Your search keyword '"Attié-Bitach, Tania"' showing total 32 results

1. Multiple congenital anomalies in two fetuses with glutathione‐synthetase deficit (GSS).

Author

Jury, Jeanne, Benoist, Jean‐François, Joubert, Madeleine, Quelin, Chloé, Besnard, Thomas, Conrad, Solène, Le Vaillant, Claudine, Bézieau, Stéphane, Isidor, Bertrand, Attié‐Bitach, Tania, Cogné, Benjamin, and Vincent, Marie

Subjects

CONGENITAL heart disease, GROWTH disorders, CLEFT palate, AMNIOTIC liquid, GENE expression

Abstract

Glutathione synthetase deficiency is a rare inborn metabolic disease usually caused by biallelic variants in GSS. Clinical severity varies from isolated hemolytic anemia, sometimes associated with chronic metabolic acidosis and 5‐oxoprolinuria, to severe neurological phenotypes with neonatal lethality. Here we report on two fetal siblings from two pregnancies with glutathione synthetase deficiency exhibiting similar multiple congenital anomalies associating phocomelia, cleft palate, intra‐uterine growth retardation, genito‐urinary malformations, and congenital heart defect. Genome sequencing showed that both fetuses were compound heterozygous for two GSS variants: the previously reported pathogenic missense substitution NM_000178.4 c.800G>A p.(Arg267Gln), and a 2.4 kb intragenic deletion NC_000020.11:g.34944530_34946833del. RNA‐seq on brain tissue revealed the out‐of‐frame deletion of the exon 3 and an almost monoallelic expression of the missense variant (88%), suggesting degradation of the deletion‐harboring allele by nonsense‐mediated mRNA decay. 5‐oxoproline (pyroglutamic acid) levels in amniotic fluid were elevated, suggesting an alteration of the gamma‐glutamyl cycle, and corroborating the pathogenicity of the two GSS variants. Only one case of glutathione synthetase deficiency with limb malformations has previously been reported, in a newborn homozygous for the c.800G>A variant. Thus, our data allow us to discuss a potential phenotypic extension of glutathione synthetase deficiency, with a possible involvement of the c.800G>A variant. [ABSTRACT FROM AUTHOR]

Published

2024

2. Fetal Presentation of MYRF‐Related Cardiac Urogenital Syndrome: An Emerging and Challenging Prenatal Diagnosis.

Author

Favier, Maud, Brischoux‐Boucher, Elise, Pyle, Louise C., Mottet, Nicolas, Auber‐Lenoir, Marion, Cattin, Julie, Dahlen, Eric, Cabrol, Christelle, Arbez‐Gindre, Francine, Attié‐Bitach, Tania, Boute, Odile, Devisme, Louise, Trost, Detlef, Boughalem, Aicha, Chitayat, David, Prasov, Lev, Chorin, Odelia, Rein‐Rothschild, Annick, Kassif, Eran, and Weissbach, Tal

Abstract

Purpose: MYRF‐related cardiac‐urogenital syndrome (MYRF‐CUGS) is a rare condition associated with heterozygous MYRF variants. The description of MYRF‐CUGS phenotype is mostly based on postnatal cases and 36 affected individuals have been published so far. We aim now to delineate the prenatal phenotype of MYRF‐CUGS by reporting clinical data from fetuses and neonates with a pathogenic MYRF variant. Methods: Detailed radiographic, pathological, clinical, and molecular data from 12 prenatal cases were collected through an international collaborative study. Adding the five fetuses previously published, we were able to study a cohort of 17 cases. Results: Main ultrasound‐accessible manifestations of MYRF‐CUGS include congenital heart defects (13/17, 76%), congenital diaphragmatic hernia (10/17, 59%) and disorders of sexual differentiation in 46, XY fetuses (7/14; 50%). Postnatal examination and/or autopsy data highlighted additional birth defects and neurological findings with a large spectrum of severity. Molecular results revealed ten previously unpublished variants, one missense and nine predicted truncating variants (three frameshift, three nonsense and three splice site variants). Conclusion: We report the first prenatal cohort of MYRF‐CUGS, allowing us to further characterize the variable expressivity of this rare disorder in fetuses. Severe congenital anomalies with a poor prognosis are more frequent than previously described in postnatal cases. Our data suggest that MYRF‐CUGS is characterized by a recurrent recognizable malformative association, accessible to prenatal diagnosis, with a significant intrafamilial phenotypic variability making genetic counseling challenging. [ABSTRACT FROM AUTHOR]

Published

2024

3. Prenatal diagnosis of SLC25A24 Fontaine progeroid syndrome: description of the fetal phenotype, genotype and detection of parental mosaicism.

Author

Pannier, Emmanuelle, Sekri, Abel, Roux, Nathalie, Vasiljevic, Alexandre, El Khattabi, Laïla, Chatron, Nicolas, Grotto, Sarah, Menzella, Delphine, Grangé, Gilles, Thébault, Florent, Massardier, Jérôme, Fourrage, Cécile, Lohmann, Laurence, Tsatsaris, Vassilis, Putoux, Audrey, Boutaud, Lucile, and Attié‐Bitach, Tania

Abstract

Background: Fontaine progeroid syndrome (FPS, OMIM 612289) is a recently identified genetic disorder stemming from pathogenic variants in the SLC25A24 gene, encoding a mitochondrial carrier protein. It encompasses Gorlin–Chaudry–Moss syndrome and Fontaine–Farriaux syndrome, primarily manifesting as craniosynostosis with brachycephaly, distinctive dysmorphic facial features, hypertrichosis, severe prenatal and postnatal growth restriction, limb shortening, and early aging with characteristic skin changes, phalangeal anomalies, and genital malformations. Cases: All known occurrences of FPS have been postnatally observed until now. Here, we present the first two prenatal cases identified during the second trimester of pregnancy. While affirming the presence of most postnatal abnormalities in prenatal cases, we note the absence of a progeroid appearance in young fetuses. Notably, our reports introduce new phenotypic features like encephalocele and nephromegaly, which were previously unseen postnatally. Moreover, paternal SLC25A24 mosaicism was detected in one case. Conclusions: We present the initial two fetal instances of FPS, complemented by thorough phenotypic and genetic assessments. Our findings expand the phenotypical spectrum of FPS, unveiling new fetal phenotypic characteristics. Furthermore, one case underscores a potential novel inheritance pattern in this disorder. Lastly, our observations emphasize the efficacy of exome/genome sequencing in both prenatal and postmortem diagnosis of rare polymalformative syndromes with a normal karyotype and array‐based comparative genomic hybridization (CGH). [ABSTRACT FROM AUTHOR]

Published

2024

4. Prenatal Diagnosis of Primrose Syndrome.

Author

Abdallah, Wael, Spaggiari, Emmanuel, Brisset, Sophie, Dard, Rodolphe, Attié Bitach, Tania, Bault, Jean Philippe, and Quibel, Thibault

