polymorphisms at the TGF-β1 locus. [ABSTRACT FROM AUTHOR]

Published

2001

14. A novel automated strategy for screening cryptic telomeric rearrangements in children with idiopathic mental retardation.

Author

Colleaux, Laurence, Rio, Marlène, Heuertz, Solange, Moindrault, Séverine, Turleau, Catherine, Ozilou, Catherine, Gosset, Philippe, Raoult, Odile, Lyonnet, Stanislas, Cormier-Daire, Valérie, Amiel, Jeanne, Le Merrer, Martine, Picq, Monique, de Blois, Marie-Christine, Prieur, Marguerite, Romana, Serge, Cornelis, François, Vekemans, Michel, and Munnich, Arnold

Subjects

INTELLECTUAL disabilities, TELOMERES, FLUORESCENCE in situ hybridization

Abstract

Cryptic unbalanced subtelomeric rearrangements are known to cause a significant proportion of idiopathic mental retardation in childhood. Because of the limited sensitivity of routine analyses, the cytogenetic detection of such rearrangements requires molecular techniques, namely FISH and comparative genomic hybridisation (CGH). An alternative approach consists in using genetic markers to detect segmental aneusomy. Here, we describe a new strategy based upon automated fluorescent genotyping to search for non mendelian segregation of telomeric microsatellites. A total of 29 individuals belonging to 24 unrelated families were screened and three abnormal patterns of segregation were detected (two rearrangements and one parental disomy). This study gives strong support to the view that cryptic telomeric rearrangements significantly contribute to idiopathic mental retardation and demonstrates that fluorescent genotyping is a very sensitive and cost-effective method to detect deletions, duplications and uniparental disomies. [ABSTRACT FROM AUTHOR]

Published

2001

15. Mutations within or upstream of the basic helix–loop–helix domain of the TWIST gene are specific to Saethre-Chotzen syndrome.

Author

El Ghouzzi, Vincent, Lajeunie, Elisabeth, Le Merrer, Martine, Cormier-Daire, Valérie, Renier, Dominique, Munnich, Arnold, and Bonaventure, Jacky

Subjects

SKULL diseases, HELIX-loop-helix motifs

Abstract

Saethre-Chotzen syndrome (ACS III) is an autosomal dominant craniosynostosis syndrome recently ascribed to mutations in the TWIST gene, a basic helix-loop-helix (b-HLH) transcription factor regulating head mesenchyme cell development during cranial neural tube formation in mouse. Studying a series of 22 unrelated ACS III patients, we have found TWIST mutations in 16/22 cases. Interestingly, these mutations consistently involved the b-HLH domain of the protein. Indeed, mutant genotypes included frameshift deletions/insertions, nonsense and missense mutations, either truncating or disrupting the b-HLH motif of the protein. This observation gives additional support to the view that most ACS III cases result from loss-of-function mutations at the TWIST locus. The P250R recurrent FGFR3 mutation was found in 2/22 cases presenting mild clinical manifestations of the disease but 4/22 cases failed to harbour TWIST or FGFR 3 mutations. Clinical re-examination of patients carrying TWIST mutations failed to reveal correlations between the mutant genotype and severity of the phenotype. Finally, since no TWIST mutations were detected in 40 cases of isolated coronal craniosynostosis, the present study suggests that TWIST mutations are specific to SaethreChotzen syndrome. Saethre-Chotzen syndrome (ACS III) is an autosomal dominant craniosynostosis syndrome recently ascribed to mutations in the TWIST gene, a basic helix-loop-helix (b-HLH) transcription factor regulating head mesenchyme cell development during cranial neural tube formation in mouse. Studying a series of 22 unrelated ACS III patients, we have found TWIST mutations in 16/22 cases. Interestingly, these mutations consistently involved the b-HLH domain of the protein. Indeed, mutant genotypes included frameshift deletions/insertions, nonsense and missense mutations, either truncating or disrupting the b-HLH motif of the protein. This observation gives additional support to the view that most ACS III cases result from... [ABSTRACT FROM AUTHOR]

Published

1999

16. Mutations in the CCN gene family member WISP3 cause progressive pseudorheumatoid dysplasia.

Author

Hurvitz, Jennifer R., Suwairi, Wafaa M., Van Hul, Wim, El-Shanti, Hatem, Superti-Furga, Andrea, Roudier, Jean, Holderbaum, Daniel, Pauli, Richard M., Herd, J. Kenneth, Hul, Els Van, Rezai-Delui, Hossien, Legius, Eric, Le Merrer, Martine, Al-Alami, Jamil, Bahabri, Sultan A., and Warman, Matthew L.

