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3. Copy number variants from 4800 exomes contribute to ~7% of genetic diagnoses in movement disorders, muscle disorders and neuropathies.

Author

Pennings, M., Meijer, Rowdy P. P., Gerrits, M., Janssen, J, Pfundt, R.P., Leeuw, N. de, Gilissen, C., Gardeitchik, T., Schouten, M.I., Voermans, N.C., Warrenburg, B.P.C. van de, Kamsteeg, E.J., Pennings, M., Meijer, Rowdy P. P., Gerrits, M., Janssen, J, Pfundt, R.P., Leeuw, N. de, Gilissen, C., Gardeitchik, T., Schouten, M.I., Voermans, N.C., Warrenburg, B.P.C. van de, and Kamsteeg, E.J.

Abstract

01 juni 2023, Contains fulltext : 293778.pdf (Publisher’s version ) (Open Access), Various groups of neurological disorders, including movement disorders and neuromuscular diseases, are clinically and genetically heterogeneous. Diagnostic panel-based exome sequencing is a routine test for these disorders. Despite the success rates of exome sequencing, it results in the detection of causative sequence variants in 'only' 25-30% of cases. Copy number variants (CNVs), i.e. deletion or duplications, explain 10-20% of individuals with multisystemic phenotypes, such as co-existing intellectual disability, but may also have a role in disorders affecting a single system (organ), like neurological disorders with normal intelligence. In this study, CNVs were extracted from clinical exome sequencing reports of 4800 probands primarily with a movement disorder, myopathy or neuropathy. In 88 (~2%) probands, phenotype-matching CNVs were detected, representing ~7% of genetically confirmed cases. CNVs varied from involvement of over 100 genes to single exons and explained X-linked, autosomal dominant, or - recessive disorders, the latter due to either a homozygous CNV or a compound heterozygous CNV with a sequence variant on the other allele. CNVs were detected affecting genes where deletions or duplications are established as a common mechanism, like PRKN (in Parkinson's disease), DMD (in Duchenne muscular dystrophy) and PMP22 (in neuropathies), but also genes in which no intragenic CNVs have been reported to date. Analysis of CNVs as part of panel-based exome sequencing for genetically heterogeneous neurological diseases provides an additional diagnostic yield of ~2% without extra laboratory costs. Therefore it is recommended to perform CNV analysis for movement disorders, muscle disease, neuropathies, or any other single-system disorder.

Published
2023

4. Respiratory insufficiency as a presenting symptom of congenital myasthenic syndromes.

Author

Udenhout, F. van den, Merkus, P.J.F.M., Verhaagen-van den Akker, S.L.J., Schouten, M.I., Erasmus, C.E., Braakman, H.M.H., Udenhout, F. van den, Merkus, P.J.F.M., Verhaagen-van den Akker, S.L.J., Schouten, M.I., Erasmus, C.E., and Braakman, H.M.H.

Abstract

Item does not contain fulltext, AIM: Respiratory insufficiency can be a presenting symptom of congenital myasthenic syndromes (CMS) but is rarely recognised as such. In this study, we aim to raise awareness of CMS to paediatricians. METHODS: We performed a retrospective case study of infants and preschool children treated in the past 5 years in Amalia Children's Hospital, Radboud University Medical Center in Nijmegen, the Netherlands for respiratory insufficiency as presenting symptom of CMS. RESULTS: Five children aged 2 weeks to 5 years experienced severe to life-threatening episodes of respiratory insufficiency, especially during viral infections, due to respiratory muscle weakness. During infections, they often also had progression of their otherwise mild ocular, facial, and limb muscle weakness. They were eventually diagnosed with genetically proven CMS. In these five children, treatment with pyridostigmine, an acetylcholinesterase inhibitor, resulted in clinical improvement. CONCLUSION: CMS should be considered in every patient with unexplained recurrent respiratory insufficiency, or with an unusually severe course of a normally mild respiratory infection, especially in combination with mild muscle weakness outside periods of illness. Early diagnosis of CMS is crucial for early treatment, which may help avoiding sudden infant death, severe respiratory insufficiency and further deterioration of the muscle strength.

Published
2023

5. Perioperative Care for Patients with Neuromuscular Disorders in the Netherlands – A Questionnaire Study Among Anaesthesiologists, Neurologists and Clinical Geneticists

Author

van den Bersselaar, L.R., primary, Gubbels, M.H.M., additional, Jungbluth, H., additional, Schouten, M.I., additional, van der Kooi, A.J., additional, Quinlivan, R., additional, Scheffer, G.J., additional, Riazi, S., additional, Snoeck, M.M.J., additional, and Voermans, N.C., additional

Published
2022
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6. Perioperative Care for Patients with Neuromuscular Disorders in the Netherlands - A Questionnaire Study Among Anaesthesiologists, Neurologists and Clinical Geneticists

Author

Bersselaar, L.R. van den, Gubbels, M.H.M., Jungbluth, H., Schouten, M.I., Kooi, A.J. van der, Quinlivan, R., Scheffer, G.J., Snoeck, M.M.J., Voermans, N.C., Bersselaar, L.R. van den, Gubbels, M.H.M., Jungbluth, H., Schouten, M.I., Kooi, A.J. van der, Quinlivan, R., Scheffer, G.J., Snoeck, M.M.J., and Voermans, N.C.

