Your search keyword '"Des Portes, V."' showing total 19 results

1. Whole-exome sequencing improves the diagnosis yield in sporadic infantile spasm syndrome.

Author

Dimassi, S., Labalme, A., Ville, D., Calender, A., Mignot, C., Boutry‐Kryza, N., de Bellescize, J., Rivier‐Ringenbach, C., Bourel‐Ponchel, E., Cheillan, D., Simonet, T., Maincent, K., Rossi, M., Till, M., Mougou‐Zerelli, S., Edery, P., Saad, A., Heron, D., des Portes, V., and Sanlaville, D.

Subjects

EXOMES, INFANTILE spasms, CHILDHOOD epilepsy, INFANT diseases, INTELLECTUAL disabilities

Abstract

Infantile spasms syndrome ( ISs) is characterized by clinical spasms with ictal electrodecrement, usually occurring before the age of 1 year and frequently associated with cognitive impairment. Etiology is widely heterogeneous, the cause remaining elusive in 40% of patients. We searched for de novo mutations in 10 probands with ISs and their parents using whole-exome sequencing ( WES). Patients had neither consanguinity nor family history of epilepsy. Common causes of ISs were excluded by brain magnetic resonance imaging ( MRI), metabolic screening, array-comparative genomic hybridization ( CGH) and testing for mutations in CDKL5, STXBP1, and for ARX duplications. We found a probably pathogenic mutation in four patients. Missense mutations in SCN2A (p. Leu1342Pro) and KCNQ2 (p. Ala306Thr) were found in two patients with no history of epilepsy before the onset of ISs. The p. Asn107Ser missense mutation of ALG13 had been previously reported in four females with ISs. The fourth mutation was an in-frame deletion (p.Phe110del) in NR2F1, a gene whose mutations cause intellectual disability, epilepsy, and optic atrophy. In addition, we found a possibly pathogenic variant in KIF3C that encodes a kinesin expressed during neural development. Our results confirm that WES improves significantly the diagnosis yield in patients with sporadic ISs. [ABSTRACT FROM AUTHOR]

Published

2016

2. Distortion of the anterior part of the interhemispheric fissure: significance and implications for prenatal diagnosis.

Author

Vinurel, N., Van Nieuwenhuyse, A., Cagneaux, M., Garel, C., Quarello, E., Brasseur, M., Picone, O., Ferry, M., Gaucherand, P., des Portes, V., and Guibaud, L.

Subjects

PRENATAL diagnosis, CEREBRAL sulci, CHROMOSOME abnormalities, NEURAL tube defects, MAGNETIC resonance imaging

Abstract

ABSTRACT In order to illustrate the significance of a new anatomical finding, distortion of the interhemispheric fissure ( DIHF) associated with impacted medial borders of the frontal lobes, we report a retrospective observational study of 13 fetuses in which DIHF was identified on prenatal imaging. In 10 cases there were associated anatomical anomalies, including mainly midline anomalies (syntelencephaly (n = 2), lobar holoprosencephaly (n = 1), Aicardi syndrome (n = 2)), but also schizencephaly (n = 1), cortical dysplasia (n = 1) and more complex cerebral malformations (n = 3), including neural tube defect in two cases. Chromosomal anomaly was identified in two cases, including 6p deletion in a case without associated central nervous system anomalies and a complex mosaicism in one of the cases with syntelencephaly. In two cases, the finding was apparently isolated on both pre- and postnatal imaging, and the children were doing well at follow-up, aged 4 and 5 years. The presence of DIHF on prenatal imaging may help in the diagnosis of cerebral anomalies, especially those involving the midline. If DIHF is apparently isolated on prenatal ultrasound, magnetic resonance imaging is recommended for careful analysis of gyration and midline, especially optic and olfactory structures. Karyotyping is also recommended. Copyright © 2013 ISUOG. Published by John Wiley & Sons Ltd [ABSTRACT FROM AUTHOR]

Published

2014

3. Implicit procedural learning in fragile X and Down syndrome.

Author

Bussy, G., Charrin, E., Brun, A., Curie, A., and des Portes, V.

