Your search keyword '"Mathijssen IB"' showing total 38 results

1. Counseling couples at risk of having a child with homozygous familial hypercholesterolemia - Clinical experience and recommendations.

Author

Tromp TR, Reijman MD, Wiegman A, Hovingh GK, Defesche JC, van Maarle MC, and Mathijssen IB

Subjects

Humans, Child, Phenotype, Prospective Studies, Counseling, Homozygote, Homozygous Familial Hypercholesterolemia, Hyperlipoproteinemia Type II drug therapy

Abstract

Homozygous familial hypercholesterolemia (HoFH) is a rare, potentially life-limiting, inherited disorder of lipoprotein metabolism characterized by extremely high low-density lipoprotein cholesterol levels. When both parents have heterozygous FH, there is a 25% chance they will conceive a child with HoFH. Here we describe our clinical experience with two such prospective parent couples who were counseled regarding reproductive options and prenatal testing for HoFH. These cases showcase how, in consultation with a molecular geneticist and pediatric cardiologist, parents may be informed of the prognosis and treatment outlook of HoFH based on the FH-variants carried, to ultimately make personal decisions on reproductive options. One couple opted for prenatal testing and termination of pregnancy in case HoFH was found, while the other accepted the risk without testing. We review the available literature on preconception counseling for HoFH and provide practical guidance to clinicians counseling at-risk couples. Optimal counseling of prospective parents may help prevent future physical and psychological problems for both parent and child., Competing Interests: Declaration of Competing Interest AW has received consulting fees from Novartis, is chair of the Steering Committee for the ORION-13 and ORION-16 trial, received payment or honoraria from Amgen, Regeneron and Novartis, and participated on a Data Safety Monitoring Board or Advisory Board of Amgen. GKH reports research grants from the Netherlands Organization for Scientific Research (vidi 016.156.445), CardioVascular Research Initiative, European Union and the Klinkerpad fonds; institutional research support from Aegerion, Amgen, AstraZeneca, Eli Lilly, Genzyme, Ionis, Kowa, Pfizer, Regeneron, Roche, Sanofi, and The Medicines Company; speaker's bureau and consulting fees from Amgen, Aegerion, Sanofi, and Regeneron until April 2019 (fees paid to the academic institution); and part-time employment at Novo Nordisk A/S, Denmark since April 2019. TRT, MDR, JCD, MCvM and IMA declare no conflicts of interest., (Copyright © 2022. Published by Elsevier Inc.)

Published

2023

2. De novo variants in the PABP domain of PABPC1 lead to developmental delay.

Author

Wegler M, Jia X, Alders M, Bouman A, Chen J, Duan X, Lauzon JL, Mathijssen IB, Sticht H, Syrbe S, Tan S, Guo H, and Abou Jamra R

Subjects

Animals, Child, Developmental Disabilities genetics, Heterozygote, Humans, Mice, Poly(A)-Binding Protein I chemistry, RNA, Messenger, RNA-Binding Proteins genetics, Exome Sequencing, Intellectual Disability genetics, Neurodevelopmental Disorders genetics, Poly(A)-Binding Protein I metabolism

Abstract

Purpose: The study aimed to investigate the role of PABPC1 in developmental delay (DD)., Methods: Children were examined by geneticists and pediatricians. Variants were identified using exome sequencing and standard downstream bioinformatics pipelines. We performed in silico molecular modeling and coimmunoprecipitation to test if the variants affect the interaction between PABPC1 and PAIP2. We performed in utero electroporation of mouse embryo brains to enlighten the function of PABPC1., Results: We describe 4 probands with an overlapping phenotype of DD, expressive speech delay, and autistic features and heterozygous de novo variants that cluster in the PABP domain of PABPC1. Further symptoms were seizures and behavioral disorders. Molecular modeling predicted that the variants are pathogenic and would lead to decreased binding affinity to messenger RNA metabolism-related proteins, such as PAIP2. Coimmunoprecipitation confirmed this because it showed a significant weakening of the interaction between mutant PABPC1 and PAIP2. Electroporation of mouse embryo brains showed that Pabpc1 knockdown decreases the proliferation of neural progenitor cells. Wild-type Pabpc1 could rescue this disturbance, whereas 3 of the 4 variants did not., Conclusion: Pathogenic variants in the PABP domain lead to DD, possibly because of interference with the translation initiation and subsequently an impaired neurogenesis in cortical development., Competing Interests: Conflict of Interest The authors declare no conflicts of interest., (Copyright © 2022 American College of Medical Genetics and Genomics. Published by Elsevier Inc. All rights reserved.)

Published

2022

3. [A female with excessive wrinkling of the hands].

Author

Melger JWJ, Knijnenburg PJC, and Mathijssen IB

Subjects

Adult, Female, Hand, Humans, Water, Young Adult, Cystic Fibrosis complications, Cystic Fibrosis diagnosis, Cystic Fibrosis genetics, Skin Aging

Abstract

A 23-year-old female complained of excessive wrinkling of her hands after brief exposure to water. The symptoms were characteristic for the diagnosis aquagenic wrinkling of the palms (AWP). This disorder is frequently associated with cystic fibrosis (CF) or CF carrier state. DNA analysis of the cystic fibrosis gene is indicated.

Published

2022

4. Germline variants in HEY2 functional domains lead to congenital heart defects and thoracic aortic aneurysms.

Author

van Walree ES, Dombrowsky G, Jansen IE, Umićević Mirkov M, Zwart R, Ilgun A, Guo D, Clur SB, Amin AS, Savage JE, van der Wal AC, Waisfisz Q, Maugeri A, Wilsdon A, Bu'Lock FA, Hurles ME, Dittrich S, Berger F, Audain Martinez E, Christoffels VM, Hitz MP, Milewicz DM, Posthuma D, Meijers-Heijboer H, Postma AV, and Mathijssen IB

Published

2022

5. Patient-Specific TBX5-G125R Variant Induces Profound Transcriptional Deregulation and Atrial Dysfunction.

Author

van Ouwerkerk AF, Bosada FM, van Duijvenboden K, Houweling AC, Scholman KT, Wakker V, Allaart CP, Uhm JS, Mathijssen IB, Baartscheer T, Postma AV, Barnett P, Verkerk AO, Boukens BJ, and Christoffels VM

Subjects

Amino Acid Substitution, Animals, Atrial Fibrillation genetics, Atrial Fibrillation metabolism, Female, Heart Atria metabolism, Humans, Male, Mice, Mice, Mutant Strains, Abnormalities, Multiple genetics, Abnormalities, Multiple metabolism, Gene Expression Regulation, Heart Defects, Congenital genetics, Heart Defects, Congenital metabolism, Heart Septal Defects, Atrial genetics, Heart Septal Defects, Atrial metabolism, Heterozygote, Lower Extremity Deformities, Congenital genetics, Lower Extremity Deformities, Congenital metabolism, Mutation, Missense, Pedigree, T-Box Domain Proteins genetics, T-Box Domain Proteins metabolism, Upper Extremity Deformities, Congenital genetics, Upper Extremity Deformities, Congenital metabolism

Abstract

Background: The pathogenic missense variant p.G125R in TBX5 (T-box transcription factor 5) causes Holt-Oram syndrome (also known as hand-heart syndrome) and early onset of atrial fibrillation. Revealing how an altered key developmental transcription factor modulates cardiac physiology in vivo will provide unique insights into the mechanisms underlying atrial fibrillation in these patients., Methods: We analyzed ECGs of an extended family pedigree of Holt-Oram syndrome patients. Next, we introduced the TBX5-p.G125R variant in the mouse genome ( Tbx5 G125R ) and performed electrophysiologic analyses (ECG, optical mapping, patch clamp, intracellular calcium measurements), transcriptomics (single-nuclei and tissue RNA sequencing), and epigenetic profiling (assay for transposase-accessible chromatin using sequencing, H3K27ac [histone H3 lysine 27 acetylation] CUT&RUN [cleavage under targets and release under nuclease sequencing])., Results: We discovered high incidence of atrial extra systoles and atrioventricular conduction disturbances in Holt-Oram syndrome patients. Tbx5 G125R/+ mice were morphologically unaffected and displayed variable RR intervals, atrial extra systoles, and susceptibility to atrial fibrillation, reminiscent of TBX5-p.G125R patients. Atrial conduction velocity was not affected but systolic and diastolic intracellular calcium concentrations were decreased and action potentials were prolonged in isolated cardiomyocytes of Tbx5 G125R/+ mice compared with controls. Transcriptional profiling of atria revealed the most profound transcriptional changes in cardiomyocytes versus other cell types, and identified over a thousand coding and noncoding transcripts that were differentially expressed. Epigenetic profiling uncovered thousands of TBX5-p.G125R-sensitive, putative regulatory elements (including enhancers) that gained accessibility in atrial cardiomyocytes. The majority of sites with increased accessibility were occupied by Tbx5. The small group of sites with reduced accessibility was enriched for DNA-binding motifs of members of the SP (specificity protein) and KLF (Krüppel-like factor) families of transcription factors. These data show that Tbx5-p.G125R induces changes in regulatory element activity, alters transcriptional regulation, and changes cardiomyocyte behavior, possibly caused by altered DNA binding and cooperativity properties., Conclusions: Our data reveal that a disease-causing missense variant in TBX5 induces profound changes in the atrial transcriptional regulatory network and epigenetic state in vivo, leading to arrhythmia reminiscent of those seen in human TBX5-p.G125R variant carriers.