Abstract

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Published
2022

7. The complexities of CACNA1A in clinical neurogenetics

Author

Hommersom, M.P., Prooije, T.H. van, Pennings, Maartje, Schouten, M.I., Bokhoven, H. van, Kamsteeg, E.J., Warrenburg, B.P.C. van de, Hommersom, M.P., Prooije, T.H. van, Pennings, Maartje, Schouten, M.I., Bokhoven, H. van, Kamsteeg, E.J., and Warrenburg, B.P.C. van de

Abstract

Item does not contain fulltext, Variants in CACNA1A are classically related to episodic ataxia type 2, familial hemiplegic migraine type 1, and spinocerebellar ataxia type 6. Over the years, CACNA1A has been associated with a broader spectrum of phenotypes. Targeted analysis and unbiased sequencing of CACNA1A result not only in clear molecular diagnoses, but also in large numbers of variants of uncertain significance (VUS), or likely pathogenic variants with a phenotype that does not directly match the CACNA1A spectrum. Over the last years, targeted and clinical exome sequencing in our center has identified 41 CACNA1A variants. Ultimately, variants were considered pathogenic or likely pathogenic in 23 cases, with most phenotypes ranging from episodic or progressive ataxia to more complex ataxia syndromes, as well as intellectual disability and epilepsy. In two cases, the causality of the variant was discarded based on non-segregation or an alternative diagnosis. In the remaining 16 cases, the variant was classified as uncertain, due to lack of opportunities for segregation analysis or uncertain association with a non-classic phenotype. Phenotypic variability and the large number of VUS make CACNA1A a challenging gene for neurogenetic diagnostics. Accessible functional read-outs are clearly needed, especially in cases with a non-classic phenotype.

Published
2022

8. Comprehensive study of 28 individuals with SIN3A-related disorder underscoring the associated mild cognitive and distinctive facial phenotype

Author

Balasubramanian, M., Dingemans, A.J.M., Albaba, S., Richardson, R., Yates, T.M., Cox, H., Douzgou, S., Armstrong, R., Sansbury, F.H., Burke, K.B., Fry, A.E., Ragge, N., Sharif, S., Foster, A., Sandre-Giovannoli, A. De, Elouej, S., Vasudevan, P., Mansour, S., Wilson, K., Stewart, H., Heide, S. van der, Nava, C., Keren, B., Demirdas, S., Brooks, A.S., Vincent, M., Isidor, B., Küry, S., Schouten, M.I., Leenders, E.K.S.M., Chung, W.K., Haeringen, A.V., Scheffner, T., Debray, F.G., White, S.M., Palafoll, M.I.V., Pfundt, R.P., Newbury-Ecob, R., Kleefstra, T., Balasubramanian, M., Dingemans, A.J.M., Albaba, S., Richardson, R., Yates, T.M., Cox, H., Douzgou, S., Armstrong, R., Sansbury, F.H., Burke, K.B., Fry, A.E., Ragge, N., Sharif, S., Foster, A., Sandre-Giovannoli, A. De, Elouej, S., Vasudevan, P., Mansour, S., Wilson, K., Stewart, H., Heide, S. van der, Nava, C., Keren, B., Demirdas, S., Brooks, A.S., Vincent, M., Isidor, B., Küry, S., Schouten, M.I., Leenders, E.K.S.M., Chung, W.K., Haeringen, A.V., Scheffner, T., Debray, F.G., White, S.M., Palafoll, M.I.V., Pfundt, R.P., Newbury-Ecob, R., and Kleefstra, T.

Abstract

Contains fulltext : 245024.pdf (Publisher’s version ) (Open Access), Witteveen-Kolk syndrome (OMIM 613406) is a recently defined neurodevelopmental syndrome caused by heterozygous loss-of-function variants in SIN3A. We define the clinical and neurodevelopmental phenotypes related to SIN3A-haploinsufficiency in 28 unreported patients. Patients with SIN3A variants adversely affecting protein function have mild intellectual disability, growth and feeding difficulties. Involvement of a multidisciplinary team including a geneticist, paediatrician and neurologist should be considered in managing these patients. Patients described here were identified through a combination of clinical evaluation and gene matching strategies (GeneMatcher and Decipher). All patients consented to participate in this study. Mean age of this cohort was 8.2 years (17 males, 11 females). Out of 16 patients ≥ 8 years old assessed, eight (50%) had mild intellectual disability (ID), four had moderate ID (22%), and one had severe ID (6%). Four (25%) did not have any cognitive impairment. Other neurological symptoms such as seizures (4/28) and hypotonia (12/28) were common. Behaviour problems were reported in a minority. In patients ≥2 years, three were diagnosed with Autism Spectrum Disorder (ASD) and four with Attention Deficit Hyperactivity Disorder (ADHD). We report 27 novel variants and one previously reported variant. 24 were truncating variants; three were missense variants and one large in-frame gain including exons 10-12.

