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1. SCN1A-deficient excitatory neuronal networks display mutation-specific phenotypes.

Author

Hugte, E.J.H. van, Lewerissa, E.I., Wu, K.M., Scheefhals, N., Parodi, G., Voorst, T.W. van, Puvogel Lütjens, S., Kogo, N., Keller, J.M., Frega, M., Schubert, D., Schelhaas, H.J., Verhoeven, J., Majoie, M., Bokhoven, H. van, Nadif Kasri, N., Hugte, E.J.H. van, Lewerissa, E.I., Wu, K.M., Scheefhals, N., Parodi, G., Voorst, T.W. van, Puvogel Lütjens, S., Kogo, N., Keller, J.M., Frega, M., Schubert, D., Schelhaas, H.J., Verhoeven, J., Majoie, M., Bokhoven, H. van, and Nadif Kasri, N.

Abstract

Contains fulltext : 300240.pdf (Publisher’s version ) (Open Access), Dravet syndrome is a severe epileptic encephalopathy, characterized by (febrile) seizures, behavioural problems and developmental delay. Eighty per cent of patients with Dravet syndrome have a mutation in SCN1A, encoding Nav1.1. Milder clinical phenotypes, such as GEFS+ (generalized epilepsy with febrile seizures plus), can also arise from SCN1A mutations. Predicting the clinical phenotypic outcome based on the type of mutation remains challenging, even when the same mutation is inherited within one family. This clinical and genetic heterogeneity adds to the difficulties of predicting disease progression and tailoring the prescription of anti-seizure medication. Understanding the neuropathology of different SCN1A mutations may help to predict the expected clinical phenotypes and inform the selection of best-fit treatments. Initially, the loss of Na+-current in inhibitory neurons was recognized specifically to result in disinhibition and consequently seizure generation. However, the extent to which excitatory neurons contribute to the pathophysiology is currently debated and might depend on the patient clinical phenotype or the specific SCN1A mutation. To examine the genotype-phenotype correlations of SCN1A mutations in relation to excitatory neurons, we investigated a panel of patient-derived excitatory neuronal networks differentiated on multi-electrode arrays. We included patients with different clinical phenotypes, harbouring various SCN1A mutations, along with a family in which the same mutation led to febrile seizures, GEFS+ or Dravet syndrome. We hitherto describe a previously unidentified functional excitatory neuronal network phenotype in the context of epilepsy, which corresponds to seizurogenic network prediction patterns elicited by proconvulsive compounds. We found that excitatory neuronal networks were affected differently, depending on the type of SCN1A mutation, but did not segregate according to clinical severity. Specifically, loss-of-function mutat

Published
2023

4. NEXMIF encephalopathy: an X-linked disorder with male and female phenotypic patterns

Author

Stamberger, H., Hammer, T.B., Gardella, E., Vlaskamp, D.R.M., Bertelsen, B., Mandelstam, S., Lange, I. de, Zhang, J., Myers, C.T., Fenger, C., Afawi, Z., Fuerte, E.P. Almanza, Andrade, D.M., Balcik, Y., Zeev, B. Ben, Bennett, M.F., Berkovic, S.F., Isidor, B., Bouman, A., Brilstra, E., Ø, L. Busk, Cairns, A., Caumes, R., Chatron, N., Dale, R.C., Geus, C. de, Edery, P., Gill, D., Granild-Jensen, J.B., Gunderson, L., Gunning, B., Heimer, G., Helle, J.R., Hildebrand, M.S., Hollingsworth, G., Kharytonov, V., Klee, E.W., Koeleman, B.P.C., Koolen, D.A., Korff, C., Küry, S., Lesca, G., Lev, D., Leventer, R.J., Mackay, M.T., Macke, E.L., McEntagart, M., Mohammad, S.S., Monin, P., Montomoli, M., Morava, E., Moutton, S., Muir, A.M., Parrini, E., Procopis, P., Ranza, E., Reed, L., Reif, P.S., Rosenow, F., Rossi, M., Sadleir, L.G., Sadoway, T., Schelhaas, H.J., Schneider, A.L., Shah, K., Shalev, R., Sisodiya, S.M., Smol, T., Stumpel, C., Stuurman, K., Symonds, J.D., Mau-Them, F.T., Verbeek, N., Verhoeven, J.S., Wallace, G., Yosovich, K., Zarate, Y.A., Zerem, A., Zuberi, S.M., Guerrini, R., Mefford, H.C., Patel, C., Zhang, Y.H., Møller, R.S., Scheffer, I.E., Stamberger, H., Hammer, T.B., Gardella, E., Vlaskamp, D.R.M., Bertelsen, B., Mandelstam, S., Lange, I. de, Zhang, J., Myers, C.T., Fenger, C., Afawi, Z., Fuerte, E.P. Almanza, Andrade, D.M., Balcik, Y., Zeev, B. Ben, Bennett, M.F., Berkovic, S.F., Isidor, B., Bouman, A., Brilstra, E., Ø, L. Busk, Cairns, A., Caumes, R., Chatron, N., Dale, R.C., Geus, C. de, Edery, P., Gill, D., Granild-Jensen, J.B., Gunderson, L., Gunning, B., Heimer, G., Helle, J.R., Hildebrand, M.S., Hollingsworth, G., Kharytonov, V., Klee, E.W., Koeleman, B.P.C., Koolen, D.A., Korff, C., Küry, S., Lesca, G., Lev, D., Leventer, R.J., Mackay, M.T., Macke, E.L., McEntagart, M., Mohammad, S.S., Monin, P., Montomoli, M., Morava, E., Moutton, S., Muir, A.M., Parrini, E., Procopis, P., Ranza, E., Reed, L., Reif, P.S., Rosenow, F., Rossi, M., Sadleir, L.G., Sadoway, T., Schelhaas, H.J., Schneider, A.L., Shah, K., Shalev, R., Sisodiya, S.M., Smol, T., Stumpel, C., Stuurman, K., Symonds, J.D., Mau-Them, F.T., Verbeek, N., Verhoeven, J.S., Wallace, G., Yosovich, K., Zarate, Y.A., Zerem, A., Zuberi, S.M., Guerrini, R., Mefford, H.C., Patel, C., Zhang, Y.H., Møller, R.S., and Scheffer, I.E.