Subjects

AGENESIS of corpus callosum, PRENATAL diagnosis, PRIMROSES, MISSENSE mutation, HUMAN abnormalities, SYNDROMES

Abstract

Primrose syndrome is a very rare congenital malformation. Symptoms of this disorder may appear during childhood, but the diagnosis is identified in adulthood in the majority of cases. The prenatal diagnosis of Primrose syndrome is not developed in the literature. We present herein a case series of 3 cases with characteristic sonographic features. A dysmorphic metopic suture, downslanting palpebral fissures, a wide forehead, and agenesis of corpus callosum are the main signs. A missense mutation in ZBTB20 identified in whole exome sequencing can confirm the prenatal diagnosis of Primrose syndrome. [ABSTRACT FROM AUTHOR]

Published

2024

5. Neu Laxova syndrome and megacystis in the first trimester: Broadening the fetal phenotype.

Author

Bourgon, Nicolas, Chen, Ruiqian, Grangé, Gilles, Grotto, Sarah, Molac, Clémence, Loeuillet, Laurence, and Attié‐Bitach, Tania

Abstract

Neu Laxova syndrome (NLS) is a rare and lethal congenital disorder characterized by severe intra‐uterine growth retardation (IUGR), ichthyosis, abnormal facial features, limb abnormalities with arthrogryposis and a wide spectrum of severe malformations of the central nervous system (CNS). NLS is due to biallelic variants in three genes previously involved in serine‐deficiency disorders (PHGDH, PSAT1 and PSPH), extending the phenotypic spectrum of these disorders. Key points: What is already known about this topic? Biallelic PHGDH variants are associated with serine‐deficiency disorders and Neu Laxova syndrome (NLS).NLS is characterized by severe IUGR, ichthyosis, abnormal facial features, limb abnormalities with arthrogryposis and a wide spectrum of severe malformations of the CNS.NLS is usually suggested in the third trimester of pregnancy or in the neonatal period. What does this study add? The study reports early and severe presentation of NLS with increased nuchal translucency and megacystis.Our findings suggest that megacystis is secondary to a neurogenic muscular atrophy, extending neuromuscular findings reported in NLS.The study highlights the intrafamilial variability of NLS. [ABSTRACT FROM AUTHOR]

Published

2023

6. Investigating genotype‐to‐phenotype correlation in CHARGE syndrome by deep phenotyping and multiparametric clustering.

Author

Dana, Jérémy, Dorval, Guillaume, Martin, Christine Saint, Belhous, Kahina, Levy, Raphael, Marlin, Sandrine, De Bie, Isabelle, Mautret‐Godefroy, Manon, Rausell, Antonio, Rio, Marlène, Boucher‐Brischoux, Elise, Attié‐Bitach, Tania, Boddaert, Nathalie, and Pingault, Véronique

Subjects

GENETIC variation, SYNDROMES, MACHINE learning, PHENOTYPES

Abstract

CHARGE syndrome, due to CHD7 pathogenic variations, is an autosomal dominant disorder characterized by a large spectrum of severity. Despite the great number of variations reported, no clear genotype‐to‐phenotype correlation has been reported. Unsupervised machine learning and clustering was undertaken using a retrospective cohort of 42 patients, after deep radiologic and clinical phenotyping, to establish genotype–phenotype correlation for CHD7‐related CHARGE syndrome. It resulted in three clusters showing phenotypes of different severities. While no clear genotype–phenotype correlation appeared within the first two clusters, a single patient was outlying the cohort data (cluster 3) with the most atypical phenotype and the most distal frameshift variant in the gene. We added two other patients with similar distal pathogenic variants and observed a tendency toward mild and/or atypical phenotypes. We hypothesized that this finding could potentially be related to escaping nonsense mediated RNA decay, but found no evidence of such decay in vivo for any of the CHD7 pathogenic variation tested. This indicates that this milder phenotype may rather result from the production of a protein retaining all functional domains. [ABSTRACT FROM AUTHOR]

Published

2023

7. Morphological and genetic causes of fetal cardiomyopathies.

Author

Kohaut, Eva, Ader, Flavie, Rooryck, Caroline, Pelluard, Fanny, Bonnière, Maryse, André, Gwenaelle, Sauvestre, Fanny, Roth, Philippe, Khraiche, Diala, Bessières, Bettina, Attié‐Bitach, Tania, and Richard, Pascale

Subjects

FETAL death, CARDIOMYOPATHIES, MYOCARDIUM, GENETIC counseling, GENETIC testing, NEWBORN infants

Abstract

Cardiomyopathies are diseases of the heart muscle with variable clinical expressivity. Most of forms are inherited as dominant trait, and with incomplete penetrance until adulthood. Severe forms of cardiomyopathies were observed during the antenatal period with a pejorative issue leading to fetal death or medical interruption of pregnancy. Variable phenotypes and genetic heterogeneity make etiologic diagnosis difficult. We report 11 families (16 cases) whose unborn, newborn or infant with early onset cardiomyopathies. Detailed morphological and histological examinations of hearts were implemented, as well as genetic analysis on a cardiac targeted NGS panel. This strategy allowed the identification of the genetic cause of the cardiomyopathy in 8/11 families. Compound heterozygous mutations in dominant adulthood cardiomyopathy genes were found in two, pathogenic variants in co‐dominant genes in one, de novo mutations in 5 including a germline mosaicism in one family. Parental testing was systematically performed to detect mutation carriers, and to manage cardiological surveillance and propose a genetic counseling. This study highlights the great diagnostic value of the genetic testing of severe antenatal cardiomyopathy both for genetic counseling and to detect presymptomatic parents at higher risk of developing cardiomyopathy. [ABSTRACT FROM AUTHOR]

Published

2023

8. Two novel variations p.(Ser1275Thr) and p.(Ser1275Arg) in FLT4 causing prenatal hereditary lymphedema type 1.

Author

Lajmi, Yosra, Loeuillet, Laurence, Petrilli, Giulia, Egloff, Charles, Nectoux, Juliette, Molac, Clémence, Roux, Nathalie, Pannier, Emmanuelle, Achaiaa, Amale, Arkoub, Zaina Ait, Chuon, Sophie, Coussement, Aurélie, Dupont, Jean Michel, Malan, Valérie, Spaggiari, Emmanuel, Razavi, Ferechte, Amiel, Jeanne, Bessières, Bettina, Grotto, Sarah, and Attié‐Bitach, Tania