Published

2022

6. Bi-allelic variants in DNA mismatch repair proteins MutS Homolog MSH4 and MSH5 cause infertility in both sexes.

Author

Wyrwoll MJ, van Walree ES, Hamer G, Rotte N, Motazacker MM, Meijers-Heijboer H, Alders M, Meißner A, Kaminsky E, Wöste M, Krallmann C, Kliesch S, Hunt TJ, Clark AT, Silber S, Stallmeyer B, Friedrich C, van Pelt AMM, Mathijssen IB, and Tüttelmann F

Subjects

Cell Cycle Proteins genetics, DNA Mismatch Repair, Female, HEK293 Cells, Humans, Male, Meiosis genetics, MutS DNA Mismatch-Binding Protein genetics, Azoospermia genetics, Infertility, Male genetics

Abstract

Study Question: Do bi-allelic variants in the genes encoding the MSH4/MSH5 heterodimer cause male infertility?, Summary Answer: We detected biallelic, (likely) pathogenic variants in MSH5 (4 men) and MSH4 (3 men) in six azoospermic men, demonstrating that genetic variants in these genes are a relevant cause of male infertility., What Is Known Already: MSH4 and MSH5 form a heterodimer, which is required for prophase of meiosis I. One variant in MSH5 and two variants in MSH4 have been described as causal for premature ovarian insufficiency (POI) in a total of five women, resulting in infertility. Recently, pathogenic variants in MSH4 have been reported in infertile men. So far, no pathogenic variants in MSH5 had been described in males., Study Design, Size, Duration: We utilized exome data from 1305 men included in the Male Reproductive Genomics (MERGE) study, including 90 males with meiotic arrest (MeiA). Independently, exome sequencing was performed in a man with MeiA from a large consanguineous family., Participants/materials, Setting, Methods: Assuming an autosomal-recessive mode of inheritance, we screened the exome data for rare, biallelic coding variants in MSH4 and MSH5. If possible, segregation analysis in the patients' families was performed. The functional consequences of identified loss-of-function (LoF) variants in MSH5 were studied using heterologous expression of the MSH5 protein in HEK293T cells. The point of arrest during meiosis was determined by γH2AX staining., Main Results and the Role of Chance: We report for the first time (likely) pathogenic, homozygous variants in MSH5 causing infertility in 2 out of 90 men with MeiA and overall in 4 out of 902 azoospermic men. Additionally, we detected biallelic variants in MSH4 in two men with MeiA and in the sister of one proband with POI. γH2AX staining revealed an arrest in early prophase of meiosis I in individuals with pathogenic MSH4 or MSH5 variants. Heterologous in vitro expression of the detected LoF variants in MSH5 showed that the variant p.(Ala620GlnTer9) resulted in MSH5 protein truncation and the variant p.(Ser26GlnfsTer42) resulted in a complete loss of MSH5., Large Scale Data: All variants have been submitted to ClinVar (SCV001468891-SCV001468896 and SCV001591030) and can also be accessed in the Male Fertility Gene Atlas (MFGA)., Limitations, Reasons for Caution: By selecting for variants in MSH4 and MSH5, we were able to determine the cause of infertility in six men and one woman, leaving most of the examined individuals without a causal diagnosis., Wider Implications of the Findings: Our findings have diagnostic value by increasing the number of genes associated with non-obstructive azoospermia with high clinical validity. The analysis of such genes has prognostic consequences for assessing whether men with azoospermia would benefit from a testicular biopsy. We also provide further evidence that MeiA in men and POI in women share the same genetic causes., Study Funding/competing Interest(s): This study was carried out within the frame of the German Research Foundation sponsored Clinical Research Unit 'Male Germ Cells: from Genes to Function' (DFG, CRU326), and supported by institutional funding of the Research Institute Amsterdam Reproduction and Development and funds from the LucaBella Foundation. The authors declare no conflict of interest., (© The Author(s) 2021. Published by Oxford University Press on behalf of European Society of Human Reproduction and Embryology. All rights reserved. For permissions, please email: journals.permissions@oup.com.)

Published

2021

7. Couples' experiences with expanded carrier screening: evaluation of a university hospital screening offer.

Author

van Dijke I, Lakeman P, Sabiri N, Rusticus H, Ottenheim CPE, Mathijssen IB, Cornel MC, and Henneman L

Subjects

Adult, Female, Genetic Counseling methods, Hospitals, University statistics & numerical data, Humans, Male, Patients psychology, Genetic Carrier Screening, Genetic Counseling psychology, Patient Participation

Abstract

Preconception carrier screening offers couples the possibility to receive information about the risk of having a child with a recessive disorder. Since 2016, an expanded carrier screening (ECS) test for 50 severe autosomal recessive disorders has been available at Amsterdam Medical Center, a Dutch university hospital. This mixed-methods study evaluated the experiences of couples that participated in the carrier screening offer, including high-risk participants, as well as participants with a general population risk. All participants received genetic counselling, and pre- (n = 132) and post-test (n = 86) questionnaires and semi-structured interviews (n = 16) were administered. The most important reason to have ECS was to spare a future child a life with a severe disorder (47%). The majority of survey respondents made an informed decision (86%), as assessed by the Multidimensional Measure of Informed Choice. Among the 86 respondents, 27 individual carriers and no new carrier couples were identified. Turn-around time of the test results was considered too long and costs were perceived as too high. Overall, mean levels of anxiety were not clinically elevated. High-risk respondents (n = 89) and pregnant respondents (n = 13) experienced higher levels of anxiety before testing, which decreased after receiving the test result. Although not clinically significant, distress was on average higher for carriers compared to non-carriers (p < 0.0001). All respondents would opt for the test again, and 80.2% would recommend it to others. The results suggest that ECS should ideally be offered before pregnancy, to minimise anxiety. This study could inform current and future implementation initiatives of preconception ECS., (© 2021. The Author(s).)

Published

2021

8. TMEM218 dysfunction causes ciliopathies, including Joubert and Meckel syndromes.

Author

Van De Weghe JC, Giordano JL, Mathijssen IB, Mojarrad M, Lugtenberg D, Miller CV, Dempsey JC, Mohajeri MSA, van Leeuwen E, Pajkrt E, Klaver CCW, Houlden H, Eslahi A, Waters AM, Bamshad MJ, Nickerson DA, Aggarwal VS, de Vries BBA, Maroofian R, and Doherty D

Abstract

The Joubert-Meckel syndrome spectrum is a continuum of recessive ciliopathy conditions caused by primary cilium dysfunction. The primary cilium is a microtubule-based, antenna-like organelle that projects from the surface of most human cell types, allowing them to respond to extracellular signals. The cilium is partitioned from the cell body by the transition zone, a known hotspot for ciliopathy-related proteins. Despite years of Joubert syndrome (JBTS) gene discovery, the genetic cause cannot be identified in up to 30% of individuals with JBTS, depending on the cohort, sequencing method, and criteria for pathogenic variants. Using exome and targeted sequencing of 655 families with JBTS, we identified three individuals from two families harboring biallelic, rare, predicted-deleterious missense TMEM218 variants. Via MatchMaker Exchange, we identified biallelic TMEM218 variants in four additional families with ciliopathy phenotypes. Of note, four of the six families carry missense variants affecting the same highly conserved amino acid position 115. Clinical features included the molar tooth sign (N = 2), occipital encephalocele (N = 5, all fetuses), retinal dystrophy (N = 4, all living individuals), polycystic kidneys (N = 2), and polydactyly (N = 2), without liver involvement. Combined with existing functional data linking TMEM218 to ciliary transition zone function, our human genetic data make a strong case for TMEM218 dysfunction as a cause of ciliopathy phenotypes including JBTS with retinal dystrophy and Meckel syndrome. Identifying all genetic causes of the Joubert-Meckel spectrum enables diagnostic testing, prognostic and recurrence risk counseling, and medical monitoring, as well as work to delineate the underlying biological mechanisms and identify targets for future therapies., Competing Interests: Declaration of interests The authors declare no competing interests.

Published

2021

9. Germline variants in HEY2 functional domains lead to congenital heart defects and thoracic aortic aneurysms.

Author

van Walree ES, Dombrowsky G, Jansen IE, Mirkov MU, Zwart R, Ilgun A, Guo D, Clur SB, Amin AS, Savage JE, van der Wal AC, Waisfisz Q, Maugeri A, Wilsdon A, Bu'Lock FA, Hurles ME, Dittrich S, Berger F, Audain Martinez E, Christoffels VM, Hitz MP, Milewicz DM, Posthuma D, Meijers-Heijboer H, Postma AV, and Mathijssen IB

Subjects

Basic Helix-Loop-Helix Transcription Factors genetics, Genetic Predisposition to Disease, Germ Cells, Humans, Pedigree, Repressor Proteins, Aortic Aneurysm, Thoracic genetics, Heart Defects, Congenital genetics

Abstract

Purpose: In this study we aimed to establish the genetic cause of a myriad of cardiovascular defects prevalent in individuals from a genetically isolated population, who were found to share a common ancestor in 1728., Methods: Trio genome sequencing was carried out in an index patient with critical congenital heart disease (CHD); family members had either exome or Sanger sequencing. To confirm enrichment, we performed a gene-based association test and meta-analysis in two independent validation cohorts: one with 2685 CHD cases versus 4370 . These controls were also ancestry-matched (same as FTAA controls), and the other with 326 cases with familial thoracic aortic aneurysms (FTAA) and dissections versus 570 ancestry-matched controls. Functional consequences of identified variants were evaluated using expression studies., Results: We identified a loss-of-function variant in the Notch target transcription factor-encoding gene HEY2. The homozygous state (n = 3) causes life-threatening congenital heart defects, while 80% of heterozygous carriers (n = 20) had cardiovascular defects, mainly CHD and FTAA of the ascending aorta. We confirm enrichment of rare risk variants in HEY2 functional domains after meta-analysis (MetaSKAT p = 0.018). Furthermore, we show that several identified variants lead to dysregulation of repression by HEY2., Conclusion: A homozygous germline loss-of-function variant in HEY2 leads to critical CHD. The majority of heterozygotes show a myriad of cardiovascular defects.

