Your search keyword '"Fryns J"' showing total 40 results

1. Congenital hydrocephalus: nosology and guidelines for clinical approach and genetic counselling.

Author

Schrander-Stumpel, C. and Fryns, J.-P.

Subjects

*HYDROCEPHALUS, *CEREBROSPINAL fluid, *PRENATAL diagnosis, *RELATIVE medical risk, *DISEASE incidence, *PREVENTION

Abstract

Unlabelled: Congenital hydrocephalus is a serious condition that can arise from multiple causes. It comprises a diverse group of conditions which result in impaired circulation and absorption of cerebrospinal fluid. Congenital malformations of the central nervous system, infections, haemorrhage, trauma, teratogens and, occasionally, tumours can all give rise to hydrocephalus. In this paper we focus on the genetic aspects of hydrocephalus, excluding neural tube defects. The incidence is 0.4-0.8 per 1000 liveborns and stillbirths. X-linked hydrocephalus comprises approximately 5% of all cases. This condition is caused by mutations in the gene at Xq28 encoding for L1, a neural cell adhesion molecule. Carrier detection and prenatal diagnosis can be offered to affected families by means of chorionic villus biopsy and linkage analysis or L1 mutation analysis. In general, recurrence risk for congenital hydrocephalus excluding X-linked hydrocephalus, is low; empiric risk figures found in various studies range from <1% to 4%. Unfortunately, prenatal diagnosis based on an early ultrasound scan is not always reliable as ventriculomegaly usually starts after 20 weeks of gestation. We stress the importance of additional clinical investigations. Prognosis in the prenatally diagnosed patients depends on additional malformations but in general, is not very good.Conclusion: Congenital hydrocephalus may be non-syndromic and syndromic. Prognosis depends primarily on the underlying cause and/or associated malformations, which have to be delineated on the basis of clinical, cytogenetic and molecular analysis. [ABSTRACT FROM AUTHOR]

Published

1998

2. DISC1 duplication in two brothers with autism and mild mental retardation.

Author

Crepel, A., Breckpot, J., Fryns, J.-P., De la Marche, W., Steyaert, J., Devriendt, K., and Peeters, H.

Subjects

*BIPOLAR disorder, *AUTISM, *INTELLECTUAL disabilities, *ASPERGER'S syndrome, *PHENOTYPES

Abstract

Crepel A, Breckpot J, Fryns J-P, De la Marche W, Steyaert J, Devriendt K, Peeters H. DISC1 duplication in two brothers with autism and mild mental retardation. We describe the identification and delineation of an inherited 2.07 Mb microduplication in 1q42.2 in two brothers with autism and mild mental retardation. Since this duplication was not present in 1577 Belgian persons, we consider this as an extremely rare variant which has the potential to provide further insight into the genetics of autism. The duplication contains seven genes including the DISC1 gene, an interesting candidate gene that has been associated to schizophrenia, bipolar disorder, autism and Asperger syndrome. In this report we describe additional analyses undertaken to investigate the causal relationship of the duplication to the autism phenotype. We conclude that the 1q42.2 microduplication probably confers susceptibility to autism in the current family. This study is a typical illustration of the difficult interpretation of causality of a very rare variant in neuropsychiatric disease and the challenge of genetic counselling in a particular family. [ABSTRACT FROM AUTHOR]

Published

2010

3. Intellectual abilities in a large sample of children with Velo-Cardio-Facial Syndrome: an update.

Author

De Smedt B, Devriendt K, Fryns J, Vogels A, Gewillig M, and Swillen A

Abstract

BACKGROUND: Learning disabilities are one of the most consistently reported features in Velo-Cardio-Facial Syndrome (VCFS). Earlier reports on IQ in children with VCFS were, however, limited by small sample sizes and ascertainment biases. The aim of the present study was therefore to replicate these earlier findings and to investigate intellectual abilities in a large sample of children with VCFS. In addition, we aimed to identify factors that may contribute to within-syndrome variability in cognitive performance, such as the mode of inheritance of the deletion, sex, the presence of a heart defect and psychiatric morbidity. METHOD: IQ data of 103 children with VCFS (56 males, 47 females) were collected. Psychiatric diagnosis was additionally recorded. RESULTS: Children with VCFS had a mean full-scale IQ (FSIQ) of 73.48 (range: 50-109). There were no effects of sex, presence of a heart defect and psychiatric condition on intellectual profile. Inheritance of the deletion affected cognitive performance in VCFS, with children with familial deletions having significant lower FSIQ than children with a de novo deletion. CONCLUSIONS: Learning disabilities are very common in children with VCFS, although marked within syndrome variability is noted. One factor contributing to this variability seems to be the mode of inheritance of the deletion. [ABSTRACT FROM AUTHOR]

Published

2007

4. Intellectual abilities in a large sample of children with Velo–Cardio–Facial Syndrome: an update.

Author

De Smedt, B., Devriendt, K., Fryns, J.‐P., Vogels, A., Gewillig, M., and Swillen, A.

Subjects

*DEVELOPMENTAL disabilities research, *PHENOTYPES, *GENETICS, *VELOCARDIOFACIAL syndrome, *FACIAL abnormalities, *GENETIC disorders

Abstract

Background Learning disabilities are one of the most consistently reported features in Velo–Cardio–Facial Syndrome (VCFS). Earlier reports on IQ in children with VCFS were, however, limited by small sample sizes and ascertainment biases. The aim of the present study was therefore to replicate these earlier findings and to investigate intellectual abilities in a large sample of children with VCFS. In addition, we aimed to identify factors that may contribute to within-syndrome variability in cognitive performance, such as the mode of inheritance of the deletion, sex, the presence of a heart defect and psychiatric morbidity. Method IQ data of 103 children with VCFS (56 males, 47 females) were collected. Psychiatric diagnosis was additionally recorded. Results Children with VCFS had a mean full-scale IQ (FSIQ) of 73.48 (range: 50–109). There were no effects of sex, presence of a heart defect and psychiatric condition on intellectual profile. Inheritance of the deletion affected cognitive performance in VCFS, with children with familial deletions having significant lower FSIQ than children with a de novo deletion. Conclusions Learning disabilities are very common in children with VCFS, although marked within syndrome variability is noted. One factor contributing to this variability seems to be the mode of inheritance of the deletion. [ABSTRACT FROM AUTHOR]

Published

2007

5. Molecular cytogenetic characterization of a constitutional complex intrachromosomal 4q rearrangement in a patient with multiple congenital anomalies.