Abstract

Background: Hereditary lymphedema 1 is a rare congenital condition, characterized by the development of chronic swelling in body parts. It is highly variable in expression and age of onset with different presentations: from feet edema to hydrops fetalis. This affection is genetically heterogeneous with autosomal dominant inheritance and incomplete penetrance due to a mutation in the FLT4 gene in most cases. Cases: In our study, we report on two fetuses harboring congenital lymphedema with FLT4 variation and review the prenatal confirmed ones of the literatures. Our cases were selected within fetuses explored by exome sequencing in a diagnosis setting. Prenatal ultrasonography showed hydrops fetalis in one case and an increased nuchal translucency with hydrothorax in the other. Comparative genomic hybridization array on amniocentesis was normal in both cases. Exome sequencing identified a variation p.(Ser1275Thr) and p.(Ser1275Arg) in fetus 1 and fetus 2 in the FLT4 gene, respectively. A de novo mutation at the same codon was reported in prenatal literature suggesting possible genotype phenotype correlation. Conclusion: Cystic hygroma/hydrops fetalis are possible manifestations of several disorders. This study illustrates how the integration of exome sequencing in prenatal clinical practice can facilitate the diagnosis and genetic counseling of heterogeneous developmental affections. [ABSTRACT FROM AUTHOR]

Published

2023

9. Retrospective evaluation of clinical and molecular data of 148 cases of esophageal atresia.

Author

Ranza, Emmanuelle, Le Gouez, Morgane, Guimier, Anne, Dunlop, Naziha Khen, Beaudoin, Sylvie, Malan, Valérie, Michot, Caroline, Baujat, Geneviève, Rio, Marlène, Cormier‐Daire, Valérie, Abadie, Véronique, Sarnacki, Sabine, Delacourt, Christophe, Lyonnet, Stanislas, Attié‐Bitach, Tania, Pingault, Véronique, Rousseau, Véronique, and Amiel, Jeanne

Abstract

Developmental abnormalities provide a unique opportunity to seek for the molecular mechanisms underlying human organogenesis. Esophageal development remains incompletely understood and elucidating causes for esophageal atresia (EA) in humans would contribute to achieve a better comprehension. Prenatal detection, syndromic classification, molecular diagnosis, and prognostic factors in EA are challenging. Some syndromes have been described to frequently include EA, such as CHARGE, EFTUD2‐mandibulofacial dysostosis, Feingold syndrome, trisomy 18, and Fanconi anemia. However, no molecular diagnosis is made in most cases, including frequent associations, such as Vertebral‐Anal‐Cardiac‐Tracheo‐Esophageal‐Renal‐Limb defects (VACTERL). This study evaluates the clinical and genetic test results of 139 neonates and 9 fetuses followed‐up at the Necker‐Enfants Malades Hospital over a 10‐years period. Overall, 52 cases were isolated EA (35%), and 96 were associated with other anomalies (65%). The latter group is divided into three subgroups: EA with a known genomic cause (9/148, 6%); EA with Vertebral‐Anal‐Cardiac‐Tracheo‐Esophageal‐Renal‐Limb defects (VACTERL) or VACTERL/Oculo‐Auriculo‐Vertebral Dysplasia (VACTERL/OAV) (22/148, 14%); EA with associated malformations including congenital heart defects, duodenal atresia, and diaphragmatic hernia without known associations or syndromes yet described (65/148, 44%). Altogether, the molecular diagnostic rate remains very low and may underlie frequent non‐Mendelian genetic models. [ABSTRACT FROM AUTHOR]

Published

2023

10. Extending the prenatal Noonan's phenotype by review of ultrasound and autopsy data.

Author

Lamouroux, Audrey, Dauge, Coralie, Wells, Constance, Mousty, Eve, Pinson, Lucile, Cavé, Hélène, Capri, Yline, Faure, Jean‐Michel, Grosjean, Frédéric, Sauvestre, Fanny, Attié‐Bitach, Tania, Pelluard, Fanny, and Geneviève, David

Abstract

Objectives: The antenatal phenotypic spectrum of Noonan Syndrome (NS) requires better characterization. Methods: This multicenter retrospective observational included 16 fetuses with molecularly confirmed NS admitted for fetopathological examination between 2009 and 2016. Results: Among 12 pathogenic variants (PV) in PTPN11 (80%), 5 (42%) fell between position c.179 and c.182. Ultrasound showed increased nuchal translucency (n = 13/16, 93%), increased nuchal fold after 15 weeks of gestation (n = 12/16, 75%), pleural effusions (n = 11/16, 69%), polyhydramnios (n = 9/16, 56%), hydrops (n = 7/16, 44%), cardiovascular (n = 6/16, 38%) and cerebral (n = 4/16, 25%) anomalies. Fetopathological examination found dysmorphic features in all cases, cardiovascular anomalies (n = 12/15, 80%), pulmonary hypoplasia (n = 10/15, 67%), effusions (n = 7/15, 47%) and neuropathological anomalies (n = 5/15, 33%). Hydrops was significantly (p = 0.02) more frequent in the four fetuses with RIT1, NRAS and RAF1 PV versus the 12 fetuses with PTPN11 PV. Conclusions: Increased nuchal translucency and nuchal fold is common in NS. Noonan Syndrome antenatal phenotype showed high in utero fetal death, hydrops, prenatal pleural effusion and pulmonary hypoplasia, although the inclusion of only deceased fetuses will have selected more severe phenotypes. Non‐specific cardiovascular and neurological abnormalities should be added to NS antenatal phenotype. Next generation sequencing will help detect more genotypes, clarifying the prenatal phenotype and identifying genotype‐phenotype correlations. Key points: What's already known about this topic? Noonan Syndrome (NS) is an autosomal dominant disorder with highly variable antenatal phenotype, which sometimes does not correlate with the severity of the postnatal phenotype, making counseling challenging.The ultrasound phenotype of NS is associated with increased nuchal translucency in first trimester and beyond the second trimester of pregnancy, polyhydramnios, pleural effusion, ascites, edema and cardiac and facial anomalies.These signs are frequent and non‐specific. What does this study add? This case series better characterizes fetuses carrying NS, identifying a wider phenotypic spectrum than originally reported. The antenatal phenotype includes non‐specific cardiovascular, renal and neurological abnormalities.This phenotype seems to be more severe than previously thought, with a high rate of hydrops, prenatal pleural effusion and pulmonary hypoplasia.Different genotypes have specific phenotypes, for example, hydrops was more associated to mutations in non‐PTPN11 targets. [ABSTRACT FROM AUTHOR]

Published

2022

11. GGCX‐related congenital combined vitamin K‐dependent clotting factors deficiency‐1: Description of a fetus with chondrodysplasia punctata.