Subjects

ANALYSIS of variance, COGNITION, FRAGILE X syndrome, GENETICS, LEARNING, MEMORY, REACTION time, RESEARCH funding, STATISTICS, DATA analysis, DOWN syndrome, CASE-control method

Abstract

Procedural learning refers to rule-based motor skill learning and storage. It involves the cerebellum, striatum and motor areas of the frontal lobe network. Fragile X syndrome, which has been linked with anatomical abnormalities within the striatum, may result in implicit procedural learning deficit. To address this issue, a serial reaction time (RT) task including six blocks of trials was performed by 14 individuals with fragile X syndrome, 12 individuals with Down syndrome and 12 mental age-matched control subjects. The first (B1) and fifth (B5) blocks were random whereas the others (B2, B3, B4 and B6) consisted of a repeated 10-step sequence. Results were analysed by Kruskal-Wallis one-way analysis of variance and Wilcoxon signed-rank test. For patients with fragile X syndrome, the RT was highly suggestive of preserved implicit learning as a significant difference was observed between blocks B5 and B6 ( P = 0.009). However, the difference of RT between B4 and B5 did not reach significance, possibly due to a subgroup of individuals who did not learn. In contrast, in the Down syndrome group, RT decreased significantly between B4 and B5 (W = 2; P = 0.003) but not between the last ordered block (B6) and the last random block (B5), suggesting a weakness in procedural learning which was sensitive to the interfering random block. implicit learning is variable in genetic syndromes and therefore relatively independent of general intellectual capacities. The results are discussed together with previous reports. [ABSTRACT FROM AUTHOR]

Published

2011

4. The Renpenning syndrome spectrum: new clinical insights supported by 13 new PQBP1-mutated males.

Author

Germanaud, D., Rossi, M., Bussy, G., Gérard, D., Hertz-Pannier, L., Blanchet, P., Dollfus, H., Giuliano, F., Bennouna-Greene, V., Sarda, P., Sigaudy, S., Curie, A., Vincent, M. C., Touraine, R., and des Portes, V.

Subjects

MICROCEPHALY, GLUTAMINE, PHENOTYPES, MUSCULAR atrophy, ANKYLOSIS, FACIAL abnormalities, X-linked intellectual disabilities, GENETICS

Abstract

D Germanaud, M Rossi, G Bussy, D Gérard, L Hertz-Pannier, P Blanchet, H Dollfus, F Giuliano, V Bennouna-Greene, P Sarda, S Sigaudy, A Curie, MC Vincent, R Touraine, V des Portes. The Renpenning syndrome spectrum: new clinical insights supported by 13 new PQBP1-mutated males. Since the first reports of polyglutamine-binding protein 1 ( PQBP1) mutations in Renpenning syndrome and related disorders, the spectrum of PQBP1-linked clinical manifestations has been outlined from rare published case reports. The phenotypic description is often obtained from medical archives, and therefore, heterogeneous. Moreover, some aspects such as brain imaging or cognitive and behavioral functioning are rarely described. In this study, 13 PQBP1-mutated French patients were subjected to a standardized clinical, cognitive and behavioral assessment. Physical measurements of their relatives were also collected. We report on a recognizable clinical and radiological phenotype. All patients presented with microcephaly, leanness and mild short stature, relative to familial measurements. Three new clinical features are described: upper back progressive muscular atrophy, metacarpophalangeal ankylosis of the thumb and velar dysfunction. The specific facial dysmorphic features included at least four of the following signs: long triangular face, large ridged nose, half-depilated eyebrows, dysplastic or protruding ears and rough slightly sparse hair. An over-aged appearance was noticed in elderly patients. Cortical gyrification was normal based on available magnetic brain imaging of six patients. PQBP1-linked microcephaly (or Renpenning syndrome) is an X-linked mental retardation syndrome, which has clinically recognizable features. [ABSTRACT FROM AUTHOR]

Published

2011

5. Abnormal Sylvian fissure on prenatal cerebral imaging: significance and correlation with neuropathological and postnatal data.

Author

Guibaud, L., Selleret, L., Larroche, J. C., Buenerd, A., Alias, F., Gaucherand, P., Des Portes, V., and Pracros, J.-P.

