Your search keyword '"de Ravel TJ"' showing total 61 results

1. Duplications of FOXG1 in 14q12 are associated with developmental epilepsy, mental retardation, and severe speech impairment

Author

Sau Wai Cheung, Katia Rocchetti, Chiara Pantaleoni, Pawel Stankiewicz, Maria Clara Bonaglia, Roberto Ciccone, Stefano D'Arrigo, Jeffrey R Hughes, Mary Bertrand, Thomy de Ravel, Nicola Brunetti-Pierri, Erika Della Mina, Christian P. Schaaf, Zhilian Xia, Naftha Jelluma, Orsetta Zuffardi, Renato Borgatti, Claudia A. L. Ruivenkamp, Parul Jayakar, Serena Belli, Alex R. Paciorkowski, V. Reid Sutton, Clinical sciences, Medical Genetics, BRUNETTI PIERRI, Nicola, Paciorkowski, Ar, Ciccone, R, Mina, Ed, Bonaglia, Mc, Borgatti, R, Schaaf, Cp, Sutton, Vr, Xia, Z, Jelluma, N, Ruivenkamp, C, Bertrand, M, de Ravel, Tj, Jayakar, P, Belli, S, Rocchetti, K, Pantaleoni, C, D'Arrigo, S, Hughes, J, Cheung, Sw, Zuffardi, O, and Stankiewicz, P.

Subjects

Adult, Male, Child, preschool, comparative genomic hybridization, Rett syndrome, Biology, Article, Epilepsy/genetics, Epilepsy, Chromosomes, Human, Pair 14/genetics, Gene Duplication, Intellectual disability, Gene duplication, Genetics, medicine, Humans, Nerve Tissue Proteins/genetics, Forkhead Transcription Factors/genetics, Genetics (clinical), Oligonucleotide Array Sequence Analysis, Infant, medicine.disease, Hypotonia, Intellectual Disability/genetics, FOXG1, Language Development Disorders/genetics, Speech delay, Female, medicine.symptom, FOXG1 developmental delay speech delay infantile spasms array CGH rett-syndrome copy number deletion family males haploinsufficiency microduplication microarray features patient, Haploinsufficiency, Developmental Disabilities/genetics

Abstract

Genome-wide high-resolution array analysis is rapidly becoming a reliable method of diagnostic investigation in individuals with mental retardation and congenital anomalies, leading to the identification of several novel microdeletion and microduplication syndromes. We have identified seven individuals with duplication on chromosome 14q11.2q13.1, who exhibited idiopathic developmental delay and cognitive impairment, severe speech delay, and developmental epilepsy. Among these cases, the minimal common duplicated region on chromosome 14q11.2q13.1 includes only three genes, FOXG1, C14orf23, and PRKD1. We propose that increased dosage of Forkhead Box G1 (FOXG1) is the best candidate to explain the abnormal neurodevelopmental phenotypes observed in our patients. Deletions and inactivating mutations of FOXG1 have been associated with a Rett-like syndrome characterized by hypotonia, irritability, developmental delay, hand stereotypies, and deceleration of head growth. FOXG1, encoding a brain-specific transcription factor, has an important role in the developing brain. In fact, in vivo studies in chicken brain demonstrated that overexpression of FOXG1 results in thickening of the neuroepithelium and outgrowth of the telencephalon and mesencephalum, secondary to a reduction in neuroepithelial cell apoptosis. European Journal of Human Genetics (2011) 19, 102-107; doi:10.1038/ejhg.2010.142; published online 25 August 2010

Published

2011

2. Genetic Mapping of the FACC Gene and Linkage Analysis in Fanconi Anaemia FamilIes

Author

Rachel Gibson, Ford, D., Jansen, S., Savoia, A., Havenga, C., Milner, R. D., Ravel, T. J., Cohn, R. J., Ball, S. E., Roberts, I., Llerena, J. C., Vorechovsky, I., Pearson, T., Birjandi, F., Hussein, S. S., Murer-Orlando, M., Easton, D. F., Mathew, C. G., Gibson, R, Ford, D, S., Jansen, Savoia, Anna, Havenga, C, Milner, Rd, DE RAVEL, Tj, Cohn, Rj, Ball, Se, Roberts, I, Llerena, Jc, Vorechovsky, I, Pearson, T, Birjandi, F, Hussein, S, MURER ORLANDO, M, Easton, Df, and Mathew, Cg

Published

1994

3. Where are the missing gene defects in inherited retinal disorders? Intronic and synonymous variants contribute at least to 4% of CACNA1F-mediated inherited retinal disorders.

Author

Zeitz C, Michiels C, Neuillé M, Friedburg C, Condroyer C, Boyard F, Antonio A, Bouzidi N, Milicevic D, Veaux R, Tourville A, Zoumba A, Seneina I, Foussard M, Andrieu C, N Preising M, Blanchard S, Saraiva JP, Mesrob L, Le Floch E, Jubin C, Meyer V, Blanché H, Boland A, Deleuze JF, Sharon D, Drumare I, Defoort-Dhellemmes S, De Baere E, Leroy BP, Zanlonghi X, Casteels I, de Ravel TJ, Balikova I, Koenekoop RK, Laffargue F, McLean R, Gottlob I, Bonneau D, Schorderet DF, L Munier F, McKibbin M, Prescott K, Pelletier V, Dollfus H, Perdomo-Trujillo Y, Faure C, Reiff C, Wissinger B, Meunier I, Kohl S, Banin E, Zrenner E, Jurklies B, Lorenz B, Sahel JA, and Audo I

Subjects

Genetic Predisposition to Disease, Hemizygote, Humans, Introns, Male, Pedigree, RNA Splicing, Silent Mutation, Calcium Channels, L-Type genetics, Eye Diseases, Hereditary genetics, Genetic Diseases, X-Linked genetics, Mutation, Myopia genetics, Night Blindness genetics, Sequence Analysis, DNA methods

Abstract

Inherited retinal disorders (IRD) represent clinically and genetically heterogeneous diseases. To date, pathogenic variants have been identified in ~260 genes. Albeit that many genes are implicated in IRD, for 30-50% of the cases, the gene defect is unknown. These cases may be explained by novel gene defects, by overlooked structural variants, by variants in intronic, promoter or more distant regulatory regions, and represent synonymous variants of known genes contributing to the dysfunction of the respective proteins. Patients with one subgroup of IRD, namely incomplete congenital stationary night blindness (icCSNB), show a very specific phenotype. The major cause of this condition is the presence of a hemizygous pathogenic variant in CACNA1F. A comprehensive study applying direct Sanger sequencing of the gene-coding regions, exome and genome sequencing applied to a large cohort of patients with a clinical diagnosis of icCSNB revealed indeed that seven of the 189 CACNA1F-related cases have intronic and synonymous disease-causing variants leading to missplicing as validated by minigene approaches. These findings highlight that gene-locus sequencing may be a very efficient method in detecting disease-causing variants in clinically well-characterized patients with a diagnosis of IRD, like icCSNB., (© 2019 Wiley Periodicals, Inc.)

Published

2019

4. FOXP1 -related intellectual disability syndrome: a recognisable entity.

Author

Meerschaut I, Rochefort D, Revençu N, Pètre J, Corsello C, Rouleau GA, Hamdan FF, Michaud JL, Morton J, Radley J, Ragge N, García-Miñaúr S, Lapunzina P, Bralo MP, Mori MÁ, Moortgat S, Benoit V, Mary S, Bockaert N, Oostra A, Vanakker O, Velinov M, de Ravel TJ, Mekahli D, Sebat J, Vaux KK, DiDonato N, Hanson-Kahn AK, Hudgins L, Dallapiccola B, Novelli A, Tarani L, Andrieux J, Parker MJ, Neas K, Ceulemans B, Schoonjans AS, Prchalova D, Havlovicova M, Hancarova M, Budisteanu M, Dheedene A, Menten B, Dion PA, Lederer D, and Callewaert B

Subjects

Autism Spectrum Disorder genetics, Face abnormalities, Female, Forkhead Transcription Factors chemistry, Forkhead Transcription Factors metabolism, Humans, Language Disorders genetics, Male, Motor Skills Disorders genetics, Mutation, Mutation, Missense, Neurodevelopmental Disorders genetics, Phenotype, Protein Stability, Repressor Proteins chemistry, Repressor Proteins metabolism, Syndrome, Transcription, Genetic, Forkhead Transcription Factors genetics, Intellectual Disability genetics, Repressor Proteins genetics

Abstract

Background: Mutations in forkhead box protein P1 ( FOXP1 ) cause intellectual disability (ID) and specific language impairment (SLI), with or without autistic features (MIM: 613670). Despite multiple case reports no specific phenotype emerged so far., Methods: We correlate clinical and molecular data of 25 novel and 23 previously reported patients with FOXP1 defects. We evaluated FOXP1 activity by an in vitro luciferase model and assessed protein stability in vitro by western blotting., Results: Patients show ID, SLI, neuromotor delay (NMD) and recurrent facial features including a high broad forehead, bent downslanting palpebral fissures, ptosis and/or blepharophimosis and a bulbous nasal tip. Behavioural problems and autistic features are common. Brain, cardiac and urogenital malformations can be associated. More severe ID and NMD, sensorineural hearing loss and feeding difficulties are more common in patients with interstitial 3p deletions (14 patients) versus patients with monogenic FOXP1 defects (34 patients). Mutations result in impaired transcriptional repression and/or reduced protein stability., Conclusions: FOXP1 -related ID syndrome is a recognisable entity with a wide clinical spectrum and frequent systemic involvement. Our data will be helpful to evaluate genotype-phenotype correlations when interpreting next-generation sequencing data obtained in patients with ID and/or SLI and will guide clinical management., Competing Interests: Competing interests: None declared., (© Article author(s) (or their employer(s) unless otherwise stated in the text of the article) 2017. All rights reserved. No commercial use is permitted unless otherwise expressly granted.)