Published

2021

10. How will new genetic technologies, such as gene editing, change reproductive decision-making? Views of high-risk couples.

Author

van Dijke I, Lakeman P, Mathijssen IB, Goddijn M, Cornel MC, and Henneman L

Subjects

Adult, Decision Making, Female, Genetic Testing ethics, Humans, Male, Gene Editing ethics, Genetic Counseling psychology, Genetic Predisposition to Disease psychology, Genetic Therapy psychology, Health Knowledge, Attitudes, Practice, Reproductive Behavior psychology

Abstract

Couples at increased risk of having offspring with a specific genetic disorder who want to avoid having an affected child have several reproductive options including prenatal diagnosis (PND) and preimplantation genetic testing (PGT). In the future, non-invasive prenatal diagnosis (NIPD), germline gene editing (GGE) and somatic gene editing (SGE) might become available. This study explores if, and how, availability of new genetic technologies, including NIPD, GGE, SGE, would change reproductive decision-making of high-risk couples. In 2018, semi-structured interviews were conducted with 25 genetically at-risk couples. Couples previously had received genetic counselling for PND and PGT, and in most cases opted for (one of) these techniques, at one Dutch Clinical Genetics Center between 2013 and 2017. Considerations participants mentioned regarding the hypothetical use of NIPD, GGE and SGE, seem similar to considerations regarding PND and PGT and are reflected in underlying concepts. These include safety and burden for mother and child, and moral considerations. Couples generally favoured NIPD over PND as this would be safe and enables earlier diagnosis. Increased opportunities of having a 'healthy' embryo and less embryo disposal were considerations in favour of GGE. Some regarded GGE as unsafe and feared slippery slope scenarios. Couples were least favourable towards SGE compared to choosing for a genetic reproductive technology, because of the perceived burden for the affected offspring. With the possibly growing number of technological options, understanding high risk couples' perspectives can assist in navigating the reproductive decision-making process. Counsellors should be prepared to counsel on more and complex reproductive options.

Published

2021

11. Development, behaviour and sensory processing in Marshall-Smith syndrome and Malan syndrome: phenotype comparison in two related syndromes.

Author

Mulder PA, van Balkom IDC, Landlust AM, Priolo M, Menke LA, Acero IH, Alkuraya FS, Arias P, Bernardini L, Bijlsma EK, Cole T, Coubes C, Dapia I, Davies S, Di Donato N, Elcioglu NH, Fahrner JA, Foster A, González NG, Huber I, Iascone M, Kaiser AS, Kamath A, Kooblall K, Lapunzina P, Liebelt J, Lynch SA, Maas SM, Mammì C, Mathijssen IB, McKee S, Mirzaa GM, Montgomery T, Neubauer D, Neumann TE, Pintomalli L, Pisanti MA, Plomp AS, Price S, Salter C, Santos-Simarro F, Sarda P, Schanze D, Segovia M, Shaw-Smith C, Smithson S, Suri M, Tatton-Brown K, Tenorio J, Thakker RV, Valdez RM, Van Haeringen A, Van Hagen JM, Zenker M, Zollino M, Dunn WW, Piening S, and Hennekam RC

Subjects

Adaptation, Psychological, Adolescent, Adult, Child, Child, Preschool, Comorbidity, Cross-Sectional Studies, Female, Follow-Up Studies, Humans, Male, Mental Disorders physiopathology, Netherlands epidemiology, Phenotype, Speech Disorders physiopathology, Syndrome, Young Adult, Abnormalities, Multiple epidemiology, Abnormalities, Multiple physiopathology, Bone Diseases, Developmental epidemiology, Bone Diseases, Developmental physiopathology, Craniofacial Abnormalities epidemiology, Craniofacial Abnormalities physiopathology, Intellectual Disability epidemiology, Intellectual Disability physiopathology, Mental Disorders epidemiology, Septo-Optic Dysplasia epidemiology, Septo-Optic Dysplasia physiopathology, Speech Disorders epidemiology

Abstract

Background: Ultrarare Marshall-Smith and Malan syndromes, caused by changes of the gene nuclear factor I X (NFIX), are characterised by intellectual disability (ID) and behavioural problems, although questions remain. Here, development and behaviour are studied and compared in a cross-sectional study, and results are presented with genetic findings., Methods: Behavioural phenotypes are compared of eight individuals with Marshall-Smith syndrome (three male individuals) and seven with Malan syndrome (four male individuals). Long-term follow-up assessment of cognition and adaptive behaviour was possible in three individuals with Marshall-Smith syndrome., Results: Marshall-Smith syndrome individuals have more severe ID, less adaptive behaviour, more impaired speech and less reciprocal interaction compared with individuals with Malan syndrome. Sensory processing difficulties occur in both syndromes. Follow-up measurement of cognition and adaptive behaviour in Marshall-Smith syndrome shows different individual learning curves over time., Conclusions: Results show significant between and within syndrome variability. Different NFIX variants underlie distinct clinical phenotypes leading to separate entities. Cognitive, adaptive and sensory impairments are common in both syndromes and increase the risk of challenging behaviour. This study highlights the value of considering behaviour within developmental and environmental context. To improve quality of life, adaptations to environment and treatment are suggested to create a better person-environment fit., (© 2020 MENCAP and International Association of the Scientific Study of Intellectual and Developmental Disabilities and John Wiley & Sons Ltd.)

Published

2020

12. Biallelic loss of function variants in COASY cause prenatal onset pontocerebellar hypoplasia, microcephaly, and arthrogryposis.

Author

van Dijk T, Ferdinandusse S, Ruiter JPN, Alders M, Mathijssen IB, Parboosingh JS, Innes AM, Meijers-Heijboer H, Poll-The BT, Bernier FP, Wanders RJA, Lamont RE, and Baas F

Subjects

Aborted Fetus abnormalities, Arthrogryposis pathology, Cells, Cultured, Cerebellar Diseases pathology, Humans, Infant, Newborn, Male, Microcephaly pathology, Syndrome, Transferases metabolism, Arthrogryposis genetics, Cerebellar Diseases genetics, Loss of Function Mutation, Microcephaly genetics, Transferases genetics

Abstract

Pontocerebellar hypoplasia (PCH) is a heterogeneous neurodegenerative disorder with a prenatal onset. Using whole-exome sequencing, we identified variants in the gene Coenzyme A (CoA) synthase (COASY) gene, an enzyme essential in CoA synthesis, in four individuals from two families with PCH, prenatal onset microcephaly, and arthrogryposis. In family 1, compound heterozygous variants were identified in COASY: c.[1549&#95;1550delAG]; [1486-3 C>G]. In family 2, all three affected siblings were homozygous for the c.1486-3 C>G variant. In both families, the variants segregated with the phenotype. RNA analysis showed that the c.1486-3 C>G variant leads to skipping of exon 7 with partial retention of intron 7, disturbing the reading frame and resulting in a premature stop codon (p.(Ala496Ilefs*20)). No CoA synthase protein was detected in patient cells by immunoblot analysis and CoA synthase activity was virtually absent. Partial CoA synthase defects were previously described as a cause of COASY Protein-Associated Neurodegeneration (CoPAN), a type of Neurodegeneration and Brain Iron Accumulation (NBIA). Here we demonstrate that near complete loss of function variants in COASY are associated with lethal PCH and arthrogryposis.

Published

2018

13. Further delineation of Malan syndrome.

Author

Priolo M, Schanze D, Tatton-Brown K, Mulder PA, Tenorio J, Kooblall K, Acero IH, Alkuraya FS, Arias P, Bernardini L, Bijlsma EK, Cole T, Coubes C, Dapia I, Davies S, Di Donato N, Elcioglu NH, Fahrner JA, Foster A, González NG, Huber I, Iascone M, Kaiser AS, Kamath A, Liebelt J, Lynch SA, Maas SM, Mammì C, Mathijssen IB, McKee S, Menke LA, Mirzaa GM, Montgomery T, Neubauer D, Neumann TE, Pintomalli L, Pisanti MA, Plomp AS, Price S, Salter C, Santos-Simarro F, Sarda P, Segovia M, Shaw-Smith C, Smithson S, Suri M, Valdez RM, Van Haeringen A, Van Hagen JM, Zollino M, Lapunzina P, Thakker RV, Zenker M, and Hennekam RC

Subjects

Abnormalities, Multiple physiopathology, Adolescent, Adult, Bone Diseases, Developmental genetics, Bone Diseases, Developmental physiopathology, Child, Child, Preschool, Chromosome Deletion, Congenital Hypothyroidism physiopathology, Craniofacial Abnormalities physiopathology, Developmental Disabilities genetics, Developmental Disabilities physiopathology, Exons genetics, Female, Hand Deformities, Congenital physiopathology, Humans, Intellectual Disability physiopathology, Male, Megalencephaly genetics, Megalencephaly physiopathology, Mutation, Missense genetics, Phenotype, Septo-Optic Dysplasia genetics, Septo-Optic Dysplasia physiopathology, Sotos Syndrome physiopathology, Young Adult, Abnormalities, Multiple genetics, Congenital Hypothyroidism genetics, Craniofacial Abnormalities genetics, Hand Deformities, Congenital genetics, Intellectual Disability genetics, NFI Transcription Factors genetics, Sotos Syndrome genetics

Abstract

Malan syndrome is an overgrowth disorder described in a limited number of individuals. We aim to delineate the entity by studying a large group of affected individuals. We gathered data on 45 affected individuals with a molecularly confirmed diagnosis through an international collaboration and compared data to the 35 previously reported individuals. Results indicate that height is > 2 SDS in infancy and childhood but in only half of affected adults. Cardinal facial characteristics include long, triangular face, macrocephaly, prominent forehead, everted lower lip, and prominent chin. Intellectual disability is universally present, behaviorally anxiety is characteristic. Malan syndrome is caused by deletions or point mutations of NFIX clustered mostly in exon 2. There is no genotype-phenotype correlation except for an increased risk for epilepsy with 19p13.2 microdeletions. Variants arose de novo, except in one family in which mother was mosaic. Variants causing Malan and Marshall-Smith syndrome can be discerned by differences in the site of stop codon formation. We conclude that Malan syndrome has a well recognizable phenotype that usually can be discerned easily from Marshall-Smith syndrome but rarely there is some overlap. Differentiation from Sotos and Weaver syndrome can be made by clinical evaluation only., (© 2018 The Authors. Human Mutation published by Wiley Periodicals, Inc.)