Abstract

Contains fulltext : 231688.pdf (Publisher’s version ) (Closed access), PURPOSE: Pathogenic variants in the X-linked gene NEXMIF (previously KIAA2022) are associated with intellectual disability (ID), autism spectrum disorder, and epilepsy. We aimed to delineate the female and male phenotypic spectrum of NEXMIF encephalopathy. METHODS: Through an international collaboration, we analyzed the phenotypes and genotypes of 87 patients with NEXMIF encephalopathy. RESULTS: Sixty-three females and 24 males (46 new patients) with NEXMIF encephalopathy were studied, with 30 novel variants. Phenotypic features included developmental delay/ID in 86/87 (99%), seizures in 71/86 (83%) and multiple comorbidities. Generalized seizures predominated including myoclonic seizures and absence seizures (both 46/70, 66%), absence with eyelid myoclonia (17/70, 24%), and atonic seizures (30/70, 43%). Males had more severe developmental impairment; females had epilepsy more frequently, and varied from unaffected to severely affected. All NEXMIF pathogenic variants led to a premature stop codon or were deleterious structural variants. Most arose de novo, although X-linked segregation occurred for both sexes. Somatic mosaicism occurred in two males and a family with suspected parental mosaicism. CONCLUSION: NEXMIF encephalopathy is an X-linked, generalized developmental and epileptic encephalopathy characterized by myoclonic-atonic epilepsy overlapping with eyelid myoclonia with absence. Some patients have developmental encephalopathy without epilepsy. Males have more severe developmental impairment. NEXMIF encephalopathy arises due to loss-of-function variants.

Published
2021

6. Hereditary spastic paraplegia due to SPAST mutations in 151 Dutch patients: new clinical aspects and 27 novel mutations

Author

de Bot, S.T., van den Elzen, R.T.M., Mensenkamp, A.R., Schelhaas, H.J., Willemsen, M.A.A.P., Knoers, N.V.A.M., Kremer, H.P.H., van de Warrenburg, B.P.C., and Scheffer, H.

Subjects
Paralysis, Spastic -- Research, Paralysis, Spastic -- Genetic aspects, Gene mutations -- Research, Gene mutations -- Physiological aspects, Health, Psychology and mental health
Published
2010

7. New cases of adult-onset Sandhoff disease with a cerebellar or lower motor neuron phenotype

Author

Delnooz, C.C.S., Lefeber, D.J., Langemeijer, S.M.C., Hoffjan, S., Dekomien, G., Zwarts, M.J., Van Engelen, B.G., Wevers, R.A., Schelhaas, H.J., and van de Warrenburg, B.P.C.

Subjects
Sandhoff disease -- Diagnosis, Sandhoff disease -- Development and progression, Sandhoff disease -- Care and treatment, Sandhoff disease -- Case studies, Cerebellar ataxia -- Case studies, Health, Psychology and mental health
Published
2010

9. Diagnostic exome sequencing in 100 consecutive patients with both epilepsy and intellectual disability

Author

Snoeijen-Schouwenaars, Francesca M., Ool, Jans S. van, Verhoeven, J.S., Mierlo, Petra van, Braakman, H.M., Smeets, E.E.J., Yntema, H.G., Brunner, H.G., Pfundt, R.P., Kamsteeg, E.J., Schelhaas, H.J., Willemsen, M.H., Snoeijen-Schouwenaars, Francesca M., Ool, Jans S. van, Verhoeven, J.S., Mierlo, Petra van, Braakman, H.M., Smeets, E.E.J., Yntema, H.G., Brunner, H.G., Pfundt, R.P., Kamsteeg, E.J., Schelhaas, H.J., and Willemsen, M.H.

Abstract

Contains fulltext : 201030.pdf (publisher's version ) (Closed access)

Published
2019

10. Mood, anxiety, and perceived quality of life in adults with epilepsy and intellectual disability

Author

Snoeijen-Schouwenaars, F.M., Snoeijen-Schouwenaars, F.M., van Ool, J.S., Tan, I.Y., Aldenkamp, A.P., Schelhaas, H.J., Hendriksen, J.G.M., Snoeijen-Schouwenaars, F.M., Snoeijen-Schouwenaars, F.M., van Ool, J.S., Tan, I.Y., Aldenkamp, A.P., Schelhaas, H.J., and Hendriksen, J.G.M.

Abstract

Objective Depression and anxiety symptoms are common among patients with epilepsy, but are relatively under-researched in patients with both epilepsy and intellectual disability (ID). The aim was to investigate whether epilepsy and ID characteristics are associated with mood, anxiety, and quality of life. Materials and Methods Adult patients with epilepsy and ID who rely on tertiary epilepsy care were included (N = 189). Mood, anxiety, and quality of life were assessed by standardized questionnaires. Epilepsy and ID characteristics were retrieved from patient charts or determined by psychometric instruments. Results Elevated levels of depressive and anxiety symptoms were present in 21.7% and 12.7%, respectively. Anxiety was significantly associated with a focal epilepsy type and ID domain discrepancy (substantial difference between two domains of adaptive behavior), but was negatively related to seizure frequency and drug load of mood-stabilizing antiepileptic drugs. Depressive symptoms were not significantly related to epilepsy characteristics, but a severe ID and ID domain discrepancy was associated with more depressive symptoms. Quality of life was significantly worse in those with multiple seizure types and ID domain discrepancy. Conclusion Whereas anxiety and quality of life are associated with individual epilepsy characteristics, this could not be confirmed for depressive symptoms in patients with epilepsy and ID, despite its high prevalence.

Published
2019

11. Classification of intellectual disability according to domains of adaptive functioning and between-domains discrepancy in adults with epilepsy

Author

van Ool, J.S., van Ool, J.S., Snoeijen-Schouwenaars, F.M., Tan, I.Y., Schelhaas, H.J., Aldenkamp, A.P., Hendriksen, J.G.M., van Ool, J.S., van Ool, J.S., Snoeijen-Schouwenaars, F.M., Tan, I.Y., Schelhaas, H.J., Aldenkamp, A.P., and Hendriksen, J.G.M.