Published

2017

5. Long-term effect of gene therapy on Leber's congenital amaurosis.

Author

Bainbridge JW, Mehat MS, Sundaram V, Robbie SJ, Barker SE, Ripamonti C, Georgiadis A, Mowat FM, Beattie SG, Gardner PJ, Feathers KL, Luong VA, Yzer S, Balaggan K, Viswanathan A, de Ravel TJ, Casteels I, Holder GE, Tyler N, Fitzke FW, Weleber RG, Nardini M, Moore AT, Thompson DA, Petersen-Jones SM, Michaelides M, van den Born LI, Stockman A, Smith AJ, Rubin G, and Ali RR

Subjects

Adolescent, Animals, Child, Dependovirus, Disease Models, Animal, Disease Progression, Dogs, Humans, Leber Congenital Amaurosis genetics, Mutation, Photoreceptor Cells, Vertebrate, Vision, Ocular, Young Adult, DNA, Complementary administration & dosage, Genetic Therapy, Genetic Vectors administration & dosage, Leber Congenital Amaurosis therapy, Retina physiology, cis-trans-Isomerases genetics

Abstract

Background: Mutations in RPE65 cause Leber's congenital amaurosis, a progressive retinal degenerative disease that severely impairs sight in children. Gene therapy can result in modest improvements in night vision, but knowledge of its efficacy in humans is limited., Methods: We performed a phase 1-2 open-label trial involving 12 participants to evaluate the safety and efficacy of gene therapy with a recombinant adeno-associated virus 2/2 (rAAV2/2) vector carrying the RPE65 complementary DNA, and measured visual function over the course of 3 years. Four participants were administered a lower dose of the vector, and 8 were administered a higher dose. In a parallel study in dogs, we investigated the relationship among vector dose, visual function, and electroretinography (ERG) findings., Results: Improvements in retinal sensitivity were evident, to varying extents, in six participants for up to 3 years, peaking at 6 to 12 months after treatment and then declining. No associated improvement in retinal function was detected by means of ERG. Three participants had intraocular inflammation, and two had clinically significant deterioration of visual acuity. The reduction in central retinal thickness varied among participants. In dogs, RPE65 gene therapy with the same vector at lower doses improved vision-guided behavior, but only higher doses resulted in improvements in retinal function that were detectable with the use of ERG., Conclusions: Gene therapy with rAAV2/2 RPE65 vector improved retinal sensitivity, albeit modestly and temporarily. Comparison with the results obtained in the dog model indicates that there is a species difference in the amount of RPE65 required to drive the visual cycle and that the demand for RPE65 in affected persons was not met to the extent required for a durable, robust effect. (Funded by the National Institute for Health Research and others; ClinicalTrials.gov number, NCT00643747.).

Published

2015

6. No evidence of locus heterogeneity in familial microcephaly with or without chorioretinopathy, lymphedema, or mental retardation syndrome.

Author

Schlögel MJ, Mendola A, Fastré E, Vasudevan P, Devriendt K, de Ravel TJ, Van Esch H, Casteels I, Arroyo Carrera I, Cristofoli F, Fieggen K, Jones K, Lipson M, Balikova I, Singer A, Soller M, Mercedes Villanueva M, Revencu N, Boon LM, Brouillard P, and Vikkula M

Subjects

Adult, Facies, Female, Heterozygote, Humans, Intellectual Disability genetics, Kinesins genetics, Lymphedema genetics, Male, Mutation, Phenotype, Retinal Dysplasia genetics, Young Adult, Microcephaly genetics

Abstract

Background: Microcephaly with or without chorioretinopathy, lymphedema, or mental retardation syndrome (MCLMR) is a rare autosomal dominant disorder with variable expressivity. It is characterized by mild-to-severe microcephaly, often associated with intellectual disability, ocular defects and lymphedema. It can be sporadic or inherited. Eighty-seven patients have been described to carry a mutation in KIF11, which encodes a homotetrameric motor kinesin, EG5., Methods: We tested 23 unreported MCLMR index patients for KIF11. We also reviewed the clinical phenotypes of all our patients as well as of those described in previously published studies., Results: We identified 14 mutations, 12 of which are novel. We detected mutations in 12 affected individuals, from 6 out of 6 familial cases, and in 8 out of 17 sporadic patients. Phenotypic evaluation of patients (our 26 + 61 earlier published = 87) revealed microcephaly in 91%, eye anomalies in 72%, intellectual disability in 67% and lymphedema in 47% of the patients. Unaffected carriers were rare (4 out of 87: 5%). Family history is not a requisite for diagnosis; 31% (16 out of 52) were de novo cases., Conclusions: All inherited cases, and 50% of sporadic cases of MCLMR are due to germline KIF11 mutations. It is possible that mosaic KIF11 mutations cause the remainder of sporadic cases, which the methods employed here were not designed to detect. On the other hand, some of them might have another mimicking disorder and genetic defect, as microcephaly is highly heterogeneous. In aggregate, KIF11 mutations likely cause the majority, if not all, of MCLMR.

Published

2015

7. Spectral sensitivity measurements reveal partial success in restoring missing rod function with gene therapy.

Author

Ripamonti C, Henning GB, Robbie SJ, Sundaram V, van den Born LI, Casteels I, de Ravel TJ, Moore AT, Smith AJ, Bainbridge JW, Ali RR, and Stockman A

Subjects

Adult, Child, Dark Adaptation physiology, Genetic Vectors, Humans, Light, Middle Aged, Photic Stimulation, Visual Acuity physiology, Visual Fields physiology, Young Adult, Dependovirus genetics, Genetic Therapy, Leber Congenital Amaurosis physiopathology, Leber Congenital Amaurosis therapy, Retinal Rod Photoreceptor Cells physiology, Vision, Ocular physiology, cis-trans-Isomerases genetics

Abstract

Restored rod visual function after gene therapy can be established unequivocally by demonstrating that, after dark adaptation, spectral sensitivity has the shape characteristic of rods and that this shape collapses to a cone-like shape before rods have recovered after an intense bleach. We used these tests to assess retinal function in eight young adults and children with early-onset severe retinal dystrophy from Phase II of a clinical gene-therapy trial for RPE65 deficiency that involved the subretinal delivery of a recombinant adeno-associated viral vector carrying RPE65. We found substantial improvements in rod sensitivity in two participants: dark-adapted spectral sensitivity was rod-like after treatment and was cone-like before rods had recovered after a bleach. After 40 min of dark adaptation, one participant showed up to 1,000-fold sensitivity improvements 4 months after treatment and the second up to 100-fold improvements 6 months after treatment. The dark-adapted spectral sensitivities of the other six participants remained cone-like and showed little improvement in sensitivity.

Published

2015

8. Nature of the visual loss in observers with Leber's congenital amaurosis caused by specific mutations in RPE65.

Author

Ripamonti C, Henning GB, Ali RR, Bainbridge JW, Robbie SJ, Sundaram V, Luong VA, van den Born LI, Casteels I, de Ravel TJ, Moore AT, and Stockman A

Subjects

Adolescent, Adult, Blindness enzymology, Blindness etiology, Child, Contrast Sensitivity, DNA Mutational Analysis, Female, Flicker Fusion, Humans, Leber Congenital Amaurosis enzymology, Leber Congenital Amaurosis genetics, Male, Photic Stimulation, Retinal Cone Photoreceptor Cells pathology, Young Adult, cis-trans-Isomerases metabolism, Blindness genetics, DNA genetics, Leber Congenital Amaurosis complications, Mutation, Retinal Cone Photoreceptor Cells enzymology, cis-trans-Isomerases genetics

Abstract

Purpose: To characterize visual losses associated with genetic mutations in the RPE65 gene that cause defects in the RPE-specific isomerase, RPE65. RPE65 is an important component of the retinoid cycle that restores 11-cis-retinal after its photoisomerization to its all-trans form. The defects investigated here cause Leber's congenital amaurosis (LCA2), an autosomal, recessively-inherited, severe, congenital-onset rod-cone dystrophy., Methods: Vision was assessed in nine patients and 10 normal controls by measuring: (1) long-wavelength sensitive (L-) cone temporal acuity (critical flicker fusion frequency or cff) as a function of target illuminance, and (2) L-cone temporal contrast sensitivity as a function of temporal frequency at a fixed-target illuminance. Measurements were made by modulating either a 650-nm light superimposed on a 480-nm background or the red phosphor of a color monitor on a background produced by the monitor's blue phosphor., Results: RPE65-mutant observers have severely reduced cffs with shallower cff versus log illuminance functions that rise with a mean slope of 4.53 Hz per decade of illuminance compared with 8.69 Hz in normal controls. Consistent with the cff differences, RPE65-mutant observers show losses in temporal contrast sensitivity that increase rapidly with temporal frequency., Conclusions: All RPE65-mutant observers have consistent and substantial losses in temporal acuity and sensitivity compared with normal observers. The losses can be characterized by the addition of two sluggish filters within the mutant visual pathway, both filters with a time constant of 29.5 ms (i.e., low-pass filters with cut-off frequencies of 5.40 Hz)., (Copyright 2014 The Association for Research in Vision and Ophthalmology, Inc.)