Published
2021

9. Clinical, genetic, and histological features of centronuclear myopathy in the Netherlands

Author

Reumers, S.F.I., Erasmus, C.E., Bouman, K., Pennings, Maartje, Schouten, M.I., Kusters, B., Duijkers, F.A., Kooi, A. van der, Jaeger, B., Verschuuren-Bemelmans, C.C., Faber, C.G., Engelen, B.G.M. van, Kamsteeg, E.J., Jungbluth, H., Voermans, N.C., Reumers, S.F.I., Erasmus, C.E., Bouman, K., Pennings, Maartje, Schouten, M.I., Kusters, B., Duijkers, F.A., Kooi, A. van der, Jaeger, B., Verschuuren-Bemelmans, C.C., Faber, C.G., Engelen, B.G.M. van, Kamsteeg, E.J., Jungbluth, H., and Voermans, N.C.

Abstract

Contains fulltext : 241356.pdf (Publisher’s version ) (Open Access), Centronuclear myopathy (CNM) is a genetically heterogeneous congenital myopathy characterized by muscle weakness, atrophy, and variable degrees of cardiorespiratory involvement. The clinical severity is largely explained by genotype (DNM2, MTM1, RYR1, BIN1, TTN, and other rarer genetic backgrounds), specific mutation(s), and age of the patient. The histopathological hallmark of CNM is the presence of internal centralized nuclei on muscle biopsy. Information on the phenotypical spectrum, subtype prevalence, and phenotype-genotype correlations is limited. To characterize CNM more comprehensively, we retrospectively assessed a national cohort of 48 CNM patients (mean age = 32 ± 24 years, range 0-80, 54% males) from the Netherlands clinically, histologically, and genetically. All information was extracted from entries in the patient's medical records, between 2000 and 2020. Frequent clinical features in addition to muscle weakness and hypotonia were fatigue and exercise intolerance in more mildly affected cases. Genetic analysis showed variants in four genes (18 DNM2, 14 MTM1, 9 RYR1, and 7 BIN1), including 16 novel variants. In addition to central nuclei, histologic examination revealed a large variability of myopathic features in the different genotypes. The identification and characterization of these patients contribute to trial readiness.

Published
2021

10. Systematic analysis of short tandem repeats in 38,095 exomes provides an additional diagnostic yield

Author

Sanden, B. van der, Corominas, J., Groot, M de, Pennings, M., Meijer, R.P., Verbeek, N., Warrenburg, B.P.C. van de, Schouten, M.I., Yntema, H.G., Vissers, L.E.L.M., Kamsteeg, E.J., Gilissen, C., Sanden, B. van der, Corominas, J., Groot, M de, Pennings, M., Meijer, R.P., Verbeek, N., Warrenburg, B.P.C. van de, Schouten, M.I., Yntema, H.G., Vissers, L.E.L.M., Kamsteeg, E.J., and Gilissen, C.

Abstract

Contains fulltext : 237911.pdf (Publisher’s version ) (Closed access), PURPOSE: Expansions of a subset of short tandem repeats (STRs) have been implicated in approximately 30 different human genetic disorders. Despite extensive application of exome sequencing (ES) in routine diagnostic genetic testing, STRs are not routinely identified from these data. METHODS: We assessed diagnostic utility of STR analysis in exome sequencing by applying ExpansionHunter to 2,867 exomes from movement disorder patients and 35,228 other clinical exomes. RESULTS: We identified 38 movement disorder patients with a possible aberrant STR length. Validation by polymerase chain reaction (PCR) and/or repeat-primed PCR technologies confirmed the presence of aberrant expansion alleles for 13 (34%). For seven of these patients the genotype was compatible with the phenotypic description, resulting in a molecular diagnosis. We subsequently tested the remainder of our diagnostic ES cohort, including over 30 clinically and genetically heterogeneous disorders. Optimized manual curation yielded 167 samples with a likely aberrant STR length. Validations confirmed 93/167 (56%) aberrant expansion alleles, of which 48 were in the pathogenic range and 45 in the premutation range. CONCLUSION: Our work provides guidance for the implementation of STR analysis in clinical ES. Our results show that systematic STR evaluation may increase diagnostic ES yield by 0.2%, and recommend making STR evaluation a routine part of ES interpretation in genetic testing laboratories.

Published
2021

11. Spectrum of Clinical Features in X-Linked Myotubular Myopathy Carriers: An International Questionnaire Study

Author

Reumers, S.F.I., Braun, F., Spillane, J.E., Böhm, J., Pennings, M., Schouten, M.I., Kooi, A.J. van der, Foley, A.R., Bönnemann, C.G., Kamsteeg, E.J., Erasmus, C.E., Schara-Schmidt, U., Jungbluth, H., Voermans, N.C., Reumers, S.F.I., Braun, F., Spillane, J.E., Böhm, J., Pennings, M., Schouten, M.I., Kooi, A.J. van der, Foley, A.R., Bönnemann, C.G., Kamsteeg, E.J., Erasmus, C.E., Schara-Schmidt, U., Jungbluth, H., and Voermans, N.C.