Subjects

FETAL abnormalities, BRAIN, MEDICAL imaging systems, NEUROLOGICAL disorders, DYSPLASIA

Abstract

The article examines fetuses at 24-34 weeks in which prenatal Sylvian fissure development was identified on prenatal cerebral imaging. The imaging data were correlated to macro- and microscopic neuropathological data or to postnatal clinical and imaging findings. According to the authors, abnormal operculization does not systematically reflect underlying cortical dysplasia and it may be related to extracorticol factors such as abnormal cerebral volume.

Published

2008

6. Plea for an anatomical approach to abnormalities of the posterior fossa in prenatal diagnosis.

Author

Guibaud, L., des Portest, V., and des Portes, V

Subjects

MEDICAL imaging systems, PRENATAL diagnosis

Abstract

The article discusses several reports published within the issue, including one on the use of two- and three-dimensional ultrasound for anatomical approach to fetal posterior fossa and another on the classification of abnormalities which include agenesis, hypoplasia and atrophy.

Published

2006

7. Prenatal cerebral ultrasound and MRI findings in glutaric aciduria Type 1: a de novo case.

Author

Mellerio, C., Marignier, S., Roth, P., Gaucherand, P., Des Portes, V., Pracros, J. P., and Guibaud, L.

Subjects

LETTERS to the editor, BRAIN diseases

Abstract

A letter to the editor is presented citing the authors' prenatal cerebral ultrasound and magnetic resonance imaging (MRI) findings from a de novo case of glutaric aciduria Type 1.

Published

2008

8. Extracerebellar ectopic brain tissue in the posterior fossa.

Author

Guibaud, L., Devonec, S., Des Portes, V., Roth, P., Gaucherand, P., and Pracros, J.-P.

Subjects

WOMEN patients, ECTOPIC pregnancy, PREGNANCY complications, RARE diseases

Abstract

This article presents the case study of a 27-year old woman at 28 weeks' gestation with the diagnosis of a round mass in the fetal posterior fossa. Tests found were highly suggestive of heterotropic or ectopic brain tissue. Surgical resection was not performed due to the atypicality of the case. The pathogenesis of this rare developmental disease is offered.

Published

2005

9. OP14.07: Outcomes of fetuses with small cerebellum on second and third trimester ultrasonography.

Author

Atallah, A., Guibaud, L., Duchemin, G., des Portes, V., and Massoud, M.

Subjects

FETAL ultrasonic imaging, NEONATAL diseases, PRENATAL care

Published

2017

10. Prenatal diagnosis of cerebellar cortical dysplasia associated with abnormalities of foliation.

Author

Massoud, M., Clerc, J., Cagneux, M., Vasiljevic, A., Massardier, J., Doret, M., Gaucherand, P., Des Portes, V., and Guibaud, L.

Subjects

PRENATAL diagnosis, DIAGNOSTIC ultrasonic imaging, MAGNETIC resonance imaging, FETAL abnormalities, THIRD trimester of pregnancy, PHOTOGRAPHS

Abstract

Several photographs showing the results of a prenatal diagnosis using ultrasound and magnetic resonance imaging (MRI) of cerebellar cortical dysplasia associated with abnormalities of foliation during the third trimester, are presented.

Published

2012

11. 'Absence of T378N mutation of ATP1A2 gene in five patients with alternating hemiplegia of childhood'.

Author

Boileau S, Vuillaume I, Sablonnière B, Marignier S, Des Portes V, Vallée L, and Auvin S

Published

2008

12. OP07.03: 'Isolated' Dandy-Walker malformation on prenatal imaging: Look for subtelomeric deletion and post-natal hydrocephalus.

Author

Guibaud, L., des Portes, V., Ville, D., and Gaucherand, P.

Subjects

*PRENATAL diagnosis, ABSTRACTS

Abstract

An abstract of the conference paper "Isolated' Dandy-Walker malformation on prenatal imaging: Look for subtelomeric deletion and post-natal hydrocephalus" by L. Guibaud and colleagues is presented.