Published

2014

9. Implantable cardioverter-defibrillators in hypertrophic cardiomyopathy: patient outcomes, rate of appropriate and inappropriate interventions, and complications.

Author

Vriesendorp PA, Schinkel AF, Van Cleemput J, Willems R, Jordaens LJ, Theuns DA, van Slegtenhorst MA, de Ravel TJ, ten Cate FJ, and Michels M

Subjects

Adult, Cardiomyopathy, Hypertrophic mortality, Death, Sudden, Cardiac prevention & control, Female, Follow-Up Studies, Humans, Male, Middle Aged, Regression Analysis, Risk Assessment, Risk Factors, Treatment Outcome, Cardiac Resynchronization Therapy statistics & numerical data, Cardiomyopathy, Hypertrophic therapy, Death, Sudden, Cardiac etiology, Defibrillators, Implantable adverse effects

Abstract

Background: Sudden cardiac death (SCD) is the most devastating complication of hypertrophic cardiomyopathy (HCM), but this can be prevented by an implantable cardioverter-defibrillator (ICD). The aim of this study is to evaluate HCM patients with ICDs for primary or secondary prevention of SCD., Methods: The study population consisted of all HCM patients with an ICD in 2 tertiary referral clinics. End points during follow-up were total and cardiac mortality, appropriate and inappropriate ICD intervention, and device-related complications. Cox-regression analysis was performed to identify predictors of outcome., Results: ICDs were implanted in 134 patients with HCM (mean age 44 ± 17 years, 34% women, 4.2 ± 4.8 years follow-up). Annualized cardiac mortality rate was 3.4% per year and associated with New York Heart Association class III or IV (HR 5.2 [2.0-14, P = .002]) and cardiac resynchronization therapy (HR 6.3 [2.1-20, P = .02]). Appropriate ICD interventions occurred in 38 patients (6.8%/year) and was associated with implantation for secondary prevention of SCD (HR 4.0 [1.8-9.1], P = .001) and male gender (HR 3.3 [1.2-9.0], P = .02). Inappropriate ICD intervention occurred in 21 patients (3.7%/year) and in 20 patients device related complications were documented (3.6%/year)., Conclusion: ICDs successfully abort life-threatening arrhythmias in HCM patients at increased risk of SCD with an annualized intervention rate of 6.8% per year. End-stage heart failure is the main cause of mortality in these patients. The annualized rate of inappropriate ICD intervention was 3.7% per year, whereas device-related complications occurred 3.6% per year., (© 2013.)

Published

2013

10. Genome-wide association analysis identifies a susceptibility locus for pulmonary arterial hypertension.

Author

Germain M, Eyries M, Montani D, Poirier O, Girerd B, Dorfmüller P, Coulet F, Nadaud S, Maugenre S, Guignabert C, Carpentier W, Vonk-Noordegraaf A, Lévy M, Chaouat A, Lambert JC, Bertrand M, Dupuy AM, Letenneur L, Lathrop M, Amouyel P, de Ravel TJ, Delcroix M, Austin ED, Robbins IM, Hemnes AR, Loyd JE, Berman-Rosenzweig E, Barst RJ, Chung WK, Simonneau G, Trégouët DA, Humbert M, and Soubrier F

Subjects

Case-Control Studies, Endothelium, Vascular metabolism, Endothelium, Vascular pathology, Familial Primary Pulmonary Hypertension, Genotype, Humans, Immunoenzyme Techniques, Phenotype, Pulmonary Artery metabolism, Pulmonary Artery pathology, RNA, Messenger genetics, Real-Time Polymerase Chain Reaction, Reverse Transcriptase Polymerase Chain Reaction, Genetic Predisposition to Disease, Genome, Human, Genome-Wide Association Study, Hypertension, Pulmonary genetics, Polymorphism, Single Nucleotide genetics, Quantitative Trait Loci

Abstract

Pulmonary arterial hypertension (PAH) is a rare, severe disease resulting from progressive obliteration of small-caliber pulmonary arteries by proliferating vascular cells. PAH can occur without recognized etiology (idiopathic PAH), be associated with a systemic disease or occur as a heritable form, with BMPR2 mutated in approximately 80% of familial and 15% of idiopathic PAH cases. We conducted a genome-wide association study (GWAS) based on 2 independent case-control studies for idiopathic and familial PAH (without BMPR2 mutations), including a total of 625 cases and 1,525 healthy individuals. We detected a significant association at the CBLN2 locus mapping to 18q22.3, with the risk allele conferring an odds ratio for PAH of 1.97 (1.59-2.45; P = 7.47 × 10(-10)). CBLN2 is expressed in the lung, and its expression is higher in explanted lungs from individuals with PAH and in endothelial cells cultured from explanted PAH lungs.

Published

2013

11. High resolution mapping of OCA2 intragenic rearrangements and identification of a founder effect associated with a deletion in Polish albino patients.

Author

Rooryck C, Morice-Picard F, Lasseaux E, Cailley D, Dollfus H, Defoort-Dhellemme S, Duban-Bedu B, de Ravel TJ, Taieb A, Lacombe D, and Arveiler B

Subjects

Albinism, Oculocutaneous ethnology, Albinism, Oculocutaneous genetics, Founder Effect, Haplotypes, Humans, Microsatellite Repeats, Oligonucleotide Array Sequence Analysis methods, White People genetics, Gene Deletion, Membrane Transport Proteins genetics

Abstract

Oculocutaneous albinism type 2 (OCA2) represents about 30% of OCA worldwide. Using quantitative multiplex fluorescent PCR and very high-resolution array-CGH focussed on the OCA2 gene and surrounding regions in 15q12, we identified new rearrangements. Deletion 1, encompassing exons 3-20, was present in three patients (including one in the homozygous state), and Deletion 2 (exons 1-20) was found in one patient (heterozygous state). The duplication (exons 3-20) was found in one patient in the homozygous state. Using 14 microsatellite markers we determined haplotypes associated with these rearrangements. Deletion 1 was associated with the same haplotype in three patients who were all of Polish origin, which is strongly in favour of a founder effect. Deletion 2 was associated with a distinct haplotype. The homozygous duplication was inherited from the two unrelated parents of the patients on two different haplotypes. Analysis of the sequences around the breakpoints of these rearrangements showed that all occurred within complex arrays of repetitive sequences. The combined use of very high-resolution array-CGH and of microsatellites (including new intragenic ones described here) constitutes a powerful approach for the precise characterization of OCA2 rearrangements, which have been found in more than 20% of OCA2 patients.

Published

2011

12. Duplications of FOXG1 in 14q12 are associated with developmental epilepsy, mental retardation, and severe speech impairment.

Author

Brunetti-Pierri N, Paciorkowski AR, Ciccone R, Della Mina E, Bonaglia MC, Borgatti R, Schaaf CP, Sutton VR, Xia Z, Jelluma N, Ruivenkamp C, Bertrand M, de Ravel TJ, Jayakar P, Belli S, Rocchetti K, Pantaleoni C, D'Arrigo S, Hughes J, Cheung SW, Zuffardi O, and Stankiewicz P

Subjects

Adult, Child, Preschool, Comparative Genomic Hybridization, Female, Humans, Infant, Male, Oligonucleotide Array Sequence Analysis, Chromosomes, Human, Pair 14 genetics, Developmental Disabilities genetics, Epilepsy genetics, Forkhead Transcription Factors genetics, Gene Duplication, Intellectual Disability genetics, Language Development Disorders genetics, Nerve Tissue Proteins genetics

Abstract

Genome-wide high-resolution array analysis is rapidly becoming a reliable method of diagnostic investigation in individuals with mental retardation and congenital anomalies, leading to the identification of several novel microdeletion and microduplication syndromes. We have identified seven individuals with duplication on chromosome 14q11.2q13.1, who exhibited idiopathic developmental delay and cognitive impairment, severe speech delay, and developmental epilepsy. Among these cases, the minimal common duplicated region on chromosome 14q11.2q13.1 includes only three genes, FOXG1, C14orf23, and PRKD1. We propose that increased dosage of Forkhead Box G1 (FOXG1) is the best candidate to explain the abnormal neurodevelopmental phenotypes observed in our patients. Deletions and inactivating mutations of FOXG1 have been associated with a Rett-like syndrome characterized by hypotonia, irritability, developmental delay, hand stereotypies, and deceleration of head growth. FOXG1, encoding a brain-specific transcription factor, has an important role in the developing brain. In fact, in vivo studies in chicken brain demonstrated that overexpression of FOXG1 results in thickening of the neuroepithelium and outgrowth of the telencephalon and mesencephalum, secondary to a reduction in neuroepithelial cell apoptosis.

Published

2011

13. Dilated cardiomyopathy caused by a novel TNNT2 mutation-added value of genetic testing in the correct identification of affected subjects.