Abstract

Item does not contain fulltext, OBJECTIVE: To characterize the spectrum of clinical features in a cohort of X-linked myotubular myopathy (XL-MTM) carriers, including prevalence, genetic features, clinical symptoms, and signs, as well as associated disease burden. METHODS: We performed a cross-sectional online questionnaire study among XL-MTM carriers. Participants were recruited from patient associations, medical centers, and registries in the United Kingdom, Germany, and the Netherlands. We used a custom-made questionnaire, the Checklist Individual Strength (CIS), the Frenchay Activities Index (FAI), the Short Form 12 (SF-12) health survey, and the McGill Pain Questionnaire. Carriers were classified as manifesting or nonmanifesting on the basis of self-reported ambulation and muscle weakness. RESULTS: The prevalence of manifesting carriers in this study population (n = 76) was 51%, subdivided into mild (independent ambulation, 39%), moderate (assisted ambulation, 9%), and severe (wheelchair dependent, 3%) phenotypes. In addition to muscle weakness, manifesting carriers frequently reported fatigue (70%) and exercise intolerance (49%). Manifesting carriers scored higher on the overall CIS (p = 0.001), the fatigue subscale (p < 0.001), and least severe pain subscale (p = 0.005) than nonmanifesting carriers. They scored lower on the FAI (p = 0.005) and the physical component of the SF-12 health survey (p < 0.001). CONCLUSIONS: The prevalence of manifesting XL-MTM carriers may be higher than currently assumed, most having a mild phenotype and a wide variety of symptoms. Manifesting carriers are particularly affected by fatigue, limitations of daily activities, pain, and reduced quality of life. Our findings should increase awareness and provide useful information for health care providers and future clinical trials.

Published
2021

12. KIF1A variants are a frequent cause of autosomal dominant hereditary spastic paraplegia

Author

Pennings, M., Schouten, M.I., Gaalen, J. van, Meijer, Rowdy P. P., Bot, S.T. de, Kriek, Marjolein, Saris, C.G.J., Vries, B.B.A. de, Schieving, J.H., Warrenburg, B.P.C. van de, Kamsteeg, E.J., Pennings, M., Schouten, M.I., Gaalen, J. van, Meijer, Rowdy P. P., Bot, S.T. de, Kriek, Marjolein, Saris, C.G.J., Vries, B.B.A. de, Schieving, J.H., Warrenburg, B.P.C. van de, and Kamsteeg, E.J.

Abstract

Contains fulltext : 214064.pdf (publisher's version ) (Open Access)

Published
2020

13. Autosomal dominant GCH1 mutations causing spastic paraplegia at disease onset

Author

Wassenberg, T., Schouten, M.I., Helmich, R.C.G., Willemsen, M.A.A.P., Kamsteeg, E.J., Warrenburg, B.P.C. van de, Wassenberg, T., Schouten, M.I., Helmich, R.C.G., Willemsen, M.A.A.P., Kamsteeg, E.J., and Warrenburg, B.P.C. van de

Abstract

Contains fulltext : 220217.pdf (Publisher’s version ) (Closed access)

Published
2020

14. A hereditary spastic paraplegia predominant phenotype caused by variants in the NEFL gene

Author

Mul, K., Schouten, M.I., Looij, E. van der, Dooijes, D., Hennekam, F.A., Notermans, N.C., Praamstra, P., Gaalen, J. van, Kamsteeg, E.J., Verbeek, N.E., Warrenburg, B.P.C. van de, Mul, K., Schouten, M.I., Looij, E. van der, Dooijes, D., Hennekam, F.A., Notermans, N.C., Praamstra, P., Gaalen, J. van, Kamsteeg, E.J., Verbeek, N.E., and Warrenburg, B.P.C. van de

Abstract

Contains fulltext : 229318.pdf (Publisher’s version ) (Open Access), INTRODUCTION: This study reports a large series of patients with a clinical picture dominated by spastic paraplegia in whom variants in the NEFL gene, a known cause for Charcot-Marie-Tooth disease, were identified. METHODS: Index patients referred for a suspicion of hereditary spastic paraplegia (HSP) were clinically assessed and genetic analysis by next-generation sequencing was undertaken. Additional family members were clinically examined and subjected to targeted testing. RESULTS: We identified two different heterozygous dominant variants in the NEFL gene in 25 patients from 14 families. Most of them (21/25) had a clinical diagnosis of HSP, often with a concomitant clinical diagnosis of polyneuropathy (16/21). Two patients were identified with a polyneuropathy with a pyramidal reflex pattern, but without spasticity. Two patients had isolated polyneuropathy. Out of the 21 patients with a diagnosis of HSP, two had co-occurring cerebellar signs. The c.262A > C p.(Thr88Pro) variant was detected in 13 families. Genealogical analysis showed shared ancestors or a similar geographical origin in 12, suggesting a founder effect. The other variant, c.296A > C p.(Asp99Ala), was found in only one family, in which limited segregation analysis could be performed. DISCUSSION: Variants in the NEFL gene can cause HSP, with or without co-existing polyneuropathy, and should be included in diagnostic testing strategies for HSP patients.