Author

Thienpont, B., Gewillig, M., Fryns, J.-P., Devriendt, K., and Vermeesch, J.

Subjects

*CYTOGENETICS, *HUMAN abnormalities, *COMPARATIVE genomic hybridization, *PHENOTYPES, *TRISOMY, *GENETICS

Abstract

Constitutional Complex Chromosomal Rearrangements (CCRs) are very rare. While the vast majority of CCRs involve more than one chromosome, only seven cases describe CCRs with four or more breakpoints within a single chromosome. Here, we present a patient with multiple congenital anomalies and mental retardation. Array Comparative Genomic Hybridisation (array CGH), FISH and Multicolour Banding FISH revealed a de novo complex rearrangement with two deletions, a duplication and an inversion of 4q. This CCR involving at least seven breakpoints is one of the most complex rearrangements of a single chromosome reported thus far. Potential mechanisms generating such complex rearrangements are discussed. Copyright © 2006 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2006

6. Ring syndrome caused by ring chromosome 7 without loss of subtelomeric sequences.

Author

Vermeesch, JR, Baten, E, Fryns, J-P, and Devriendt, K

Subjects

*CHROMOSOME abnormalities, *MEDICAL genetics

Abstract

Ring chromosome 7 is an unusual chromosome anomaly. Here we describe a patient with ring chromosome 7 and we show that both subtelomeres are still present. The diagnosis agrees with ‘ring syndrome’. This report helps to further delineate the clinical manifestations of ‘ring syndrome’ and to distinguish the phenotypic consequences of the presence of a ring chromosome 7 from the phenotypic consequences of terminal chromosome 7 submicroscopic deletions. [ABSTRACT FROM AUTHOR]

Published

2002

7. A case of left isomerism with early fetal decompensation.

Author

Witters, I., Debois, P., Fryns, J. P., Devriendt, K., and Gewillig, M.

Subjects

*LETTERS to the editor, *FETAL heart abnormalities

Abstract

A letter to the editor is presented about a case of left isomerism with fetal heart abnormalities.

Published

2007

8. Holoprosencephaly and ZIC2 microdeletions: novel clinical and epidemiological specificities delineated.

Author

Chabchoub, E, Willekens, D, Vermeesch, JR, and Fryns, J-P

Subjects

*HOLOPROSENCEPHALY, *DELETION mutation, *GENETIC mutation, *HUMAN cytogenetics, *PHENOTYPES, *HETEROGENEITY

Abstract

Chabchoub E, Willekens D, Vermeesch JR, Fryns J-P. Holoprosencephaly and ZIC2 microdeletions: novel clinical and epidemiological specificities delineated. Holoprosencephaly (HPE), the most common malformation of the human brain results from abnormal cleavage of the forebrain during the early embryonic developmental stages. The spectrum of malformations in HPE is wide, ranging from the classical cyclopia/proboscis to fairly asymptomatic forms [i.e. a single maxillary central incisor (SMCI)]. HPE may be caused by environmental or genetic factors. ZIC2 (13q32) was the second gene identified in which mutations cause HPE and recently a specific phenotype was ascribed to ZIC2-mutation HPE. Earlier, we reported a boy presenting HPE and deafness. Cytogenetic analyses were normal. Using array-comparative genomic hybridization (aCGH), we found a de novo 129 kb del(13)(q32) encompassing ZIC2 and ZIC5. There is no evidence for the involvement of ZIC5 in human diseases. We reviewed the literature for ZIC2- ZIC5 deletions and their involvement in neural tube defects (NTDs). Interestingly, we found evidence for a specific facial phenotype for ZIC2 gene deletion patients distinct from those with point mutations. In addition, based on the clinical data together with pathology, imaging and functional studies, we suggest an outline for a model explaining the genetic heterogeneity of ZIC2- ZIC5-associated NTDs and propose further studies for validation. [ABSTRACT FROM AUTHOR]

Published

2012

9. Mutations of the UPF3B gene, which encodes a protein widely expressed in neurons, are associated with nonspecific mental retardation with or without autism.

Author

Laumonnier, F., Shoubridge, C., Antar, C., Nguyen, L. S., Van Esch, H., Kleefstra, T., Briault, S., Fryns, J. P., Hamel, B., Chelly, J., Ropers, H. H., Ronce, N., Blesson, S., Moraine, C., G.écz, J., and Raynaud, M.

Subjects

*INTELLECTUAL disabilities, *AUTISM, *X chromosome abnormalities, *NEURAL transmission, *QUANTITATIVE research, *MESSENGER RNA, *HIPPOCAMPUS (Brain)

Abstract

Mutations in the UPF3B gene, which encodes a protein involved in nonsense-mediated mRNA decay, have recently been described in four families with specific (Lujan–Fryns and FG syndromes), nonspecific X-linked mental retardation (XLMR) and autism. To further elucidate the contribution of UPF3B to mental retardation (MR), we screened its coding sequence in 397 families collected by the EuroMRX consortium. We identified one nonsense mutation, c.1081C>T/p.Arg361*, in a family with nonspecific MR (MRX62) and two amino-acid substitutions in two other, unrelated families with MR and/or autism (c.1136G>A/p.Arg379His and c.1103G>A/p.Arg368Gln). Functional studies using lymphoblastoid cell lines from affected patients revealed that c.1081C>T mutation resulted in UPF3B mRNA degradation and consequent absence of the UPF3B protein. We also studied the subcellular localization of the wild-type and mutated UPF3B proteins in mouse primary hippocampal neurons. We did not detect any obvious difference in the localization between the wild-type UPF3B and the proteins carrying the two missense changes identified. However, we show that UPF3B is widely expressed in neurons and also presents in dendritic spines, which are essential structures for proper neurotransmission and thus learning and memory processes. Our results demonstrate that in addition to Lujan–Fryns and FG syndromes, UPF3B protein truncation mutations can cause also nonspecific XLMR. We also identify comorbidity of MR and autism in another family with UPF3B mutation. The neuronal localization pattern of the UPF3B protein and its function in mRNA surveillance suggests a potential function in the regulation of the expression and degradation of various mRNAs present at the synapse. [ABSTRACT FROM AUTHOR]