Author

Van Acker H, De Sutter J, Vandekerckhove K, de Ravel TJ, Verhaaren H, and De Backer J

Subjects

Female, Genetic Testing, Humans, Pedigree, Young Adult, Cardiomyopathy, Dilated genetics, Mutation, Troponin T genetics

Abstract

Diagnosing familial dilated cardiomyopathy requires careful family history taking and clinical evaluation in first degree relatives. Based on the results of these findings the diagnosis may be established in the proband. However, due to the age-dependent expression of the disease, doubt may persist regarding the exact status of other family members, especially in young individuals. Here we present a family with DCM in whom we identified an underlying cardiac troponin T (TNNT2) mutation. Genetic testing was essential for the detection of asymptomatic carriers as well as for exclusion of the disease in other family members., (Copyright © 2009 Elsevier Ireland Ltd. All rights reserved.)

Published

2010

14. Deletions in the VPS13B (COH1) gene as a cause of Cohen syndrome.

Author

Balikova I, Lehesjoki AE, de Ravel TJ, Thienpont B, Chandler KE, Clayton-Smith J, Träskelin AL, Fryns JP, and Vermeesch JR

Subjects

Abnormalities, Multiple pathology, Adult, Base Sequence, Child, DNA Mutational Analysis, Humans, Intellectual Disability genetics, Intellectual Disability pathology, Male, Microcephaly genetics, Microcephaly pathology, Neutropenia genetics, Neutropenia pathology, Phenotype, Syndrome, Vesicular Transport Proteins metabolism, Abnormalities, Multiple genetics, Sequence Deletion, Vesicular Transport Proteins genetics

Abstract

Cohen syndrome is an autosomal recessive disorder that is characterized by mental retardation, facial dysmorphism, microcephaly, retinal dystrophy, truncal obesity, joint laxity and intermittent neutropenia. Mutations in the VPS13B (COH1) gene underlie Cohen syndrome. In approximately 70% of the patients mutations in the gene are identified on both alleles, while in about 30% only a mutation in a single allele or no mutant allele is detected. The VPS13B locus was recently added to the growing list of benign copy number variants. We hypothesized that patients with unexplained Cohen syndrome would harbour deletions affecting the VPS13B locus. We screened 35 patients from 26 families with targeted array CGH and identified 7 copy number alterations: 2 homozygous and 5 heterozygous deletions. Our results show that deletions are an important cause of Cohen syndrome and screening for copy number alterations of VPS13B should be an integral part of the diagnostic work-up of these patients. These findings have important consequences for the diagnosis of patients with genetic disorders in general since, as we highlight, rare benign copy number variants can underly autosomal recessive disorders and lead to disease in homozygous state or in compound heterozygosity with another mutation.

Published

2009

15. Further delineation of the 15q13 microdeletion and duplication syndromes: a clinical spectrum varying from non-pathogenic to a severe outcome.

Author

van Bon BW, Mefford HC, Menten B, Koolen DA, Sharp AJ, Nillesen WM, Innis JW, de Ravel TJ, Mercer CL, Fichera M, Stewart H, Connell LE, Ounap K, Lachlan K, Castle B, Van der Aa N, van Ravenswaaij C, Nobrega MA, Serra-Juhé C, Simonic I, de Leeuw N, Pfundt R, Bongers EM, Baker C, Finnemore P, Huang S, Maloney VK, Crolla JA, van Kalmthout M, Elia M, Vandeweyer G, Fryns JP, Janssens S, Foulds N, Reitano S, Smith K, Parkel S, Loeys B, Woods CG, Oostra A, Speleman F, Pereira AC, Kurg A, Willatt L, Knight SJ, Vermeesch JR, Romano C, Barber JC, Mortier G, Pérez-Jurado LA, Kooy F, Brunner HG, Eichler EE, Kleefstra T, and de Vries BB

Subjects

Adolescent, Adult, Child, Child, Preschool, Chromosome Disorders pathology, Female, Humans, Infant, Infant, Newborn, Intellectual Disability genetics, Intellectual Disability pathology, Male, Oligonucleotide Array Sequence Analysis, Pedigree, Pregnancy, Syndrome, Chromosome Aberrations, Chromosome Deletion, Chromosome Disorders genetics, Chromosomes, Human, Pair 15 genetics, Gene Duplication

Abstract

Background: Recurrent 15q13.3 microdeletions were recently identified with identical proximal (BP4) and distal (BP5) breakpoints and associated with mild to moderate mental retardation and epilepsy., Methods: To assess further the clinical implications of this novel 15q13.3 microdeletion syndrome, 18 new probands with a deletion were molecularly and clinically characterised. In addition, we evaluated the characteristics of a family with a more proximal deletion between BP3 and BP4. Finally, four patients with a duplication in the BP3-BP4-BP5 region were included in this study to ascertain the clinical significance of duplications in this region., Results: The 15q13.3 microdeletion in our series was associated with a highly variable intra- and inter-familial phenotype. At least 11 of the 18 deletions identified were inherited. Moreover, 7 of 10 siblings from four different families also had this deletion: one had a mild developmental delay, four had only learning problems during childhood, but functioned well in daily life as adults, whereas the other two had no learning problems at all. In contrast to previous findings, seizures were not a common feature in our series (only 2 of 17 living probands). Three patients with deletions had cardiac defects and deletion of the KLF13 gene, located in the critical region, may contribute to these abnormalities. The limited data from the single family with the more proximal BP3-BP4 deletion suggest this deletion may have little clinical significance. Patients with duplications of the BP3-BP4-BP5 region did not share a recognisable phenotype, but psychiatric disease was noted in 2 of 4 patients., Conclusions: Overall, our findings broaden the phenotypic spectrum associated with 15q13.3 deletions and suggest that, in some individuals, deletion of 15q13.3 is not sufficient to cause disease. The existence of microdeletion syndromes, associated with an unpredictable and variable phenotypic outcome, will pose the clinician with diagnostic difficulties and challenge the commonly used paradigm in the diagnostic setting that aberrations inherited from a phenotypically normal parent are usually without clinical consequences.

Published

2009

16. Early detection of chromosome 9q22.32q31.1 microdeletion and the nevoid basal cell carcinoma syndrome.

Author

de Ravel TJ, Ameye L, Ballon K, Borghgraef M, Vermeesch JR, and Devriendt K

Subjects

Abnormalities, Multiple genetics, Carcinoma, Basal Cell genetics, Humans, Infant, Intellectual Disability, Male, Motor Skills Disorders, Patched Receptors, Patched-1 Receptor, Receptors, Cell Surface genetics, Speech Disorders, Syndrome, Chromosome Deletion, Chromosome Disorders genetics, Chromosomes, Human, Pair 9

Abstract

We report on a patient with a microdeletion of chromosome region 9q22.32q31.1 including the PTCH1 gene (human homologue of the Drosophila patched 1 gene), review the findings in the reported patients with similar array CGH findings, and highlight the non nevoid basal cell carcinoma/non-Gorlin syndrome findings at an earlier age. These are macrocephaly, neonatal hypotonia, severe psychomotor retardation with markedly delayed motor milestones and speech development, epicanthic folds, a thin upper lip, a short and wide/webbed neck, pectus excavatum and (kypho)scoliosis. These features should alert the physician to an early diagnosis of the microdeletion and allow the initiation of essential clinical management hereof.

Published

2009

17. Another patient with a de novo deletion further delineates the 2q33.1 microdeletion syndrome.

Author

de Ravel TJ, Balikova I, Thiry P, Vermeesch JR, and Frijns JP

Subjects

Abnormalities, Multiple genetics, Humans, Male, Syndrome, Young Adult, Chromosome Deletion, Chromosome Disorders genetics, Chromosomes, Human, Pair 2

Abstract

A male patient, who had intra-uterine growth retardation, a low birth weight and hypotonia due to a chromosome 2q33.1 deletion, is described. At the age of 20 years, he displays short stature, microcephaly, a high forehead, microstomia, large teeth and is hypertonic. He is severely mentally retarded, has not developed speech, is hyperactive, anxious and at times aggressive. Full tiling array showed a de novo 14 Mb deletion at chromosome region 2q32.3q33.2, further delineating the 2q33.1 microdeletion syndrome.

Published

2009

18. Mutation analysis in Costello syndrome: functional and structural characterization of the HRAS p.Lys117Arg mutation.

Author

Denayer E, Parret A, Chmara M, Schubbert S, Vogels A, Devriendt K, Frijns JP, Rybin V, de Ravel TJ, Shannon K, Cools J, Scheffzek K, and Legius E

Subjects

Base Sequence, Cell Line, Cell Proliferation, Child, Child, Preschool, Codon, DNA Mutational Analysis, Guanosine Diphosphate metabolism, Humans, Hydrolysis, Infant, Infant, Newborn, Molecular Sequence Data, Mutant Proteins chemistry, Syndrome, Abnormalities, Multiple genetics, Arginine genetics, Lysine genetics, Mutation genetics, Proto-Oncogene Proteins p21(ras) chemistry, Proto-Oncogene Proteins p21(ras) genetics

Abstract

Costello syndrome is a mental retardation syndrome characterized by high birth weight, postnatal growth retardation, coarse face, loose skin, cardiovascular problems, and tumor predisposition. De novo heterozygous missense mutations in HRAS codon 12 and 13 disturbing the intrinsic GTP hydrolysis cause Costello syndrome. We report a patient with typical Costello syndrome and a novel heterozygous missense mutation in codon 117 (c.350A>G, p.Lys117Arg) of the HRAS gene, resulting in constitutive activation of the RAS/MAPK pathway similar to the typical p.Gly12Ser and p.Gly12Ala mutations. Recombinant HRAS p.Lys117Arg demonstrates normal intrinsic GTP hydrolysis and responsiveness to GTPase-activating proteins, but the nucleotide dissociation rate is increased 80-fold. Consistent with the biochemical data, the crystal structure of the p.Lys117Arg mutant indicates an altered interaction pattern of the side chain that is associated with unfavorable nucleotide binding properties. Together, these data show that a RAS mutation that only perturbs guanine nucleotide binding has similar functional consequences as mutations that impair GTP hydrolysis and causes human disease., ((c) 2007 Wiley-Liss, Inc.)

