Your search keyword '"Redeker EJ"' showing total 23 results

1. Successful Growth Hormone Therapy in Cornelia de Lange Syndrome.

Author

de Graaf M, Kant SG, Wit JM, Willem Redeker EJ, Eduard Santen GW, Henriëtta Verkerk AJM, Uitterlinden AG, Losekoot M, and Oostdijk W

Subjects

Body Height drug effects, Child, De Lange Syndrome complications, Dwarfism drug therapy, Dwarfism etiology, Hormone Replacement Therapy, Humans, Infant, Small for Gestational Age growth & development, Male, Treatment Outcome, De Lange Syndrome drug therapy, Human Growth Hormone therapeutic use

Abstract

Cornelia de Lange syndrome (CdLS) is a both clinically and genetically heterogeneous syndrome. In its classical form, it is characterised by distinctive facial features, intra-uterine growth retardation, short stature, developmental delay, and anomalies in multiple organ systems. NIPBL, SMC1A, SMC3, RAD21 and HDAC8, all involved in the cohesin pathway, have been identified to cause CdLS. Growth hormone (GH) secretion has been reported as normal, and to our knowledge, there are no reports on the effect of recombinant human GH treatment in CdLS patients. We present a patient born small for gestational age with persistent severe growth retardation [height -3.4 standard deviation score (SDS)] and mild dysmorphic features, who was treated with GH from 4.3 years of age onward and was diagnosed 6 years later with CdLS using whole-exome sequencing. Treatment led to a height gain of 1.6 SDS over 8 years. Treatment was interrupted shortly due to high serum insulin-like growth factor-1 serum values. In conclusion, GH therapy may be effective and safe for short children with CdLS.

Published

2017

2. Uptake of prenatal diagnostic testing for retinoblastoma compared to other hereditary cancer syndromes in the Netherlands.

Author

Dommering CJ, Henneman L, van der Hout AH, Jonker MA, Tops CM, van den Ouweland AM, van der Luijt RB, Mensenkamp AR, Hogervorst FB, Redeker EJ, de Die-Smulders CE, Moll AC, and Meijers-Heijboer H

Subjects

DNA Mutational Analysis, Early Detection of Cancer methods, Female, Genetic Counseling, Humans, Mutation, Neoplastic Syndromes, Hereditary genetics, Netherlands, Pregnancy, Prenatal Diagnosis methods, Retinoblastoma genetics, Retrospective Studies, Surveys and Questionnaires, Early Detection of Cancer statistics & numerical data, Genes, Retinoblastoma genetics, Genetic Testing statistics & numerical data, Neoplastic Syndromes, Hereditary diagnosis, Prenatal Diagnosis statistics & numerical data, Retinoblastoma diagnosis

Abstract

Since the 1980s the genetic cause of many hereditary tumor syndromes has been elucidated. As a consequence, carriers of a deleterious mutation in these genes may opt for prenatal diagnoses (PND). We studied the uptake of prenatal diagnosis for five hereditary cancer syndromes in the Netherlands. Uptake for retinoblastoma (Rb) was compared with uptake for Von Hippel-Lindau disease (VHL), Li-Fraumeni syndrome (LFS), familial adenomatous polyposis (FAP), and hereditary breast ovarian cancer (HBOC). A questionnaire was completed by all nine DNA-diagnostic laboratories assessing the number of independent mutation-positive families identified from the start of diagnostic testing until May 2013, and the number of PNDs performed for these syndromes within these families. Of 187 families with a known Rb-gene mutation, 22 had performed PND (11.8%), this was significantly higher than uptake for FAP (1.6%) and HBOC (<0.2%). For VHL (6.5%) and LFS (4.9%) the difference was not statistically significant. PND for Rb started 3 years after introduction of diagnostic DNA testing and remained stable over the years. For the other cancer syndromes PND started 10-15 years after the introduction and uptake for PND showed an increase after 2009. We conclude that uptake of PND for Rb was significantly higher than for FAP and HBOC, but not different from VHL and LFS. Early onset, high penetrance, lack of preventive surgery and perceived burden of disease may explain these differences.

Published

2017

3. Whole-exome sequencing is a powerful approach for establishing the etiological diagnosis in patients with intellectual disability and microcephaly.

Author

Rump P, Jazayeri O, van Dijk-Bos KK, Johansson LF, van Essen AJ, Verheij JB, Veenstra-Knol HE, Redeker EJ, Mannens MM, Swertz MA, Alizadeh BZ, van Ravenswaaij-Arts CM, Sinke RJ, and Sikkema-Raddatz B

Subjects

Adolescent, Adult, Child, Child, Preschool, Female, Humans, Infant, Male, Middle Aged, Young Adult, Exome genetics, Intellectual Disability complications, Intellectual Disability genetics, Microcephaly complications, Microcephaly genetics, Sequence Analysis, DNA methods

Abstract

Background: Clinical and genetic heterogeneity in monogenetic disorders represents a major diagnostic challenge. Although the presence of particular clinical features may aid in identifying a specific cause in some cases, the majority of patients remain undiagnosed. Here, we investigated the utility of whole-exome sequencing as a diagnostic approach for establishing a molecular diagnosis in a highly heterogeneous group of patients with varied intellectual disability and microcephaly., Methods: Whole-exome sequencing was performed in 38 patients, including three sib-pairs, in addition to or in parallel with genetic analyses that were performed during the diagnostic work-up of the study participants., Results: In ten out of these 35 families (29 %), we found mutations in genes already known to be related to a disorder in which microcephaly is a main feature. Two unrelated patients had mutations in the ASPM gene. In seven other patients we found mutations in RAB3GAP1, RNASEH2B, KIF11, ERCC8, CASK, DYRK1A and BRCA2. In one of the sib-pairs, mutations were found in the RTTN gene. Mutations were present in seven out of our ten families with an established etiological diagnosis with recessive inheritance., Conclusions: We demonstrate that whole-exome sequencing is a powerful tool for the diagnostic evaluation of patients with highly heterogeneous neurodevelopmental disorders such as intellectual disability with microcephaly. Our results confirm that autosomal recessive disorders are highly prevalent among patients with microcephaly.