Subjects

GENES, CYSTEINE proteinases, CELL growth, GENETIC mutation

Abstract

Members of the CCN (for CTGF, cyr61/cef10, nov) gene family encode cysteine-rich secreted proteins with roles in cell growth and differentiation. Cell-specific and tissue-specific differences in the expression and function of different CCN family members suggest they have non-redundant roles. Using a positional-candidate approach, we found that mutations in the CCN family member WISP3 are associated with the autosomal recessive skeletal disorder progressive pseudorheumatoid dysplasia (PPD; MIM 208230). PPD is an autosomal recessive disorder that may be initially misdiagnosed as juvenile rheumatoid arthritis. Its population incidence has been estimated at 1 per million in the United Kingdom, but it is likely to be higher in the Middle East and Gulf States. Affected individuals are asymptomatic in early childhood. Signs and symptoms of disease typically develop between three and eight years of age. Clinically and radiographically, patients experience continued cartilage loss and destructive bone changes as they age, in several instances necessitating joint replacement surgery by the third decade of life. Extraskeletal manifestations have not been reported in PPD. Cartilage appears to be the primary affected tissue, and in one patient, a biopsy of the iliac crest revealed abnormal nests of chondrocytes and loss of normal cell columnar organization in growth zones. We have identified nine different WISP3 mutations in unrelated, affected individuals, indicating that the gene is essential for normal post-natal skeletal growth and cartilage homeostasis. [ABSTRACT FROM AUTHOR]

Published

1999

17. Presentation of six cases of Stüve-Wiedemann syndrome.

Author

Cormier-Daire, Valérie, Munnich, A., Lyonnet, Stanislas, Rustin, Pierre, Delezoide, Anne-Lise, Maroteaux, Pierre, and Le Merrer, Martine

Abstract

Stüve-Wiedemann syndrome (SWS) is a rare disorder characterized by bowing of the long bones, camptodactyly, respiratory distress, hyperthermic episodes and early lethality. We report six additional cases of SWS, suggesting that this syndrome is homogeneous. All patients had feeding and swallowing difficulties, respiratory insufficiency, dysmorphic features and radiolucent metaphyses with abnormal trabecular pattern. Recurrent episodes of unexplained fever was the cause of death in almost all cases. Parental consanguinity and recurrence in sibs is highly suggestive of autosomal recessive inheritance. [ABSTRACT FROM AUTHOR]

Published

1998

18. Metaphyseal anadysplasia type II: a new regressive metaphyseal dysplasia.

Author

Le Merrer, Martine and Maroteaux, Pierre

Abstract

We report on six unrelated children, three boys and three girls, with a metaphyseal dysplasia of early onset and spontaneous regressing evolution. During the first months of life the children present with enlargement of costochondral junctions and knobby wrists. On radiographs the metaphyseal changes of the knees are specific with fine irregularities. The femoral necks are blurred but not hypoplastic. The stature is not affected and there are no metabolic abnormalities. The radiographic findings regress during growth and the abnormalities disappear after the age of ten years. These metaphyseal changes and their mode of inheritance are different from previous cases described as anadysplasia. We propose therefore to delineate this syndrome as a new type of regressive metaphyseal dysplasia and to name it anadysplasia type II. [ABSTRACT FROM AUTHOR]

Published

1998

19. X-linked spastic paraplegia and Pelizaeus-Merzbacher disease are allelic disorders at the proteolipid protein locus.

Author

Saugier-Veber, Pascale, Munnich, Arnold, Bonneau, Dominique, Rozet, Jean-Michel, Le Merrer, Martine, Gil, Roger, and Boespflug-Tanguy, Odile

Published

1994

20. Truncating mutations in the last exon of NOTCH2 cause a rare skeletal disorder with osteoporosis.

Author

Isidor, ,13Bertrand, Lindenbaum, Pierre, Pichon, Olivier, Bézieau, Stéphane, Dina, Christian, Jacquemont, Sébastien, Martin-Coignard, Dominique, Thauvin-Robinet, Christel, Le Merrer, Martine, Mandel, Jean-Louis, David, Albert, Faivre, Laurence, Cormier-Daire, Valérie, Redon, Richard, and Le Caignec, Cédric

Subjects

GENETIC mutation, EXONS (Genetics), OSTEOPOROSIS, BONE resorption, MESSENGER RNA, PATIENTS