Abstract

Background In the Diagnostic and Statistical Manual of Mental Disorders-Fifth edition (DSM-5), the diagnostic criteria of intellectual disability (ID) include three domains of adaptive deficits: the conceptual, social and practical. Substantial intra-individual differences between domains can be considered an ID domain discrepancy. Method We explored the associations between ID domains, discrepancies and epilepsy in 189 adults (mean age = 47.9; SD = 15.6). Each DSM-5 ID domain was assessed separately, using subscales of the Vineland II for the social and practical domains, and psychological instruments, including intelligence tests, for the conceptual domain. A set of standardised criteria is proposed to identify an ID domain discrepancy. Results An ID domain discrepancy seemed to be present in about one-third of subjects and was particularly present in subjects with moderate ID (53.4%). Impairment in the social domain was most often the reason for the discrepancy. The presence of a discrepancy was significantly related to a focal (localised) epilepsy type (OR = 2.3, P = .028) and a mixed seizure type (OR = 1.4, P = .009). Epilepsy characteristics that are indicative of a more severe and refractory epilepsy, including various seizure types, a high seizure frequency, a combined epilepsy type (both focal and generalised epilepsy) and an early age at onset, were significantly related to more severe impairments in conceptual, social and practical adaptive behaviour (all P values <.01). Conclusions With a substantial proportion of the subjects who had both ID and epilepsy with an ID discrepancy, professionals should be aware of this and take all domains of ID into account when studying or working with this vulnerable population.

Published
2019

12. De Novo Pathogenic Variants in CACNA1E Cause Developmental and Epileptic Encephalopathy with Contractures, Macrocephaly, and Dyskinesias

Author

Helbig, K.L., Lauerer, R.J., Bahr, J.C., Souza, I.A., Myers, C.T., Uysal, B., Schwarz, N., Gandini, M.A., Huang, S., Keren, B., Mignot, C., Afenjar, A., Villemeur, T. Billette de, Heron, D., Nava, C., Valence, S., Buratti, J., Fagerberg, C.R., Soerensen, K.P., Kibaek, M., Kamsteeg, E.J., Koolen, D.A., Gunning, B., Schelhaas, H.J., Kruer, M.C., Fox, J., Bakhtiari, S., Jarrar, R., Padilla-Lopez, S., Lindstrom, K., Jin, S.C., Zeng, X., Bilguvar, K., Papavasileiou, A., Xin, Q., Zhu, C., Boysen, K., Vairo, F., Lanpher, B.C., Klee, E.W., Tillema, J.M., Payne, E.T., Cousin, M.A., Kruisselbrink, T.M., Wick, M.J., Baker, J., Haan, E., Smith, N., Corbett, M.A., MacLennan, A.H., Gecz, J., Biskup, S., Goldmann, E., Rodan, L.H., Kichula, E., Segal, E., Jackson, K.E., Asamoah, A., Dimmock, D., McCarrier, J., Botto, L.D., Filloux, F., Tvrdik, T., Cascino, G.D., Klingerman, S., Neumann, C., Wang, R., Jacobsen, J.C., Nolan, M.A., Snell, R.G., Lehnert, K., Sadleir, L.G., Anderlid, B.M., Kvarnung, M., Guerrini, R., Friez, M.J., Lyons, M.J., Leonhard, J., Kringlen, G., Casas, K., Achkar, C.M. El, Smith, L.A., Rotenberg, A., Poduri, A., Sanchis-Juan, A., Carss, K.J., Rankin, J., Zeman, A., Raymond, F.L., Blyth, M., Kerr, B., Ruiz, K., Urquhart, J., Hughes, I., Banka, S., Hedrich, U.B.S., Scheffer, I.E., Helbig, I., Zamponi, G.W., Lerche, H., et al., Helbig, K.L., Lauerer, R.J., Bahr, J.C., Souza, I.A., Myers, C.T., Uysal, B., Schwarz, N., Gandini, M.A., Huang, S., Keren, B., Mignot, C., Afenjar, A., Villemeur, T. Billette de, Heron, D., Nava, C., Valence, S., Buratti, J., Fagerberg, C.R., Soerensen, K.P., Kibaek, M., Kamsteeg, E.J., Koolen, D.A., Gunning, B., Schelhaas, H.J., Kruer, M.C., Fox, J., Bakhtiari, S., Jarrar, R., Padilla-Lopez, S., Lindstrom, K., Jin, S.C., Zeng, X., Bilguvar, K., Papavasileiou, A., Xin, Q., Zhu, C., Boysen, K., Vairo, F., Lanpher, B.C., Klee, E.W., Tillema, J.M., Payne, E.T., Cousin, M.A., Kruisselbrink, T.M., Wick, M.J., Baker, J., Haan, E., Smith, N., Corbett, M.A., MacLennan, A.H., Gecz, J., Biskup, S., Goldmann, E., Rodan, L.H., Kichula, E., Segal, E., Jackson, K.E., Asamoah, A., Dimmock, D., McCarrier, J., Botto, L.D., Filloux, F., Tvrdik, T., Cascino, G.D., Klingerman, S., Neumann, C., Wang, R., Jacobsen, J.C., Nolan, M.A., Snell, R.G., Lehnert, K., Sadleir, L.G., Anderlid, B.M., Kvarnung, M., Guerrini, R., Friez, M.J., Lyons, M.J., Leonhard, J., Kringlen, G., Casas, K., Achkar, C.M. El, Smith, L.A., Rotenberg, A., Poduri, A., Sanchis-Juan, A., Carss, K.J., Rankin, J., Zeman, A., Raymond, F.L., Blyth, M., Kerr, B., Ruiz, K., Urquhart, J., Hughes, I., Banka, S., Hedrich, U.B.S., Scheffer, I.E., Helbig, I., Zamponi, G.W., and Lerche, H., et al.

Abstract

Item does not contain fulltext, Developmental and epileptic encephalopathies (DEEs) are severe neurodevelopmental disorders often beginning in infancy or early childhood that are characterized by intractable seizures, abundant epileptiform activity on EEG, and developmental impairment or regression. CACNA1E is highly expressed in the central nervous system and encodes the alpha1-subunit of the voltage-gated CaV2.3 channel, which conducts high voltage-activated R-type calcium currents that initiate synaptic transmission. Using next-generation sequencing techniques, we identified de novo CACNA1E variants in 30 individuals with DEE, characterized by refractory infantile-onset seizures, severe hypotonia, and profound developmental impairment, often with congenital contractures, macrocephaly, hyperkinetic movement disorders, and early death. Most of the 14, partially recurring, variants cluster within the cytoplasmic ends of all four S6 segments, which form the presumed CaV2.3 channel activation gate. Functional analysis of several S6 variants revealed consistent gain-of-function effects comprising facilitated voltage-dependent activation and slowed inactivation. Another variant located in the domain II S4-S5 linker results in facilitated activation and increased current density. Five participants achieved seizure freedom on the anti-epileptic drug topiramate, which blocks R-type calcium channels. We establish pathogenic variants in CACNA1E as a cause of DEEs and suggest facilitated R-type calcium currents as a disease mechanism for human epilepsy and developmental disorders.