Published

2018

14. Homozygous DMRT2 variant associates with severe rib malformations in a newborn.

Author

Bouman A, Waisfisz Q, Admiraal J, van de Loo M, van Rijn RR, Micha D, Oostra RJ, and Mathijssen IB

Subjects

Alleles, Fatal Outcome, Genetic Association Studies, Genetic Predisposition to Disease, Heterozygote, Humans, Infant, Newborn, Male, Radiography, Ribs diagnostic imaging, Spine diagnostic imaging, Tomography, Spiral Computed, Exome Sequencing, Abnormalities, Multiple diagnosis, Abnormalities, Multiple genetics, DNA-Binding Proteins genetics, Hernia, Diaphragmatic diagnosis, Hernia, Diaphragmatic genetics, Homozygote, Mutation, Phenotype, Ribs abnormalities, Spine abnormalities, Transcription Factors genetics

Abstract

Spondylocostal dysostosis (SCD) is a rare disorder characterized by vertebral segmentation defects and malformations of the ribs. SCD patients have some degree of (kypho)scoliosis, short stature and suffer from respiratory impairment due to the reduced size of their thoracic cage. Mutations in DLL3, MESP2, LFNG, HES7, TBX6, and RIPPLY2 are known to cause different subtypes of SCD. Here, we report on a male neonate with an apparent distinct SCD-like phenotype only partly overlapping the previously described SCD subtypes. The proband presented with severe rib malformations (missing, fused, bifid, and hypoplastic ribs), vertebral malformations (intervertebral fusions of the laminae and irregular ossification of the vertebral bodies), and a mild scoliosis. Clear segmentation defects of the vertebral bodies were lacking. Other dysmorphic features were present as well. Severe respiratory insufficiency was present from birth. Whole exome sequencing identified a homozygous start-loss variant in DMRT2 (NM&#95;006557.6: c.1A > T p.[Met1?]) being a likely cause of the SCD-like phenotype in the proband. Mutations in DMRT2 (OMIM#604935) have not been described in relation to SCD-related phenotypes in humans before. However, Dmrt2 knock-out mice exhibit severe rib and vertebral defects that strikingly overlap with the radiological phenotype of the proband reported here. Therefore, it seems plausible that mutations in DMRT2 are associated with a different (novel) subtype of SCD mainly characterized by severe rib anomalies but lacking clear segmentation defects of the vertebral bodies., (© 2018 Wiley Periodicals, Inc.)

Published

2018

15. Preconception carrier screening for multiple disorders: evaluation of a screening offer in a Dutch founder population.

Author

Mathijssen IB, Holtkamp KCA, Ottenheim CPE, van Eeten-Nijman JMC, Lakeman P, Meijers-Heijboer H, van Maarle MC, and Henneman L

Subjects

Adult, Awareness, Female, Founder Effect, Humans, Male, Genetic Counseling psychology, Genetic Testing, Health Knowledge, Attitudes, Practice, Heterozygote, Population genetics, Preconception Care

Abstract

Technological developments have enabled carrier screening for multiple disorders. This study evaluated experiences with a preconception carrier screening offer for four recessive disorders in a Dutch founder population. Questionnaires were completed by 182 attendees pretesting and posttesting and by 137 non-attendees. Semistructured interviews were conducted with seven of the eight carrier couples. Attendees were mainly informed about the existence of screening by friends/colleagues (49%) and family members (44%). Familiarity with the genetic disorders was high. Knowledge after counseling increased (p < 0.001); however, still 9%, compared to 29% before counseling, wrongly mentioned an increased risk of having an affected child if both parents are carriers of different disorders. Most attendees (97%) recalled their test results correctly, but two couples reported being carrier of another disorder than reported. Overall, 63% felt worried while waiting for results but anxiety levels returned to normal afterwards. In all, 2/39 (5%) carriers felt less healthy. Screened individuals were very satisfied; they did not regret testing (97%) and would recommend testing to others (97%). The majority (94%) stated that couples should always have a pretest consultation, preferably by a genetic counselor rather than their general practitioner (83%). All carrier couples made reproductive decisions based on their results. Main reason for non-attendance was unawareness of the screening offer. With expanded carrier screening, adequately informing couples pretest and posttesting is of foremost importance. Close influencers (family/friends) can be used to raise awareness of a screening offer. Our findings provide lessons for the implementation of expanded carrier screening panels in other communities and other settings.

Published

2018

16. With expanded carrier screening, founder populations run the risk of being overlooked.

Author

Mathijssen IB, van Maarle MC, Kleiss IIM, Redeker EJW, Ten Kate LP, Henneman L, and Meijers-Heijboer H

Abstract

Genetically isolated populations exist worldwide. Specific genetic disorders, including rare autosomal recessive disorders may have high prevalences in these populations. We searched for Dutch genetically isolated populations and their autosomal recessive founder mutations. We investigated whether these founder mutations are covered in the (preconception) expanded carrier screening tests of five carrier screening providers. Our results show that the great majority of founder mutations are not covered in these screening panels, and these panels may thus not be appropriate for use in founder populations. It is therefore important to be aware of founder mutations in a population when offering carrier tests.

Published

2017

17. Factors for successful implementation of population-based expanded carrier screening: learning from existing initiatives.

Author

Holtkamp KCA, Mathijssen IB, Lakeman P, van Maarle MC, Dondorp WJ, Henneman L, and Cornel MC

Subjects

Adolescent, Adult, Female, Humans, Jews genetics, Male, Netherlands, Young Adult, Genetic Testing methods, Heterozygote, Mass Screening methods

Abstract

Background: Carrier screening for autosomal recessive disorders aims to facilitate reproductive decision-making by identifying couples with a 1-in-4 risk in every pregnancy of having an affected child. Except for a few countries or regions, carrier screening is not widely offered and is mostly ancestry-based. Technological advances enable carrier screening for multiple diseases simultaneously allowing universal screening regardless of ancestry (population-based expanded carrier screening). It is important to study how this can be successfully implemented. This study therefore aims to identify critical factors involved in successful implementation, from a user perspective, by learning from already implemented initiatives., Methods: Factors associated with successful implementation were identified by: (i) a literature review and (ii) two case studies; studying experiences with carrier screening in two high-risk communities (a Dutch founder population and the Ashkenazi Jewish population), including a survey among community members., Results: Factors identified were familiarity with (specific) genetic diseases and its availability, high perceived benefits of screening (e.g. screening avoids much suffering), acceptance of reproductive options, perceived risk of being a carrier and low perceived social barriers (e.g. stigmatization). In contrast to the Jewish community, the initial demand for screening in the Dutch founder population did not entirely come from the community itself. However, the large social cohesion of the community facilitated the implementation process., Conclusion: To ensure successful implementation of population-based expanded carrier screening, efforts should be made to increase knowledge about genetic diseases, create awareness and address personal benefits of screening in a non-directive way., (© The Author 2016. Published by Oxford University Press on behalf of the European Public Health Association.)

Published

2017

18. The phenotypic spectrum of Schaaf-Yang syndrome: 18 new affected individuals from 14 families.

Author

Fountain MD, Aten E, Cho MT, Juusola J, Walkiewicz MA, Ray JW, Xia F, Yang Y, Graham BH, Bacino CA, Potocki L, van Haeringen A, Ruivenkamp CA, Mancias P, Northrup H, Kukolich MK, Weiss MM, van Ravenswaaij-Arts CM, Mathijssen IB, Levesque S, Meeks N, Rosenfeld JA, Lemke D, Hamosh A, Lewis SK, Race S, Stewart LL, Hay B, Lewis AM, Guerreiro RL, Bras JT, Martins MP, Derksen-Lubsen G, Peeters E, Stumpel C, Stegmann S, Bok LA, Santen GW, and Schaaf CP

Subjects

Adolescent, Adult, Autism Spectrum Disorder physiopathology, Child, Child, Preschool, Chromosomes, Human, Pair 15, Developmental Disabilities physiopathology, Female, Gene Expression, Genomic Imprinting, Humans, Infant, Infant, Newborn, Intellectual Disability physiopathology, Male, Mutation, Phenotype, Prader-Willi Syndrome physiopathology, Autism Spectrum Disorder genetics, Developmental Disabilities genetics, Intellectual Disability genetics, Prader-Willi Syndrome genetics, Proteins genetics

Abstract

Purpose: Truncating mutations in the maternally imprinted, paternally expressed gene MAGEL2, which is located in the Prader-Willi critical region 15q11-13, have recently been reported to cause Schaaf-Yang syndrome, a Prader-Willi-like disease that manifests as developmental delay/intellectual disability, hypotonia, feeding difficulties, and autism spectrum disorder. The causality of the reported variants in the context of the patients' phenotypes was questioned, as MAGEL2 whole-gene deletions seem to cause little or no clinical phenotype., Methods: Here we report a total of 18 newly identified individuals with Schaaf-Yang syndrome from 14 families, including 1 family with 3 individuals found to be affected with a truncating variant of MAGEL2, 11 individuals who are clinically affected but were not tested molecularly, and a presymptomatic fetal sibling carrying the pathogenic MAGEL2 variant., Results: All cases harbor truncating mutations of MAGEL2, and nucleotides c.1990-1996 arise as a mutational hotspot, with 10 individuals and 1 fetus harboring a c.1996dupC (p.Q666fs) mutation and 2 fetuses harboring a c.1996delC (p.Q666fs) mutation. The phenotypic spectrum of Schaaf-Yang syndrome ranges from fetal akinesia to neurobehavioral disease and contractures of the small finger joints., Conclusion: This study provides strong evidence for the pathogenicity of truncating mutations of the paternal allele of MAGEL2, refines the associated clinical phenotypes, and highlights implications for genetic counseling for affected families.Genet Med 19 1, 45-52.