Published

2008

19. What's new in karyotyping? The move towards array comparative genomic hybridisation (CGH).

Author

de Ravel TJ, Devriendt K, Fryns JP, and Vermeesch JR

Subjects

Abnormalities, Multiple genetics, Female, Genetic Variation, Genotype, Humans, Intellectual Disability genetics, Neoplasms genetics, Phenotype, Pregnancy, Prenatal Diagnosis, Translocation, Genetic, Karyotyping, Nucleic Acid Hybridization, Oligonucleotide Array Sequence Analysis trends

Abstract

Molecular karyotyping by array comparative genomic hybridisation (array CGH) has doubled the detection rate of pathogenic chromosomal imbalances in patients. This has been possible by increasing the resolution level from the 5 Mb obtained using the conventional karyotype to as low as 100 kb by array technology. Moreover, the technology revealed that over 12% of the human genome includes sub-microscopic benign copy number variable regions. These new findings have implications in genetic counselling and patient management.

Published

2007

20. Identification of a novel BBS gene (BBS12) highlights the major role of a vertebrate-specific branch of chaperonin-related proteins in Bardet-Biedl syndrome.

Author

Stoetzel C, Muller J, Laurier V, Davis EE, Zaghloul NA, Vicaire S, Jacquelin C, Plewniak F, Leitch CC, Sarda P, Hamel C, de Ravel TJ, Lewis RA, Friederich E, Thibault C, Danse JM, Verloes A, Bonneau D, Katsanis N, Poch O, Mandel JL, and Dollfus H

Subjects

Animals, Chaperonins physiology, Chromosomes, Human, Pair 4 genetics, Embryo, Nonmammalian abnormalities, Group II Chaperonins, Homozygote, Humans, Models, Molecular, Mutation, Oligonucleotide Array Sequence Analysis, Pedigree, Polymorphism, Single Nucleotide, Zebrafish abnormalities, Zebrafish embryology, Zebrafish genetics, Bardet-Biedl Syndrome genetics, Chaperonins genetics

Abstract

Bardet-Biedl syndrome (BBS) is primarily an autosomal recessive ciliopathy characterized by progressive retinal degeneration, obesity, cognitive impairment, polydactyly, and kidney anomalies. The disorder is genetically heterogeneous, with 11 BBS genes identified to date, which account for ~70% of affected families. We have combined single-nucleotide-polymorphism array homozygosity mapping with in silico analysis to identify a new BBS gene, BBS12. Patients from two Gypsy families were homozygous and haploidentical in a 6-Mb region of chromosome 4q27. FLJ35630 was selected as a candidate gene, because it was predicted to encode a protein with similarity to members of the type II chaperonin superfamily, which includes BBS6 and BBS10. We found pathogenic mutations in both Gypsy families, as well as in 14 other families of various ethnic backgrounds, indicating that BBS12 accounts for approximately 5% of all BBS cases. BBS12 is vertebrate specific and, together with BBS6 and BBS10, defines a novel branch of the type II chaperonin superfamily. These three genes are characterized by unusually rapid evolution and are likely to perform ciliary functions specific to vertebrates that are important in the pathophysiology of the syndrome, and together they account for about one-third of the total BBS mutational load. Consistent with this notion, suppression of each family member in zebrafish yielded gastrulation-movement defects characteristic of other BBS morphants, whereas simultaneous suppression of all three members resulted in severely affected embryos, possibly hinting at partial functional redundancy within this protein family.

Published

2007

21. BBS10 encodes a vertebrate-specific chaperonin-like protein and is a major BBS locus.

Author

Stoetzel C, Laurier V, Davis EE, Muller J, Rix S, Badano JL, Leitch CC, Salem N, Chouery E, Corbani S, Jalk N, Vicaire S, Sarda P, Hamel C, Lacombe D, Holder M, Odent S, Holder S, Brooks AS, Elcioglu NH, Silva ED, Rossillion B, Sigaudy S, de Ravel TJ, Lewis RA, Leheup B, Verloes A, Amati-Bonneau P, Mégarbané A, Poch O, Bonneau D, Beales PL, Mandel JL, Katsanis N, and Dollfus H

Subjects

Cohort Studies, Humans, Mutation, Proteins metabolism, Bardet-Biedl Syndrome genetics, Proteins genetics

Abstract

Bardet-Biedl syndrome (BBS) is a genetically heterogeneous ciliopathy. Although nine BBS genes have been cloned, they explain only 40-50% of the total mutational load. Here we report a major new BBS locus, BBS10, that encodes a previously unknown, rapidly evolving vertebrate-specific chaperonin-like protein. We found BBS10 to be mutated in about 20% of an unselected cohort of families of various ethnic origins, including some families with mutations in other BBS genes, consistent with oligogenic inheritance. In zebrafish, mild suppression of bbs10 exacerbated the phenotypes of other bbs morphants.

Published

2006

22. CHARGE syndrome: the phenotypic spectrum of mutations in the CHD7 gene.

Author

Jongmans MC, Admiraal RJ, van der Donk KP, Vissers LE, Baas AF, Kapusta L, van Hagen JM, Donnai D, de Ravel TJ, Veltman JA, Geurts van Kessel A, De Vries BB, Brunner HG, Hoefsloot LH, and van Ravenswaaij CM

Subjects

Adolescent, Adult, Central Nervous System Diseases diagnosis, Central Nervous System Diseases genetics, Child, Child, Preschool, Choanal Atresia diagnosis, Choanal Atresia genetics, Coloboma diagnosis, Coloboma genetics, DNA Mutational Analysis, Female, Genetic Testing, Gestational Age, Heart Defects, Congenital diagnosis, Heart Defects, Congenital genetics, Humans, Infant, Infant, Newborn, Male, Mouth Diseases diagnosis, Mouth Diseases genetics, Phenotype, Spinal Diseases diagnosis, Spinal Diseases genetics, Syndrome, Vestibular Diseases diagnosis, Vestibular Diseases genetics, Abnormalities, Multiple diagnosis, Abnormalities, Multiple genetics, DNA Helicases genetics, DNA-Binding Proteins genetics, Mutation

Abstract

Background: CHARGE syndrome is a non-random clustering of congenital anomalies including coloboma, heart defects, choanal atresia, retarded growth and development, genital hypoplasia, ear anomalies, and deafness. A consistent feature in CHARGE syndrome is semicircular canal hypoplasia resulting in vestibular areflexia. Other commonly associated congenital anomalies are facial nerve palsy, cleft lip/palate, and tracheo-oesophageal fistula. Specific behavioural problems, including autistic-like behaviour, have been described. The CHD7 gene on chromosome 8q12.1 was recently discovered as a major gene involved in the aetiology of this syndrome., Methods: The coding regions of CHD7 were screened for mutations in 107 index patients with clinical features suggestive of CHARGE syndrome. Clinical data of the mutation positive patients were sampled to study the phenotypic spectrum of mutations in the CHD7 gene., Results: Mutations were identified in 69 patients. Here we describe the clinical features of 47 of these patients, including two sib pairs. Most mutations were unique and were scattered throughout the gene. All patients but one fulfilled the current diagnostic criteria for CHARGE syndrome. No genotype-phenotype correlations were apparent in this cohort, which is best demonstrated by the differences in clinical presentation in sib pairs with identical mutations. Somatic mosaicism was detected in the unaffected mother of a sib pair, supporting the existence of germline mosaicism., Conclusions: CHD7 mutations account for the majority of the cases with CHARGE syndrome, with a broad clinical variability and without an obvious genotype-phenotype correlation. In one case evidence for germline mosaicism was provided.