Published

2010

10. Novel PORCN mutations in focal dermal hypoplasia.

Author

Froyen, G., Govaerts, K., van Esch, H., Verbeeck, J., Tuomi, M.-L., Heikkilä, H., Torniainen, S., Devriendt, K., Fryns, J.-P., Marynen, P., Järvel, I., and Ala-Mello, S.

Subjects

*GENETIC disorders, *CHROMOSOME abnormalities, *GENETIC mutation, *GENETICS, *PHENOTYPES

Abstract

Focal dermal hypoplasia (FDH), Goltz or Goltz–Gorlin syndrome, is an X-linked dominant multisystem disorder characterized primarily by involvement of the skin, skeletal system and eyes. We screened for mutations in the PORCN gene in eight patients of Belgian and Finnish origin with firm clinical suspicion of FDH. First, we performed quantitative PCR (qPCR) analysis to define the copy number at this locus. Next, we sequenced the coding regions and flanking intronic sequences of the PORCN gene. Three de novo mutations were identified in our patients with FDH: a 150-kb deletion removing six genes including PORCN, as defined by qPCR and X-array-CGH, and two heterozygous missense mutations; c.992T>G (p.L331R) in exon 11 and c.1094G>A (p.R365Q) in exon 13 of the gene. Both point mutations changed highly conserved amino acids and were not found in 300 control X chromosomes. The three patients in whom mutations were identified all present with characteristic dermal findings together with limb manifestations, which were not seen in our mutation-negative patients. The clinical characteristics of our patients with PORCN mutations were compared with the previously reported mutation-positive cases. In this report, we summarize the literature on PORCN mutations and associated phenotypes. [ABSTRACT FROM AUTHOR]

Published

2009

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

Author

de Ravel, T. J. L., Balikova, I., Thienpont, B., Hannes, F., Maas, N., Fryns, J. -P., Devriendt, K., and Vermeesch, J. R.

Subjects

*KARYOTYPES, *HUMAN abnormalities, *CHROMOSOME abnormalities, *INTELLECTUAL disabilities, *FAMILIAL diseases, *HUMAN genome

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 © 2006 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2006

12. Alterations of uromodulin biology: a common denominator of the genetically heterogeneous FJHN/MCKD syndrome.

Author

Vylet'al, P., Kublová, M., Kalbáčová, M., Hodaňová, K., Barešová, V., Stibůrková, B., Sikora, J., Hůlková, H., Živný, J., Majewski, J., Simmonds, A., Fryns, J.-P., Venkat-Raman, G., Elleder, M., and Kmoch, S.

Subjects

*HYPERURICEMIA, *GLYCOSYLATION, *PHENOTYPES, *KIDNEY tubules, *CYSTIC kidney disease, *DISEASES

Abstract

Autosomal dominant hyperuricemia, gout, renal cysts, and progressive renal insufficiency are hallmarks of a disease complex comprising familial juvenile hyperuricemic nephropathy and medullary cystic kidney diseases type 1 and type 2. In some families the disease is associated with mutations of the gene coding for uromodulin, but the link between the genetic heterogeneity and mechanism(s) leading to the common phenotype symptoms is not clear. In 19 families, we investigated relevant biochemical parameters, performed linkage analysis to known disease loci, sequenced uromodulin gene, expressed and characterized mutant uromodulin proteins, and performed immunohistochemical and electronoptical investigation in kidney tissues. We proved genetic heterogeneity of the disease. Uromodulin mutations were identified in six families. Expressed, mutant proteins showed distinct glycosylation patterns, impaired intracellular trafficking, and decreased ability to be exposed on the plasma membrane, which corresponded with the observations in the patient's kidney tissue. We found a reduction in urinary uromodulin excretion as a common feature shared by almost all of the families. This was associated with case-specific differences in the uromodulin immunohistochemical staining patterns in kidney. Our results suggest that various genetic defects interfere with uromodulin biology, which could lead to the development of the common disease phenotype. ‘Uromodulin-associated kidney diseases’ may be thus a more appropriate term for this syndrome.Kidney International (2006) 70, 1155–1169. doi:10.1038/sj.ki.5001728; published online 2 August 2006 [ABSTRACT FROM AUTHOR]

Published

2006

13. Novel GJA1 mutations in patients with oculo-dento-digital dysplasia (ODDD)

Author

Debeer, Ph., Van Esch, H., Huysmans, C., Pijkels, E., De Smet, L., Van de Ven, W., Devriendt, K., and Fryns, J.-P.

Subjects

*DYSPLASIA, *FAMILIES, *CELLULAR pathology, *PEDIATRIC physiology

Abstract

Abstract: Oculo-dento-digital dysplasia (ODDD) is an autosomal dominant disorder characterized by developmental anomalies of the face, the eyes, the limbs and the teeth. Patients with ODDD usually present with complete syndactyly of the fourth and fifth fingers (type III syndactyly), ocular changes, abnormalities of primary and permanent dentition and specific craniofacial malformations. Mutations in GJA1, a gene that encodes the gap junction protein connexin 43, are responsible for ODDD. Gap junctions are assemblies of intercellular channels that allow exchange of various ions and signaling molecules between cells. In this way, gap junctions play an important regulatory role in a variety of physiologic and developmental processes. We identified three novel and one previously described GJA1 mutation in two large ODDD families and two sporadic ODDD cases. [Copyright &y& Elsevier]

Published

2005

14. Deletions Involving Long-Range Conserved Nongenic Sequences Upstream and Downstream of FOXL2 as a Novel Disease-Causing Mechanism in Blepharophimosis Syndrome.