Published

2017

19. LONG-TERM FOLLOW-UP OF PATIENTS WITH RETINITIS PIGMENTOSA TYPE 12 CAUSED BY CRB1 MUTATIONS: A Severe Phenotype With Considerable Interindividual Variability.

Author

Mathijssen IB, Florijn RJ, van den Born LI, Zekveld-Vroon RC, Ten Brink JB, Plomp AS, Baas F, Meijers-Heijboer H, Bergen AA, and van Schooneveld MJ

Subjects

Adolescent, Adult, Aged, Electroretinography, Female, Follow-Up Studies, Humans, Male, Middle Aged, Phenotype, Retinitis Pigmentosa genetics, Retinitis Pigmentosa pathology, Retinitis Pigmentosa physiopathology, Tomography, Optical Coherence, Vision Disorders etiology, Vision Disorders physiopathology, Visual Acuity physiology, Visual Fields physiology, Young Adult, Eye Proteins genetics, Membrane Proteins genetics, Mutation, Nerve Tissue Proteins genetics

Abstract

Purpose: To examine the long-term clinical course and variability in a large pedigree segregating CRB1 type autosomal recessive retinitis pigmentosa., Methods: An observational case study of 30 patients with CRB1 type autosomal recessive retinitis pigmentosa, homozygous for the CRB1 c.3122T > C; p.(Met1041Thr) mutation from a Dutch genetically isolated population in which the CRB1 gene was originally identified. The authors evaluated medical records, analyzed a questionnaire, and performed a comprehensive ophthalmic examination, including optical coherence tomography., Results: Mean follow-up was 19 years (range 0-45 years, SD 15 years). With aging, patients showed progressive visual decline, deterioration of visual fields, increasing narrowing of the anterior chamber, increased prevalence of cataract, and an increase in the amount of intraretinal pigmentations. Fifty percent of patients had a visual acuity of ≤0.3 at Age 18 and of ≤0.1 at Age 35. Electroretinogram responses were severely reduced or absent already at a young age and optical coherence tomography showed increased retinal thickness with often cystoid maculopathy at young age, and thinning of the retina and disorientation of the photoreceptor layer in the late stages. The clinical course showed considerable interindividual variability, but intraindividual similarity between both eyes was the rule., Conclusion: The wide and variable clinical spectrum in patients with the same CRB1 mutation supports the hypothesis that the CRB1 type autosomal recessive retinitis pigmentosa-phenotype is modulated by other factors. The clinical variability will make it harder to evaluate the effect of (upcoming) therapies for retinitis pigmentosa, although because of the intraindividual similarity between both eyes, the contralateral eye can be used as an excellent internal control.

Published

2017

20. Noninvasive prenatal diagnosis of Huntington disease: detection of the paternally inherited expanded CAG repeat in maternal plasma.

Author

van den Oever JM, Bijlsma EK, Feenstra I, Muntjewerff N, Mathijssen IB, Bakker E, van Belzen MJ, and Boon EM

Subjects

Female, Humans, Huntingtin Protein, Huntington Disease blood, Huntington Disease genetics, Male, Pregnancy, Huntington Disease diagnosis, Maternal Serum Screening Tests, Nerve Tissue Proteins genetics

Abstract

Objective: With a shift towards noninvasive testing, we have explored and validated the use of noninvasive prenatal diagnosis (NIPD) for Huntington disease (HD)., Methods: Fifteen couples have been included, assessing a total of n = 20 pregnancies. Fetal paternally inherited CAG repeat length was determined in total cell-free DNA from maternal plasma using a direct approach by PCR and subsequent fragment analysis., Results: All fetal HD (n = 7) and intermediate (n = 3) CAG repeats could be detected in maternal plasma. Detection of repeats in the normal range (n = 10) was successful in n = 5 cases where the paternal repeat size could be distinguished from maternal repeat patterns after fragment analysis. In all other cases (n = 5), the paternal peaks coincided with the maternal peak pattern. All NIPD results were concordant with results from routine diagnostics on fetal genomic DNA from chorionic villi., Conclusion: In this validation study, we demonstrated that all fetuses at risk for HD could be identified noninvasively in maternal plasma. Additionally, we have confirmed results from previously described case reports that NIPD for HD can be performed using a direct approach by PCR. For future diagnostics, parental CAG profiles can be used to predict the success rate for NIPD prior to testing., (© 2015 John Wiley & Sons, Ltd.)

Published

2015

21. Identification of a Dutch founder mutation in MUSK causing fetal akinesia deformation sequence.

Author

Tan-Sindhunata MB, Mathijssen IB, Smit M, Baas F, de Vries JI, van der Voorn JP, Kluijt I, Hagen MA, Blom EW, Sistermans E, Meijers-Heijboer H, Waisfisz Q, Weiss MM, and Groffen AJ

Subjects

Alleles, Amino Acid Sequence, Arthrogryposis diagnosis, Arthrogryposis pathology, Base Sequence, Female, Fetus, Gene Expression, Gene Frequency, Genes, Lethal, Genetic Testing, Homozygote, Humans, Male, Molecular Sequence Data, Motor Endplate pathology, Muscle Cells metabolism, Muscle Cells pathology, Netherlands, Pedigree, Prenatal Diagnosis, Primary Cell Culture, Receptors, Cholinergic chemistry, Arthrogryposis genetics, Founder Effect, Motor Endplate genetics, Mutation, Receptor Protein-Tyrosine Kinases genetics, Receptors, Cholinergic genetics

Abstract

Fetal akinesia deformation sequence (FADS) refers to a clinically and genetically heterogeneous group of disorders with congenital malformations related to impaired fetal movement. FADS can result from mutations in CHRNG, CHRNA1, CHRND, DOK7 and RAPSN; however, these genes only account for a minority of cases. Here we identify MUSK as a novel cause of lethal FADS. Fourteen affected fetuses from a Dutch genetic isolate were traced back to common ancestors 11 generations ago. Homozygosity mapping in two fetuses revealed MUSK as a candidate gene. All tested cases carried an identical homozygous variant c.1724T>C; p.(Ile575Thr) in the intracellular domain of MUSK. The carrier frequency in the genetic isolate was 8%, exclusively found in heterozygous carriers. Consistent with the established role of MUSK as a tyrosine kinase that orchestrates neuromuscular synaptogenesis, the fetal myopathy was accompanied by impaired acetylcholine receptor clustering and reduced tyrosine kinase activity at motor nerve endings. A functional assay in myocytes derived from human fetuses confirmed that the variant blocks MUSK-dependent motor endplate formation. Taken together, the results strongly support a causal role of this founder mutation in MUSK, further expanding the gene set associated with FADS and offering new opportunities for prenatal genetic testing.

Published

2015

22. Phenotype and genotype in 103 patients with tricho-rhino-phalangeal syndrome.

Author

Maas SM, Shaw AC, Bikker H, Lüdecke HJ, van der Tuin K, Badura-Stronka M, Belligni E, Biamino E, Bonati MT, Carvalho DR, Cobben J, de Man SA, Den Hollander NS, Di Donato N, Garavelli L, Grønborg S, Herkert JC, Hoogeboom AJ, Jamsheer A, Latos-Bielenska A, Maat-Kievit A, Magnani C, Marcelis C, Mathijssen IB, Nielsen M, Otten E, Ousager LB, Pilch J, Plomp A, Poke G, Poluha A, Posmyk R, Rieubland C, Silengo M, Simon M, Steichen E, Stumpel C, Szakszon K, Polonkai E, van den Ende J, van der Steen A, van Essen T, van Haeringen A, van Hagen JM, Verheij JB, Mannens MM, and Hennekam RC

Subjects

Abnormalities, Multiple pathology, Adolescent, Adult, Aged, Child, Child, Preschool, Female, Genetic Association Studies, Humans, Infant, Langer-Giedion Syndrome pathology, Male, Middle Aged, Mutation, Missense, Repressor Proteins, Young Adult, Abnormalities, Multiple genetics, DNA-Binding Proteins genetics, Langer-Giedion Syndrome genetics, Transcription Factors genetics