Published
2018

13. Characterization of glycosylphosphatidylinositol biosynthesis defects by clinical features, flow cytometry, and automated image analysis

Author

Knaus, A. (Alexej), Pantel, J.T. (Jean Tori), Pendziwiat, M. (Manuela), Hajjir, N. (Nurulhuda), Zhao, M. (Max), Hsieh, T.-C. (Tzung-Chien), Schubach, M. (Max), Gurovich, Y. (Yaron), Fleischer, N. (Nicole), Jäger, M. (Marten), Köhler, S. (Sebastian), Muhle, H. (Hiltrud), Korff, C. (Christian), Møller, R.S. (Rikke S.), Bayat, A. (Allan), Calvas, P. (Patrick), Chassaing, N. (Nicolas), Warren, H. (Hannah), Skinner, S. (Steven), Louie, R. (Raymond), Evers, C. (Christina), Bohn, M. (Marc), Christen, H.-J. (Hans-Jürgen), Born, M. (Myrthe) van den, Obersztyn, E. (Ewa), Charzewska, A. (Agnieszka), Endziniene, M. (Milda), Kortüm, F. (Fanny), Brown, N. (Natasha), Robinson, P.N. (Peter N.), Schelhaas, H.J. (Helenius), Weber, Y. (Yvonne), Helbig, I. (Ingo), Mundlos, S. (Stefan), Horn, D. (Denise), Krawitz, P., Knaus, A. (Alexej), Pantel, J.T. (Jean Tori), Pendziwiat, M. (Manuela), Hajjir, N. (Nurulhuda), Zhao, M. (Max), Hsieh, T.-C. (Tzung-Chien), Schubach, M. (Max), Gurovich, Y. (Yaron), Fleischer, N. (Nicole), Jäger, M. (Marten), Köhler, S. (Sebastian), Muhle, H. (Hiltrud), Korff, C. (Christian), Møller, R.S. (Rikke S.), Bayat, A. (Allan), Calvas, P. (Patrick), Chassaing, N. (Nicolas), Warren, H. (Hannah), Skinner, S. (Steven), Louie, R. (Raymond), Evers, C. (Christina), Bohn, M. (Marc), Christen, H.-J. (Hans-Jürgen), Born, M. (Myrthe) van den, Obersztyn, E. (Ewa), Charzewska, A. (Agnieszka), Endziniene, M. (Milda), Kortüm, F. (Fanny), Brown, N. (Natasha), Robinson, P.N. (Peter N.), Schelhaas, H.J. (Helenius), Weber, Y. (Yvonne), Helbig, I. (Ingo), Mundlos, S. (Stefan), Horn, D. (Denise), and Krawitz, P.

Abstract

Background: Glycosylphosphatidylinositol biosynthesis defects (GPIBDs) cause a group of phenotypically overlapping recessive syndromes with intellectual disability, for which pathogenic mutations have been described in 16 genes of the corresponding molecular pathway. An elevated serum activity of alkaline phosphatase (AP), a GPI-linked enzyme, has been used to assign GPIBDs to the phenotypic series of hyperphosphatasia with mental retardation syndrome (HPMRS) and to distinguish them from another subset of GPIBDs, termed multiple congenital anomalies hypotonia seizures syndrome (MCAHS). However, the increasing number of individuals with a GPIBD shows that hyperphosphatasia is a variable feature that is not ideal for a clinical classification. Methods: We studied the discriminatory power of multiple GPI-linked substrates that were assessed by flow cytometry in blood cells and fibroblasts of 39 and 14 individuals with a GPIBD, respectively. On the phenotypic level, we evaluated the frequency of occurrence of clinical symptoms and analyzed the performance of computer-assisted image analysis of the facial gestalt in 91 individuals. Results: We found that certain malformations such as Morbus Hirschsprung and diaphragmatic defects are more likely to be associated with particular gene defects (PIGV, PGAP3, PIGN). However, especially at the severe end of the clinical spectrum of HPMRS, there is a high phenotypic overlap with MCAHS. Elevation of AP has also been documented in some of the individuals with MCAHS, namely those with PIGA mutations. Although the impairment of GPI-linked substrates is supposed to play the key role in the pathophysiology of GPIBDs, we could not observe gene-specific profiles for flow cytometric markers or a correlation between their cell surface levels and the severity of the phenotype. In contrast, it was facial recognition software that achieved the highest accuracy in predicting the disease-causing gene in a GPIBD. Conclusions: Due to the overlap

Published
2018
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15. Phenytoin as a last-resort treatment in SCN8A encephalopathy.

Author

Braakman, H.M., Erasmus, C.E., Haaxma, C.A., Willemsen, M.H., Schelhaas, H.J., Braakman, H.M., Erasmus, C.E., Haaxma, C.A., Willemsen, M.H., and Schelhaas, H.J.

Abstract

Contains fulltext : 175085.pdf (publisher's version ) (Open Access)

Published
2017

17. Normal values for quantitative muscle ultrasonography in adults

Author

Arts, I.M.P., Pillen, S., Schelhaas, H.J., Overeem, S., and Zwarts, M.J.

Subjects
Health aging / healthy living [IGMD 5], Functional Neurogenomics [DCN 2]
Abstract

Contains fulltext : 89861.pdf (Publisher’s version ) (Closed access) Ultrasonography can detect structural muscle changes caused by neuromuscular disease. Quantitative analysis is the preferred method to determine if ultrasound findings are within normal limits, but normative data are incomplete. The purpose of this study was to provide normative muscle ultrasonography data for muscle thickness and echo intensity for five different muscle groups in adults. Bilateral scans of the sternocleidomastoid, biceps brachii/brachialis, forearm flexor group, quadriceps femoris, and tibialis anterior were made in 95 volunteers, aged 17-90 years. Both muscle thickness and echo intensity showed gender differences and a muscle-specific non-linear correlation with age. The muscles of the upper extremities showed right-left differences. These data demonstrate the effect of age on muscle characteristics and provide normative values that can be used in clinical practice. 01 januari 2010

Published
2010

18. Survival profiles of patients with frontotemporal dementia and motor neuron disease

Author

Hu, W.T., Seelaar, H., Josephs, K.A., Knopman, D.S., Boeve, B.F., Sorenson, E.J., McCluskey, L., Elman, L., Schelhaas, H.J., Parisi, J.E., Kuesters, B., Lee, V.M., Trojanowski, J.Q., Petersen, R.C., Swieten, J.C. van, and Grossman, M.