Published

2016

4. Targeted carrier screening for four recessive disorders: high detection rate within a founder population.

Author

Mathijssen IB, Henneman L, van Eeten-Nijman JM, Lakeman P, Ottenheim CP, Redeker EJ, Ottenhof W, Meijers-Heijboer H, and van Maarle MC

Subjects

Adolescent, Adult, Arthrogryposis diagnosis, Arthrogryposis genetics, Chondrodysplasia Punctata, Rhizomelic diagnosis, Chondrodysplasia Punctata, Rhizomelic genetics, Female, Founder Effect, Genetic Counseling, Humans, Male, Middle Aged, Netherlands, Olivopontocerebellar Atrophies diagnosis, Olivopontocerebellar Atrophies genetics, Osteogenesis Imperfecta diagnosis, Osteogenesis Imperfecta genetics, Pedigree, Peroxisomal Targeting Signal 2 Receptor deficiency, Pregnancy, Young Adult, Genes, Recessive, Genetic Carrier Screening methods, Genetic Testing methods

Abstract

In a genetically isolated community in the Netherlands four severe recessive genetic disorders occur at relatively high frequency (pontocerebellar hypoplasia type 2 (PCH2), fetal akinesia deformation sequence (FADS), rhizomelic chondrodysplasia punctata type 1 (RCDP1), and osteogenesis imperfecta (OI) type IIB/III. Over the past decades multiple patients with these disorders have been identified. This warranted the start of a preconception outpatient clinic, in 2012, aimed at couples planning a pregnancy. The aim of our study was to evaluate the offer of targeted genetic carrier screening as a method to identify high-risk couples for having affected offspring in this high-risk subpopulation. In one year, 203 individuals (92 couples and 19 individuals) were counseled. In total, 65 of 196 (33.2%) tested individuals were carriers of at least one disease, five (7.7%) of them being carriers of two diseases. Carrier frequencies of PCH2, FADS, RCDP1, and OI were 14.3%, 11.2%, 6.1%, and 4.1% respectively. In individuals with a positive family history for one of the diseases, the carrier frequency was 57.8%; for those with a negative family history this was 25.8%. Four PCH2 carrier-couples were identified. Thus, targeted (preconception) carrier screening in this genetically isolated population in which a high prevalence of specific disorders occurs detects a high number of carriers, and is likely to be more effective compared to cascade genetic testing. Our findings and set-up can be seen as a model for carrier screening in other high-risk subpopulations and contributes to the discussion about the way carrier screening can be offered and organized in the general population., (Copyright © 2015 Elsevier Masson SAS. All rights reserved.)

Published

2015

5. High rate of mosaicism in individuals with Cornelia de Lange syndrome.

Author

Huisman SA, Redeker EJ, Maas SM, Mannens MM, and Hennekam RC

Subjects

Base Sequence, Cell Cycle Proteins genetics, Chromosomal Proteins, Non-Histone genetics, Humans, Molecular Sequence Data, Mouth Mucosa cytology, Sequence Analysis, DNA, Structural Maintenance of Chromosome Protein 1, De Lange Syndrome genetics, Mosaicism, Proteins genetics

Abstract

Background: Cornelia de Lange syndrome (CdLS) is a well known malformation syndrome for which five causative genes are known, accounting for ∼55-65% of cases. In this study, we hypothesised that mosaicism might explain some of the ∼35-45% of cases without detectable mutation in DNA derived from lymphocytes; we investigated the frequency of NIPBL mutations in buccal cells in individuals negative for mutations in any of the five genes in lymphocytes; and we evaluated the efficiency of obtaining DNA from buccal swabs and the best strategy for optimal mutation detection in CdLS., Methods: Buccal swabs were obtained from eight mutation positive and 13 mutation negative individuals with clinically diagnosed CdLS, following informed consent. We then forwarded instructions and a single mouth swab to the families; if subsequently insufficient DNA was obtained, we re-sent two mouth swabs. Buccal cells were screened for NIPBL mutations using Sanger sequencing techniques., Results: Sufficient DNA for analysis was obtained in 21/22 individuals. In all six tested individuals with a known NIPBL mutation and in two with a known SMC1A mutation, the mutation was confirmed in buccal cells. In 10 of the 13 tested individuals without detectable mutation in lymphocytes a NIPBL mutation could be detected in buccal cells. Clinically there were no significant differences between patients with a germline and mosaic NIPBL mutation., Conclusions: Somatic mosaicism for an NIPBL mutation is frequent (10/44; 23%) clinically in reliably diagnosed CdLS individuals. Obtaining buccal swabs at the time a blood sample is obtained will facilitate adequate molecular analysis of clinically diagnosed CdLS patients.