Abstract

Tricho-rhino-phalangeal syndrome (TRPS) is characterized by craniofacial and skeletal abnormalities, and subdivided in TRPS I, caused by mutations in TRPS1, and TRPS II, caused by a contiguous gene deletion affecting (amongst others) TRPS1 and EXT1. We performed a collaborative international study to delineate phenotype, natural history, variability, and genotype-phenotype correlations in more detail. We gathered information on 103 cytogenetically or molecularly confirmed affected individuals. TRPS I was present in 85 individuals (22 missense mutations, 62 other mutations), TRPS II in 14, and in 5 it remained uncertain whether TRPS1 was partially or completely deleted. Main features defining the facial phenotype include fine and sparse hair, thick and broad eyebrows, especially the medial portion, a broad nasal ridge and tip, underdeveloped nasal alae, and a broad columella. The facial manifestations in patients with TRPS I and TRPS II do not show a significant difference. In the limbs the main findings are short hands and feet, hypermobility, and a tendency for isolated metacarpals and metatarsals to be shortened. Nails of fingers and toes are typically thin and dystrophic. The radiological hallmark are the cone-shaped epiphyses and in TRPS II multiple exostoses. Osteopenia is common in both, as is reduced linear growth, both prenatally and postnatally. Variability for all findings, also within a single family, can be marked. Morbidity mostly concerns joint problems, manifesting in increased or decreased mobility, pain and in a minority an increased fracture rate. The hips can be markedly affected at a (very) young age. Intellectual disability is uncommon in TRPS I and, if present, usually mild. In TRPS II intellectual disability is present in most but not all, and again typically mild to moderate in severity. Missense mutations are located exclusively in exon 6 and 7 of TRPS1. Other mutations are located anywhere in exons 4-7. Whole gene deletions are common but have variable breakpoints. Most of the phenotype in patients with TRPS II is explained by the deletion of TRPS1 and EXT1, but haploinsufficiency of RAD21 is also likely to contribute. Genotype-phenotype studies showed that mutations located in exon 6 may have somewhat more pronounced facial characteristics and more marked shortening of hands and feet compared to mutations located elsewhere in TRPS1, but numbers are too small to allow firm conclusions., (Copyright © 2015 Elsevier Masson SAS. All rights reserved.)

Published

2015

23. 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

24. Variants in CUL4B are associated with cerebral malformations.

Author

Vulto-van Silfhout AT, Nakagawa T, Bahi-Buisson N, Haas SA, Hu H, Bienek M, Vissers LE, Gilissen C, Tzschach A, Busche A, Müsebeck J, Rump P, Mathijssen IB, Avela K, Somer M, Doagu F, Philips AK, Rauch A, Baumer A, Voesenek K, Poirier K, Vigneron J, Amram D, Odent S, Nawara M, Obersztyn E, Lenart J, Charzewska A, Lebrun N, Fischer U, Nillesen WM, Yntema HG, Järvelä I, Ropers HH, de Vries BB, Brunner HG, van Bokhoven H, Raymond FL, Willemsen MA, Chelly J, Xiong Y, Barkovich AJ, Kalscheuer VM, Kleefstra T, and de Brouwer AP

Subjects

Adolescent, Adult, Cell Cycle Proteins, Cells, Cultured, Child, Child, Preschool, Genetic Association Studies, HEK293 Cells, Humans, Infant, Male, Malformations of Cortical Development metabolism, Malformations of Cortical Development pathology, Mental Retardation, X-Linked metabolism, Mental Retardation, X-Linked pathology, Middle Aged, Pedigree, Sequence Analysis, DNA, Young Adult, Brain pathology, Cullin Proteins genetics, Cullin Proteins metabolism, Malformations of Cortical Development genetics, Mental Retardation, X-Linked genetics, Nerve Tissue Proteins metabolism

Abstract

Variants in cullin 4B (CUL4B) are a known cause of syndromic X-linked intellectual disability. Here, we describe an additional 25 patients from 11 families with variants in CUL4B. We identified nine different novel variants in these families and confirmed the pathogenicity of all nontruncating variants. Neuroimaging data, available for 15 patients, showed the presence of cerebral malformations in ten patients. The cerebral anomalies comprised malformations of cortical development (MCD), ventriculomegaly, and diminished white matter volume. The phenotypic heterogeneity of the cerebral malformations might result from the involvement of CUL-4B in various cellular pathways essential for normal brain development. Accordingly, we show that CUL-4B interacts with WDR62, a protein in which variants were previously identified in patients with microcephaly and a wide range of MCD. This interaction might contribute to the development of cerebral malformations in patients with variants in CUL4B., (© 2014 WILEY PERIODICALS, INC.)

Published

2015

25. Prenatal diagnostic testing of the Noonan syndrome genes in fetuses with abnormal ultrasound findings.

Author

Croonen EA, Nillesen WM, Stuurman KE, Oudesluijs G, van de Laar IM, Martens L, Ockeloen C, Mathijssen IB, Schepens M, Ruiterkamp-Versteeg M, Scheffer H, Faas BH, van der Burgt I, and Yntema HG

Subjects

Abortion, Eugenic, DNA Mutational Analysis, Female, Humans, Karyotype, Molecular Diagnostic Techniques, Noonan Syndrome diagnostic imaging, Nuchal Translucency Measurement, Pregnancy, Protein Tyrosine Phosphatase, Non-Receptor Type 11 genetics, Proto-Oncogene Proteins genetics, Proto-Oncogene Proteins c-raf genetics, Proto-Oncogene Proteins p21(ras), ras Proteins genetics, Noonan Syndrome genetics

Abstract

In recent studies on prenatal testing for Noonan syndrome (NS) in fetuses with an increased nuchal translucency (NT) and a normal karyotype, mutations have been reported in 9-16% of cases. In this study, DNA of 75 fetuses with a normal karyotype and abnormal ultrasound findings was tested in a diagnostic setting for mutations in (a subset of) the four most commonly mutated NS genes. A de novo mutation in either PTPN11, KRAS or RAF1 was detected in 13 fetuses (17.3%). Ultrasound findings were increased NT, distended jugular lymphatic sacs (JLS), hydrothorax, renal anomalies, polyhydramnios, cystic hygroma, cardiac anomalies, hydrops fetalis and ascites. A second group, consisting of anonymized DNA of 60 other fetuses with sonographic abnormalities, was tested for mutations in 10 NS genes. In this group, five possible pathogenic mutations have been identified (in PTPN11 (n=2), RAF1, BRAF and MAP2K1 (each n=1)). We recommend prenatal testing of PTPN11, KRAS and RAF1 in pregnancies with an increased NT and at least one of the following additional features: polyhydramnios, hydrops fetalis, renal anomalies, distended JLS, hydrothorax, cardiac anomalies, cystic hygroma and ascites. If possible, mutation analysis of BRAF and MAP2K1 should be considered.

Published

2013

26. Prenatal diagnosis of a trisomy 7/trisomy 13 mosaicism.

Author

Huijsdens-van Amsterdam K, Barge-Schaapveld DQ, Mathijssen IB, Alders M, Pajkrt E, and Knegt AC

Abstract

Double aneuploidy mosaicism of two different aneuploidy cell lines is rare. We describe for the first time a double trisomy mosaicism, involving chromosomes 7 and 13 in a fetus presenting with multiple congenital anomalies. No evidence for chimerism was found by DNA genotyping. The origin of both trisomies are consistent with isodisomy of maternal origin. Therefore, it is most likely that the double trisomy mosaicism arose from two independent events very early in embryonic development. The trisomy 7 and 13 cells were shown to be of maternal origin.

Published

2012

27. Audit of 10 years of referrals for fetal echocardiography.

Author

Clur SA, Van Brussel PM, Mathijssen IB, Pajkrt E, Ottenkamp J, and Bilardo CM

Subjects

Echocardiography trends, Female, Heart Defects, Congenital mortality, Humans, Medical Audit, Nuchal Translucency Measurement, Pregnancy, Referral and Consultation, Retrospective Studies, Echocardiography statistics & numerical data, Heart Defects, Congenital diagnostic imaging

Abstract

Objectives: To evaluate trends over time, indications, diagnoses, noncardiac defects and outcome of fetuses referred for tertiary level echocardiography., Methods: Retrospective study of fetal echocardiograms performed between April 1999 and 2009., Results: Of the 623 fetuses included, 301 (48%) had cardiac pathology. Congenital heart defects (CHDs) were found in 243/301 (81%), mostly in the severe spectrum. Of the fetuses with CHDs, 26% (63/243) had chromosomal anomalies. The chromosomally normal fetuses with CHDs had a mortality rate of 43% (77/180) and 23% (41/180) had extra-cardiac anomalies. The termination of pregnancy (TOP) rate for all cardiac pathology was 24.9% (75/301) and for CHDs 29.6% (72/243). The TOP rates for CHDs diagnosed before 19 and 24 weeks gestation were 61% (28/46) and 44% (68/155), respectively. An increase in referrals followed the introduction of a national screening program, (nuchal translucency (NT) and routine structural ultrasound screening). The main referral indication was an increased NT (>95th percentile; 32% of cases). CHDs were found in 81/239 (34%) fetuses with an increased NT., Conclusions: Referral indications for fetal echocardiography were appropriate (almost 50% had cardiac pathology). The mortality was high. Fetal outcome and TOP decisions correlated with CHD severity and presence of noncardiac defects. An increased NT is a strong marker for CHDs., (Copyright © 2011 John Wiley & Sons, Ltd.)

Published

2011

28. Targeted ultrasound examination and DNA testing for Noonan syndrome, in fetuses with increased nuchal translucency and normal karyotype.