Subjects
Perception and Action [DCN 1], Alzheimer Centre [NCEBP 11], Functional Neurogenomics [DCN 2]
Abstract

Contains fulltext : 81426.pdf (Publisher’s version ) (Closed access) BACKGROUND: Frontotemporal dementia and amyotrophic lateral sclerosis are neurodegenerative diseases associated with TAR DNA-binding protein 43- and ubiquitin-immunoreactive pathologic lesions. OBJECTIVE: To determine whether survival is influenced by symptom of onset in patients with frontotemporal dementia and amyotrophic lateral sclerosis. DESIGN, SETTING, AND PATIENTS: Retrospective review of patients with both cognitive impairment and motor neuron disease consecutively evaluated at 4 academic medical centers in 2 countries. MAIN OUTCOME MEASURES: Clinical phenotypes and survival patterns of patients. RESULTS: A total of 87 patients were identified, including 60 who developed cognitive symptoms first, 19 who developed motor symptoms first, and 8 who had simultaneous onset of cognitive and motor symptoms. Among the 59 deceased patients, we identified 2 distinct subgroups of patients according to survival. Long-term survivors had cognitive onset and delayed emergence of motor symptoms after a long monosymptomatic phase and had significantly longer survival than the typical survivors (mean, 67.5 months vs 28.2 months, respectively; P < .001). Typical survivors can have simultaneous or discrete onset of cognitive and motor symptoms, and the simultaneous-onset patients had shorter survival (mean, 19.2 months) than those with distinct cognitive or motor onset (mean, 28.6 months) (P = .005). CONCLUSIONS: Distinct patterns of survival profiles exist in patients with frontotemporal dementia and motor neuron disease, and overall survival may depend on the relative timing of the emergence of secondary symptoms.

Published
2009

21. A LRSAM1 mutation links Charcot-Marie-Tooth type 2 to Parkinson's disease

Author

Aerts, M.B., Weterman, M.A., Quadri, M., Schelhaas, H.J., Bloem, B.R., Esselink, R.A., Baas, F., Bonifati, V., Warrenburg, B.P.C. van de, Aerts, M.B., Weterman, M.A., Quadri, M., Schelhaas, H.J., Bloem, B.R., Esselink, R.A., Baas, F., Bonifati, V., and Warrenburg, B.P.C. van de

Abstract

Contains fulltext : 168294.pdf (publisher's version ) (Open Access), LRSAM1 mutations have been found in recessive and dominant forms of Charcot-Marie-Tooth disease. Within one generation of the original Dutch family in which the dominant LRSAM1 mutation was identified, three of the five affected family members have developed Parkinson's disease between ages 50 and 65 years, many years after neuropathy onset. We speculate that this late-onset parkinsonism is part of the LRSAM1 phenotype, thus associating a hitherto peripheral nerve disease with a central nervous system phenotype. How the mutated Lrsam1 protein, which normally has E3 ubiquitin ligase activity and is expressed in the nervous system, impacts on substantia nigra neurons is unclear.

Published
2016

22. Botulinum toxin-A injections vs radiotherapy for drooling in ALS

Author

Weikamp, J.G., Schinagl, D.A.X., Verstappen, C.C., Schelhaas, H.J., Swart, B.J.M. de, Kalf, J.G., Weikamp, J.G., Schinagl, D.A.X., Verstappen, C.C., Schelhaas, H.J., Swart, B.J.M. de, and Kalf, J.G.

Abstract

Item does not contain fulltext, OBJECTIVES: Botulinum neurotoxin (BoNT) injections in the salivary glands and radiotherapy (RT) on these glands are commonly used to alleviate severe drooling in patients with amyotrophic lateral sclerosis (ALS). This study compares BoNT type A with RT based on patient-rated evaluations. MATERIALS & METHODS: A prospective randomized controlled pilot study to compare RT (n = 10; on the parotid and the posterior part of the submandibular glands) with BoNT-A treatment (n = 10; in the parotid glands only, because of the risk of increasing oropharyngeal weakness) in patients with ALS. The primary outcome was the drooling status (burden of drooling), and our secondary interests were the degree of salivation, global change of drooling after treatment, and level of satisfaction with the treatment and negative experiences. RESULTS: There were no statistically significant between-treatment differences for the drooling status after treatment. Only at twelve weeks more saliva reduction was achieved by RT (P = 0.02). Patients treated with RT also described more transient negative experiences (like pain in mandible) directly after treatment. Subgroup analysis showed that patients with very severe dysphagia (no oral intake) were less satisfied and experienced a lower global change of drooling after treatment. CONCLUSIONS: This pilot study showed no significant difference in the burden of drooling between the treatments. However, with RT more saliva reduction was achieved, including negative experiences directly after treatment, but without the risk of decreasing oropharyngeal function. In addition, patients with very severe dysphagia do not seem to benefit from either treatment.

Published
2016

23. Tau Rather than TDP-43 Proteins are Potential Cerebrospinal Fluid Biomarkers for Frontotemporal Lobar Degeneration Subtypes: A Pilot Study

Author

Kuiperij, H.B., Versleijen, A.A., Beenes, M., Verwey, N.A., Benussi, L., Paterlini, A., Binetti, G., Teunissen, C.E., Raaphorst, J., Schelhaas, H.J., Kusters, B., Pijnenburg, Y.A.L., Ghidoni, R., Verbeek, M.M., Kuiperij, H.B., Versleijen, A.A., Beenes, M., Verwey, N.A., Benussi, L., Paterlini, A., Binetti, G., Teunissen, C.E., Raaphorst, J., Schelhaas, H.J., Kusters, B., Pijnenburg, Y.A.L., Ghidoni, R., and Verbeek, M.M.