Author

Mathonnet, Alix, Cunat, Séverine, Allias, Fabienne, Caillot, Sandrine, Thonnon, Cyrielle, Till, Marianne, Attié‐Bitach, Tania, Touraine, Renaud, Meunier, Sandrine, Cartellier, Charline, Rossi, Massimiliano, Attia, Jocelyne, and Putoux, Audrey

Abstract

Congenital combined vitamin K‐dependent clotting factors deficiency (VKCFD) is a rare autosomal recessive disease resulting in hemorrhagic symptoms usually associated with developmental disorders and bone abnormalities. Pathogenic variants in two genes encoding enzymes of the vitamin K cycle, GGCX and VKORC1, can lead to this disorder. We present the case of a male fetus with a brachytelephalangic chondrodysplasia punctata (CDP), absence of nasal bone, growth restriction, and bilateral ventriculomegaly at 18 weeks of gestation. Pathological examination showed a Binder phenotype, hypoplastic distal phalanges, stippled epiphyses, and brain abnormalities suggestive of a brain hemorrhage. Two GGCX pathogenic variants inherited respectively from the mother and the father were identified. To our knowledge, this is the first prenatal description of VKCFD. Even if it remains a rare etiology, which is mostly described in children or adult patients, VKCFD should be considered in fetuses with CDP. [ABSTRACT FROM AUTHOR]

Published

2022

12. EFTUD2 missense variants disrupt protein function and splicing in mandibulofacial dysostosis Guion‐Almeida type.

Author

Thomas, Huw B., Wood, Katherine A., Buczek, Weronika A., Gordon, Christopher T., Pingault, Véronique, Attié‐Bitach, Tania, Hentges, Kathryn E., Varghese, Vinod C., Amiel, Jeanne, Newman, William G., and O'Keefe, Raymond T.

Abstract

Pathogenic variants in the core spliceosome U5 small nuclear ribonucleoprotein gene EFTUD2/SNU114 cause the craniofacial disorder mandibulofacial dysostosis Guion‐Almeida type (MFDGA). MFDGA‐associated variants in EFTUD2 comprise large deletions encompassing EFTUD2, intragenic deletions and single nucleotide truncating or missense variants. These variants are predicted to result in haploinsufficiency by loss‐of‐function of the variant allele. While the contribution of deletions within EFTUD2 to allele loss‐of‐function are self‐evident, the mechanisms by which missense variants are disease‐causing have not been characterized functionally. Combining bioinformatics software prediction, yeast functional growth assays, and a minigene (MG) splicing assay, we have characterized how MFDGA missense variants result in EFTUD2 loss‐of‐function. Only four of 19 assessed missense variants cause EFTUD2 loss‐of‐function through altered protein function when modeled in yeast. Of the remaining 15 missense variants, five altered the normal splicing pattern of EFTUD2 pre‐messenger RNA predominantly through exon skipping or cryptic splice site activation, leading to the introduction of a premature termination codon. Comparison of bioinformatic predictors for each missense variant revealed a disparity amongst different software packages and, in many cases, an inability to correctly predict changes in splicing subsequently determined by MG interrogation. This study highlights the need for laboratory‐based validation of bioinformatic predictions for EFTUD2 missense variants. [ABSTRACT FROM AUTHOR]

Published

2020

13. TAR syndrome: Clinical and molecular characterization of a cohort of 26 patients and description of novel noncoding variants of RBM8A.

Author

Boussion, Simon, Escande, Fabienne, Jourdain, Anne‐Sophie, Smol, Thomas, Brunelle, Perrine, Duhamel, Céline, Alembik, Yves, Attié‐Bitach, Tania, Baujat, Geneviève, Bazin, Anne, Bonnière, Maryse, Carassou, Philippe, Carles, Dominique, Devisme, Louise, Goizet, Cyril, Goldenberg, Alice, Grotto, Sarah, Guichet, Agnès, Jouk, Pierre‐Simon, and Loeuillet, Laurence

Abstract

Thrombocytopenia‐absent radius (TAR) syndrome is characterized by radial defect and neonatal thrombocytopenia. It is caused by biallelic variants of RBM8A gene (1q21.1) with the association of a null allele and a hypomorphic noncoding variant. RBM8A encodes Y14, a core protein of the exon junction complex involved in messenger RNA maturation. To date, only two hypomorphic variants have been identified. We report on a cohort of 26 patients affected with TAR syndrome and carrying biallelic variants in RBM8A. Half patients carried a 1q21.1 deletion and one of the two known hypomorphic variants. Four novel noncoding variants of RBM8A were identified in the remaining patients. We developed experimental models enabling their functional characterization in vitro. Two variants, located respectively in the 5′‐untranslated region (5′‐UTR) and 3′‐UTR regions, are responsible for a diminished expression whereas two intronic variants alter splicing. Our results bring new insights into the molecular knowledge of TAR syndrome and enabled us to propose genetic counseling for patients' families. [ABSTRACT FROM AUTHOR]

Published

2020

14. Prenatal diagnosis of cerebro‐oculo‐facio‐skeletal syndrome: Report of three fetuses and review of the literature.

Author

Le Van Quyen, Pauline, Calmels, Nadège, Bonnière, Maryse, Chartier, Suzanne, Razavi, Féréchté, Chelly, Jamel, El Chehadeh, Salima, Baer, Sarah, Boutaud, Lucile, Bacrot, Séverine, Obringer, Cathy, Favre, Romain, Attié‐Bitach, Tania, Laugel, Vincent, and Antal, Maria C.

Abstract

Cerebro‐oculo‐facio‐skeletal syndrome (COFS) is a rare autosomal recessive neurodegenerative disease belonging to the family of DNA repair disorders, characterized by microcephaly, congenital cataracts, facial dysmorphism and arthrogryposis. Here, we describe the detailed morphological and microscopic phenotype of three fetuses from two families harboring ERCC5/XPG likely pathogenic variants, and review the five previously reported fetal cases. In addition to the classical features of COFS, the fetuses display thymus hyperplasia, splenomegaly and increased hematopoiesis. Microencephaly is present in the three fetuses with delayed development of the gyri, but normal microscopic anatomy at the supratentorial level. Microscopic anomalies reminiscent of pontocerebellar hypoplasia are present at the infratentorial level. In conclusion, COFS syndrome should be considered in fetuses when intrauterine growth retardation is associated with microcephaly, arthrogryposis and ocular anomalies. Further studies are needed to better understand XPG functions during human development. [ABSTRACT FROM AUTHOR]

Published

2020

15. Mutations in IFT80 cause SRPS Type IV. Report of two families and review.

Author

Bizaoui, Varoona, Huber, Céline, Kohaut, Eva, Roume, Joelle, Bonnière, Maryse, Attié‐Bitach, Tania, and Cormier‐Daire, Valérie

Abstract

We report novel causative mutations in the IFT80 gene identified in four fetuses from two unrelated families with Beemer‐Langer syndrome (BLS) or BLS‐like phenotypes. We discuss the implication of the IFT80 gene in ciliopathies, and its diagnostic value for BLS among other SRPS. [ABSTRACT FROM AUTHOR]

Published

2019

16. Fetal phenotype of Rubinstein‐Taybi syndrome caused by CREBBP mutations.

Author

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

Subjects

HUMAN phenotype, FETUS, RUBINSTEIN-Taybi syndrome, HUMAN abnormalities, GALLBLADDER, GENETIC mutation

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. [ABSTRACT FROM AUTHOR]