Published

2006

23. Microarray-based mutation detection and phenotypic characterization of patients with Leber congenital amaurosis.

Author

Yzer S, Leroy BP, De Baere E, de Ravel TJ, Zonneveld MN, Voesenek K, Kellner U, Ciriano JP, de Faber JT, Rohrschneider K, Roepman R, den Hollander AI, Cruysberg JR, Meire F, Casteels I, van Moll-Ramirez NG, Allikmets R, van den Born LI, and Cremers FP

Subjects

Adaptor Proteins, Signal Transducing, Alcohol Oxidoreductases genetics, Child, Child, Preschool, DNA Mutational Analysis, Female, Genetic Testing methods, Genotype, Humans, Infant, Male, Phenotype, Retinitis Pigmentosa congenital, Retinitis Pigmentosa genetics, cis-trans-Isomerases, Blindness congenital, Blindness genetics, Carrier Proteins genetics, Eye Proteins genetics, Guanylate Cyclase genetics, Membrane Proteins genetics, Mutation, Nerve Tissue Proteins genetics, Oligonucleotide Array Sequence Analysis methods, Receptors, Cell Surface genetics

Abstract

Purpose: To test the efficiency of a microarray chip as a diagnostic tool in a cohort of northwestern European patients with Leber congenital amaurosis (LCA) and to perform a genotype-phenotype analysis in patients in whom pathologic mutations were identified., Methods: DNAs from 58 patients with LCA were analyzed using a microarray chip containing previously identified disease-associated sequence variants in six LCA genes. Mutations identified by chip analysis were confirmed by sequence analysis. On identification of one mutation, all protein coding exons of the relevant genes were sequenced. In addition, sequence analysis of the RDH12 gene was performed in 22 patients. Patients with mutations were phenotyped., Results: Pathogenic mutations were identified in 19 of the 58 patients with LCA (32.8%). Four novel sequence variants were identified. Mutations were most frequently found in CRB1 (15.5%), followed by GUCY2D (10.3%). The p.R768W mutation was found in 8 of 10 GUCY2D alleles, suggesting that it is a founder mutation in the northwest of Europe. In early childhood, patients with AIPL1 or GUCY2D mutations show normal fundi. Those with AIPL1-associated LCA progress to an RP-like fundus before the age of 8, whereas patients with GUCY2D-associated LCA still have relatively normal fundi in their mid-20s. Patients with CRB1 mutations present with distinct fundus abnormalities at birth and consistently show characteristics of RP12. Pathogenic GUCY2D mutations result in the most severe form of LCA., Conclusions: Microarray-based mutation detection allowed the identification of 32% of LCA sequence variants and represents an efficient first-pass screening tool. Mutations in CRB1, and to a lesser extent, in GUCY2D, underlie most LCA cases in this cohort. The present study establishes a genotype-phenotype correlation for AIPL1, CRB1, and GUCY2D.

Published

2006

24. Molecular karyotyping of patients with MCA/MR: the blurred boundary between normal and pathogenic variation.

Author

de Ravel TJ, Balikova I, Thienpont B, Hannes F, Maas N, Fryns JP, Devriendt K, and Vermeesch JR

Subjects

Adult, Child, Child, Preschool, Chromosome Aberrations, Female, Genome, Human, Humans, Infant, Intellectual Disability genetics, Male, Phenotype, Computational Biology methods, Genetic Variation, Karyotyping methods, Nucleic Acid Hybridization

Abstract

Molecular karyotyping has revealed that microdeletions/duplications in the human genome are a major cause of multiple congenital anomalies associated with mental retardation (MCA/MR). The identification of a de novo chromosomal imbalance in a patient with MCA/MR is usually considered causal for the phenotype while a chromosomal imbalance inherited from a phenotypically normal parent is considered as a benign variation and not related to the disorder. Around 40% of imbalances in patients with MCA/MR in this series is inherited from a healthy parent and the majority of these appear to be (extremely) rare variants. As some of these contain known disease-causing genes and have also been found to be de novo in MCA/MR patients, this challenges the general view that such familial variants are innocent and of no major phenotypic consequence. Rather, we argue, that human genomes can be tolerant of genomic copy number variations depending on the genetic and environmental background and that different mechanisms play a role in determining whether these chromosomal imbalances manifest themselves., (Copyright (c) 2006 S. Karger AG, Basel.)

Published

2006

25. Unconventional intronic splice site mutation in SCN5A associates with cardiac sodium channelopathy.

Author

Rossenbacker T, Schollen E, Kuipéri C, de Ravel TJ, Devriendt K, Matthijs G, Collen D, Heidbüchel H, and Carmeliet P

Subjects

Adolescent, Adult, Aged, Alleles, Child, DNA Mutational Analysis, Female, Humans, Male, Middle Aged, Models, Biological, NAV1.5 Voltage-Gated Sodium Channel, Pedigree, RNA Splicing physiology, Syndrome, Arrhythmias, Cardiac genetics, Introns genetics, Muscle Proteins genetics, Mutation, RNA Splice Sites genetics, Sodium Channels genetics

Abstract

Background: Mutations in the cardiac sodium channel, SCN5A, have been associated with one type of long-QT syndrome, with isolated cardiac conduction defects and Brugada syndrome. The sodium channelopathies exhibit marked variation in clinical phenotypes. The mechanisms underlying the phenotypical diversity, however, remain unknown. Exonic SCN5A mutations can be detected in 20% of Brugada syndrome patients., Results: An intronic mutation (c.4810+3_4810+6dupGGGT) in the SCN5A gene, located outside the consensus splice site, was detected in this study in a family with a highly variable clinical phenotype of Brugada syndrome and/or conduction disease and in a patient with Brugada syndrome. The mutation was not found in a control panel of 100 (200 alleles) ethnically matched normal control subjects. We provide in vivo and in vitro evidence that the mutation can disrupt the splice donor site, activate a cryptic splice site, and create a novel splice site. Notably, our data show that normal transcripts can be also derived from the mutant allele., Conclusions: This is the first report of an unconventional intronic splice site mutation in the SCN5A gene leading to cardiac sodium channelopathy. We speculate that its phenotypical diversity might be determined by the ratio of normal/abnormal transcripts derived from the mutant allele.

Published

2005

26. Follow-up of adult males with chromosome 18p deletion.

Author

de Ravel TJ, Thiry P, and Fryns JP

Subjects

Abnormalities, Multiple pathology, Abnormalities, Multiple physiopathology, Adult, Female, Follow-Up Studies, Humans, Intellectual Disability physiopathology, Male, Middle Aged, Phenotype, Syndrome, Abnormalities, Multiple genetics, Chromosome Deletion, Chromosomes, Human, Pair 18 genetics, Intellectual Disability genetics

Abstract

The 18p- syndrome has been known for over 40 years, the first report being by de Grouchy et al. [Comptes Rendus Hebdomadaires Séances l'Acad Sci 256 (1963) 1028]. Mental retardation of varying severity is the most constant feature. Over 100 cases have been reported. The eldest patients have been 50 years [Hum Genet 63 (1983) 139; Clin Genet 2 (1971) 338]. Follow-up of two adult patients, then 22 and 42 years [Ann Génét 29 (1986) 107], now 42 and 62 years of age, is reported. Further case reports are required in order to better define the evolution of adult patients with the 18p- syndrome.

Published

2005

27. A further mutation of the FGFR2 tyrosine kinase domain in mild Crouzon syndrome.

Author

de Ravel TJ, Taylor IB, Van Oostveldt AJ, Fryns JP, and Wilkie AO

Subjects

Acrocephalosyndactylia diagnosis, Adult, Amino Acid Sequence, Amino Acid Substitution, Child, Child, Preschool, Craniofacial Dysostosis diagnosis, Female, Heterozygote, Humans, Male, Middle Aged, Molecular Sequence Data, Pedigree, Polymerase Chain Reaction, Receptor, Fibroblast Growth Factor, Type 2, Sequence Homology, Amino Acid, Acrocephalosyndactylia genetics, Craniofacial Dysostosis genetics, Mutation, Missense genetics, Receptor Protein-Tyrosine Kinases genetics, Receptors, Fibroblast Growth Factor genetics

Abstract

We report a family heterozygous for a newly identified mutation in the tyrosine kinase I domain of the FGFR2 gene (1576A > G, encoding the missense substitution Lys526Glu), associated with variable expressivity of Crouzon syndrome, including clinical nonpenetrance. Our observations expand both the clinical and molecular spectrum of this unusual subset of FGFR2 mutations.

Published

2005

28. Post-zygotic origin of isochromosome 12p.

Author

de Ravel TJ, Keymolen K, van Assche E, Wittevronghel I, Moerman P, Salden I, Matthijs G, Fryns JP, and Vermeesch JR

Subjects

Adult, Alleles, Amniotic Fluid cytology, Cells, Cultured, Chorionic Villi ultrastructure, Chromosome Banding, DNA analysis, Female, Fibroblasts, Gestational Age, Humans, In Situ Hybridization, Fluorescence, Karyotyping, Pregnancy, Chromosomes, Human, Pair 12 genetics, Isochromosomes genetics, Prenatal Diagnosis, Zygote

Abstract

Objective: Advance knowledge about the mechanism of isochromosome formation., Methods: Echographic examination of the foetus. G- and/or T-banded chromosome and FISH analysis using chromosome 12p subtelomeric probes on short- and long-term CVS cultures, amniocytes and foetal fibroblasts. Polymorphic CA repeat analysis on DNA from the foetus and both parents., Results: Short-term CVS cultures showed a 46,XX karyotype, whilst long-term CVS cultures showed a 47,XX,+12 karyotype. FISH on amniocytes indicated 2, 3 and 4 signals. Foetal fibroblasts showed both 47,XX,+12 and 47,XX,+i(12)(p10) karyotypes. DNA analysis revealed the isochromosome to be paternal in origin, whilst the other two foetal chromosomes 12 were maternal, part iso- and part heterodisomy., Conclusion: The cytogenetic and DNA constitution of the foetus indicated the isochromosome 12p to be of paternal origin, and implied post-zygotic formation of the isochromosome 12p in the Pallister-Killian syndrome., (Copyright (c) 2004 John Wiley & Sons, Ltd.)