Published
2020

15. Panel-Based Exome Sequencing for Neuromuscular Disorders as a Diagnostic Service

Author

Westra, D., Schouten, M.I., Stunnenberg, B.C., Kusters, B., Saris, C.G.J., Erasmus, C.E., Engelen, B.G.M. van, Bulk, S., Verschuuren-Bemelmans, C.C., Gerkes, E.H., Geus, C. de, Zwaag, P.A. van der, Chan, S., Chung, B., Barge-Schaapveld, D., Kriek, M., Sznajer, Y., Spaendonck-Zwarts, K.Y. van, Kooi, A.J. van der, Krause, A., Schonewolf-Greulich, B., Die-Smulders, C.E. de, Sallevelt, S., Krapels, I.P.C., Rasmussen, M., Maystadt, I., Kievit, A.J., Witting, N., Pennings, M., Meijer, R.I., Gillissen, C., Kamsteeg, E.J., Voermans, N.C., Westra, D., Schouten, M.I., Stunnenberg, B.C., Kusters, B., Saris, C.G.J., Erasmus, C.E., Engelen, B.G.M. van, Bulk, S., Verschuuren-Bemelmans, C.C., Gerkes, E.H., Geus, C. de, Zwaag, P.A. van der, Chan, S., Chung, B., Barge-Schaapveld, D., Kriek, M., Sznajer, Y., Spaendonck-Zwarts, K.Y. van, Kooi, A.J. van der, Krause, A., Schonewolf-Greulich, B., Die-Smulders, C.E. de, Sallevelt, S., Krapels, I.P.C., Rasmussen, M., Maystadt, I., Kievit, A.J., Witting, N., Pennings, M., Meijer, R.I., Gillissen, C., Kamsteeg, E.J., and Voermans, N.C.

Abstract

Contains fulltext : 204157.pdf (publisher's version ) (Closed access), BACKGROUND: Neuromuscular disorders (NMDs) are clinically and genetically heterogeneous. Accurate molecular genetic diagnosis can improve clinical management, provides appropriate genetic counseling and testing of relatives, and allows potential therapeutic trials. OBJECTIVE: To establish the clinical utility of panel-based whole exome sequencing (WES) in NMDs in a population with children and adults with various neuromuscular symptoms. METHODS: Clinical exome sequencing, followed by diagnostic interpretation of variants in genes associated with NMDs, was performed in a cohort of 396 patients suspected of having a genetic cause with a variable age of onset, neuromuscular phenotype, and inheritance pattern. Many had previously undergone targeted gene testing without results. RESULTS: Disease-causing variants were identified in 75/396 patients (19%), with variants in the three COL6-genes (COL6A1, COL6A2 and COL6A3) as the most common cause of the identified muscle disorder, followed by variants in the RYR1 gene. Together, these four genes account for almost 25% of cases in whom a definite genetic cause was identified. Furthermore, likely pathogenic variants and/or variants of uncertain significance were identified in 95 of the patients (24%), in whom functional and/or segregation analysis should be used to confirm or reject the pathogenicity. In 18% of the cases with a disease-causing variant of which we received additional clinical information, we identified a genetic cause in genes of which the associated phenotypes did not match that of the patients. Hence, the advantage of panel-based WES is its unbiased approach. CONCLUSION: Whole exome sequencing, followed by filtering for NMD genes, offers an unbiased approach for the genetic diagnostics of NMD patients. This approach could be used as a first-tier test in neuromuscular disorders with a high suspicion of a genetic cause. With uncertain results, functional testing and segregation analysis are needed to complete t

Published
2019

16. Clinical Presentation of a Complex Neurodevelopmental Disorder Caused by Mutations in ADNP

Author

Dijck, A. Van, Vulto-van Silfhout, A.T., Cappuyns, E., Werf, I.M. van der, Mancini, G.M.S., Tzschach, A., Bernier, R., Gozes, I., Eichler, E.E., Romano, C, Lindstrand, A., Nordgren, A., Kvarnung, M., Kleefstra, T., Vries, B.B. de, Kury, S., Rosenfeld, J.A., Meuwissen, M.E., Vandeweyer, G., Kooy, R.F., Schouten, M.I., Willemsen, M.H., Marcelis, C.L., Ockeloen, C.W., Burgt, I. van der, Feenstra, I., Manning, M.A., Slattery, L., Dijck, A. Van, Vulto-van Silfhout, A.T., Cappuyns, E., Werf, I.M. van der, Mancini, G.M.S., Tzschach, A., Bernier, R., Gozes, I., Eichler, E.E., Romano, C, Lindstrand, A., Nordgren, A., Kvarnung, M., Kleefstra, T., Vries, B.B. de, Kury, S., Rosenfeld, J.A., Meuwissen, M.E., Vandeweyer, G., Kooy, R.F., Schouten, M.I., Willemsen, M.H., Marcelis, C.L., Ockeloen, C.W., Burgt, I. van der, Feenstra, I., Manning, M.A., and Slattery, L.