Published

2013

6. Microfluidic amplification as a tool for massive parallel sequencing of the familial hypercholesterolemia genes.

Author

Hollants S, Redeker EJ, and Matthijs G

Subjects

Apolipoproteins B genetics, Humans, Microfluidic Analytical Techniques, Mutation, Oligonucleotide Array Sequence Analysis, Polymerase Chain Reaction, Proprotein Convertase 9, Proprotein Convertases genetics, Receptors, LDL genetics, Sequence Analysis, DNA, Serine Endopeptidases genetics, Hyperlipoproteinemia Type II genetics

Abstract

Background: Familial hypercholesterolemia (FH) is an autosomal dominant disorder that affects cholesterol metabolism and is an important risk factor for heart disease. Three different genes were causally linked to this disorder: LDLR (low density lipoprotein receptor), APOB [apolipoprotein B (including Ag(x) antigen)], and PCSK9 (proprotein convertase subtilisin/kexin type 9). We evaluated a new amplicon preparation tool for resequencing these genes on next generation sequencing (NGS) platforms., Methods: For the 3 genes, 38 primer pairs were designed and loaded on the Fluidigm Access Array, a microfluidic array in which a PCR was performed. We amplified 144 DNA samples (73 positive controls and 71 patient samples) and performed 3 sequencing runs on a GS FLX Titanium system from Roche 454, using pyrosequencing. Data were analyzed with the SeqNext module of the Sequence Pilot software., Result: From the 38 amplicons, 37 were amplified successfully, without any further optimization. Sequencing resulted in a mean coverage of the individual amplicons of 71-fold, 74-fold, and 117-fold for the 3 runs, respectively. In the positive controls, all known mutations were identified. In 29% of the patient samples, a pathogenic point mutation or small deletion/insertion was found. Large rearrangements were not detectable with NGS, but were picked up by multiplex ligation-dependent probe amplification., Conclusions: Combining a microfluidic amplification system with massive parallel sequencing is an effective method for mutation scanning in FH patients, which can be implemented in diagnostics. For data analysis, we propose a minimum variant frequency threshold of 20% and a minimum coverage of 25-fold.

Published

2012

7. Risk of colorectal and endometrial cancers in EPCAM deletion-positive Lynch syndrome: a cohort study.

Author

Kempers MJ, Kuiper RP, Ockeloen CW, Chappuis PO, Hutter P, Rahner N, Schackert HK, Steinke V, Holinski-Feder E, Morak M, Kloor M, Büttner R, Verwiel ET, van Krieken JH, Nagtegaal ID, Goossens M, van der Post RS, Niessen RC, Sijmons RH, Kluijt I, Hogervorst FB, Leter EM, Gille JJ, Aalfs CM, Redeker EJ, Hes FJ, Tops CM, van Nesselrooij BP, van Gijn ME, Gómez García EB, Eccles DM, Bunyan DJ, Syngal S, Stoffel EM, Culver JO, Palomares MR, Graham T, Velsher L, Papp J, Oláh E, Chan TL, Leung SY, van Kessel AG, Kiemeney LA, Hoogerbrugge N, and Ligtenberg MJ

Subjects

Adolescent, Adult, Aged, Cohort Studies, Colorectal Neoplasms etiology, Endometrial Neoplasms etiology, Epithelial Cell Adhesion Molecule, Female, Gene Deletion, Humans, Male, Middle Aged, MutS Homolog 2 Protein genetics, Promoter Regions, Genetic, Risk, Antigens, Neoplasm genetics, Cell Adhesion Molecules genetics, Colorectal Neoplasms genetics, Endometrial Neoplasms genetics, Sequence Deletion

Abstract

Background: Lynch syndrome is caused by germline mutations in MSH2, MLH1, MSH6, and PMS2 mismatch-repair genes and leads to a high risk of colorectal and endometrial cancer. We previously showed that constitutional 3' end deletions of EPCAM can cause Lynch syndrome through epigenetic silencing of MSH2 in EPCAM-expressing tissues, resulting in tissue-specific MSH2 deficiency. We aim to establish the risk of cancer associated with such EPCAM deletions., Methods: We obtained clinical data for 194 carriers of a 3' end EPCAM deletion from 41 families known to us at the Radboud University Nijmegen Medical Centre, Nijmegen, Netherlands and compared cancer risk with data from a previously described cohort of 473 carriers from 91 families with mutations in MLH1, MSH2, MSH6, or a combined EPCAM-MSH2 deletion., Findings: 93 of the 194 EPCAM deletion carriers were diagnosed with colorectal cancer; three of the 92 women with EPCAM deletions were diagnosed with endometrial cancer. Carriers of an EPCAM deletion had a 75% (95% CI 65-85) cumulative risk of colorectal cancer before the age of 70 years (mean age at diagnosis 43 years [SD 12]), which did not differ significantly from that of carriers of combined EPCAM-MSH2 deletion (69% [95% CI 47-91], p=0·8609) or mutations in MSH2 (77% [64-90], p=0·5892) or MLH1 (79% [68-90], p=0·5492), but was higher than noted for carriers of MSH6 mutation (50% [38-62], p<0·0001). By contrast, women with EPCAM deletions had a 12% [0-27] cumulative risk of endometrial cancer, which was lower than was that noted for carriers of a combined EPCAM-MSH2 deletion (55% [20-90], p<0·0001) or of a mutation in MSH2 (51% [33-69], p=0·0006) or MSH6 (34% [20-48], p=0·0309), but did not differ significantly from that noted for MLH1 (33% [15-51], p=0·1193) mutation carriers. This risk seems to be restricted to deletions that extend close to the MSH2 gene promoter. Of 194 carriers of an EPCAM deletion, three had duodenal cancer and four had pancreatic cancer., Interpretation: EPCAM deletion carriers have a high risk of colorectal cancer; only those with deletions extending close to the MSH2 promoter have an increased risk of endometrial cancer. These results underscore the effect of mosaic MSH2 deficiency, leading to variable cancer risks, and could form the basis of an optimised protocol for the recognition and targeted prevention of cancer in EPCAM deletion carriers., (Copyright © 2011 Elsevier Ltd. All rights reserved.)