Author

Beysen, D., Raes, J., Leroy, B. P., Lucassen, A., Yates, J. R. W., Clayton-Smith, J., Ilyina, H., Brooks, S. Sklower, Christin-Maitre, S., Fellous, M., Fryns, J. P., Kim, J. R., Lapunzina, P., Lemyre, F., Meire, F., Messiaen, L. M., Oley, C., Splitt, M., Thomson, J., and Van de Peer, Y.

Subjects

*GENES, *GENE expression, *GENETIC regulation, *GENETIC code, *NUCLEOTIDE sequence, *BINDING sites

Abstract

The expression of a gene requires not only a normal coding sequence but also intact regulatory regions, which can be located at large distances from the target genes, as demonstrated for an increasing number of developmental genes. In previous mutation studies of the role of FOXL2 in blepharophimosis syndrome (BPES), we identified intragenic mutations in 70% of our patients. Three translocation breakpoints upstream of FOXL2 in patients with BPES suggested a position effect. Here, we identified novel microdeletions outside of FOXL2 in cases of sporadic and familial BPES. Specifically, four rearrangements, with an overlap of 126 kb, are located 230 kb upstream of FOXL2, telomeric to the reported translocation breakpoints. Moreover, the shortest region of deletion overlap (SRO) contains several conserved nongenic sequences (CNGs) harboring putative transcription-factor binding sites and representing potential long-range cis-regulatory elements. Interestingly, the human region orthologous to the 12-kb sequence deleted in the polled intersex syndrome in goat, which is an animal model for BPES, is contained in this SRO, providing evidence of human-goat conservation of FOXL2 expression and of the mutational mechanism. Surprisingly, in a fifth family with BPES, one rearrangement was found downstream of FOXL2. In addition, we report nine novel rearrangements encompassing FOXL2 that range from partial gene deletions to submicroscopic deletions. Overall, genomic rearrangements encompassing or outside of FOXL2 account for 16% of all molecular defects found in our families with BPES. In summary, this is the first report of extragenic deletions in BPES, providing further evidence of potential long-range cis-regulatory elements regulating FOXL2 expression. It contributes to the enlarging group of developmental diseases caused by defective distant regulation of gene expression. Finally, we demonstrate that CNGs are candidate regions for genomic rearrangements in developmental genes. [ABSTRACT FROM AUTHOR]

Published

2005

15. The del(2)(q32.2q33) deletion syndrome defined by clinical and molecular characterization of four patients

Author

Van Buggenhout, G., Van Ravenswaaij-Arts, C., MC Maas, N., Thoelen, R., Vogels, A., Smeets, Dominique, Salden, I., Matthijs, G., Fryns, J.-P., and Vermeesch, J.R.

Subjects

*GENETICS, *DEVELOPMENTAL disabilities, *PEOPLE with intellectual disabilities, *HEREDITY

Abstract

Abstract: We report four patients with an interstitial deletion of chromosome 2q32 → 2q33. They presented similar clinical findings including pre- and postnatal growth retardation, distinct facial dysmorphism, thin and sparse hair and fair built, micrognathia, cleft or high palate, relative macroglossia, dacrocystitis, persisting feeding difficulties, inguinal hernia and broad based gait. All were severely mentally retarded. Three patients had a specific behavioral phenotype with hyperactivity and motor restlessness, chaotic behavior, happy-personality but with periods of aggression and anxiety, sleeping problems and self-mutilation. (head-banging). Array CGH and fluorescence in situ hybridization (FISH) allowed us to delineate the deletion size and showed that the four patients share a 8.1 Mb minimal deleted region. Reviewing additional nine case reports of patients with similar deletions showed striking phenotypic similarities which enabled the delineation of the 2q32.2q33 syndrome. Deletion of 2q32 has been also associated with the wrinkly skin syndrome (WWS) and isolated cleft palate. Although the patients presented here shared many aspects of WWS, they did not had the wrinkly skin. All patients had a cleft or high palate, most likely as a result of hemizygosity for SATB2. A potential commonly deleted interval of the three patients with behavioral problems, excluding the deletion in the patient without behavioral problems, is at most 0.5 Mb in size harboring only two genes. [Copyright &y& Elsevier]

Published

2005

16. Behavioural, academic and neuropsychological profile of normally gifted Neurofibromatosis type 1 children.

Author

Descheemaeker, M.‐J., Ghesquière, P., Symons, H., Fryns, J. P., and Legius, E.

Subjects

*NEUROPSYCHOLOGY, *NEUROFIBROMATOSIS, *PHAKOMATOSES, *NEUROFIBROMA, *LANGUAGE disorders, *READING disability

Abstract

In the present study the neuropsychological, academic and social-emotional profiles were examined in Neurofibromatosis type 1 (NF1) children17 NF1 children (ages 7–11) with NF1 without serious medical problems and with a full scale IQ (FSIQ) above 70.Wechsler Intelligence Scale for Children-Revised (WISC-R), academic tests and an exhaustive neuropsychological test battery were administered in all children. Parents and teachers filled out the Child Behavioural Checklist (CBCL) and Teacher Report Form (TRF), respectively, the NF1 children the Experienced Competence Scale for Children (ECSC).Nearly 50% (8/17) of the children showed learning disabilities, when corrected for IQ in the academic evaluations. Isolated impaired literacy skills, particularly spelling problems, were most frequent (4/8), whereas a pure arithmetic learning disability was rare (1/8). Three children presented both learning disabilities. Results on academic and neuropsychological tests did not fit the well-known types of learning disabilities– nonverbal learning disability (NLD) and dyslexia. Nearly all NF1 children showed visual perceptual and executive dysfunctions. In this study, teachers more frequently reported behavioural problems in NF1 children than parents, as opposed to literature data in a general population. The correspondence of the perception of internalizing problems between the children and teachers was greater than between children and their parents. No correlation was found between the performances on the WISC-R, specific neuropsychological results, academic performances and behavioural problems. The Deficiency in Attention, Motor and Perception (DAMP) concept seems most appropriate in order to describe the neuropsychological deficits and their repercussions on behavioural and academic performances seen in NF1 children. [ABSTRACT FROM AUTHOR]