Abstract

Contains fulltext : 202777.pdf (publisher's version ) (Closed access), BACKGROUND: In genome-wide screening studies for de novo mutations underlying autism and intellectual disability, mutations in the ADNP gene are consistently reported among the most frequent. ADNP mutations have been identified in children with autism spectrum disorder comorbid with intellectual disability, distinctive facial features, and deficits in multiple organ systems. However, a comprehensive clinical description of the Helsmoortel-Van der Aa syndrome is lacking. METHODS: We identified a worldwide cohort of 78 individuals with likely disruptive mutations in ADNP from January 2014 to October 2016 through systematic literature search, by contacting collaborators, and through direct interaction with parents. Clinicians filled in a structured questionnaire on genetic and clinical findings to enable correlations between genotype and phenotype. Clinical photographs and specialist reports were gathered. Parents were interviewed to complement the written questionnaires. RESULTS: We report on the detailed clinical characterization of a large cohort of individuals with an ADNP mutation and demonstrate a distinctive combination of clinical features, including mild to severe intellectual disability, autism, severe speech and motor delay, and common facial characteristics. Brain abnormalities, behavioral problems, sleep disturbance, epilepsy, hypotonia, visual problems, congenital heart defects, gastrointestinal problems, short stature, and hormonal deficiencies are common comorbidities. Strikingly, individuals with the recurrent p.Tyr719* mutation were more severely affected. CONCLUSIONS: This overview defines the full clinical spectrum of individuals with ADNP mutations, a specific autism subtype. We show that individuals with mutations in ADNP have many overlapping clinical features that are distinctive from those of other autism and/or intellectual disability syndromes. In addition, our data show preliminary evidence of a correlation between genotype and phenotype.

Published
2019

17. Biallelic variants in LARS2 and KARS cause deafness and (ovario)leukodystrophy

Author

Knaap, M.S. van der, Bugiani, M., Mendes, M.I., Riley, L.G., Smith, D.E., Rudinger-Thirion, J., Frugier, M., Breur, M., Crawford, J., Gaalen, J. van, Schouten, M.I., Willems, M., Waisfisz, Q., Mau-Them, F.T., Rodenburg, R.J.T., Taft, R.J., Keren, B., Christodoulou, J., Depienne, C., Simons, C., Salomons, G.S., Mochel, F., Knaap, M.S. van der, Bugiani, M., Mendes, M.I., Riley, L.G., Smith, D.E., Rudinger-Thirion, J., Frugier, M., Breur, M., Crawford, J., Gaalen, J. van, Schouten, M.I., Willems, M., Waisfisz, Q., Mau-Them, F.T., Rodenburg, R.J.T., Taft, R.J., Keren, B., Christodoulou, J., Depienne, C., Simons, C., Salomons, G.S., and Mochel, F.

Abstract

Contains fulltext : 202716.pdf (publisher's version ) (Closed access), OBJECTIVE: To describe the leukodystrophy caused by pathogenic variants in LARS2 and KARS, encoding mitochondrial leucyl transfer RNA (tRNA) synthase and mitochondrial and cytoplasmic lysyl tRNA synthase, respectively. METHODS: We composed a group of 5 patients with leukodystrophy, in whom whole-genome or whole-exome sequencing revealed pathogenic variants in LARS2 or KARS. Clinical information, brain MRIs, and postmortem brain autopsy data were collected. We assessed aminoacylation activities of purified mutant recombinant mitochondrial leucyl tRNA synthase and performed aminoacylation assays on patients' lymphoblasts and fibroblasts. RESULTS: Patients had a combination of early-onset deafness and later-onset neurologic deterioration caused by progressive brain white matter abnormalities on MRI. Female patients with LARS2 pathogenic variants had premature ovarian failure. In 2 patients, MRI showed additional signs of early-onset vascular abnormalities. In 2 other patients with LARS2 and KARS pathogenic variants, magnetic resonance spectroscopy revealed elevated white matter lactate, suggesting mitochondrial disease. Pathology in one patient with LARS2 pathogenic variants displayed evidence of primary disease of oligodendrocytes and astrocytes with lack of myelin and deficient astrogliosis. Aminoacylation activities of purified recombinant mutant leucyl tRNA synthase showed a 3-fold loss of catalytic efficiency. Aminoacylation assays on patients' lymphoblasts and fibroblasts showed about 50% reduction of enzyme activity. CONCLUSION: This study adds LARS2 and KARS pathogenic variants as gene defects that may underlie deafness, ovarian failure, and leukodystrophy with mitochondrial signature. We discuss the specific MRI characteristics shared by leukodystrophies caused by mitochondrial tRNA synthase defects. We propose to add aminoacylation assays as biochemical diagnostic tools for leukodystrophies.

Published
2019

18. Functional impairments, fatigue and quality of life in RYR1-related myopathies: A questionnaire study

Author

Ruitenbeek, E. van, Custers, J.A.E., Verhaak, C.M., Snoeck, M., Erasmus, C.E., Kamsteeg, E.J., Schouten, M.I., Engelen, B.G.M. van, Jungbluth, H., Voermans, N.C., Ruitenbeek, E. van, Custers, J.A.E., Verhaak, C.M., Snoeck, M., Erasmus, C.E., Kamsteeg, E.J., Schouten, M.I., Engelen, B.G.M. van, Jungbluth, H., and Voermans, N.C.