Abstract

Hajdu-Cheney syndrome is a rare autosomal dominant skeletal disorder with facial anomalies, osteoporosis and acro-osteolysis. We sequenced the exomes of six unrelated individuals with this syndrome and identified heterozygous nonsense and frameshift mutations in NOTCH2 in five of them. All mutations cluster to the last coding exon of the gene, suggesting that the mutant mRNA products escape nonsense-mediated decay and that the resulting truncated NOTCH2 proteins act in a gain-of-function manner. [ABSTRACT FROM AUTHOR]

Published

2011

21. Thromboxane synthase mutations in an increased bone density disorder (Ghosal syndrome).

Author

Geneviève, David, Proulle, Valérie, Isidor, Bertrand, Bellais, Samuel, Serre, Valérie, Djouadi, Fatima, Picard, Capucine, Vignon-Savoye, Capucine, Bader-Meunier, Brigitte, Blanche, Stéphane, de Vernejoul, Marie-Christine, Legeai-Mallet, Laurence, Fischer, Anne-Marie, Le Merrer, Martine, Dreyfus, Marie, Gaussem, Pascale, Munnich, Arnold, and Cormier-Daire, Valérie

Subjects

DYSPLASIA, GENETIC disorders, BONE density, THROMBOXANES, GENETIC mutation

Abstract

Studying consanguineous families with Ghosal hematodiaphyseal dysplasia syndrome (GHDD), a disorder of increased bone density, we identified mutations in TBXAS1, which encodes thromboxane synthase (TXAS). TXAS, an enzyme of the arachidonic acid cascade, produces thromboxane A2 (TXA2). Platelets from subjects with GHDD showed a specific deficit in arachidonic acid–produced aggregation. We also found that TXAS and TXA2 modulated expression of TNFSF11 and TNFRSF11B (encoding RANKL and osteoprotegerin (OPG), respectively) in primary cultured osteoblasts. [ABSTRACT FROM AUTHOR]

Published

2008

22. Wolcott-Rallison syndrome: a case with endocrine and exocrine pancreatic deficiency and pancreatic hypotrophy.

Author

Castelnau, Pierre, Le Merrer, Martine, Diatloff-Zito, Catherine, Marquis, Eve, Tête, Marie-Joseph, Robert, Jean-Jacques, Castelnau, P, Le Merrer, M, Diatloff-Zito, C, Marquis, E, Tête, M J, and Robert, J J

Subjects

*SYNDROMES, *RADIOGRAPHY, *DYSPLASIA

Abstract

Clinical analysis and genetic investigations of new cases of Wolcott-Rallison syndrome are needed to evaluate the role of the gene(s) directly or indirectly implicated in pancreas development and in the aetiology of the syndrome. [ABSTRACT FROM AUTHOR]

Published

2000

23. New dysplasia or achondrogenesis type 1B? The importance of histology and molecular biology in delineating skeletal dysplasias.

Author

Unger, Sheila, Le Merrer, Martine, Meinecke, Peter, Chitayat, David, Rossi, Antonio, and Superti-Furga, Andrea

Subjects

LETTERS to the editor, DYSPLASIA

Abstract

Presents a letter to the editor about histology and microbiology in delineating skeletal dysplasias.

Published

2001

24. Clinical utility gene card for: Hypophosphatasia - update 2013.

Author

Mornet, Etienne, Hofmann, Christine, Bloch-Zupan, Agnès, Girschick, Hermann, and Le Merrer, Martine

Subjects

HYPOPHOSPHATASIA, GENETIC testing, GENETIC counseling, DELETION mutation, PATHOGENIC microorganisms, THERAPEUTICS

Abstract

The article discusses the developments in the genetics research related to treatment for hypophosphatasia (HP), rathbun disease and phosphoethanolaminuria. Topics include the different disease-causing mutations reported in the ALPL gene mutations, analytical techniques for mutation screening, and fundamental use of genetic testing in genetic counselling.

Published

2014

25. Clinical utility gene card for: hypophosphatasia.

Author

Mornet, Etienne, Beck, Christine, Bloch-Zupan, Agnès, Girschick, Hermann, and Le Merrer, Martine

Subjects

HYPOPHOSPHATASIA, HUMAN chromosome abnormality diagnosis

Abstract

The article offers information on the clinical utility gene card for diagnosis of hypophosphatasia (HP) in which prevalence of severe cases was one in 100,000 based on the study conducted in Toronto, Ontario.

Published

2011

26. FGFR2 mutations in Pfeiffer syndrome.

Author

Lajeunie, Elisabeth, Ma, Hong Wei, Bonaventure, Jacky, Munnich, Arnold, Le Merrer, Martine, and Renier, Dominique

Published

1995