Abstract

Item does not contain fulltext, BACKGROUND: Frontotemporal dementia (FTD) is a heterogeneous disease both at the clinical, genetic, and pathobiological level. The underlying pathological spectrum (termed FTLD, frontotemporal lobar degeneration) is in most cases defined by accumulation of either tau (FTLD-tau) or TDP-43 proteins (FTLD-TDP). Biomarkers to differentiate these subtypes are not yet available, whereas these are essential requirements to study the natural course of disease and for homogeneous inclusion of patients in clinical studies. OBJECTIVE: To study if a combination of total (t-) and phosphorylated (p-)tau, and t-TDP-43 and p-TDP-43 proteins in cerebrospinal fluid (CSF) is suitable to discriminate FTLD-tau and FTLD-TDP subtypes. METHODS: We developed immunoassays for the quantification of t-TDP-43 and p-TDP-43 proteins and used commercially available assays for the quantification of t-tau and p-tau proteins. We quantified these proteins in ventricular CSF samples from neuropathologically defined FTLD-tau and FTLD-TDP cases to study the reflection of underlying brain pathology in CSF composition, and in lumbar CSF samples from FTLD-tau and FTLD-TDP patients to study the diagnostic potential of CSF biomarkers. RESULTS: In ventricular CSF, t-TDP-43 and t-tau levels, when combined into one model, were significantly different between neuropathologically-defined FTLD-tau and FTLD-TDP cases. In a pilot study using lumbar CSF, the p-tau/t-tau ratio, but not t-TDP-43 levels, were significantly different between FTLD-TDP and FTLD-tau patients. CONCLUSION: We conclude that with current available methods, CSF tau, rather than TDP-43 proteins, may have diagnostic value in the differentiation of FTLD patients with either tau or TDP-43 pathology.

Published
2016

24. A LRSAM1 mutation links Charcot-Marie-Tooth type 2 to Parkinson's disease

Author

Aerts, M.B. (Marjolein B.), Weterman, M.A.J., Quadri, M. (Marialuisa), Schelhaas, H.J. (Helenius), Bloem, B.R. (Bastiaan), Esselink, R.A. (Rianne A.), Baas, F. (Frank), Bonifati, V. (Vincenzo), Warrenburg, B. (Bart) van de, Aerts, M.B. (Marjolein B.), Weterman, M.A.J., Quadri, M. (Marialuisa), Schelhaas, H.J. (Helenius), Bloem, B.R. (Bastiaan), Esselink, R.A. (Rianne A.), Baas, F. (Frank), Bonifati, V. (Vincenzo), and Warrenburg, B. (Bart) van de

Abstract

LRSAM1 mutations have been found in recessive and dominant forms of Charcot-Marie-Tooth disease. Within one generation of the original Dutch family in which the dominant LRSAM1 mutation was identified, three of the five affected family members have developed Parkinson's disease between ages 50 and 65 years, many years after neuropathy onset. We speculate that this late-onset parkinsonism is part of the LRSAM1 phenotype, thus associating a hitherto peripheral nerve disease with a central nervous system phenotype. How the mutated Lrsam1 protein, which normally has E3 ubiquitin ligase activity and is expressed in the nervous system, impacts on substantia nigra neurons is unclear.

Published
2016
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25. Letter: Recruitment of patients with both epilepsy and intellectual disability

Author

Mierlo, P. van, Snoeijen-Schouwenaars, F.M., Veendrick, M.J., Tan, I.Y., Willemsen, M.H., Schelhaas, H.J., Kleine, B.U., Mierlo, P. van, Snoeijen-Schouwenaars, F.M., Veendrick, M.J., Tan, I.Y., Willemsen, M.H., Schelhaas, H.J., and Kleine, B.U.

Abstract

Item does not contain fulltext

Published
2015

26. Autism and behavior in adult patients with Dravet syndrome (DS)

Author

Berkvens, J.J., Veugen, I., Veendrick-Meekes, M.J., Snoeijen-Schouwenaars, F.M., Schelhaas, H.J., Willemsen, M.H., Tan, I.Y., Aldenkamp, A.P., Berkvens, J.J., Veugen, I., Veendrick-Meekes, M.J., Snoeijen-Schouwenaars, F.M., Schelhaas, H.J., Willemsen, M.H., Tan, I.Y., and Aldenkamp, A.P.

Abstract

Item does not contain fulltext, INTRODUCTION: Autism and behavioral characteristics in adults with Dravet syndrome (DS) have rarely been systematically studied. METHOD: Three scales were used to assess the outcomes of DS in adulthood in terms of autism and behavior. All the adult patients with DS, nine male and four female, aged between 18 and 60years, living at the Epilepsy Center Kempenhaeghe in The Netherlands were included in the study. In addition, the past medical history of each patient was systematically screened for diagnoses like autism, Pervasive Development Disorder-Not Otherwise Specified (PDD-NOS), autism spectrum disorder (ASD), hyperactivity, Attention Deficit Hyperactivity Disorder (ADHD), and self-mutilation. Information concerning past and current use of psychoactive drugs was also evaluated. RESULTS: Eight patients (61.5%) were classified as having autism spectrum disorder (ASD) according to the AVZ-R or according to the medical record. Self-mutilation was seen in four patients (30.8%), hyperactivity in none. Three patients (23.1%) currently used psychoactive drugs. CONCLUSION: Autism spectrum disorders persist in adult patients with DS, while certain characteristics associated with behavioral problems, such as hyperactivity or use of psychoactive medication, seem to be less prominent than in childhood.

Published
2015

28. Cumulative effect of 5 daily sessions of theta burst stimulation on corticospinal excitability in amyotrophic lateral sclerosis

Author

Munneke, M., Rongen, J.J., Overeem, S., Schelhaas, H.J., Zwarts, M.J., Stegeman, D.F., Kinesiology, and Research Institute MOVE

Subjects
SDG 3 - Good Health and Well-being, DCN MP - Plasticity and memory, Quality of nursing and allied health care [NCEBP 6], parasitic diseases, DCN MP - Plasticity and memory NCEBP 4 - Quality of hospital and integrated care, Tissue engineering and pathology [NCMLS 3]
Abstract

Contains fulltext : 125297.pdf (Publisher’s version ) (Closed access) INTRODUCTION: Excitotoxicity plays an important role in the pathogenesis of the preferential motor neuron death observed in amyotrophic lateral sclerosis (ALS). Continuous theta burst stimulation (cTBS) by transcranial magnetic stimulation has an inhibitory effect on corticospinal excitability (CSE). We characterized the neurophysiological changes induced by cTBS in ALS. METHODS: The patients received 5 daily sessions of cTBS. CSE was assessed at baseline and after each session of cTBS. RESULTS: The amplitude of a single pulse motor evoked potential was significantly decreased (34%) over the days. The amplitude returned to baseline a week after the last session. The resting motor threshold increased significantly, whereas intracortical inhibition and facilitation did not change over the sessions. CONCLUSIONS: Daily cTBS has a cumulative depressing effect on CSE in patients with ALS. These results suggest that modulation of CSE in ALS is possible, but repetitive sessions are needed to maintain the effect.