Published

2004

29. Novel pore mutation in SCN5A manifests as a spectrum of phenotypes ranging from atrial flutter, conduction disease, and Brugada syndrome to sudden cardiac death.

Author

Rossenbacker T, Carroll SJ, Liu H, Kuipéri C, de Ravel TJ, Devriendt K, Carmeliet P, Kass RS, and Heidbüchel H

Subjects

Adolescent, Adult, DNA Mutational Analysis, Electrocardiography, Female, Heterozygote, Humans, Male, Middle Aged, Mutation, NAV1.5 Voltage-Gated Sodium Channel, Phenotype, Syndrome, Atrial Flutter genetics, Bundle-Branch Block genetics, Heart Conduction System physiopathology, Sodium Channels genetics, Ventricular Fibrillation genetics

Abstract

Objectives: The purpose of this study was to determine the clinical and biophysical characteristics of a novel SCN5A mutation., Background: Brugada syndrome and isolated cardiac conduction defect have been linked to SCN5A mutations., Methods: Eleven members of a western European family underwent electrophysiologic investigations and mutation analysis of the SCN5A gene. Wild-type and mutant SCN5A channels were expressed in HEK293 cells, and whole cell currents were studied using patch clamp procedures., Results: A novel mutation, R376H, in the first pore segment of SCN5A variably causes Brugada syndrome and/or conduction disease in a single family. Biophysical analysis demonstrated a significant current reduction for the mutant, a pathophysiologic profile consistent with Brugada syndrome and isolated cardiac conduction defect. Among 11 family members, 9 were carriers of the mutation. The proband's initial presentation was a saddleback Brugada ECG, atrial flutter, and diffuse conduction disturbances. He had no inducible ventricular arrhythmias but experienced sudden cardiac death. His brother was affected by atrial flutter and had a clear conduction disorder, but he did not display baseline or evocable ECG signs of Brugada syndrome. He received an implantable cardioverter-defibrillator that delivered one appropriate shock after 1 year of follow-up. The phenotype in the family members was highly variable and ranged from noninducible and inducible asymptomatic carriers of the mutations to isolated conduction disease and to symptomatic Brugada syndrome., Conclusions: We describe the functional characterization of a novel SCN5A pore mutation, R376H, with variable clinical expression in the same family. Differentiating between electrophysiologic entities (Brugada syndrome-isolated cardiac conduction defect) is more challenging. Recognition of factors modifying the clinical presentation may be important for clinical decision making.

Published

2004

30. Macrocephaly, mental retardation, dysmorphism, and spastic paraplegia.

Author

de Ravel TJ, Van Driessche J, and Fryns JP

Subjects

Adult, Female, Humans, Brain abnormalities, Facies, Intellectual Disability pathology, Paraplegia pathology

Published

2004

31. Bilateral complete radioulnar synostosis associated with ectrodactyly and sensorineural hearing loss: a variant of SHFM1.

Author

Debeer P, Vandenbossche L, de Ravel TJ, Desloovere C, De Smet L, Huysmans C, Thoelen R, Vermeesch J, Van de Ven WJ, and Fryns JP

Subjects

Abnormalities, Multiple genetics, Foot Deformities, Congenital genetics, Hand Deformities, Congenital genetics, Humans, Infant, Newborn, Male, Radiography, Synostosis genetics, Abnormalities, Multiple diagnostic imaging, Foot Deformities, Congenital diagnostic imaging, Hand Deformities, Congenital diagnostic imaging, Hearing Loss, Sensorineural genetics, Radius diagnostic imaging, Synostosis diagnostic imaging, Ulna diagnostic imaging

Published

2004

32. Complex chromosome re-arrangement 45,X,t(Y;9) in a girl with sex reversal and mental retardation.

Author

de Ravel TJ, Fryns JP, Van Driessche J, and Vermeesch JR

Subjects

Abnormalities, Multiple pathology, Child, Chromosome Banding, Female, Humans, In Situ Hybridization, Fluorescence, Karyotyping, Abnormalities, Multiple genetics, Chromosomes, Human, Pair 9 genetics, Chromosomes, Human, Y genetics, Disorders of Sex Development, Intellectual Disability pathology, Translocation, Genetic

Abstract

A girl with mental retardation and multiple minor anomalies was found to have a complex chromosome 9p re-arrangement comprising a deleted, translocated Y chromosome, a deletion of the sex reversal gene region (DMRT1) at 9p, together with an inverted duplication of the more proximal part of 9p. The karyotype was 45,X,der(Y;9)(Ypter-->Yq12::9p21.1-->9p22.2::9p22.2-->9qter) de novo. The karyotypic male, phenotypic female had a dysgerminoma of the left dysplastic ovary. The patient had typical 'trisomy 9p' syndrome, and we propose that the critical region for this phenotype is located between 9p22.1 and 9p22.2., (Copyright 2003 Wiley-Liss, Inc.)

Published

2004

33. De novo interstitial tandem duplication of chromosome 20p12.1p13.

Author

de Ravel TJ, Vermeesch JR, and Fryns JP

Subjects

Child, Preschool, Chromosome Banding, Female, Gene Duplication, Humans, In Situ Hybridization, Fluorescence, Karyotyping, Chromosome Aberrations, Chromosomes, Human, Pair 20 genetics

Abstract

We report the first case of an individual with a de novo interstitial tandem duplication of the short arm of chromosome 20p12.1p13, discuss the clinical features, and propose the possible underlying mechanism of formation., (Copyright 2002 Wiley-Liss, Inc.)

Published

2003

34. Apparently new autosomal dominant Spondyloepimetaphyseal dysplasia: gonadal mosaicism onset.

Author

de Ravel TJ, De Smet L, and Fryns JP

Subjects

Adolescent, Adult, Child, Preschool, Collagen Type II genetics, Family Health, Female, Genes, Dominant, Hip Joint abnormalities, Humans, Knee Joint abnormalities, Spine abnormalities, Mosaicism genetics, Mosaicism pathology, Osteochondrodysplasias genetics, Osteochondrodysplasias pathology

Abstract

We report a family in which an apparently previously undescribed form of Spondyloepimetaphyseal dysplasia (SEMD) presented after probable gonadal mosaicism occurred and is inherited in an autosomal dominant mode. The other autosomal dominant SEMDs are compared.

Published

2002

35. Human homologues of Osr1 and Osr2 are not involved in a syndrome with distal limb deficiencies, oral abnormalities, and renal defects.

Author

Debeer P, de Ravel TJ, Devriendt K, Fryns JP, Huysmans C, and Van de Ven WJ

Subjects

Animals, Humans, Kidney abnormalities, Limb Deformities, Congenital genetics, Mice, Molecular Sequence Data, Mouth Abnormalities genetics, Organ Specificity genetics, Polymerase Chain Reaction, Abnormalities, Multiple genetics, Transcription Factors genetics

Published

2002

36. Familial adenomatous polyposis in two Black South African families.

Author

Grobbelaar JJ, Wilken E, de Ravel TJ, Nicholson DL, and Kotze MJ

Subjects

Adult, Autoradiography, Black People genetics, Female, Genetic Heterogeneity, Humans, Male, Middle Aged, Pedigree, South Africa, Adenomatous Polyposis Coli genetics

Abstract

The apparent low incidence of colon cancer in the Black population of South Africa has been ascribed to a non-Western diet. The present authors report the identification of two common 5-bp deletions at codons 1309 and 1061 of the adenomatous polyposis coli (APC) gene in a Xhosa and Zulu patient, respectively. The in vitro transcription/translation test (PTT) and a non-radioactive heteroduplex method, which facilitates resolution of enzymatically amplified DNA by agarose gel electrophoresis, were used for mutation detection. This study represents the first report of APC mutations in indigenous Black individuals clinically diagnosed with familial adenomatous polyposis coli (FAP). The two deletion mutations are responsible for FAP in 35% of affected South Africans, a frequency similar to that described in several other non-African populations. The apparently low incidence of colon cancer in the African population may be ascribed either to the rare occurrence of the 'second hit' needed for polyp formation or to a lower incidence of mutations in the APC gene.

Published

2002

37. Cohen syndrome and rheumatoid arthritis.

Author

De Ravel TJ, Azou M, and Fryns JR

Subjects

Humans, Infant, Newborn, Male, Syndrome, Abnormalities, Multiple, Arthritis, Juvenile congenital, Facies, Microcephaly

Published

2002

38. "A new association of mental retardation, short stature, unusual face, radio-ulnar synostosis and retinal pigment abnormalities": Cohen syndrome with thrombocytopenia.

Author

De Ravel TJ, Dillen K, and Fryns JP

Subjects

Humans, Male, Middle Aged, Syndrome, Abnormalities, Multiple pathology, Body Height, Facies, Intellectual Disability pathology, Retinal Pigments metabolism, Siblings, Thrombocytopenia pathology

Published

2002

39. Hemifacial microsomia in two patients further supporting chromosomal mosaicism as a causative factor.

Author

de Ravel TJ, Legius E, Brems H, Van Hoestenberghe R, Gillis PH, and Fryns JP

Subjects

Humans, Infant, Newborn, Male, Meiosis, Chromosome Aberrations, Chromosomes, Human, Pair 22, Chromosomes, Human, Pair 9, Facial Asymmetry genetics, Mosaicism pathology

Abstract

We report two cases with hemifacial microsomia with body asymmetry associated with mosaic trisomies. The child with mosaic trisomy 9 had skin pigmentary changes. In the boy with mosaic trisomy 22, the extra chromosome 22 originated from a maternal meiosis I error.