Published

2011

8. Leiden Open Variation Database of the MUTYH gene.

Author

Out AA, Tops CM, Nielsen M, Weiss MM, van Minderhout IJ, Fokkema IF, Buisine MP, Claes K, Colas C, Fodde R, Fostira F, Franken PF, Gaustadnes M, Heinimann K, Hodgson SV, Hogervorst FB, Holinski-Feder E, Lagerstedt-Robinson K, Olschwang S, van den Ouweland AM, Redeker EJ, Scott RJ, Vankeirsbilck B, Grønlund RV, Wijnen JT, Wikman FP, Aretz S, Sampson JR, Devilee P, den Dunnen JT, and Hes FJ

Subjects

Adenomatous Polyposis Coli genetics, Alternative Splicing, Amino Acid Sequence, Base Sequence, DNA genetics, DNA Glycosylases chemistry, Genetic Association Studies, Genetic Predisposition to Disease, Humans, Molecular Sequence Data, Mutation, Netherlands, Protein Isoforms chemistry, Protein Isoforms genetics, Protein Structure, Tertiary, DNA Glycosylases genetics, Databases, Genetic, Genetic Variation

Abstract

The MUTYH gene encodes a DNA glycosylase involved in base excision repair (BER). Biallelic pathogenic MUTYH variants have been associated with colorectal polyposis and cancer. The pathogenicity of a few variants is beyond doubt, including c.536A4G/p.Tyr179Cys and c.1187G4A/p.Gly396Asp (previously c.494A4G/p.Tyr165Cys and c.1145G4A/p.Gly382Asp).However, for a substantial fraction of the detected variants, the clinical significance remains uncertain,compromising molecular diagnostics and thereby genetic counseling. We have established an interactive MUTYH gene sequence variant database (www.lovd.nl/MUTYH) with the aim of collecting and sharing MUTYH genotype and phenotype data worldwide. To support standard variant description, we chose NM&#95;001128425.1 as the reference sequence. The database includes records with variants per individual, linked to available phenotype and geographic origin data as well as records with in vitro functional and in silico test data. As of April 2010, the database contains 1968 published and 423 unpublished submitted entries, and 230 and 61 unique variants,respectively. This open-access repository allows all involved to quickly share all variants encountered and communicate potential consequences, which will be especially useful to classify variants of uncertain significance.

Published

2010

9. Multiplex ligation-dependent probe amplification (MLPA) enhances the molecular diagnosis of aniridia and related disorders.

Author

Redeker EJ, de Visser AS, Bergen AA, and Mannens MM

Subjects

Exons genetics, Eye Proteins genetics, Homeodomain Proteins genetics, Humans, In Situ Hybridization, Fluorescence, PAX6 Transcription Factor, Paired Box Transcription Factors genetics, Point Mutation genetics, Repressor Proteins genetics, Sequence Deletion, Aniridia diagnosis, Aniridia genetics, Polymerase Chain Reaction methods, WAGR Syndrome diagnosis, WAGR Syndrome genetics

Abstract

Mutations in the PAX6 gene have been implicated in aniridia, a congenital malformation of the eye with severe hypoplasia of the iris. However, not all aniridia cases can be explained by mutations in the PAX6 gene. The purpose of this study was to enhance the molecular diagnosis of aniridia using multiplex ligation-dependent probe amplification (MLPA). Total genomic DNA was isolated from peripheral blood of 70 unrelated probands affected with aniridia. Polymerase chain reaction (PCR) was performed followed by automated bidirectional sequencing. Additionally, MLPA was performed. We identified 24 different point mutations in the PAX6 gene in 34 patients after sequencing. In eight additional patients, we identified a deletion of one or more exons of the PAX6 gene or in the 3' regulatory region of the PAX6 gene using MLPA. This work demonstrates the necessity to screen for larger deletions in the region of the PAX6 gene in addition to the sequencing of exons in the PAX6 gene. The mutation detection rate will increase from 49% to 60%. This shows that MLPA substantially enhances the molecular diagnosis of aniridia.