Published

2009

13. OC10.04: Distortion of the anterior part of the interhemispheric fissure. Significance and impact on prenatal diagnosis.

Author

Guibaud, L., Quarello, E., Ferry, M., Picone, O., des Portes, V., and Gaucherand, P.

Subjects

ABSTRACTS, PRENATAL diagnosis

Abstract

An abstract of the conference paper "Distortion of the anterior part of the interhemispheric fissure. Significance and impact on prenatal diagnosis" by L. Guibaud and colleagues is presented.

Published

2009

14. Further delineation of the clinical spectrum of de novo TRIM8 truncating mutations.

Author

Assoum M, Lines MA, Elpeleg O, Darmency V, Whiting S, Edvardson S, Devinsky O, Heinzen E, Hernan RR, Antignac C, Deleuze JF, Des Portes V, Bertholet-Thomas A, Belot A, Geller E, Lemesle M, Duffourd Y, Thauvin-Robinet C, Thevenon J, Chung W, Lowenstein DH, and Faivre L

Subjects

Adolescent, Amino Acid Sequence, Carrier Proteins chemistry, Child, Child, Preschool, Female, Humans, Infant, Infant, Newborn, Male, Nerve Tissue Proteins chemistry, Carrier Proteins genetics, Mutation genetics, Nerve Tissue Proteins genetics

Abstract

De novo mutations of the TRIM8 gene, which codes for a tripartite motif protein, have been identified using whole exome sequencing (WES) in two patients with epileptic encephalopathy (EE), but these reports were not sufficient to conclude that TRIM8 was a novel gene responsible for EE. Here we report four additional patients presenting with EE and de novo truncating mutations of TRIM8 detected by WES, and give further details of the patient previously reported by the Epi4K consortium. Epilepsy of variable severity was diagnosed in children aged 2 months to 3.5 years of age. All patients had developmental delay of variable severity with no or very limited language, often associated with behavioral anomalies and unspecific facial features or MRI brain abnormalities. The phenotypic variability observed in these patients appeared related to the severity of the epilepsy. One patient presented pharmacoresistant EE with regression, recurrent infections and nephrotic syndrome, compatible with the brain and kidney expression of TRIM8. Interestingly, all mutations were located at the highly conserved C-terminus section of TRIM8. This collaborative study confirms that TRIM8 is a novel gene responsible for EE, possibly associated with nephrotic syndrome. This report brings new evidence on the pathogenicity of TRIM8 mutations and highlights the value of data-sharing to delineate the phenotypic characteristics and biological basis of extremely rare disorders., (© 2018 Wiley Periodicals, Inc.)

Published

2018

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

Author

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

Subjects

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

Abstract

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

Published

2016

16. Complex mosaic CDKL5 deletion with two distinct mutant alleles in a 4-year-old girl.

Author

Boutry-Kryza N, Ville D, Labalme A, Calender A, Dupont JM, Touraine R, Edery P, des Portes V, Sanlaville D, and Lesca G

Subjects

Child, Preschool, Chromosome Breakpoints, Comparative Genomic Hybridization, DNA Mutational Analysis, Exons, Female, Gene Duplication, Genetic Association Studies, Humans, Infant, Infant, Newborn, Rett Syndrome diagnosis, Rett Syndrome genetics, Spasms, Infantile diagnosis, Spasms, Infantile genetics, X Chromosome Inactivation, Alleles, Gene Deletion, Mosaicism, Mutation, Protein Serine-Threonine Kinases genetics

Abstract

Mutations of the CDKL5 gene cause early epileptic encephalopathy. Patients manifest refractory epilepsy, beginning before the age of 3 months, which is associated with severe psychomotor delay and features that overlap with Rett syndrome. We report here a patient with mosaicism for CDKL5 exonic deletion, with the presence of two mutant alleles. The affected 4-year-old girl presented with infantile spasms, beginning at the age of 9 months, but subsequent progression of the disease was consistent with the classical CDKL5-related phenotype. A deletion of exons 17 and 18 was suspected on the basis of Multiplex Ligation Probe Amplification analysis, but unexpected results for cDNA analysis, which showed the presence of an abnormal transcript with the deletion of exon 18 only, led us to suspect that two distinct events might have occurred. We used custom array-CGH to determine the size and breakpoints of these deletions. Exon 18 was deleted from one of the abnormal alleles, and exon 17 was deleted from the other. A Fork Stalling and Template Switching (FoSTeS) mechanism was proposed to explain the two events, given the presence of regions of microhomology at the breakpoints. We propose here an original involvement of the FoSTeS mechanism to explain the co-occurrence of these two events in the CDKL5 gene in a single patient. This patient highlights the difficulties involved in the detection of such abnormalities, particularly when they occur in a mosaic state and involve two distinct mutational events in a single gene., (© 2014 Wiley Periodicals, Inc.)