Published

2019

17. A clinical and histopathological study of malformations observed in fetuses infected by the Zika virus.

Author

Beaufrère, Aurélie, Bessières, Bettina, Bonnière, Maryse, Driessen, Marine, Alfano, Christian, Couderc, Thérèse, Thiry, Marc, Thelen, Nicolas, Lecuit, Marc, Attié‐Bitach, Tania, Vekemans, Michel, Ville, Yves, Nguyen, Laurent, Leruez‐Ville, Marianne, and Encha‐Razavi, Férechté

Subjects

HISTOPATHOLOGY, FETAL abnormalities, ZIKA virus infections, MICROCEPHALY, DISEASE prevalence, PUBLIC health

Abstract

Background: The recent outbreak of Zika virus (ZIKV) infection and the associated increased prevalence of microcephaly in Brazil underline the impact of viral infections on embryo fetal development. The aim of the present study is to provide a detailed clinical and histopathological study of the fetal disruption caused by the ZIKV, with a special focus on the associated neuropathological findings. Methods: A detailed feto‐placental examination, as well as neuropathological and neurobiological studies were performed on three fetuses collected after pregnancy termination between 22 and 25 weeks of gestation (WG), because brain malformations associated with a maternal and fetal ZIKV infection was diagnosed. Results: In all three cases, the maternal infection occurred during the first trimester of pregnancy. A small head was observed on the ultrasound examination of the second trimester of pregnancy and led to the diagnosis of ZIKV fetopathy and pregnancy termination. The fetal histopathological examination was unremarkable on the viscera but showed on the testis an interstitial lymphocytic infiltrate. The placenta contained a Hofbauer cells hyperplasia with signs of inflammation. Neuropathological findings included a meningoencephalitis and an ex vacuo hydrocephalus. Immunohistochemical studies showed the presence of T lymphocytic and histiocytic meningitis associated with an abundant cerebral astroglial and macrophagic reaction. In situ hybridization demonstrated, abundant ZIKV particles within the cerebral parenchyma mainly in the ventricular/subventricular zone and in the cortical plate. In addition massive cells death and endoplasmic reticulum damage were present. Conclusion: The present study reports on the clinical and histopathological findings observed in three fetuses infected by the ZIKV. It emphasizes the severity of brain damages and the minimal visceral and placental changes observed upon ZIKV infection. This confirms the selective neurotropism of ZIKV. Finally, it allows us to describe the cascade of multifactorial developmental defects leading to microcephaly. [ABSTRACT FROM AUTHOR]

Published

2019

18. Loss of function IFT27 variants associated with an unclassified lethal fetal ciliopathy with renal agenesis.

Author

Quélin, Chloé, Loget, Philippe, Boutaud, Lucile, Elkhartoufi, Nadia, Milon, Joelle, Odent, Sylvie, Fradin, Mélanie, Demurger, Florence, Pasquier, Laurent, Thomas, Sophie, and Attié‐Bitach, Tania

Abstract

Ciliopathies comprise a group of clinically heterogeneous and overlapping disorders with a wide spectrum of phenotypes ranging from prenatal lethality to adult‐onset disorders. Pathogenic variants in more than 100 ciliary protein‐encoding genes have been described, most notably those involved in intraflagellar transport (IFT) which comprises two protein complexes, responsible for retrograde (IFT‐A) and anterograde transport (IFT‐B). Here we describe a fetus with an unclassified severe ciliopathy phenotype including short ribs, polydactyly, bilateral renal agenesis, and imperforate anus, with compound heterozygosity for c.118_125del, p.(Thr40Glyfs*11) and a c.352 +1G > T in IFT27, which encodes a small GTPase component of the IFT‐B complex. We conclude that bilateral renal agenesis is a rare feature of this severe ciliopathy and this report highlights the phenotypic overlap of Pallister–Hall syndrome and ciliopathies. The phenotype in patients with IFT27 gene variants is wide ranging from Bardet–Biedl syndrome to a lethal phenotype. [ABSTRACT FROM AUTHOR]

Published

2018

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

Author

Legendre, Marine, Abadie, Véronique, Attié‐Bitach, Tania, Philip, Nicole, Busa, Tiffany, Bonneau, Dominique, Colin, Estelle, Dollfus, Hélène, Lacombe, Didier, Toutain, Annick, Blesson, Sophie, Julia, Sophie, Martin‐Coignard, Dominique, Geneviève, David, Leheup, Bruno, Odent, Sylvie, Jouk, Pierre‐Simon, Mercier, Sandra, Faivre, Laurence, and Vincent‐Delorme, Catherine

Published

2017

20. Fetal Cerebral Ventricular Dilatation: Etiopathogenic Study of 130 Observations.

Author

Darouich, Sihem, Boutaud, Lucile, Bessières, Bettina, Bonnière, Maryse, Martinovic, Jelena, Mechler, Charlotte, Alby, Caroline, Bernard, Jean‐Pierre, Roth, Philippe, Ville, Yves, Malan, Valerie, Vekemans, Michel, Attié‐Bitach, Tania, and Encha‐Razavi, Férechté

Abstract

Background Fetal cerebral ventricular dilatation (CVD) is a common abnormal prenatal finding that often predicts a poor prognosis. The etiology involves both genetic and nongenetic factors with diverse pathogenic mechanisms. We describe the neuropathological features of CVD in a large cohort of fetuses. The goals are to determine the physiopathological mechanisms and etiologies. Methods We retrospectively analyzed a series of 130 fetuses examined at the Necker University Hospital following termination of pregnancy between January 2000 and December 2014. Chiari II and Dandy-Walker malformations were excluded from our study population. Karyotype and/or array comparative genomic hybridization were performed in all cases. Targeted Sanger sequencing or next generation sequencing were carried out in 34 and 5 cases, respectively. Results We distinguished four groups of pathological entities: (1) midbrain/hindbrain patterning defects (54 cases, 42%), mainly related to aqueduct of Sylvius anomalies (atresia or stenosis); (2) cerebral cytoarchitectonic disorders (16 cases, 12%), essentially resulting from arachnoidal neuroglial ectopia; (3) hemorrhagic and perfusion failure (42 cases, 32%); and (4) nonspecific CVD (18 cases, 14%), without apparent obstruction, cortical malformation, or clastic injury. Although the pathogenic mechanisms of CVD were identified in 86% of cases, the causes, both acquired and genetic, were recognized in 21% of cases only. Conclusion The neuropathological analysis is a powerful tool in the diagnosis of the fetal CVD pathogenic mechanisms and to identify homogeneous groups. The paucity of molecular diagnosis, notably in the major groups of midbrain/hindbrain patterning defects and hemorrhagic and perfusion failure, highlights the needs of future research to improve our current knowledge on CVD causes. Birth Defects Research 109:1586-1595, 2017. © 2017 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2017

21. Clinical, genetic and neuropathological findings in a series of 138 fetuses with a corpus callosum malformation.

Author

Alby, Caroline, Malan, Valérie, Boutaud, Lucile, Marangoni, Maria Angela, Bessières, Bettina, Bonniere, Maryse, Ichkou, Amale, Elkhartoufi, Nadia, Bahi‐Buisson, Nadia, Sonigo, Pascale, Millischer, Anne‐Elodie, Thomas, Sophie, Ville, Yves, Vekemans, Michel, Encha‐Razavi, Férechté, and Attié‐Bitach, Tania