Published

2008

10. DNA analysis of the SH3BP2 gene in patients with aggressive central giant cell granuloma.

Author

de Lange J, van Maarle MC, van den Akker HP, and Redeker EJ

Subjects

Cherubism genetics, DNA Mutational Analysis, Diagnosis, Differential, Female, Granuloma, Giant Cell blood, Humans, Jaw Diseases blood, Male, Mutation, Polymerase Chain Reaction, Adaptor Proteins, Signal Transducing genetics, Granuloma, Giant Cell genetics, Jaw Diseases genetics

Abstract

A mutation of the SH3BP2 gene is known to cause cherubism. As there are clinical and histopathological similarities between central giant cell granuloma and cherubism, we made a constitutional DNA analysis of the SH3BP2 gene in four patients with aggressive giant cell granuloma (having one or more of the following features pain, paraesthesia, rapid growth, or root resorption). We found no mutations in the SH3BP2 gene, which indicates that cherubism is a separate entity. However, a somatic mutation in a specific group of cells could cause the focal lesions in giant cell granuloma. Further DNA analysis of the tissue of giant cell granulomas therefore seems indicated.

Published

2007

11. Increased DNA damage sensitivity of Cornelia de Lange syndrome cells: evidence for impaired recombinational repair.

Author

Vrouwe MG, Elghalbzouri-Maghrani E, Meijers M, Schouten P, Godthelp BC, Bhuiyan ZA, Redeker EJ, Mannens MM, Mullenders LH, Pastink A, and Darroudi F

Subjects

Cell Cycle Proteins, Cells, Cultured, Chromosome Aberrations, G2 Phase, Histones metabolism, Humans, Mitomycin pharmacology, Nucleic Acid Synthesis Inhibitors pharmacology, Proteins genetics, Proteins metabolism, Rad51 Recombinase metabolism, Radiation, Ionizing, Recombination, Genetic, DNA Damage, DNA Repair physiology, De Lange Syndrome genetics

Abstract

Cornelia de Lange syndrome (CdLS) is a rare dominantly inherited multisystem disorder affecting both physical and mental development. Heterozygous mutations in the NIPBL gene were found in about half of CdLS cases. Scc2, the fungal ortholog of the NIPBL gene product, is essential for establishing sister chromatid cohesion. In yeast, the absence of cohesion leads to chromosome mis-segregation and defective repair of DNA double-strand breaks. To evaluate possible DNA repair defects in CdLS cells, we characterized the cellular responses to DNA-damaging agents. We show that cells derived from CdLS patients, both with and without detectable NIPBL mutations, have an increased sensitivity for mitomycin C (MMC). Exposure of CdLS fibroblast and B-lymphoblastoid cells to MMC leads to enhanced cell killing and reduced proliferation and, in the case of primary fibroblasts, an increased number of chromosomal aberrations. After X-ray exposure increased numbers of chromosomal aberrations were also detected, but only in cells irradiated in the G(2)-phase of the cell cycle when repair of double-strand breaks is dependent on the establishment of sister chromatid cohesion. Repair at the G(1) stage is not affected in CdLS cells. Our studies indicate that CdLS cells have a reduced capacity to tolerate DNA damage, presumably as a result of reduced DNA repair through homologous recombination.

Published

2007

12. Large genomic rearrangements in NIPBL are infrequent in Cornelia de Lange syndrome.

Author

Bhuiyan ZA, Stewart H, Redeker EJ, Mannens MM, and Hennekam RC

Subjects

Adolescent, Adult, Cell Cycle Proteins, Child, Child, Preschool, Chromosomes, Human, Pair 9 genetics, Cohort Studies, DNA Mutational Analysis methods, Female, Genome, Human, Humans, Infant, Male, Middle Aged, Nucleic Acid Amplification Techniques methods, Pedigree, Phenotype, De Lange Syndrome genetics, Exons genetics, Gene Deletion, Gene Rearrangement, Proteins genetics

Abstract

Cornelia de Lange Syndrome (CdLS) is a multiple congenital anomaly syndrome characterized by a distinctive facial appearance, malformations of the upper limbs, and delay in growth and development. Mutations in NIPBL are associated with CdLS in 27-56% of cases and have been reported as point mutations, small insertions and deletions in coding regions, regulatory regions and at splice junctions. All previous studies used PCR-based exon-scanning methodologies that do not allow detection of large genomic rearrangements. We studied the relative copy number of NIPBL exons in a series of 50 CdLS probands, negative for NIPBL mutations, by multiplex ligation-dependent probe amplification (MLPA). In a single patient, we found a 5.2 kb deletion encompassing exons 41-42 of NIPBL. Our studies indicate that large NIPBL rearrangements do occur in CdLS but are likely to be infrequent events.

Published

2007

13. A new mutation in the SH3BP2 gene showing reduced penetrance in a family affected with cherubism.

Author

de Lange J, van Maarle MC, van den Akker HP, and Redeker EJ

Subjects

Amino Acid Substitution, DNA Mutational Analysis, Female, Humans, Male, Mutation, Missense, Pedigree, Penetrance, Point Mutation, Proline genetics, Threonine genetics, Turkey, Adaptor Proteins, Signal Transducing genetics, Cherubism genetics

Published

2007

14. Molecular genetic testing for familial hypercholesterolemia in the Netherlands: a stepwise screening strategy enhances the mutation detection rate.