Published
2013
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30. VAPB and C9orf72 mutations in 1 familial amyotrophic lateral sclerosis patient

Author

van Blitterswijk, M., Es, M.A. van, Koppers, M., van Rheenen, W., Medic, J., Schelhaas, H.J., van der Kooi, A.J., Visser, M. de, Veldink, J.H., and Berg, L.H. van den

Subjects
DCN MP - Plasticity and memory
Abstract

Item does not contain fulltext Previously, we have reported amyotrophic lateral sclerosis (ALS) families with multiple mutations in major ALS-associated genes. These findings provided evidence for an oligogenic basis of ALS. In our present study, we screened a cohort of 755 sporadic ALS patients, 111 familial ALS patients (97 families), and 765 control subjects of Dutch descent for mutations in vesicle-associated membrane protein B (VAPB). We have identified 1 novel VAPB mutation (p.V234I) in a familial ALS patient known to have a chromosome 9 open reading frame 72 (C9orf72) repeat expansion. This p.V234I mutation was absent in control subjects, located in a region with high evolutionary conservation, and predicted to have damaging effects. Taken together, these findings provide additional evidence for an oligogenic basis of ALS.

Published
2012

31. UNC13A is a modifier of survival in amyotrophic lateral sclerosis

Author

Diekstra, F.P., Vught, P.W. van, Rheenen, W. van, Koppers, M., Pasterkamp, R.J., Es, M.A. van, Schelhaas, H.J., Visser, M. de, Robberecht, W., Damme, P. van, Andersen, P.M., Berg, L.H. van den, and Veldink, J.H.

Subjects
DCN MP - Plasticity and memory
Abstract

Item does not contain fulltext A large genome-wide screen in patients with sporadic amyotrophic lateral sclerosis (ALS) showed that the common variant rs12608932 in gene UNC13A was associated with disease susceptibility. UNC13A regulates the release of neurotransmitters, including glutamate. Genetic risk factors that, in addition, modify survival, provide promising therapeutic targets in ALS, a disease whose etiology remains largely elusive. We examined whether UNC13A was associated with survival of ALS patients in a cohort of 450 sporadic ALS patients and 524 unaffected controls from a population-based study of ALS in The Netherlands. Additionally, survival data were collected from individuals of Dutch, Belgian, or Swedish descent (1767 cases, 1817 controls) who had participated in a previously published genome-wide association study of ALS. We related survival to rs12608932 genotype. In both cohorts, the minor allele of rs12608932 in UNC13A was not only associated with susceptibility but also with shorter survival of ALS patients. Our results further corroborate the role of UNC13A in ALS pathogenesis. 01 maart 2012

Published
2012

32. Mutations in KCND3 gene cause spinocerebellar ataxia type 19

Author

Duarri, A., Jezierska, J., Fokkens, M., Meijer, M., Schelhaas, H.J., Dunnen, W. den, van Dijk, F., Verschuuren-Bemelmans, C., Hageman, G., Van de Vlies, P., Kusters, B., Warrenburg, B.P.C. van de, Kremer, B., Wijmenga, C., Swertz, M.A., Kampinga, H.H., Boddeke, E., and Verbeek, D.S.

Subjects
DCN MP - Plasticity and memory, ONCOL 3 - Translational research DCN MP - Plasticity and memory
Abstract

Item does not contain fulltext

Published
2012

33. UBQLN2 in familial amyotrophic lateral sclerosis in The Netherlands

Author

Doormaal, P.T. van, Rheenen, W. van, Blitterswijk, M. van, Schellevis, R.D., Schelhaas, H.J., Visser, M. de, Kooi, A.J. van der, Veldink, J.H., and Berg, L.H. van den

Subjects
DCN MP - Plasticity and memory
Abstract

Item does not contain fulltext Recently it was discovered that mutations in the UBQLN2 gene were a cause of an X-linked dominant type of familial amyotrophic lateral sclerosis (ALS). We investigated the frequency of mutations in this gene in a cohort of 92 families with ALS in the Netherlands. Eight families were excluded because of male-to-male transmission. In the remaining 84 familial ALS cases no mutations were discovered in UBQLN2. Hence, UBQLN2 was not found to be a cause of familial ALS in the Netherlands. 01 september 2012

Published
2012

34. VCP mutations in familial and sporadic amyotrophic lateral sclerosis

Author

Koppers, M., Blitterswijk, M.M. van, Vlam, L., Rowicka, P.A., Vught, P.W. van, Groen, E.J., Spliet, W.G., Engelen-Lee, J. van, Schelhaas, H.J., Visser, M. de, Kooi, A.J. van der, Pol, W.L. van der, Pasterkamp, R.J., Veldink, J.H., and Berg, L.H. van den

Subjects
DCN MP - Plasticity and memory
Abstract

Item does not contain fulltext Mutations in the valosin-containing protein (VCP) gene were recently reported to be the cause of 1%-2% of familial amyotrophic lateral sclerosis (ALS) cases. VCP mutations are known to cause inclusion body myopathy (IBM) with Paget's disease (PDB) and frontotemporal dementia (FTD). The presence of VCP mutations in patients with sporadic ALS, sporadic ALS-FTD, and progressive muscular atrophy (PMA), a known clinical mimic of inclusion body myopathy, is not known. To determine the identity and frequency of VCP mutations we screened a cohort of 93 familial ALS, 754 sporadic ALS, 58 sporadic ALS-FTD, and 264 progressive muscular atrophy patients for mutations in the VCP gene. Two nonsynonymous mutations were detected; 1 known mutation (p.R159H) in a patient with familial ALS with several family members suffering from FTD, and 1 mutation (p.I114V) in a patient with sporadic ALS. Conservation analysis and protein prediction software indicate the p.I114V mutation to be a rare benign polymorphism. VCP mutations are a rare cause of familial ALS. The role of VCP mutations in sporadic ALS, if present, appears limited. 01 april 2012