Abstract

BACKGROUND Corpus callosum malformation (CCM) is the most frequent brain malformation observed at birth. Because CCM is a highly heterogeneous condition, the prognosis of fetuses diagnosed prenatally remains uncertain, making prenatal counseling difficult. METHODS AND RESULTS We evaluated retrospectively a total of 138 fetuses, 117 with CCM observed on prenatal imaging examination, and 21 after postmortem autopsy. On ultrasound and/or magnetic resonance imaging, CCM was either isolated ( N = 40) or associated with other neurological ( N = 57) or extra cerebral findings ( N = 21/20, respectively). RESULTS Most fetuses ( N = 132) remained without a diagnosis at the time of pregnancy termination. This emphasizes the need to establish a neuropathological classification and to perform a genomic screening using comparative genomic hybridization. A neuropathological examination performed on 138 cases revealed a spectrum of CCMs, classified as follows: agenesis of corpus callosum (55), CC hypoplasia (30), CC dysmorphism (24), and CCM associated with a malformation of cortical development (29). Of interest, after fetopathological examination, only 16/40 malformations were classified as isolated, highlighting the importance of the autopsy following termination of pregnancy. Among the 138 cases, the underlying etiology was found in 46 cases: diabetes (one case), cytomegalovirus infection (one case), 23 chromosome abnormalities, and 21 mendelian conditions. CONCLUSION In our series of 138 cases of CCM, prenatal and postmortem examinations identified a variety of genetic causes. However, no diagnosis could be established in 67% of cases. The classification based on the underlying neurodevelopmental defects paves the way for further genetic studies and genotype-phenotype correlations. Birth Defects Research (Part A) 106:36-46, 2016. © 2015 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2016

22. Phenotypic spectrum of STRA6 mutations: from Matthew-Wood syndrome to non-lethal anophthalmia.

Author

Chassaing, Nicolas, Golzio, Christelle, Odent, Sylvie, Lequeux, Léopoldine, Vigouroux, Adeline, Martinovic-Bouriel, Jelena, Tiziano, Francesco Danilo, Masini, Lucia, Piro, Francesca, Maragliano, Giovanna, Delezoide, Anne-Lise, Attié-Bitach, Tania, Manouvrier-Hanu, Sylvie, Etchevers, Heather C., and Calvas, Patrick

Abstract

Matthew-Wood, Spear, PDAC or MCOPS9 syndrome are alternative names used to refer to combinations of microphthalmia/anophthalmia, malformative cardiac defects, pulmonary dysgenesis, and diaphragmatic hernia. Recently, mutations in STRA6, encoding a membrane receptor for vitamin A-bearing plasma retinol binding protein, have been identified in such patients. We performed STRA6 molecular analysis in three fetuses and one child diagnosed with Matthew-Wood syndrome and in three siblings where two adult living brothers are affected with combinations of clinical anophthalmia, tetralogy of Fallot, and mental retardation. Among these patients, six novel mutations were identified, bringing the current total of known STRA6 mutations to seventeen. We extensively reviewed clinical data pertaining to all twenty-one reported patients with STRA6 mutations (the seven of this report and fourteen described elsewhere) and discuss additional features that may be part of the syndrome. The clinical spectrum associated with STRA6 deficiency is even more variable than initially described. © 2009 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published

2009

23. Hydrothorax in fetal cases of Opitz G/BBB diagnosis: Extending the phenotype?

Author

Tessier, Aude, Boutaud, Lucile, Bruel, Ange‐Line, Thauvin‐Robinet, Christel, Roth, Philippe, Malan, Valérie, Beaujard, Marie‐Paule, Achaiaa, Amale, Oliveira, Judite, Steffann, Julie, Encha‐Razavi, Ferechte, Faivre, Laurence, Bessières, Bettina, and Attié‐Bitach, Tania

Subjects

HYDROTHORAX, HYDROPS fetalis, BLOOD-brain barrier, DIAGNOSIS, PHENOTYPES, GRAY matter (Nerve tissue)

Abstract

We report two fetal cases carrying a de novo I MID1 i mutation and presenting with severe hydrothorax, suggesting the expansion of the phenotype of Opitz GBBB syndrome GLO:8DU/01dec20:cge13840-toc-0001.jpg PHOTO (COLOR): . gl DATA AVAILABILITY STATEMENT No shared research data. Additionally, autopsy revealed hypertelorism, large forehead, wide nasal bridge, lower set ears, large anterior fontanelle, hypospadias, vermis hypoplasia and enlarged forth ventricle (see Figure 1). 2 Patton MA, Baraitser M, Nickolaides K, Rodeck CH, Gamsu H. Prenatal treatment of fetal hydrops associated with the hypertelorism-dysphagia syndrome (opitz-g syndrome). [Extracted from the article]

Published

2020

24. Cytogenetic and histological features of a human embryo with homogeneous chromosome 8 trisomy.

Author

Golzio, Christelle, Guirchoun, Jessica, Ozilou, Catherine, Thomas, Sophie, Goudefroye, Géraldine, Morichon-Delvallez, Nicole, Vekemans, Michel, Attié-Bitach, Tania, and Etchevers, Heather C.

Abstract

Background Homogeneous and complete trisomy 8 is extremely rare. With one recent neonatal exception, all reported cases have been mosaic, due to mitotic non-disjunction during early zygotic development. We report a case of chromosome 8 trisomy in a human embryo examined at Carnegie stage 11 (25 days post-fertilization). It presented severe cardiovascular and central nervous system malformations. Methods The unusual bifid heart in this embryo spurred a detailed histological examination, karyotyping of a chorionic villus sample and subsequent FISH on inter-phase nuclei of intra-embryonic sections. Results Trophoblast cells had a karyotype of 47,XX, +8. Within the embryo proper, FISH demonstrated that the trisomy 8 was homogeneous in embryonic as well as extra-embryonic tissues. FQ-PCR supports a meiosis I origin of non-disjunction. In sections, the pharyngeal arches (including cardiac outflow tract), forebrain, mesonephros and liver were absent. Somites and yolk sac blood vessels were irregularly shaped. Conclusion We show that homogeneous, intra-embryonic trisomy 8 is compatible with implantation and early human development. Molecular pathways that may be compromised and their impact on organogenesis are discussed. Copyright © 2006 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2006

25. Fatty acid oxidation in the human fetus: Implications for fetal and adult disease.

Author

Oey, Nadia, Ruiter, Jos, Attié-Bitach, Tania, IJlst, Lodewijk, Wanders, Ronald, and Wijburg, Frits