Author

Lombardi MP, Redeker EJ, van Gent DH, Smeele KL, Weerdesteijn R, and Mannens MM

Subjects

Adolescent, Adult, Child, Child, Preschool, Chromatography, High Pressure Liquid, Combinatorial Chemistry Techniques methods, Female, Humans, Hyperlipoproteinemia Type II epidemiology, Male, Middle Aged, Molecular Probe Techniques, Netherlands epidemiology, Point Mutation, Sequence Analysis, DNA, Translocation, Genetic, Apolipoproteins B genetics, DNA Mutational Analysis, Genetic Testing methods, Hyperlipoproteinemia Type II genetics, Molecular Diagnostic Techniques methods, Receptors, LDL genetics

Abstract

Familial hypercholesterolemia (FH) has been identified as a major risk factor for coronary vascular disease and is associated with mutations in the low-density liporotein receptor (LDLR) and apolipoprotein B (APOB) gene. The molecular basis of FH in the Dutch population is well understood. Approximately 160 different LDLR and APOB gene defects have been identified with a panel of 9 LDLR gene and 1 APOB gene frequently occurring mutations accounting for approximately 30% of all clinically diagnosed FH cases. As molecular diagnosis of FH is becoming increasingly widely applied, a variety of mutation detection rates is reported, ranging from as low as 30% and up to 80%. This variability appears to depend on the clinical criteria applied to identify patients with FH and on the strategies and methodologies used for mutation screening. In this study we describe the application of a stepwise screening approach, combining different methodologies, to detect mutations of the LDLR gene and APOB gene in 1465 patients with FH. A mutation was found in approximately 44% of the patients, which demonstrates that this is an effective strategy for the molecular diagnosis of FH.

Published

2006

15. Prospective screening for subtelomeric rearrangements in children with mental retardation of unknown aetiology: the Amsterdam experience.

Author

van Karnebeek CD, Koevoets C, Sluijter S, Bijlsma EK, Smeets DF, Redeker EJ, Hennekam RC, and Hoovers JM

Subjects

Adolescent, Child, Child, Preschool, Chromosome Banding, Chromosomes, Artificial, Bacterial genetics, Chromosomes, Artificial, P1 Bacteriophage genetics, Cohort Studies, Female, Humans, Infant, Male, Metaphase genetics, Netherlands, Nucleic Acid Hybridization, Prospective Studies, Tandem Repeat Sequences genetics, Chromosome Aberrations, Genetic Testing methods, Intellectual Disability etiology, Intellectual Disability genetics, Telomere genetics

Abstract

Objective: The frequency of subtelomeric rearrangements in patients with unexplained mental retardation (MR) is uncertain, as most studies have been retrospective and case retrieval may have been biased towards cases more likely to have a chromosome anomaly. To ascertain the frequency of cytogenetic anomalies, including subtelomeric rearrangements, we prospectively screened a consecutive cohort of cases with unexplained MR in an academic tertiary centre., Methods: Inclusion criteria were: age <18 years at referral, IQ<85, no aetiological diagnosis after complete examination, which included karyotyping with high resolution banding (HRB)., Results: In 266 karyotyped children, anomalies were detected in 20 (7.5%, seven numerical, 13 structural); 39 cases were analysed by FISH for specific interstitial microdeletions, and anomalies were found in nine (23%). FISH analyses for subtelomeric microdeletions were performed in 184 children (44% moderate-profound MR, 51% familial MR), and one rearrangement (0.5%) was identified in a non-familial MR female with mild MR (de novo deletion 12q24.33-qter). The number of probable polymorphisms was considerable: 2qter (n=7), Xpter (n=3), and Ypter (n=1). A significantly higher total number of malformations and minor anomalies was present in the cytogenetic anomaly group compared to the group without cytogenetic anomalies., Conclusions: The total frequency of cytogenetic anomalies in this prospective study was high (1:10), but the frequency of subtelomeric rearrangements was low. The most likely explanations are the high quality of HRB cytogenetic studies and the lack of clinical selection bias. Conventional cytogenetic analyses, combined with targeted microdeletion testing, remain the single most effective way of additional investigation in mentally retarded children, also in a tertiary centre.

Published

2002

16. An aetiological study of 25 mentally retarded adults with autism.

Author

van Karnebeek CD, van Gelderen I, Nijhof GJ, Abeling NG, Vreken P, Redeker EJ, van Eeghen AM, Hoovers JM, and Hennekam RC

Subjects

Adolescent, Adult, Autistic Disorder diagnosis, Autistic Disorder etiology, Electroencephalography, Female, Gene Duplication, Genetic Testing, Hospitals, Psychiatric, Humans, In Situ Hybridization, Fluorescence, Intellectual Disability diagnosis, Intellectual Disability etiology, Male, Middle Aged, Netherlands, Syndrome, Autistic Disorder complications, Autistic Disorder genetics, Intellectual Disability complications, Intellectual Disability genetics

Published

2002

17. Molecular genetic testing for familial hypercholesterolemia: spectrum of LDL receptor gene mutations in The Netherlands.

Author

Lombardi MP, Redeker EJ, Defesche JC, Kamerling SW, Trip MD, Mannens MM, Havekes LM, and Kastelein JJ

Subjects

Child, DNA Mutational Analysis, Exons, Gene Deletion, Genetic Testing, Heterozygote, Humans, Introns, Mutation, Missense, Netherlands, RNA Splicing, Hyperlipoproteinemia Type II genetics, Mutation, Receptors, LDL genetics