Published

2001

40. An unbalanced translocation 46,XX,+der(18)t(18;21)(q12.2;q11.2)mat,-21 associated with maternal isodisomy 18pter-->18q12.2.

Author

de Ravel TJ, Matthijs G, and Fryns J

Subjects

Centromere genetics, Child, Preschool, Crossing Over, Genetic genetics, Female, Humans, In Situ Hybridization, Fluorescence, Infant, Infant, Newborn, Karyotyping, Male, Phenotype, Polymorphism, Genetic genetics, Abnormalities, Multiple genetics, Chromosomes, Human, Pair 18 genetics, Chromosomes, Human, Pair 21 genetics, Translocation, Genetic genetics, Uniparental Disomy genetics

Abstract

We report a patient with a 46,XX,+der(18)t(18;21)(q12.2;q11.2)mat,-21 karyotype, in whom the rarely seen adjacent-2 segregation (according to the predicted pachytene diagram model) as well as two cross-overs, resulted in maternal isodisomy 18pter-->18q12.2.

Published

2001

41. The ICF syndrome: new case and update.

Author

De Ravel TJ, Deckers E, Alliet PL, Petit P, and Fryns JP

Subjects

Child, Preschool, Chromosome Aberrations, Chromosomes, Human, Pair 1, Chromosomes, Human, Pair 16, Female, Genetic Heterogeneity, Humans, Karyotyping, Male, Syndrome, gamma-Globulins therapeutic use, Agammaglobulinemia genetics, Agammaglobulinemia therapy, Centromere, Face abnormalities

Abstract

The ICF syndrome: New case and update: We report the clinical progress in a 5-year-old boy with the <> (ICF) syndrome. Early diagnosis and intervention has led to a good outcome. DNMT3B mutation analysis was negative, supporting genetic heterogeneity in this condition.

Published

2001

42. Possible isochromosome 22 leading to trisomy 22.

Author

Manasse BF, Pfaffenzeller WM, Gurtunca N, and de Ravel TJ

Subjects

Adult, Face diagnostic imaging, Female, Genitalia, Female diagnostic imaging, Growth Disorders genetics, Humans, Infant, Newborn, Karyotyping, Male, Monosomy, Phenotype, Pregnancy, Pregnancy Complications, Ultrasonography, Abnormalities, Multiple genetics, Chromosomes, Human, Pair 22 genetics, Face abnormalities, Genitalia, Female abnormalities, Heart Septal Defects, Atrial genetics, Heart Septal Defects, Ventricular genetics, Isochromosomes genetics, Trisomy genetics

Abstract

We describe the first case of trisomy 22 resulting from a monocentric, possible isochromosome 22. The female infant had multiple anomalies including an abnormal face, ambiguous genitalia, and both ventricular and atrial septal defects. Survival was short., (Copyright 2000 Wiley-Liss, Inc.)

Published

2000

43. Idiopathic multicentric osteolysis presents early and is not linked to chromosome 18q21.1.

Author

De Ravel TJ, Matthijs G, Holvoet M, Wouters C, Legius E, and Fryns JP

Subjects

Adult, Child, DNA genetics, Family Health, Female, Foot Deformities, Genetic Linkage, Hand Deformities, Humans, Lod Score, Male, Maxillofacial Abnormalities, Microsatellite Repeats, Osteolysis, Essential pathology, Pedigree, Chromosomes, Human, Pair 18 genetics, Osteolysis, Essential genetics

Published

2000

44. The Pallister-Killian syndrome is reliably diagnosed by FISH on buccal mucosa.

Author

Manasse BF, Lekgate N, Pfaffenzeller WM, and de Ravel TJ

Subjects

Abnormalities, Multiple genetics, Child, Developmental Disabilities genetics, Humans, In Situ Hybridization, Fluorescence, Intellectual Disability genetics, Syndrome, Abnormalities, Multiple diagnosis, Chromosomes, Human, Pair 12, Developmental Disabilities diagnosis, Intellectual Disability diagnosis, Mosaicism, Mouth Mucosa

Abstract

The Pallister-Killian syndrome is a rare disorder, which is clinically diagnosed and usually confirmed by the detection of mosaicism for an isochromosome 12p in fibroblast cultures. To date FISH on buccal mucosa has been used in only three cases and this detected high levels of mosaicism for the isochromosome. We review one previously reported case [Woodman et al. (1995) Genet Couns 6:33-36] and report a further seven clinically suspected cases in which the diagnoses were confirmed by FISH on buccal mucosa, and recommend that this tissue be used routinely for laboratory confirmation. The presence of the isochromosome 12p at levels as low as 1% is acceptable.

Published

2000

45. Trichorhinophalangeal syndrome type II: case report.

Author

Lambie L and de Ravel TJ

Subjects

Child, Preschool, Cytogenetics, Gene Deletion, Genetic Counseling, Humans, Langer-Giedion Syndrome genetics, Male, Mutation genetics, Prognosis, South Africa, Langer-Giedion Syndrome diagnosis, Langer-Giedion Syndrome therapy

Abstract

Patients with the trichorhinophalangeal syndrome type II, also known as the Langer-Giedion syndrome, may present to the health care-givers or physicians in various specialties and need to be recognised in order that accurate diagnosis, management and counselling about prognosis and recurrence risks may be carried out. A case of young male with this condition is presented.

Published

2000

46. Amniocentesis--too dangerous and too late?

Author

Viljoen D, Kromberg J, de Ravel TJ, Krause A, Donaldson S, Craig P, and Oliveira V

Subjects

Abortion, Legal psychology, Adult, Chromosome Aberrations psychology, Chromosome Disorders, Female, Genetic Counseling psychology, Genetic Counseling standards, Humans, Pregnancy, Amniocentesis psychology, Maternal Age, Pregnancy, High-Risk

Published

1999

47. Trisomy 18 with total cranio-rachischisis and thoraco-abdominoschisis.

Author

Donaldson SJ, Wright CA, and de Ravel TJ

Subjects

Anencephaly genetics, Female, Humans, Male, Pregnancy, Abdomen abnormalities, Abnormalities, Multiple pathology, Anencephaly pathology, Chromosomes, Human, Pair 18, Thorax abnormalities, Trisomy pathology

Abstract

We describe a further case of trisomy 18 with total cranio-rachischisis and radial agenesis, and report the first case with thoraco-abdominoschisis. We review these rare findings in trisomy 18.

Published

1999

48. Hydrolethalus syndrome in a non-Finnish family: confirmation of the entity and early prenatal diagnosis.

Author

de Ravel TJ, van der Griendt MC, Evan P, and Wright CA

Subjects

Alleles, Female, Finland, Germany ethnology, Humans, Male, Portugal ethnology, Pregnancy, Pregnancy Trimester, First, South Africa, Syndrome, Abnormalities, Multiple diagnostic imaging, Hydrocephalus diagnostic imaging, Polyhydramnios diagnostic imaging, Ultrasonography, Prenatal

Abstract

We present a family in which the first affected child presented with a 'milder' form of the hydrolethalus syndrome and survived to seven months, and two subsequent pregnancies with typical features detected early by ultrasound evaluation. We propose that the 'milder' cases are indeed true cases of the hydrolethalus syndrome and that allelic variability may be responsible for these 'non-typically Finnish' findings. We also demonstrate that, especially in families where there has been a previously affected fetus, echographic diagnosis can be made in the first trimester, as early as the 11th week of gestation.

Published

1999

49. Brachydactyly type B with its distinct facies and 'Cooks syndrome' are the same entity.

Author

de Ravel TJ, Berkowitz DE, Wagner JM, and Jenkins T

Subjects

Child, Female, Humans, Male, Syndrome, Facies, Fingers abnormalities, Foot Deformities, Congenital pathology, Hand Deformities, Congenital pathology, Nuclear Family

Abstract

A sibling pair with brachydactyly type B born to a normal non-consanguineous couple are described and the severity of their condition discussed. It is proposed that a subgroup of individuals with brachydactyly type B principally involving the nails and distal phalanges, and also having distinct facies, might be identical to individuals having 'Cooks syndrome'.

Published

1999

50. Trisomy 8 mosaicism: a further five cases illustrating marked clinical and cytogenetic variability.

Author

Jordan MA, Marques I, Rosendorff J, and de Ravel TJ

Subjects

Adolescent, Adult, Chromosome Banding, Female, Humans, In Situ Hybridization, Fluorescence, Infant, Intellectual Disability, Intelligence, Male, Phenotype, Abnormalities, Multiple diagnosis, Abnormalities, Multiple pathology, Abnormalities, Multiple psychology, Chromosomes, Human, Pair 8, Mosaicism, Trisomy

Abstract

Trisomy 8 mosaicism is extremely variable in its phenotypic and cytogenic expression. We present five patients clearly demonstrating the lack of correlation between clinical and laboratory findings, and show that the aneuploid cell lines decreases with time in relation to the normal. This poses a counseling dilemma.

Published

1998