Author

Bakker M, Pajkrt E, Mathijssen IB, and Bilardo CM

Subjects

Adult, Craniofacial Abnormalities, Female, Gestational Age, Heart Defects, Congenital diagnostic imaging, Humans, Lymphangioma, Cystic diagnostic imaging, Male, Mutation, Polyhydramnios diagnostic imaging, Pregnancy, Prenatal Diagnosis, Protein Tyrosine Phosphatase, Non-Receptor Type 11 genetics, DNA analysis, Karyotype, Noonan Syndrome diagnostic imaging, Noonan Syndrome genetics, Nuchal Translucency Measurement, Ultrasonography, Prenatal

Abstract

Objective: To define sonographic criteria that may improve the prenatal diagnosis of Noonan syndrome by targeted DNA testing., Methods: We searched our Fetal Medicine Unit records for all cases with a final diagnosis of Noonan syndrome. A literature review was undertaken to identify the sonographic features of Noonan syndrome fetuses. Information was pooled to define the most common features., Results: In our database, we identified three cases of Noonan syndrome. The diagnosis was suspected prenatally in two of them. Thirty-nine cases were identified in the literature. In the presented cases we show that suspicion of Noonan syndrome should arise when, after an increased nuchal translucency, ultrasound investigation in the second trimester shows a persistant nuchal fold (NF) or cystic hygroma in combination with at least one of the following features: hydrops fetalis, pleural effusion, cardiac anomalies, polyhydramnios or specific facial abnormalities., Conclusion: Prenatal ultrasound findings in Noonan syndrome can be subtle and aspecific, but when specific characteristics are present additional targeted DNA analysis is indicated., (Copyright © 2011 John Wiley & Sons, Ltd.)

Published

2011

29. A novel autosomal dominant condition consisting of congenital heart defects and low atrial rhythm maps to chromosome 9q.

Author

van de Meerakker JB, van Engelen K, Mathijssen IB, Lekanne dit Deprez RH, Lam J, Wilde AA, Baars MJ, Mannens MM, Mulder BJ, Moorman AF, and Postma AV

Subjects

Adolescent, Adult, Aged, Aged, 80 and over, Child, Child, Preschool, Comparative Genomic Hybridization, Female, Genetic Linkage, Humans, Infant, Infant, Newborn, Kruppel-Like Factor 4, Male, Middle Aged, Mutation genetics, Pedigree, Young Adult, Chromosomes, Human, Pair 9 genetics, Genes, Dominant genetics, Heart Atria physiopathology, Heart Defects, Congenital genetics

Abstract

Congenital heart defects (CHDs) occur mostly sporadic, but familial CHD cases have been reported. Mutations in several genes, including NKX2.5, GATA4 and NOTCH1, were identified in families and patients with CHD, but the mechanisms underlying CHD are largely unknown. We performed genome-wide linkage analysis in a large four-generation family with autosomal dominant CHD (including atrial septal defect type I and II, tetralogy of Fallot and persistent left superior vena cava) and low atrial rhythm, a unique phenotype that has not been described before. We obtained phenotypic information including electrocardiography, echocardiography and DNA of 23 family members. Genome-wide linkage analysis on 12 affected, 5 unaffected individuals and 1 obligate carrier demonstrated significant linkage only to chromosome 9q21-33 with a multipoint maximum LOD score of 4.1 at marker D9S1690, between markers D9S167 and D9S1682. This 48-cM critical interval corresponds to 39 Mb and contains 402 genes. Sequence analysis of nine candidate genes in this region (INVS, TMOD1, TGFBR1, KLF4, IPPK, BARX1, PTCH1, MEGF9 and S1PR3) revealed no mutations, nor were genomic imbalances detected using array comparative genomic hybridization. In conclusion, we describe a large family with CHD and low atrial rhythm with a significant LOD score to chromosome 9q. The phenotype is representative of a mild form of left atrial isomerism or a developmental defect of the sinus node and surrounding tissue. Because the mechanisms underlying CHD are largely unknown, this study represents an important step towards the discovery of genes implied in cardiogenesis.

Published

2011

30. Characteristics and outcome and the omphalocele circumference/abdominal circumference ratio in prenatally diagnosed fetal omphalocele.

Author

Kleinrouweler CE, Kuijper CF, van Zalen-Sprock MM, Mathijssen IB, Bilardo CM, and Pajkrt E

Subjects

Adolescent, Adult, Delivery, Obstetric statistics & numerical data, Female, Fetal Diseases diagnostic imaging, Hernia, Umbilical diagnostic imaging, Hernia, Umbilical surgery, Humans, Infant, Newborn, Male, Netherlands epidemiology, Retrospective Studies, Ultrasonography, Prenatal, Waist Circumference, Young Adult, Fetal Diseases epidemiology, Hernia, Umbilical epidemiology

Abstract

Objective: To evaluate the outcome of fetuses with prenatally diagnosed omphalocele and to investigate the predictive value of the omphalocele circumference/abdominal circumference (OC/AC) ratio - a measure for the relative size of the omphalocele., Materials and Methods: This study includes all fetuses prenatally diagnosed with omphalocele at our centre between 1995 and 2007. Medical records and footage of ultrasound examinations were reviewed. Omphalocele was classified in four groups: isolated, chromosomal, syndromic, and multiple anomalies., Results: Eighty-eight cases were identified: 21 (24%) were isolated and 67 had additional structural anomalies. Of the 44 fetuses (50%) with chromosomal anomalies, 2 had omphalocele as a solitary finding. Fifty-three pregnancies (60%) were terminated because of the size of the lesion or associated structural or chromosomal anomalies. Twenty-one cases resulted in a live birth, of which 17 were vaginal deliveries (81%, all uncomplicated) including 3 cases of giant omphalocele (≥5 cm). The OC/AC ratio was found predictive for herniation of the liver, respiratory insufficiency and type of surgical reconstruction. Currently, 12/88 fetuses (14%) are alive and well, including 2 infants with multiple anomalies., Conclusion: Identification of omphalocele should arouse suspicion of genetic abnormalities, even in cases that appear isolated. The OC/AC ratio may influence counselling regarding the postnatal course., (Copyright © 2011 S. Karger AG, Basel.)

Published

2011

31. Functional analysis of novel TBX5 T-box mutations associated with Holt-Oram syndrome.

Author

Boogerd CJ, Dooijes D, Ilgun A, Mathijssen IB, Hordijk R, van de Laar IM, Rump P, Veenstra-Knol HE, Moorman AF, Barnett P, and Postma AV

Subjects

Abnormalities, Multiple genetics, Abnormalities, Multiple metabolism, Amino Acid Sequence, Animals, Atrial Natriuretic Factor genetics, Binding Sites, Case-Control Studies, Cell Line, DNA Mutational Analysis, Electrophoretic Mobility Shift Assay, Fibroblast Growth Factor 10 genetics, GATA4 Transcription Factor genetics, GATA4 Transcription Factor metabolism, Genotype, Heart Defects, Congenital metabolism, Heart Septal Defects, Atrial genetics, Heart Septal Defects, Atrial metabolism, Homeodomain Proteins genetics, Homeodomain Proteins metabolism, Humans, Immunoprecipitation, Lower Extremity Deformities, Congenital genetics, Lower Extremity Deformities, Congenital metabolism, Models, Molecular, Molecular Sequence Data, Phenotype, Promoter Regions, Genetic, Protein Binding, Protein Conformation, Rats, Recombinant Fusion Proteins metabolism, T-Box Domain Proteins chemistry, T-Box Domain Proteins metabolism, Transfection, Upper Extremity Deformities, Congenital metabolism, Heart Defects, Congenital genetics, Mutation, Missense, T-Box Domain Proteins genetics, Upper Extremity Deformities, Congenital genetics

Abstract

Aims: Holt-Oram syndrome (HOS) is a heart/hand syndrome clinically characterized by upper limb and cardiac malformations. Mutations in T-box transcription factor 5 (TBX5) underlie this syndrome, the majority of which lead to premature stops. In this study, we present our functional analyses of five (novel) missense TBX5 mutations identified in HOS patients, most of whom presented with severe cardiac malformations., Methods and Results: Functional characterization of mutant proteins shows a dramatic loss of DNA-binding capacity, as well as diminished binding to known cardiac interaction partners NKX2-5 and GATA4. The disturbance of these interactions leads to a loss of function, as measured by the reduced activation of Nppa and FGF10 in rat heart derived cells, although with variable severity. Two out of the five mutations are peculiar: one, p.H220del, is associated with additional extra-cardiac defects, perhaps by interfering with other T-box dependant pathways, and another, p.I106V, leads to limb defects only, which is supported by its normal interaction with cardiac-specific interaction partners., Conclusion: Overall, our data are consistent with the hypothesis that these novel missense mutations in TBX5 lead to functional haploinsufficiency and result in a reduced transcriptional activation of target genes, which is likely central to the pathogenesis of HOS.