Abstract

Mutations in the LDL receptor are responsible for familial hypercholesterolemia (FH). At present, more than 600 mutations of the LDL receptor gene are known to underlie FH. However, the array of mutations varies considerably in different populations. Therefore, the delineation of essentially all LDL receptor gene mutations in a population represents a prerequisite for the implementation of nation-wide genetic testing for FH. In this study, the frequency and geographical distribution of 13 known mutations were evaluated in a cohort of 1223 FH patients. We identified 358 mutation carriers, representing 29% of the FH cohort. Four mutations (N543H-2393de19, 1359--1G-->A, 313 + 1 G-->A and W23X) occurred with a relatively high frequency, accounting for 22.4% of the entire study cohort. Two of these common FH mutations (N543H-2393de19 and 1359 - 1G-->A) showed a preferential geographic distribution. Second, to further expand the array of LDL receptor gene mutations, we conducted mutation analysis by denaturing gradient gel electrophoresis (DGGE) in 141 children with definite FH. A mutation was identified in 111 patients, involving 16 new single base substitutions and four small deletions and insertions, which brings the number of different FH-causing mutations in our country up to 61. Our data indicate that an estimate of the prevalence of specific mutations, as well as the compilation of a database of all FH-causing mutations in a given country, can facilitate selection of the most appropriate molecular diagnostic approach.

Published

2000

18. DNA diagnosis in a family with autosomal dominant aniridia.

Author

Verbraak FD, Mannens MA, Redeker EJ, Saunders GF, and Bleeker-Wagemakers EM

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Aniridia diagnosis, Chromosomes, Human, Pair 11, Family, Female, Gene Expression, Genetic Linkage genetics, Genetic Variation genetics, Glaucoma genetics, Humans, Male, Middle Aged, Nystagmus, Pathologic genetics, Pedigree, Visual Acuity, Aniridia genetics, DNA analysis

Abstract

A large family with autosomal dominant aniridia is described. One of the family members presented with reduced visual acuity, nystagmus, slightly distorted macular reflex, but normal irides and clear media. Because of the high variability in expression of aniridia, even within family, a diagnosis of aniridia could not be excluded. However linkage analysis using tightly linked chromosome 11p13 markers flanking the aniridia locus (catalase, D11S151, and D11S325) made it highly unlikely that this patient inherited the aniridia gene from his affected mother.

Published

1991

19. Structure and composition of synaptonemal complexes, isolated from rat spermatocytes.

Author

Heyting C, Dietrich AJ, Redeker EJ, and Vink AC

Subjects

Animals, Chromosomes ultrastructure, Male, Microscopy, Electron, Nucleoproteins isolation & purification, Rats, Spermatocytes analysis, Meiosis, Spermatocytes ultrastructure

Abstract

Synaptonemal complexes (SCs) (structures involved in chromosome pairing during meiosis) were isolated and purified from rat spermatocytes for the purpose of biochemical and morphological analysis. Spermatocytes were lysed in a medium, containing Triton X-100, EDTA and DTT; the resulting swollen nuclei were disrupted by DNAse II, and the suspension was centrifuged through 1.5 M sucrose. The resulting preparation consisted for at least 60% of free SCs, as judged from electron micrographs of agar filtrates. The purified SCs still possessed lateral and transversal elements and attachment plaques. A small fraction also contained a central element. Particularly in diplotene SCs, the lateral elements clearly consisted of two subelements, which are connected by thinner fibres. The lateral elements may fall apart into a network of thinner fibres, presumably as a result of degradation during isolation. On SDS-polyacrylamide gels, the major protein components of purified SCs had relative mobilities (Mrs) of 67 to 60 and 57 to 55 kDa; in addition, there were minor proteins with Mrs of 90, 35, 33, 28, and 26 kDa, and varying amounts of histones. The 67 to 60 kDa proteins comigrate with lamins of rat liver pore complexes and laminae. A possible relationship between SCs and pore complexes and laminae is discussed.

Published

1985

20. Identification of two major components of the lateral elements of synaptonemal complexes of the rat.

Author

Heyting C, Moens PB, van Raamsdonk W, Dietrich AJ, Vink AC, and Redeker EJ

Subjects

Animals, Antibodies, Monoclonal, Antigen-Antibody Complex analysis, Immunoenzyme Techniques, Male, Microscopy, Electron, Rats, Spermatocytes ultrastructure, Meiosis, Spermatocytes cytology, Synaptonemal Complex

Abstract

This paper describes the identification of two major components of the lateral elements of synaptonemal complexes of the rat by immunocytochemical techniques. We prepared monoclonal antibodies against synaptonemal complexes (SCs) by immunization of mice with purified SCs. One of these antibodies, II52F10, reacts with a 30 and a 33 kDa polypeptide, which are major components of purified SCs. Using this antibody, we studied the localization of its antigens light microscopically, by means of the indirect immunoperoxidase technique, as well as ultrastructurally, by means of the immunogold labeling technique. The immunolocalization was carried out on whole-mount preparations of lysed spermatocytes. The antibody reacts with paired as well as unpaired segments of zygotene, pachytene and diplotene SCs. In light microscopic preparations, the attachment plaques, particularly those of late pachytene and diplotene SCs, also appear to react strongly. In electron micrographs the lateral elements in paired as well as unpaired segments could be seen to react. No reaction was observed in the attachment plaques; however, in late pachytene and diplotene SCs the swollen terminal segments of the lateral elements did react with the antibody. Thus, we conclude that a 30 and a 33 kDa polypeptide make part of the lateral elements of synaptonemal complexes of the rat.