Published

2005

17. Chromosomal anomalies in individuals with autism: a strategy towards the identification of genes involved in autism.

Author

Castermans D, Wilquet V, Steyaert J, Van De Ven W, Fryns J, and Devriendt K

Abstract

We review the different strategies currently used to try to identify susceptibility genes for idiopathic autism. Although identification of genes is usually straightforward in Mendelian disorders, it has proved to be much more difficult to establish in polygenic disorders like autism. Neither genome screens of affected siblings nor the large number of association studies using candidate genes have resulted in finding autism susceptibility genes. We focus on the alternative approach of 'positional cloning' through chromosomal aberrations in individuals with autism. In particular, balanced aberrations such as reciprocal translocations or inversions offer a unique opportunity, since only the genes in the breakpoint regions are candidate genes. This approach, in combination with others, is likely to produce results in the coming years. [ABSTRACT FROM AUTHOR]

Published

2004

18. Speech and language in Wolf-Hirschhorn syndrome: a case-study.

Author

Van Borsel J, De Grande S, Van Buggenhout G, and Fryns J

Published

2004

19. A physical map of the chromosome 12 centromere.

Author

Duhamel, H., Raeymaekers, P., Van Zand, K., Verhasselt, P., Fryns, J. P., Vermeesch, J. R., and Marynen, P.

Subjects

*HUMAN chromosome 12, *CENTROMERE, *HUMAN genome, *HUMAN gene mapping, *MICROSATELLITE repeats

Abstract

While current sequencing efforts consider the detection of alpha satellite repeats as logical end points for map construction, detailed maps of most pericentromeric regions are lacking to confirm this hypothesis. Here we identify the different alpha satellite families present at the pericentromeric region of chromosome 12. The order, size and location of these repeats is established using radiation hybrid analysis, pulsed field gel analysis and FISH and the maps are integrated with current sequence information. For the different classes of alpha satellites present at the chromosome 12 centromere the paralogs in the human genome were mapped by FISH. Unique sequences flanking the alpha satellite repeats were identified, some of which are not represented in the current draft sequence. This mapping effort localises the different alpha satellite repeats within the pericentromeric region and anchors them in the current maps. The novel sequences identified may serve as the end point for the ongoing sequencing efforts. Copyright © 2003 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2003

20. PA26 is a candidate gene for heterotaxia in humans: identification of a novel PA26-related gene family in human and mouse.

Author

Peeters, H., Debeer, P., Bairoch, A., Wilquet, V., Huysmans, C., Parthoens, E., Fryns, J. P., Gewillig, M., Nakamura, Y., Niikawa, N., Van de Ven, W., and Devriendt, K.

Subjects

*GENE expression, *EPSTEIN-Barr virus, *ONCOGENIC DNA viruses, *VIRAL cell transformation, *CELL lines, *GENETIC mutation

Abstract

Heterotaxia is an aetiologically heterogeneous condition caused by an abnormal left-right axis formation, resulting in reversed left-right polarity of one or more organ systems. In a patient with heterotaxia and a de novo reciprocal translocation t(6;18)(q21;q21), we found that the PA26 gene was disrupted by the 6q21 breakpoint. Northern blot analysis showed decreased expression of the PA26 gene in an Epstein-Barr virus-transformed cell line of this patient. During early embryogenesis of Xenopus, the orthologue of PA26, XPA26 is exclusively expressed in the notochord, a midline structure. This further supports a possible role of PA26 in human situs determination. Mutation analysis of human PA26 gene in 40 unrelated individuals with unexplained heterotaxia failed to identify mutations, indicating that PA26 mutations are not a frequent cause of heterotaxia in humans. Analysis of the PA26 gene structure resulted in the identification of a novel PA26-related gene family, which we have named the sestrin family, and which comprises three closely related genes in human and in mouse. [ABSTRACT FROM AUTHOR]

Published

2003

21. X-linked mental retardation: vanishing boundaries between non-specific (MRX) and syndromic (MRXS) forms.

Author

Frints, SGM, Froyen, G, Marynen, P, and Fryns, J-P

Subjects

*INTELLECTUAL disabilities, *GENETIC mutation

Abstract

This review covers the history and nosology of X-linked mental retardation (XLMR) in which the following, largely clinically based, subclassification was used: fragile X syndrome (FRAXA), syndromic forms (MRXS) and non-specific forms (MRX). After the discovery of the FMR2 gene at the FRAXE site, 10 MRX genes have been identified in the last 6 years. A short description is given of the strategies used to identify the genes that cause mental retardation (MR). Furthermore, their potential functions and the association with MR will be discussed. It is emphasized that mutations in several of these MR genes can result in non-specific, as well as in syndromic forms of XLMR. Present findings stress the importance of accurate clinical evaluation. Most considerably, genotype–phenotype correlation studies of affected individuals in XLMR families with MRX gene mutations are necessary to define the criteria of MRX vs MRXS subclassification. [ABSTRACT FROM AUTHOR]

Published

2002

22. Involvement of a palindromic chromosome 22-specific low-copy repeat in a constitutional t(X; 22)(q27;q11).

Author

Debeer, P, Mols, R, Huysmans, C, Devriendt, K, Van de Ven, WJM, and Fryns, J-P

Subjects

*CHROMOSOMES, *GENETICS

Abstract

Segmental duplications or low-copy repeats (LCRs) on chromosome 22q11 have been implicated in several chromosomal rearrangements. The presence of AT-rich regions in these duplications may lead to the formation of hairpin structures, which facilitate chromosomal rearrangement. Here we report the involvement of such a low-copy repeat in a t(X;22) associated with a neural tube defect. Molecular analysis of the chromosomal breakpoints revealed that the chromosome 22 breakpoint maps in the palindromic non-AT-rich NF1 -like region of low-copy repeat B (LCR-B). No palindromic region was encountered near the breakpoint on chromosome X. Our findings confirm that there is no single mechanism leading to translocations with chromosome 22q11 involvement. Because LCR-B does not contain genes involved in neural tube development, we believe that the gene responsible for the observed phenotype is most likely localized on chromosome X. [ABSTRACT FROM AUTHOR]