Abstract

Contains fulltext : 202034.pdf (publisher's version ) (Closed access)

Published
2019

20. Clinical exome sequencing for cerebellar ataxia and spastic paraplegia uncovers novel gene-disease associations and unanticipated rare disorders [Corrigendum]

Author

Warrenburg, B.P.C. van de, Schouten, M.I., Bot, S.T. de, Vermeer, S., Meijer, R., Pennings, M., Gilissen, C., Willemsen, M.A.A.P., Scheffer, H., and Kamsteeg, E.J.

Subjects
Disorders of movement Donders Center for Medical Neuroscience [Radboudumc 3], Sensory disorders Donders Center for Medical Neuroscience [Radboudumc 12], Rare cancers Radboud Institute for Health Sciences [Radboudumc 9]
Abstract

Item does not contain fulltext 1 p.

Published
2017

21. Chromosomal contacts connect loci associated with autism, BMI and head circumference phenotypes

Author

Loviglio, M.N., Leleu, M., Mannik, K., Passeggeri, M., Giannuzzi, G., Werf, I. van der, Waszak, S.M., Zazhytska, M., Roberts-Caldeira, I., Gheldof, N., Migliavacca, E., Alfaiz, A.A., Hippolyte, L., Maillard, A.M., Dijck, A. Van, Kooy, R.F., Sanlaville, D., Rosenfeld, J.A., Shaffer, L.G., Andrieux, J., Marshall, C., Scherer, S.W., Shen, Y., Gusella, J.F., Thorsteinsdottir, U., Thorleifsson, G., Dermitzakis, E.T., Deplancke, B., Beckmann, J.S., Rougemont, J., Jacquemont, S., Reymond, A., Vulto-van Silfhout, A.T., Schouten, M.I., Pfundt, R.P., Leeuw, N. de, et al., Loviglio, M.N., Leleu, M., Mannik, K., Passeggeri, M., Giannuzzi, G., Werf, I. van der, Waszak, S.M., Zazhytska, M., Roberts-Caldeira, I., Gheldof, N., Migliavacca, E., Alfaiz, A.A., Hippolyte, L., Maillard, A.M., Dijck, A. Van, Kooy, R.F., Sanlaville, D., Rosenfeld, J.A., Shaffer, L.G., Andrieux, J., Marshall, C., Scherer, S.W., Shen, Y., Gusella, J.F., Thorsteinsdottir, U., Thorleifsson, G., Dermitzakis, E.T., Deplancke, B., Beckmann, J.S., Rougemont, J., Jacquemont, S., Reymond, A., Vulto-van Silfhout, A.T., Schouten, M.I., Pfundt, R.P., Leeuw, N. de, and et al.

Abstract

Contains fulltext : 174530.pdf (publisher's version ) (Open Access), Copy number variants (CNVs) are major contributors to genomic imbalance disorders. Phenotyping of 137 unrelated deletion and reciprocal duplication carriers of the distal 16p11.2 220 kb BP2-BP3 interval showed that these rearrangements are associated with autism spectrum disorders and mirror phenotypes of obesity/underweight and macrocephaly/microcephaly. Such phenotypes were previously associated with rearrangements of the non-overlapping proximal 16p11.2 600 kb BP4-BP5 interval. These two CNV-prone regions at 16p11.2 are reciprocally engaged in complex chromatin looping, as successfully confirmed by 4C-seq, fluorescence in situ hybridization and Hi-C, as well as coordinated expression and regulation of encompassed genes. We observed that genes differentially expressed in 16p11.2 BP4-BP5 CNV carriers are concomitantly modified in their chromatin interactions, suggesting that disruption of chromatin interplays could participate in the observed phenotypes. We also identified cis- and trans-acting chromatin contacts to other genomic regions previously associated with analogous phenotypes. For example, we uncovered that individuals with reciprocal rearrangements of the trans-contacted 2p15 locus similarly display mirror phenotypes on head circumference and weight. Our results indicate that chromosomal contacts' maps could uncover functionally and clinically related genes.

Published
2017

22. Clinical exome sequencing for cerebellar ataxia and spastic paraplegia uncovers novel gene-disease associations and unanticipated rare disorders

Author

Warrenburg, B.P.C. van de, Schouten, M.I., Bot, S.T. de, Vermeer, S., Meijer, R., Pennings, M., Gilissen, C., Willemsen, M.A.A.P., Scheffer, H., Kamsteeg, E.J., Warrenburg, B.P.C. van de, Schouten, M.I., Bot, S.T. de, Vermeer, S., Meijer, R., Pennings, M., Gilissen, C., Willemsen, M.A.A.P., Scheffer, H., and Kamsteeg, E.J.