Abstract

Studies in the last few years have shown a remarkably high activity of fatty acid oxidation (FAO) enzymes in human placenta. We have recently shown mRNA expression as well as enzymatic activity of long-chain FAO enzymes in the human embryo and fetus. In this study we show activity of the FAO enzymes carnitine palmitoyltranferase 1, medium-chain acyl-CoA dehydrogenase and short-chain hydroxyacyl-CoA dehydrogenase in embryonic and fetal tissues. In addition, we show the presence of different acylcarnitines in fetal liver and kidney, which substantiates the notion that the mitochondrial FAO enzymes are not only present in human fetal tissues but also metabolically active. In a glucose-rich environment FAO might be necessary for additional ATP production from fatty acids, but also for the breakdown of fatty acids that are products of the turnover of membranes in the growing fetus. The importance of FAO in the human embryo and fetus is further stressed by the fact that a higher frequency of prematurity, intrauterine growth retardation, fetal morbidity and intrauterine death is noted in long-chain FAO defects. Furthermore, in animal studies, gestational loss during early embryonic development has been observed as a consequence of disturbed FAO. Finally, there are indications that regulation of activity of FAO during fetal development might not only be important for fetal life but may also have implications for health and disease in adulthood. [ABSTRACT FROM AUTHOR]

Published

2006

26. Molecular screening of the ZFHX1B gene in prenatally diagnosed isolated agenesis of the corpus callosum.

Author

Espinosa-Parrilla, Yolanda, Encha-Razavi, Férechté, Attié-Bitach, Tania, Martinovic, Jelena, Morichon-Delvallez, Nicole, Munnich, Arnold, Vekemans, Michel, Lyonnet, Stanislas, and Amiel, Jeanne

Abstract

Objective Agenesis of the corpus callosum (ACC) is the most common malformation of the central nervous system and may be associated with mental retardation. ACC is found in 40% of the cases of Mowat-Wilson syndrome (MWS), a polytopic embryonic defect including a distinctive facial gestalt, severe mental retardation, epilepsy and postnatal microcephaly as constant features. Other manifestations involve Hirschsprung disease, cardiac defects, renal abnormalities and hypospadias. Among this broad spectrum of malformations recently associated with haploinsufficiency of the zinc finger homeobox 1B gene ( ZFHX1B), ACC can therefore be the only feature to be detected prenatally. Thus, we studied a group of 18 fetuses terminated for ACC and performed mutational analysis of the ZFHX1B gene in six selected cases. Methods Diagnosis of agenesis of the ACC was performed by prenatal echography survey. Screening for ZFHX1B deletions was performed by poly (CA) microsatellite markers studies and real-time semi-quantitative PCR. Mutational analysis was performed by single-strand conformation polymorphisms analysis (SSCP). Results Neither deletion encompassing the ZFHX1B locus nor mutation could be detected in any of the six fetuses analysed. Conclusion ZFHX1B is not a major gene in isolated ACC. However, analysis of MWS should be considered in the differential diagnosis of ACC, especially when the facial features raise the possibility of MWS. Copyright © 2004 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2004

27. Prenatal diagnosis of carnitine palmitoyltransferase 2 deficiency in chorionic villi: a novel approach.

Author

Vekemans, Bernadette Chadefaux, Bonnefont, Jean-Paul, Aupetit, Joëlle, Royer, Ghislaine, Droin, Véronique, Attié-Bitach, Tania, Saudubray, Jean-Marie, and Thuillier, Laure

Abstract

Carnitine palmitoyltransferase 2 (CPT2) deficiency, the most common autosomal recessive inherited disease of the mitochondrial long-chain fatty acid (LCFA) β-oxidation, may result in three distinct clinical phenotypes, namely, a mild adult muscular form, a severe infantile hepatocardiomuscular disease, and a neonatal form, which includes dysmorphic features in addition to hepatocardiomuscular symptoms. Both the latter forms are life-threatening diseases, and prenatal diagnosis (PND) can be offered to couples at a one-fourth risk of having an affected child. PND of CPT2 deficiency hitherto relied mostly on mutation detection from fresh chorionic villi (10 weeks' gestation), since CPT2 activity could be assayed on cultured amniocytes only (16-17 weeks' gestation). We devised a CPT2 activity assay from 10 mg of chorionic villi sampling (CVS). Combining this enzymatic assay to haplotype study using polymorphic markers linked to the CPT2 gene, we were able to carry out within 2 days, CPT2 deficiency PND, in two unrelated families, using a CVS performed at the 11th week of gestation. Copyright © 2003 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2003

28. Cerebral dysgenesis does not exclude OFD I syndrome.

Author

Thauvin-Robinet, Christel, Lesca, Gaëtan, Aral, Bernard, Gigot, Nadège, Lambert, Sandy, Gueneau, Lucie, Macca, Marina, Franco, Brunella, Huet, Frédéric, Zabot, Marie-Thérèse, Attié-Bitach, Tania, Attia-Sobol, Jocelyne, and Faivre, Laurence

Published

2011

29. Novel de novo ZBTB20 mutations in three cases with Primrose syndrome and constant corpus callosum anomalies.

Author

Alby C, Boutaud L, Bessières B, Serre V, Rio M, Cormier-Daire V, de Oliveira J, Ichkou A, Mouthon L, Gordon CT, Bonnière M, Mechler C, Nitschke P, Bole C, Lyonnet S, Bahi-Buisson N, Boddaert N, Colleaux L, Roth P, Ville Y, Vekemans M, Encha-Razavi F, Attié-Bitach T, and Thomas S

Subjects

Adolescent, Amino Acid Sequence, Brain abnormalities, Brain diagnostic imaging, Child, Female, High-Throughput Nucleotide Sequencing, Humans, Infant, Newborn, Male, Nerve Tissue Proteins chemistry, Nucleic Acid Conformation, Pedigree, Phenotype, Protein Conformation, Reproducibility of Results, Sequence Analysis, DNA, Transcription Factors chemistry, Abnormalities, Multiple diagnosis, Abnormalities, Multiple genetics, Agenesis of Corpus Callosum diagnosis, Agenesis of Corpus Callosum genetics, Calcinosis diagnosis, Calcinosis genetics, Ear Diseases diagnosis, Ear Diseases genetics, Intellectual Disability diagnosis, Intellectual Disability genetics, Muscular Atrophy diagnosis, Muscular Atrophy genetics, Mutation, Nerve Tissue Proteins genetics, Transcription Factors genetics

Abstract

Corpus callosum (CC) is the major brain commissure connecting homologous areas of cerebral hemispheres. CC anomalies (CCAs) are the most frequent brain anomalies leading to variable neurodevelopmental outcomes making genetic counseling difficult in the absence of a known etiology that might inform the prognosis. Here, we used whole exome sequencing, and a targeted capture panel of syndromic CCA known causal and candidate genes to screen a cohort of 64 fetuses with CCA observed upon autopsy, and 34 children with CCA and intellectual disability. In one fetus and two patients, we identified three novel de novo mutations in ZBTB20, which was previously shown to be causal in Primrose syndrome. In addition to CCA, all cases presented with additional features of Primrose syndrome including facial dysmorphism and macrocephaly or megalencephaly. All three variations occurred within two out of the five zinc finger domains of the transcriptional repressor ZBTB20. Through homology modeling, these variants are predicted to result in local destabilization of each zinc finger domain suggesting subsequent abnormal repression of ZBTB20 target genes. Neurohistopathological analysis of the fetal case showed abnormal regionalization of the hippocampal formation as well as a reduced density of cortical upper layers where originate most callosal projections. Here, we report novel de novo ZBTB20 mutations in three independent cases with characteristic features of Primrose syndrome including constant CCA. Neurohistopathological findings in fetal case corroborate the observed key role of ZBTB20 during hippocampal and neocortical development. Finally, this study highlights the crucial role of ZBTB20 in CC development in human., (© 2018 Wiley Periodicals, Inc.)