Published

2010

32. A gain-of-function TBX5 mutation is associated with atypical Holt-Oram syndrome and paroxysmal atrial fibrillation.

Author

Postma AV, van de Meerakker JB, Mathijssen IB, Barnett P, Christoffels VM, Ilgun A, Lam J, Wilde AA, Lekanne Deprez RH, and Moorman AF

Subjects

Abnormalities, Multiple, Adolescent, Adult, Age of Onset, Animals, Atrial Fibrillation diagnosis, Binding, Competitive, Cells, Cultured, Child, DNA metabolism, DNA pharmacology, Electrocardiography, Female, Gene Expression Regulation, Gene Transfer Techniques, Genetic Linkage, Genetic Testing, Homeobox Protein Nkx-2.5, Homeodomain Proteins metabolism, Humans, Male, Mice, Pedigree, Phenotype, Protein Transport genetics, Rats, Syndrome, T-Box Domain Proteins chemistry, T-Box Domain Proteins metabolism, Transcription Factors metabolism, Two-Hybrid System Techniques, Atrial Fibrillation genetics, Mutation, T-Box Domain Proteins genetics

Abstract

Holt-Oram syndrome (HOS) is a heart/hand syndrome clinically characterized by upper limb and cardiac malformations. Mutations in T-box transcription factor 5 (TBX5) underlie this syndrome. Here, we describe a large atypical HOS family in which affected patients have mild skeletal deformations and paroxysmal atrial fibrillation, but few have congenital heart disease. Sequencing of TBX5 revealed a novel mutation, c.373G>A, resulting in the missense mutation p.Gly125Arg, in all investigated affected family members, cosegregating with the disease. We demonstrate that the mutation results in normal Nkx2-5 interaction, is correctly targeted to the nucleus, has significantly enhanced DNA binding and activation of both the Nppa(Anf) and Cx40 promoter, and significantly augments expression of Nppa, Cx40, Kcnj2, and Tbx3 in comparison with wild-type TBX5. Thus, contrary to previously published HOS mutations, the p.G125R TBX5 mutation results in a gain-of-function. We speculate that the gain-of-function mechanism underlies the mild skeletal phenotype and paroxysmal atrial fibrillation and suggest a possible role of TBX5 in the development of (paroxysmal) atrial fibrillation based on a gain-of-function either through a direct stimulation of target genes via TBX5 or indirectly via TBX5 stimulated TBX3. These findings may warrant a renewed look at the phenotypes of families and individuals hitherto not classified as HOS or as atypical but presenting with paroxysmal atrial fibrillation, because these may possibly be the result of additional TBX5 gain-of-function mutations.

Published

2008

33. Structural heart defects associated with an increased nuchal translucency: 9 years experience in a referral centre.

Author

Clur SA, Mathijssen IB, Pajkrt E, Cook A, Laurini RN, Ottenkamp J, and Bilardo CM

Subjects

Chromosomes, Human, Pair 18, Chromosomes, Human, X, Down Syndrome complications, Down Syndrome epidemiology, Female, Heart Defects, Congenital complications, Humans, Monosomy, Pregnancy, Referral and Consultation, Retrospective Studies, Trisomy, Ultrasonography, Prenatal, Abnormalities, Multiple epidemiology, Chromosome Aberrations statistics & numerical data, Heart Defects, Congenital epidemiology, Nuchal Translucency Measurement

Abstract

Objective: To investigate the congenital heart disease (CHD) found in association with an increased nuchal translucency (NT) at 11-14 weeks of gestation in chromosomally normal and abnormal fetuses., Methods: Patients referred from January 1998 until May 2007 with an increased NT (> or = 95th percentile) where CHD was diagnosed were included. Chromosome analysis, fetal and postnatal echocardiography were performed. A postmortem examination followed pregnancy termination when possible., Results: Major CHD was identified in 68 of 967 fetuses with an increased NT (median NT 4.8 mm, range 2.5-22 mm). Major CHD was found in 34 of 693 fetuses (4.9%) with a normal karyotype and increased NT (median 5.2 mm, range 2.5-9.6 mm). CHD frequency increased from 1.9%, with NT between 2.5 and 3.5 mm, to 27.7% when NT was > or = 6.5 mm. Septal defects predominated (20%) when NT was < or = 3.5 mm. With NT > 3.5 mm an equal distribution of CHD types was seen. Major CHD was identified in 34 of the 274 fetuses with an abnormal karyotype and increased NT (median 4.2 mm, range 2.5-22 mm)., Conclusions: A variety of CHD is associated with an increased NT in the first trimester of pregnancy. Conotruncal defects, branchial arch derivative defects, left and right obstructive lesions (inflow and outflow) and shunts were seen., (Copyright (c) 2008 John Wiley & Sons, Ltd.)

Published

2008

34. Testicular cancer in a patient with Primrose syndrome.

Author

Mathijssen IB, van Hasselt-van der Velde J, and Hennekam RC

Subjects

Abnormalities, Multiple genetics, Abnormalities, Multiple pathology, Adolescent, Adult, Ear, External abnormalities, Facies, Hearing Loss diagnosis, Hearing Loss genetics, Hearing Loss pathology, Humans, Intellectual Disability genetics, Intellectual Disability pathology, Male, Palate, Hard abnormalities, Syndrome, Testicular Neoplasms genetics, Testicular Neoplasms pathology, Abnormalities, Multiple diagnosis, Hair abnormalities, Intellectual Disability diagnosis, Joints abnormalities, Testicular Neoplasms diagnosis

Abstract

A mentally retarded, adult man was found to have joint contractures, sparse body hair, hearing loss, dysmorphic facial features, large calcified pinnae and a huge torus palatinus. All features are similar to those earlier described in patients with Primrose syndrome. In addition he developed a germ cell tumour of his right testicle at age 27 years. A comparison is provided between the main findings in the four previously reported cases with Primrose syndrome and the current patient. Calcification of the pinnae is an infrequent symptom in the general population, and a torus palatinus of limited size is commonly found but a torus of the size reported here is extremely unusual. Both symptoms are excellent handles for diagnosing this entity. It remains as yet uncertain whether an increased risk to malignancies forms part of this syndrome or is only a consequence of cryptorchidism in this patient.

Published

2006

35. Unilateral symbrachydactyly of the foot.

Author

Mathijssen IB, Cossey V, Fryns JP, De Smet L, and Devriendt K

Subjects

Foot Deformities, Congenital embryology, Foot Deformities, Congenital etiology, Genetic Counseling, Humans, Infant, Newborn, Male, Foot Deformities, Congenital pathology

Published

2006

36. Array comparative genomic hybridization analysis of a familial duplication of chromosome 13q: a recognizable syndrome.

Author

Mathijssen IB, Hoovers JM, Mul AN, Man HY, Ket JL, and Hennekam RC

Subjects

Abnormalities, Multiple genetics, Abnormalities, Multiple pathology, Adolescent, Adult, Child, Child, Preschool, Chromosome Banding, Family Health, Female, Gene Duplication, Genome, Human, Genotype, Hearing Loss pathology, Humans, In Situ Hybridization, Fluorescence, Intellectual Disability pathology, Karyotyping, Male, Middle Aged, Pedigree, Phenotype, Syndrome, Tooth Abnormalities, Chromosome Aberrations, Chromosomes, Human, Pair 13 genetics, Nucleic Acid Hybridization methods

Abstract

We report on a family with six persons in three generations who have mild mental retardation, behavioral problems, seizures, hearing loss, strabismus, dental anomalies, hypermobility, juvenile hallux valgus, and mild dysmorphic features. Classical cytogenetic analysis showed a partial duplication of chromosome 13q, array comparative genomic hybridization showed the duplication to span approximately 21 Mb, ranging from chromosome band 13q21.31 to 13q31.1. The relatively mild presentation of this large duplication may be explained by the relative paucity of genes in the chromosome region involved. Genotype-phenotype correlations in patients with similar partial 13q duplications are inconsistent. Emerging cytogenetic techniques will allow more reliable genotype-phenotype correlations., (Copyright (c) 2005 Wiley-Liss, Inc.)

Published

2005

37. Iris heterochromia: a variable feature in Verloes-Koulischer-oral-acral syndrome.

Author

Mathijssen IB, Fryns JP, Devriendt K, Sznajer Y, and Van Eygen M

Subjects

Child, Preschool, Humans, Male, Maxilla abnormalities, Maxilla diagnostic imaging, Pigmentation Disorders pathology, Radiography, Syndrome, Abnormalities, Multiple pathology, Alveolar Process abnormalities, Hand Deformities, Congenital pathology, Iris abnormalities, Lip abnormalities

Published

2005

38. Genotype-phenotype correlation in patients suspected of having Sotos syndrome.

Author

de Boer L, Kant SG, Karperien M, van Beers L, Tjon J, Vink GR, van Tol D, Dauwerse H, le Cessie S, Beemer FA, van der Burgt I, Hamel BC, Hennekam RC, Kuhnle U, Mathijssen IB, Veenstra-Knol HE, Stumpel CT, Breuning MH, and Wit JM

Subjects

Adolescent, Adult, Child, Child, Preschool, Female, Genotype, Heart Defects, Congenital genetics, Histone Methyltransferases, Histone-Lysine N-Methyltransferase, Humans, Infant, Intracellular Signaling Peptides and Proteins genetics, Male, Middle Aged, Mutation, Nuclear Proteins genetics, Pedigree, Syndrome, Abnormalities, Multiple genetics, Abnormalities, Multiple pathology, Craniofacial Abnormalities genetics, Craniofacial Abnormalities pathology, Intellectual Disability genetics, Phenotype

Abstract

Background: Deletions and mutations in the NSD1 gene are the major cause of Sotos syndrome. We wanted to evaluate the genotype-phenotype correlation in patients suspected of having Sotos syndrome and determine the best discriminating parameters for the presence of a NSD1 gene alteration., Methods: Mutation and fluorescence in situ hybridization analysis was performed on blood samples of 59 patients who were clinically scored into 3 groups. Clinical data were compared between patients with and without NSD1 alterations. With logistic regression analysis the best combination of predictive variables was obtained., Results: In the groups of typical, dubious and atypical Sotos syndrome, 81, 36 and 0% of the patients, respectively, showed NSD1 gene alterations. Four deletions were detected. In 23 patients (2 families) 19 mutations were detected (1 splicing defect, 3 non-sense, 7 frameshift and 8 missense mutations). The best predictive parameters for a NSD1 gene alteration were frontal bossing, down-slanted palpebral fissures, pointed chin and overgrowth. Higher incidences of feeding problems and cardiac anomalies were found. The parameters, delayed development and advanced bone age, did not differ between the 2 subgroups., Conclusions: In our patients suspected of having Sotos syndrome, facial features and overgrowth were highly predictive of a NSD1 gene aberration, whereas developmental delay and advanced bone age were not., (Copyright (c) 2004 S. Karger AG, Basel.)

Published

2004