Abstract

Contains fulltext : 167657.pdf (Publisher’s version ) (Open Access), Cerebellar ataxia (CA) and hereditary spastic paraplegia (HSP) are two of the most prevalent motor disorders with extensive locus and allelic heterogeneity. We implemented clinical exome sequencing, followed by filtering data for a 'movement disorders' gene panel, as a generic test to increase variant detection in 76 patients with these disorders. Segregation analysis or phenotypic re-evaluation was utilized to substantiate findings. Disease-causing variants were identified in 9 of 28 CA patients, and 8 of 48 HSP patients. In addition, possibly disease-causing variants were identified in 1 and 8 of the remaining CA and HSP patients, respectively. In 10 patients with CA, the total disease-causing or possibly disease-causing variants were detected in 8 different genes, whereas 16 HSP patients had such variants in 12 different genes. In the majority of cases, the identified variants were compatible with the patient phenotype. Interestingly, in some patients variants were identified in genes hitherto related to other movement disorders, such as TH variants in two siblings with HSP. In addition, rare disorders were uncovered, for example, a second case of HSP caused by a VCP variant. For some patients, exome sequencing results had implications for treatment, exemplified by the favorable L-DOPA treatment in a patient with HSP due to ATP13A2 variants (Parkinson type 9). Thus, clinical exome sequencing in this cohort of CA and HSP patients suggests broadening of disease spectra, revealed novel gene-disease associations, and uncovered unanticipated rare disorders. In addition, clinical exome sequencing results have shown their value in guiding practical patient management.

Published
2016

23. The Genetic Homogeneity of CAPOS Syndrome: Four New Patients With the c.2452G>A (p.Glu818Lys) Mutation in the ATP1A3 Gene

Author

Maas, R.P.P.W.M., Schieving, J.H., Schouten, M.I., Kamsteeg, E.J., Warrenburg, B.P.C. van de, Maas, R.P.P.W.M., Schieving, J.H., Schouten, M.I., Kamsteeg, E.J., and Warrenburg, B.P.C. van de

Abstract

Item does not contain fulltext, BACKGROUND: The clinical syndrome of cerebellar ataxia, areflexia, pes cavus, optic atrophy, and sensorineural hearing loss (CAPOS) was first described 20 years ago, but it was only recently that whole exome sequencing unveiled the causative mutation in the ATP1A3 gene. We present four patients from the seventh and eighth family identified worldwide, provide a critical review of all patients published thus far, and speculate about the pathophysiologic processes underlying the acute neurological manifestations. CLINICAL OBSERVATIONS: The individuals presented here experienced one to three paroxysmal, short-lasting episodes in childhood with cerebellar symptoms and signs, hypotonia, ophthalmoparesis, motor weakness, areflexia, and/or lethargy that were consistently associated with febrile illness. An underlying c.2452G>A mutation in the ATP1A3 gene was found in all four individuals. Besides the persisting CAPOS features, other possibly related sequelae included dystonia, myoclonus, and emotional and behavioral changes. After initiation of acetazolamide in two patients, no further episodes occurred. CONCLUSION: Targeted sequencing of the ATP1A3 gene is recommended in children exhibiting paroxysmal, fever-induced ataxia and in adults with a more or less stationary or slowly progressive cerebellar syndrome since childhood accompanied by mixed combinations of areflexia, pes cavus, profound visual impairment, and/or sensorineural hearing loss. Similar to some other types of episodic ataxia, acetazolamide may be considered in patients with CAPOS syndrome to prevent or attenuate bouts of ataxia, but this requires further study.

Published
2016

24. Interpretatie van integratie. Een verkennend onderzoek naar de consistentie van politieke partijen in het integratiedebat

Author

Schouten, M.I., Graaf, W. de (Thesis Advisor), Schouten, M.I., and Graaf, W. de (Thesis Advisor)

Abstract

Er bestaan veel interpretaties van het begrip integratie. Vaak wordt integratie ook in één adem genoemd met andere onderwerpen, zoals huwelijksmigratie, onderwijs, huisvestiging, discriminatie, criminaliteit en normen en waarden. Ondanks de breedte van het onderwerp valt er wel een algemene opvatting in het integratiedebat te ontdekken. Die is door de jaren heen sterk veranderd, maar de huidige algemene opvatting is dat immigranten ‘mee moeten doen met de samenleving’. Ze moeten de taal leren, aan het werk en de Nederlandse normen en waarden overnemen. Binnen deze algemene opvatting zitten weer verschillen tussen de diverse politieke partijen. Dat heeft natuurlijk vooral te maken met de geschiedenis en de ideologie van de politieke partijen. Maar hoe consistent zijn partijen in hun opvattingen over integratie? Blijven zij in een debat stevig aan hun eigen standpunten vasthouden? Of zijn hun opvattingen in de praktijk heel anders dan dat zij op papier hebben gezet? En passen hun standpunten wel bij hun eigen ideologie? In dit onderzoek wordt ingegaan op de achtergrond en ideologie van vijf politieke partijen. Vervolgens wordt gekeken welke standpunten deze politieke partijen in verkiezingsprogramma’s, nota’s en op hun websites innemen over integratie. Tot slot wordt er een debat over het integratievraagstuk geanalyseerd om te kijken hoe standpunten van politieke partijen tot uiting komen. Het blijkt dat er geenszins sprake is van één vloeiende lijn tussen partij-ideologie, standpunten op papier en het debat. En dat maakt het integratiedebat er niet makkelijker op; voor de partijen niet, maar ook voor de burgers niet.

Published
2009

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