Published

2018

30. PAX2 mutations in fetal renal hypodysplasia.

Author

Martinovic-Bouriel J, Benachi A, Bonnière M, Brahimi N, Esculpavit C, Morichon N, Vekemans M, Antignac C, Salomon R, Encha-Razavi F, Attié-Bitach T, and Gubler MC

Subjects

Adolescent, Adult, DNA Mutational Analysis, Eye pathology, Eye Abnormalities genetics, Eye Abnormalities pathology, Female, Humans, Kidney pathology, Pregnancy, Fetus abnormalities, Kidney abnormalities, Kidney Diseases genetics, Kidney Diseases pathology, Mutation genetics, PAX2 Transcription Factor genetics

Abstract

Papillorenal syndrome also known as renal-coloboma syndrome (OMIM 120330) is an autosomal dominant condition comprising optic nerve anomaly and renal oligomeganephronic hypoplasia. This reduced number of nephron generations with compensatory glomerular hypertrophy leads towards chronic insufficiency with renal failure. We report on two fetuses with PAX2 mutations presenting at 24 and 18 weeks' gestation, respectively, born into two different sibships. In our first patient, termination of pregnancy was elected for anhydramnios and suspicion of renal agenesis in the healthy couple with an unremarkable previous clinical history. This fetus had bilateral asymmetric kidney anomalies including a small multicystic left kidney, and an extremely hypoplastic right kidney. Histology showed dysplastic lesions in the left kidney, contrasting with rather normal organization in the hypoplastic right kidney. Ocular examination disclosed bilateral optic nerve coloboma. The association of these anomalies, highly suggestive of the papillorenal syndrome, led us to perform the molecular study of the PAX2 gene. Direct sequencing of the PAX2 coding sequence identified a de novo single G deletion of nucleotide 935 in exon 3 of the PAX2 resulting in a frameshift mutation (c.392delG, p.Ser131Thrfs*28). In the second family, the presence of a maternally inherited PAX2 mutation led to a decision for termination of pregnancy. The 18-week gestation fetus presented the papillorenal syndrome including hypoplastic kidneys and optic nerve coloboma. In order to address the PAX2 involvement in isolated renal "disease," 18 fetuses fulfilling criteria were screened: 10/18 had uni- or bilateral agenesis, 6/18 had bilateral multicystic dysplasia with enlarged kidneys, and 2/18 presented bilateral severe hypodysplasia confirmed on fetopathological examination. To the best of our knowledge, our first patient represents an unreported fetal diagnosis of papillorenal syndrome, and another example of the impact of oriented fetopathological examination in genetic counseling of the parents., ((c) 2010 Wiley-Liss, Inc.)

Published

2010

31. De novo trisomy 20p of paternal origin.

Author

Chaabouni M, Turleau C, Karboul L, Jemaa LB, Maazoul F, Attié-Bitach T, Romana S, and Chaabouni H

Subjects

Child, Preschool, Chromosome Banding, Facial Asymmetry genetics, Fingers abnormalities, Humans, In Situ Hybridization, Fluorescence, Male, Polydactyly genetics, Chromosomes, Human, Pair 20, Fathers, Trisomy genetics

Abstract

We report on a case of a de novo trisomy 20p in a 5-year-old boy. The patient presented with dysmorphic features, mental retardation, poor coordination, cardiac malformation, kyphosis, hypospadias, cryptorchidism, and preaxial hexadactyly. No growth delay was noticed. Standard karyotype and FISH techniques allowed the characterization of the chromosome rearrangement showing a duplication spanning almost the whole short arm of chromosome 20. Therefore the karyotype was interpreted as 46,XY,der(20)(pter --> q13.3::p11.2 --> pter). Molecular studies identified the duplication of paternal origin. This is one of the rare reports with almost pure trisomy 20p characterized at the molecular level. Its phenotype is compared to other similar cases described in the literature.

Published

2007

32. Matthew-Wood syndrome: report of two new cases supporting autosomal recessive inheritance and exclusion of FGF10 and FGFR2.

Author

Martinovic-Bouriel J, Bernabé-Dupont C, Golzio C, Grattagliano-Bessières B, Malan V, Bonnière M, Esculpavit C, Fallet-Bianco C, Mirlesse V, Le Bidois J, Aubry MC, Vekemans M, Morichon N, Etchevers H, Attié-Bitach T, Encha-Razavi F, and Benachi A

Subjects

Abnormalities, Multiple diagnosis, Abnormalities, Multiple pathology, Adult, Anophthalmos diagnosis, Chromosome Disorders diagnosis, Chromosome Disorders pathology, Female, Genes, Recessive, Humans, Male, Microphthalmos diagnosis, Pregnancy, Prenatal Diagnosis, Syndrome, Abnormalities, Multiple genetics, Anophthalmos genetics, Fibroblast Growth Factor 10 genetics, Lung abnormalities, Microphthalmos genetics, Receptor, Fibroblast Growth Factor, Type 2 genetics

Abstract

We describe two fetal cases of microphthalmia/anophthalmia, pulmonary agenesis, and diaphragmatic defect. This rare association is known as Matthew-Wood syndrome (MWS; MIM 601186) or by the acronym "PMD" (Pulmonary agenesis, Microphthalmia, Diaphragmatic defect). Fewer than ten pre- and perinatal diagnoses of Matthew-Wood syndrome have been described to date. The cause is unknown, and the mode of transmission remains unclear. Most cases have been reported as isolated and sporadic, although recurrence among sibs has been observed once. Our two cases both occurred in consanguineous families, further supporting autosomal recessive transmission. In addition, in one family at least one of the elder sibs presented an evocatively similar phenotype. The spatiotemporal expression pattern of the FGF10 and FGFR2 genes in human embryos and the reported phenotypes of knockout mice for these genes spurred us to examine their coding sequences in our two cases of MWS. While in our patients, no causative sequence variations were identified in FGF10 or FGFR2, this cognate ligand-receptor pair and its downstream effectors remain functional candidates for MWS and similar associations of congenital ocular, diaphragmatic and pulmonary malformations., ((c) 2007 Wiley-Liss, Inc.)

Published

2007