Published

2002

23. Autosomal dominant isolated velopharyngeal insufficiency.

Author

Vantrappen, G, Rommel, N, Wellens, W, Cremers, CWRJ, Fryns, J-P, and Devriendt, K

Subjects

*VELOPHARYNGEAL insufficiency, *SOFT palate, *FAMILIAL diseases

Abstract

Describes a family with autosomal dominant isolated velopharyngeal incompetence, a velopgharyngeal disorder. Manifestations of the disease; Hypernasal speech of the patients; Role of soft palate in the velopharyngeal insufficiency.

Published

2002

24. Prader–Willi syndrome: new insights in the behavioural and psychiatric spectrum.

Author

Descheemaeker, M. J, Vogels, A, Govers, V, Borghgraef, M, Willekens, D, Swillen, A, Verhoeven, W, and Fryns, J. P

Subjects

*PRADER-Willi syndrome, *PSYCHOSES, *PATHOLOGICAL psychology

Abstract

AbstractPrader–Willi syndrome (PWS) is a genetic disorder caused by the loss of the paternal contribution of the proximal part (15q11–q13) of the long arm of chromosome 15 (i.e. deletion, disomy and imprinting mutation). The syndrome is associated with distinct physical dysmorphism, as well as with specific behavioural and psychopathological characteristics. Psychiatric symptoms in adolescence and adulthood have been described, including acute cycloid psychosis, and obsessive compulsive, bipolar and pervasive developmental disorders. At the Centre for Human Genetics in Leuven, Belgium, 53 individuals (31 children and adolescents, and 22 adults) have been followed up for 15 years by a special multidisciplinary team. Attention was given to their medical, cognitive, behavioural and emotional development, and the evolution of psychiatric disorders in adolescence and adulthood. This study describes the psychiatric problems in four patients diagnosed with acute cycloid psychosis and traces their development from infancy to adolescence. Four other individuals needed psychiatric evaluation and treatment, and could be diagnosed as having unspecified bipolar disorder, also termed unstable mood disorder. Both groups were compared, and significant differences in early development and later evolution into adulthood were noted. The individuals with PWS who later developed psychotic episodes were described as active and extrovert toddlers, and showed autistic behaviour during their primary school education. Their intellectual functioning was in the moderate to severely retarded range. The individuals with PWS who later developed an unstable mood disorder were described as rather passive and introvert toddlers, and they presented less disturbed behaviour during their primary school education. The intellectual functioning of these subjects was in the normal to borderline range. [ABSTRACT FROM AUTHOR]

Published

2002

25. Physical map of a 1.5 Mb region on 12p11.2 harbouring a synpolydactyly associated chromosomal breakpoint.

Author

Debeer, Ph, Schoenmakers, E F P M, Thoelen, R, Holvoet, M, Kuittinen, T, Fabry, G, Fryns, J-P, Goodman, F R, and Van de Ven, W J M

Subjects

*ABNORMALITIES in the anatomical extremities, *GENETIC mutation, *HUMAN genetics

Abstract

Synpolydactyly (SPD) is a rare malformation of the distal limbs known to be caused by mutations in HOXD13. We have previously described a complex form of SPD associated with synostoses in three members of a Belgian family, which co-segregates with a t(12;22)(p11.2;q13.3) chromosomal translocation. The chromosome 12 breakpoint of this translocation maps to 12p11.2 between markers D12S1034 and D12S1596. Here we show that a mutation in the HOXD13 gene is not responsible for the phenotype, and present a physical map of the region around the 12p11.2 breakpoint. Starting from D12S1034 and D12S1596, we have established a contig approximately 1.5 Mb in length, containing 13 YAC clones, 16 BAC clones, and 11 cosmid clones. FISH analysis shows that cosmid LL12NCO1-149H4 maps across the breakpoint, and Southern blot experiments using fragments of this cosmid as probes identify a rearranged BamHI fragment in the patients carrying the translocation. A search for expressed sequences within the contig have so far revealed one CpG island, seven anonymous ESTs and three previously characterised genes, DAD-R, KRAG and HT21, all of which were found not to be directly disrupted by the translocation. The gene represented by EST R72964 was found to be disrupted by the translocation. These findings lay the groundwork for further efforts to characterise a gene critical for normal distal limb development that is perturbed by this translocation. [ABSTRACT FROM AUTHOR]

Published

2000

26. Molecular cloning of Xp11 breakpoints in two unrelated mentally retarded females with X;autosome translocations.

Author

Nothwang, H.G., Schröer, A., Maarel, S. Van Der, Kubart, S., Schneider, S., Rieβelmann, L., Menzel, C., Hinzmann, B., Vogt, D., Rosenthal, A., Fryns, J.-P., Tommerup, E N., Haaf, T., Ropers, H.H., and Wirth, J.

Subjects

*INTELLECTUAL disabilities, *X chromosome, *SOUTHERN blot, *PHENOTYPES, *GENETICS, *POPULATION

Abstract

Mental retardation is a very common and extremely heterogeneous disorder that affects about 3% of the human population. Its molecular basis is largely unknown, but many loci have been mapped to the X chromosome. We report on two mentally retarded females with X;autosome translocations and breakpoints in Xp11, viz., t(X;17)(p11;p13) and t(X;20)(p11;q13). (Fiber-) FISH analysis assigned the breakpoints to different subbands, Xp11.4 and Xp11.23, separated by approximately 8 Mb. High-resolution mapping of the X- chromosome breakpoints using Southern blot hybridization resulted in the isolation of breakpoint-spanning genomic subclones of 3 kb and 0.5 kb. The Xp11.4 breakpoint is contained within a single copy sequence, whereas the Xp11.23 breakpoint sequence resembles an L1 repetitive element. Several expressed sequences map close to the breakpoints, but none was found to be inactivated. Therefore, mechanisms other than disruption of X-chromosome genes likely cause the phenotypes. Copyright © 2000 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2000

27. Vesico-ureteral reflux: a genetic condition?

Author

Devriendt, K., Groenen, P., Van Esch, H., van Dijck, M., Van de Ven, W., Fryns, J. P., and Proesmans, W.