Published

2014

17. Clinical and neurocognitive characterization of a family with a novel MED12 gene frameshift mutation.

Author

Lesca G, Moizard MP, Bussy G, Boggio D, Hu H, Haas SA, Ropers HH, Kalscheuer VM, Des Portes V, Labalme A, Sanlaville D, Edery P, Raynaud M, and Lespinasse J

Subjects

14-3-3 Proteins genetics, Abnormalities, Multiple physiopathology, Adult, Aged, Agenesis of Corpus Callosum physiopathology, Anus, Imperforate physiopathology, Blepharophimosis physiopathology, Blepharoptosis physiopathology, Chromosomes, Human, X genetics, Constipation physiopathology, Exons, Female, Frameshift Mutation, Heart Defects, Congenital physiopathology, Humans, Intellectual Disability physiopathology, Male, Mental Retardation, X-Linked physiopathology, Middle Aged, Muscle Hypotonia genetics, Muscle Hypotonia physiopathology, Mutation, X Chromosome Inactivation genetics, Abnormalities, Multiple genetics, Agenesis of Corpus Callosum genetics, Anus, Imperforate genetics, Blepharophimosis genetics, Blepharoptosis genetics, Constipation genetics, Genetic Diseases, X-Linked, Heart Defects, Congenital genetics, Intellectual Disability genetics, Mediator Complex genetics, Mental Retardation, X-Linked genetics, Muscle Hypotonia congenital

Abstract

FG syndrome, Lujan syndrome, and Ohdo syndrome, the Maat-Kievit-Brunner type, have been described as distinct syndromes with overlapping non-specific features and different missense mutations of the MED12 gene have been reported in all of them. We report a family including 10 males and 1 female affected with profound non-specific intellectual disability (ID) which was linked to a 30-cM region extending from Xp11.21 (ALAS2) to Xq22.3 (COL4A5). Parallel sequencing of all X-chromosome exons identified a frameshift mutation (c.5898dupC) of MED12. Mutated mRNA was not affected by non-sense mediated RNA decay and induced an additional abnormal isoform due to activation of cryptic splice-sites in exon 41. Dysmorphic features common to most affected males were long narrow face, high forehead, flat malar area, high nasal bridge, and short philtrum. Language was absent or very limited. Most patients had a friendly personality. Cognitive impairment, varying from borderline to profound ID was similarly observed in seven heterozygous females. There was no correlation between cognitive function and X-chromosome inactivation profiles in blood cells. The severe degree of ID in male patients, as well as variable cognitive impairment in heterozygous females suggests that the duplication observed in the present family may have a more severe effect on MED12 function than missense mutations. In a cognitively impaired male from this family, who also presented with tall stature and dysmorphism and did not have the MED12 mutation, a 600-kb duplication at 17p13.3 including the YWHAE gene, was found in a mosaic state., (© 2013 Wiley Periodicals, Inc.)