Published

1987

21. Two major components of synaptonemal complexes are specific for meiotic prophase nuclei.

Author

Heyting C, Dettmers RJ, Dietrich AJ, Redeker EJ, and Vink AC

Subjects

Animals, Fluorescent Antibody Technique, Male, Molecular Weight, Nuclear Proteins analysis, Prophase, Rats, Cell Nucleus ultrastructure, Meiosis, Spermatids cytology, Spermatocytes cytology, Spermatogonia cytology, Spermatozoa cytology, Synaptonemal Complex

Abstract

Monoclonal antibody II52F10 was elicited against purified synaptonemal complexes (SCs); it recognizes two major components of the lateral elements of SCs, namely an Mr = 30,000 and an Mr = 33,000 protein. We studied the distribution of the antigens of II52F10 within tissues and cells of the male rat by immunoblot analysis and immunocytochemical techniques. Nuclear proteins from various cell types, including spermatogonia and spermatids, did not react with antibody II52F10 on immunoblots; the same holds for proteins from isolated mitotic chromosomes. As expected, an Mr = 30,000 and an Mr = 33,000 protein from spermatocyte nuclei did react with the antibody. In cryostat sections of liver, brain, muscle and gut we could not detect any reaction with II52F10. In the testis the reaction was confined to SCs or SC fragments. Partly on the basis of indirect evidence we identified the antigen-containing cells as zygotene up to and including post-diffuse diplotene spermatocytes. The persistence of some antigen-containing fragments in the earliest stages of spermatids could not be excluded. We conclude that the lateral elements (LEs) of SCs are not assembled by rearrangement of pre-existing components of the nucleus: at least two of their major components are newly synthesized, presumably during zygotene. Furthermore we conclude partly from indirect evidence that the major components of the LEs of SCs are not involved in the chromosome condensation processes that take place during the earliest stages of meiotic prophase.

Published

1988

22. Synaptonemal complex proteins.

Author

Heyting C, Dietrich AJ, Moens PB, Dettmers RJ, Offenberg HH, Redeker EJ, and Vink AC

Subjects

Animals, Antibodies, Monoclonal, Blotting, Western, Electrophoresis, Polyacrylamide Gel, Immunoenzyme Techniques, Immunohistochemistry, Male, Molecular Weight, Nuclear Proteins ultrastructure, Rats, Spermatocytes ultrastructure, Synaptonemal Complex immunology, Meiosis physiology, Nuclear Proteins isolation & purification, Synaptonemal Complex physiology

Abstract

Synaptonemal complexes were isolated from rate spermatocytes for the purpose of biochemical and morphological analysis. Several monoclonal antibodies were elicited against purified synaptonemal complexes to study the composition and assembly of these structures. Four classes of antibodies could be discriminated according to the polypeptides that they recognize on Western blots of purified synaptonemal complexes, namely antibodies recognizing (i) a 190-kDa polypeptide; (ii) a 30- and a 33-kDa polypeptide; (iii) two polypeptides with molecular weights of about 120 kDa; and (iv) polypeptides with molecular weights of 66-55 kDa. The localization of these antigens within spermatocytes was analyzed light microscopically, by means of the immunoperoxidase technique and ultrastructurally, by immunogold labelling of surface-spread spermatocytes. The 66- to 55-kDa polypeptides are not confined to synaptonemal complexes; rather, these polypeptides appear to be chromosomal components. The 190-, 30-, and 33-kDa polypeptides make part of the lateral elements of paired as well as unpaired segments of synaptonemal complexes. The 120-kDa polypeptides were localized on the inner edge of the lateral elements, specifically in paired segments of synaptonemal complexes. The distribution of the 190-, 120-, 30-, and 33-kDa polypeptides within the testis was analyzed by immunofluorescence staining of cryostat sections. All these polypeptides turned out to be specific for nuclei of zygotene up to and including diplotene spermatocytes. Only in some early spermatids could the 190-, 30-, and 33-kDa polypeptides be detected, presumably in remnants of synaptonemal complexes.(ABSTRACT TRUNCATED AT 250 WORDS)

Published

1989

23. Amniotic fluid gel acetylcholinesterase determination in prenatal diagnosis: dark field illumination as a method for improving the detection of precipitation bands.

Author

Leschot NJ, Heyting C, Schaik MV, and Redeker EJ

Subjects

Anencephaly diagnosis, Chemical Precipitation, Electrophoresis, Polyacrylamide Gel, Female, Hernia, Umbilical diagnosis, Humans, Meckel Diverticulum diagnosis, Pregnancy, Spina Bifida Occulta diagnosis, Staining and Labeling, Transillumination, alpha-Fetoproteins analysis, Acetylcholinesterase analysis, Amniocentesis, Amniotic Fluid enzymology, Neural Tube Defects diagnosis

Abstract

This paper describes a sensitive method for the detection of precipitation bands in the qualitative acetylcholinesterase (AChe) gel test. This method--dark field illumination--is compared with two existing methods of detection: epi-illumination of unstained gels and transillumination of dithio-oxamide stained gels. The comparison has been carried out on a selected series of 271 amniotic fluid samples, taken before the 22nd week of gestation. All 96 samples from normal pregnancies were scored as negative with all three visualization methods. For the detection of neural tube defects (NTD) and omphaloceles, dark field illumination proved to be more efficient than epi-illumination or dithio-oxamide staining. In case of another congenital defect, we obtained a positive result with dark field illumination, and a negative one with the other detection methods. It is concluded that dark field illumination was shown to be the most sensitive method for the detection of precipitation bands.

Published

1985