Subjects

*VESICO-ureteral reflux, *GENE expression, *VECTOR-pathogen relationships, *KIDNEY abnormalities, *CHROMOSOME abnormalities, *GENEALOGY, *GENES, *GENETIC techniques, *URETERS, *URETERIC obstruction

Abstract

Vesico-ureteral reflux (VUR) is a frequent condition, but in most instances, the precise cause is unknown. We here review the evidence of a genetic aetiology of VUR, inherited as an autosomal dominant trait, with variable expression. We discuss the possible pathogenetic relationship between VUR and other types of uropathies and possible strategies towards the identification of genes underlying VUR are presented. The isolation of the gene(s) responsible for uropathies will not only lead to a better insight into the embryology of the urological system, the pathogenesis of uropathies, but also to a renewed interest from clinicians in congenital uropathies. [ABSTRACT FROM AUTHOR]

Published

1998

28. Physical mapping of the t(12;22) translocation breakpoints in a family with a complex type of 3/3′/4 synpolydactyly.

Author

Debeer, P., Schoenmakers, E. F. P. M., Thoelen, R., Fryns, J. -P., and van de Ven, W. J. M.

Subjects

*GENE mapping, *CHROMOSOMAL translocation, *GENETIC disorders, *SOMATIC hybrids, *HAND abnormalities, *SYNDACTYLY

Abstract

We previously reported clinical and radiological findings in a Belgian family with a complex type of synpolydactyly associated with metacarpal and metatarsal synostoses, cosegregating with a balanced t(12;22). Recently, expansions of a polyalanine stretch within the first exon of the HOXD13 gene, which resides on chromosome 2q31, have been shown to cause synpolydactyly (SPD). Using exon amplification followed by direct sequencing, we were able to exclude the direct involvement of the HOXD13 gene in this family. As a first step toward the positional cloning of a candidate disease gene on chromosome 12 and/or 22 responsible for the type of complex synpolydactyly observed in this family, we report here the construction of a somatic cell hybrid retaining only the der(22) of the t(12;22)(p11.3;q13.3). STS content mapping and FISH experiments allowed us to position the chromosomal breakpoints between markers D12S1596 and D12S1034 on chromosome 12 and markers N73F4 and D22S158 on chromosome 22. [ABSTRACT FROM AUTHOR]

Published

1998

29. Chromosome healing of constitutional chromosome deletions studied by microdissection.

Author

Vermeesch, J.R., Faizetti, D., Buggenhout, G. Van, Fryns, J.-P., and Marynen, P.

Subjects

*CHROMOSOMES, *MICRODISSECTION, *GENES, *GENETICS, *TELOMERES, *TELOMERASE

Abstract

Broken chromosomes are highly unstable and are subject to chromosome fusion or loss. As an exception, healing of human chromosomes occurs which can lead to constitutional or acquired terminal chromosome deletion disorders. Both de novo telomere addition at the breakpoint and telomere capture have been implicated as healing mechanisms. We investigated the origin of the novel ends of chromosomes 4p and 5p in a patient with the Wolf-Hirschhorn syndrome and in 4 patients with the Cri-du-Chat syndrome by chromosome microdissection. Our results suggest that de novo telomere synthesis by telomerase is the main mechanism of chromosome healing in constitutional chromosome deletions. [ABSTRACT FROM AUTHOR]

Published

1998

30. Detection of an unusual 17p13.3 microdeletion by array comparative genomic hybridisation in a patient with lissencephaly.

Author

Chabchoub, E., de Ravel, T., Thoelen, R., Vermeesch, J. R., Fryns, J .-P., and Esch, H. Van

Subjects

*LETTERS to the editor, *LISSENCEPHALY

Abstract

A letter to the editor is presented in response to the article "Detection of an Unusual 17p13.3 Microdeletion By Array Comparative Genomic Hybridisation in a Patient With Lissencephaly" in the 2006 issue.

Published

2006

31. ARX mutation in a boy with transsphenoidal encephalocele and hypopituitarism.

Author

Van Esch, H, K3Poirier, de Zegher, F, Holvoet, M, Bienvenu, T, Chelly, J, Devriendt, K, and Fryns, J-P

Subjects

*LETTERS to the editor, *ENCEPHALOCELE

Abstract

Presents a letter to the editor on the causal role of the Aristaless-related homeobox gene in the origin of the encephalocele and endocrine defects in a patient.

Published

2004

32. Twin reversed arterial perfusion sequence presenting as intrauterine cyst.

Author

Witters, I., Coumans, A., Willekes, C., and Fryns, J. P.

Subjects

*PREGNANCY complications, *FETAL heart abnormalities, *AMNIOCENTESIS, *KARYOTYPES, *UTERINE tumors

Abstract

The article presents a case study involving a dichorionic triamniotic triplet pregnancy with an acardiac twin in the monochorionic pair showing an intrauterine cyst. It mentions that the gestation was discovered after elicitation of ovulation. It also notes that one of the twins fetuses particularly a male indicated malformation of the heart along with the execution of amniocentesis to determine normal molecular karyotypes.

Published

2013

33. Prenatal diagnosis of schizencephaly after inhalation of organic solvents.

Author

Witters, I., Cannie, M., Casaers, P., Devriend, K., and Fryns, J.-P.

Subjects

*LETTERS to the editor, *PRENATAL diagnosis

Abstract

A letter to the editor is presented about the prenatal diagnosis of schizencephaly after inhalation of organic solvents.