Published

2013

18. Specific clinical and brain MRI features in mentally retarded patients with mutations in the Oligophrenin-1 gene.

Author

des Portes V, Boddaert N, Sacco S, Briault S, Maincent K, Bahi N, Gomot M, Ronce N, Bursztyn J, Adamsbaum C, Zilbovicius M, Chelly J, and Moraine C

Subjects

Adult, Cerebellum pathology, Epilepsy complications, Female, Frameshift Mutation, Humans, Magnetic Resonance Imaging, Male, Mental Retardation, X-Linked complications, Mental Retardation, X-Linked genetics, Muscle Hypotonia complications, Vision Disorders complications, Cerebellum abnormalities, Cytoskeletal Proteins genetics, GTPase-Activating Proteins genetics, Mental Retardation, X-Linked diagnosis, Mutation, Nuclear Proteins genetics

Abstract

Oligophrenin-1 (OPHN-1) gene disruption is known as responsible for so called "non-specific" X-linked mental retardation (MR) Billuart et al. [1998: Nature 392:923-926]. In order to search for a possible specific clinical and radiological profile for mutation in the OPHN-1 gene, clinical and 3D brain MRI studies were performed in the two families with a known mutation in OPHN-1 reported so far: a 19-year-old female with an X;12 balanced translocation encompassing OPHN-1, and four affected males of family MRX60 sharing a frameshift mutation in OPHN-1. Clinical data shared by affected individuals were neonatal hypotonia with motor delay but no obvious ataxia, marked strabismus, early onset complex partial seizures, and moderate to severe MR. Brain MRIs performed in three individuals exhibited a specific vermian dysgenesis including an incomplete sulcation of anterior and posterior vermis with the most prominent defect in lobules VI and VII. In addition, a non-specific cerebral cortico-subcortical atrophy was also observed. These clinical and radiological features suggest a distinct clinico-radiological syndrome. These preliminary data need to be confirmed in other families and will be helpful for further targeted mutation screening of the OPHN-1 gene in male patients with similar clinico-radiological features. In addition, OPHN-1 inactivation should be considered as a relevant model of developmental vermis disorganization, leading to a better understanding of the possible role of the cerebellum in MR., (Copyright 2003 Wiley-Liss, Inc.)

Published

2004

19. Inv(X)(p21.1;q22.1) in a man with mental retardation, short stature, general muscle wasting, and facial dysmorphism: clinical study and mutation analysis of the NXF5 gene.

Author

Frints SG, Jun L, Fryns JP, Devriendt K, Teulingkx R, Van den Berghe L, De Vos B, Borghgraef M, Chelly J, Des Portes V, Van Bokhoven H, Hamel B, Ropers HH, Kalscheuer V, Raynaud M, Moraine C, Marynen P, and Froyen G

Subjects

Abnormalities, Multiple diagnosis, Active Transport, Cell Nucleus, Base Sequence, Chromosome Breakage, Cloning, Molecular, Gene Expression, Humans, In Situ Hybridization, Fluorescence, Male, Mental Retardation, X-Linked metabolism, Middle Aged, Molecular Sequence Data, Nucleocytoplasmic Transport Proteins, RNA metabolism, Sequence Homology, Nucleic Acid, Syndrome, Abnormalities, Multiple genetics, Chromosome Inversion, Chromosomes, Human, X, Mental Retardation, X-Linked genetics, Mutation genetics, Nuclear Proteins genetics, RNA-Binding Proteins genetics

Abstract

We describe a 59-year-old male (patient A059) with moderate to severe mental retardation (MR) and a pericentric inversion of the X-chromosome: inv(X)(p21.1;q22.1). He had short stature, pectus excavatum, general muscle wasting, and facial dysmorphism. Until now, no other patients with similar clinical features have been described in the literature. Molecular analysis of both breakpoints led to the identification of a novel "Nuclear RNA export factor" (NXF) gene cluster on Xq22.1. Within this cluster, the NXF5 gene was interrupted with subsequent loss of gene expression. Hence, mutation analysis of the NXF5 and its neighboring homologue, the NXF2 gene was performed in 45 men with various forms of syndromic X-linked MR (XLMR) and in 70 patients with nonspecific XLMR. In the NXF5 gene four nucleotide changes: one intronic, two silent, and one missense (K23E), were identified. In the NXF2 gene two changes (one intronic and one silent) were found. Although none of these changes were causative mutations, we propose that NXF5 is a good candidate gene for this syndromic form of XLMR, given the suspected role of NXF proteins is within mRNA export/transport in neurons. Therefore, mutation screening of the NXF gene family in phenotypically identical patients is recommended., (Copyright 2003 Wiley-Liss, Inc.)

Published

2003