Published

2007

34. Increased nuchal translucency thickness in thrombocytopenia-absent-radius syndrome.

Author

Witters, I., Claerhout, P., Frynss, J. P., and Fryns, J P

Subjects

*LETTERS to the editor, *THROMBOCYTOPENIA

Abstract

A letter to the editor is presented in response to the article about nuchal translucency thickness in thrombocytopenia-absent-radius syndrome that was published in the previous issue.

Published

2005

35. Anogenital malformation with ambiguous genitalia as part of the OEIS complex.

Author

Witters, I., Deprest, J., van Hole, C., Hanssens, M., Devlieger, H., and Fryns, J. P.

Subjects

*LETTERS to the editor, *GENITAL abnormalities

Abstract

A letter to the editor is presented about a 30-year-old woman diagnosed with anogenital malformation and ambiguous genitalia.

Published

2004

36. Preaxial polydactyly type 1 and severe language deficit in maternal uniparental disomy of chromosome 7.

Author

Potgieter, Steph, Matthijs, Gert, De Cock, Paul, Fryns, Jean-Pierre, Potgieter, S, Matthijs, G, De Cock, P, and Fryns, J P

Subjects

*LANGUAGE disorders, *CHROMOSOME analysis

Abstract

Presents a case of maternal uniparental disomy of chromosome VII with unilateral preaxial polydactylyl type I and severe language deficit. Clinical phenotype of the specific condition; Analysis of markers in chromosome VII; Result of the haplotype analysis.

Published

2000

37. Parental perception of sleep behaviour and sleep disorders in children with VCFS and their siblings.

Author

Swillen A, Berghs I, Schoeters A, Fryns J, Hellinkcx W, and Devriendt K

Published

2008

38. Molecular karyotyping is important in determining the cause of behavioural phenotypes.

Author

de Ravel TJL, Swillen A, Willekens D, Descheemaeker M, Govers V, Borghgraef M, Vermeesch JR, and Fryns J

Published

2008

39. Parental perception of sleep behaviour and sleep disorders in children with VCFS and their siblings.

Author

Swillen, A., Berghs, I., Schoeters, A., Fryns, J.‐P., Hellinkcx, W., and Devriendt, K.

Subjects

*SLEEP disorders in children, *BEHAVIOR disorders in children, *SYNDROMES in children, *NARCOLEPSY, *SLEEP apnea syndromes

Abstract

Background: Disrupted sleep in children may lead to multiple behavioural problems that affect the individual and the family. The aim of this study was to compare sleep behaviour and sleep disorders in children with VCFS with those of their siblings and to determine the severity and pattern of the sleep problems. Method: Parents completed the Children’s Sleep Habits Questionnaire (CSHQ) (Owens et al., 2000) for 31 children with VCFS (mean age 10 years). This instrument has good psychometric properties and validity. It includes items relating to a number of key sleep domains grouped conceptually into eight subscales reflecting: (1) Bedtime Resistance; (2) Sleep Onset Delay; (3) Sleep Duration; (4) Sleep Anxiety; (5) Night Wakings; (6) Parasomnias; (7) Sleep Disordered Breathing; (8) Daytime Sleepiness. Total Sleep Disturbance Score includes all items of the eight subscales. Higher scores are indicative of more disturbed sleep. Results: The severity of sleep problems in the VCFS group was reported by parents as being significantly higher than in the sibling group (mean score 42.97 and 36.55, respectively; p < 0.001). Values for five of eight sleep subscales including bedtime resistance, sleep anxiety, night waking, parasomnias and daytime sleepiness were significantly (p < 0.001) higher in the VCFS group. Conclusion: Parents report that sleep problems are significantly more severe in children with VCFS compared to their siblings, and that the pattern appears diverse. Sleep problems in children with VCFS require further research and clinical attention. [ABSTRACT FROM AUTHOR]

Published

2008

40. Molecular karyotyping is important in determining the cause of behavioural phenotypes.

Author

De Ravel, T. J. L., Swillen, A., Willekens, D., Descheemaeker, M.‐J., Govers, V., Borghgraef, M., Vermeesch, J. R., and Fryns, J.‐P.

Subjects

*KARYOTYPES, *CYTOGENETICS, *PHENOTYPES, *SYNDROMES, *AUTISM

Abstract

Background: The cytogenetic delineation and behavioural phenotype of syndromes has evolved from the chromosome level, through FISH (microdeletions syndromes, such as PWS, VCFS, SMS, del1p36) to molecular karyotyping (array CGH). The new syndromes being outlined in recent years account for rarer microdeletions and microduplications, in which the behavioural phenotype is not always well characterized. Method: We have screened by array CGH more than 2000 patients, of which almost 400 have cytogenetic imbalances. We present a subset of these patients, in which the behaviour was an important component of the motivation for molecular karyotyping. Results: Three case studies: 1) A boy with severe feeding problems, speech delay, stereotypic and autistic behaviour. He is dysmorphic and has an intellectual disability. Molecular karyotyping showed a de novo microdeletion of chromosome 15q13.2. 2) A 3-year old girl with difficult behaviour, including negative vocalizations, aggression and repetitive rocking. She has poor weight gain, difficulty in falling asleep and wakes early. She is dysmorphic, has a developmental IQ of 67, a paternally inherited microdeletion of chromosome 9p21.3 and a de novo microduplication of chromosome 17p11.2. 3) A 5-year old girl with intellectual disability who participates in interactive play but remains slow in task execution. Her balance is poor when standing and walking, She does not evidence satiety for food and constantly air-swallows. Molecular karyotyping revealed a de novo microdeletion of chromosome 9qter. Conclusion: The molecular karyotyping results encourage its use in finding the cause of intellectual disability. With the assistance of international collaboration via common databases, such as Decipher, pinpointing and understanding the underlying genes contributing to the overall clinical picture, especially behaviour, will become a reality. [ABSTRACT FROM AUTHOR]

Published

2008