Published
2012

35. Transcranial direct current stimulation does not modulate motor cortex excitability in patients with amyotrophic lateral sclerosis

Author

Munneke, M., Stegeman, D.F., Hengeveld, Y.A., Rongen, J.J., Schelhaas, H.J., Zwarts, M.J., Kinesiology, and Research Institute MOVE

Subjects
Functional Neurogenomics Quality of hospital and integrated care [DCN 2], SDG 3 - Good Health and Well-being, Quality of nursing and allied health care [NCEBP 6], Perception and Action [DCN 1], Functional Neurogenomics [DCN 2]
Abstract

Contains fulltext : 98484.pdf (Publisher’s version ) (Closed access) INTRODUCTION: Amyotrophic lateral sclerosis (ALS) is a progressive disease caused by the degeneration of upper and lower motor neurons. The etiology of ALS is unclear, but there is evidence that loss of cortical inhibition could be related to motor neuron degeneration. We sought to determine whether cathodal transcranial direct current stimulation (tDCS) can reduce cortical excitability in patients with ALS. METHODS: Three sessions of cathodal tDCS, lasting 7, 11, or 15 minutes, were performed in 10 patients and 10 healthy controls. Corticospinal excitability was measured before and after the tDCS. RESULTS: Cathodal tDCS induced a consistent decrease in corticospinal excitability in healthy controls, but not in ALS patients. CONCLUSIONS: The failure of tDCS to produce an excitability shift in the patients supports the potential diagnostic value of tDCS as a marker of upper motor neuron involvement. However, variation in corticospinal excitability measurements both inter- and intraindividually will limit its usefulness.

Published
2011
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36. Serum angiogenin levels are elevated in ALS, but not Parkinson's disease

Author

Es, M.A. van, Veldink, J.H., Schelhaas, H.J., Bloem, B.R., Sodaar, P., Nuenen, B.F.L. van, Verbeek, M.M., Warrenburg, B.P.C. van de, and Berg, L.H. van den

Subjects
Disorders of movement Donders Center for Medical Neuroscience [Radboudumc 3]
Abstract

Item does not contain fulltext

Published
2014

37. [Amyotrophic lateral sclerosis]

Author

Veldink, J.H., Weikamp, J.G., Schelhaas, H.J., and Berg, L.H. van den

Subjects
Functional Neurogenomics [DCN 2]
Abstract

Contains fulltext : 87415.pdf (Publisher’s version ) (Open Access) Amyotrophic lateral sclerosis is one of the most severe and disabling diseases of the nervous system. Amyotrophic lateral sclerosis leads to the progressive weakening of the muscles in the arms, legs, face, mouth and trunk. The onset of the disease is insidious, starting with weakness in the hands or feet or with slurred speech. The weakness worsens and patients pass away as a result of weakness of the respiratory muscles on average within 3 years of the onset of the disease. In the Netherlands, approximately 400 patients are diagnosed with amyotrophic lateral sclerosis every year. There is no diagnostic test for this neuro-muscular disease; the diagnosis is established by excluding other disorders that resemble amyotrophic lateral sclerosis. Only one drug is able to inhibit the progression of the disease to any extent: riluzole. Treatment, therefore, is mainly focused on supportive measures and those which enhance the quality of life optimally.

Published
2010

38. Age-related changes in motor unit number estimates in adult patients with Charcot-Marie-Tooth type 1A

Author

Dijk, J.P. van, Verhamme, C., Schaik, I.N. van, Schelhaas, H.J., Mans, E., Bour, L.J., Stegeman, D.F., Zwarts, M.J., Kinesiology, Research Institute MOVE, Amsterdam Neuroscience, Neurology, and Amsterdam institute for Infection and Immunity

Subjects
Functional Neurogenomics [DCN 2]
Abstract

Contains fulltext : 88007.pdf (Publisher’s version ) (Closed access) BACKGROUND: Charcot-Marie-Tooth disease type 1A (CMT1A) is known as a demyelinating hereditary neuropathy. Secondary axonal dysfunction is the most important determinant of disease severity. In adult patients, clinical progression may be because of further axonal deterioration as was shown with compound muscle action potential (CMAP) amplitude reductions over time. The motor unit number estimation (MUNE) technique may be more accurate to determine the number of axons as it is not disturbed by the effect of reinnervation. The purpose of this study was to investigate the number and size of motor units in relation to age in patients and controls. METHODS: In a cross-sectional design, we assessed arm and hand strength and performed electrophysiological examinations, including CMAP amplitudes and MUNE of the thenar muscles using high-density surface EMG in 69 adult patients with CMT1A and 55 age-matched healthy controls. RESULTS: In patients, lower CMAP amplitudes and MUNE values were related to hand weakness. The CMAP amplitude and MUNE value of the thenar muscles were significantly lower in patients than in controls. CMAP amplitudes declined with age in controls, but not in patients. MUNE values declined with age in both patients and controls. CONCLUSIONS: The age-dependent decrease in the number of motor units was not significantly different between patients with CMT1A and controls, indicating that loss of motor units in adult patients is limited. 01 augustus 2010

Published
2010
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39. First patho-anatomical investigation of the brain of a SCA19 patient

Author

Seidel, K., Kusters, B., Dunnen, W.F. den, Bouzrou, M., Hageman, G., Korf, H.W., Schelhaas, H.J., Verbeek, D., Rub, U., Seidel, K., Kusters, B., Dunnen, W.F. den, Bouzrou, M., Hageman, G., Korf, H.W., Schelhaas, H.J., Verbeek, D., and Rub, U.

Abstract

Item does not contain fulltext

Published
2014

40. Measuring and modulating the brain with non-invasive stimulation

Author

Stegeman, D.F., Schelhaas, H.J., Munneke, M.A.M., Stegeman, D.F., Schelhaas, H.J., and Munneke, M.A.M.

Abstract

Radboud Universiteit Nijmegen, 3 oktober 2014, Promotor : Stegeman, D.F. Co-promotor : Schelhaas, H.J., Contains fulltext : 130300.pdf (publisher's version ) (Open Access), The overall goal of the studies in this thesis was the use of non-invasive brain stimulation for measuring and modulating corticospinal excitability and to study the possibility of therapeutic modulation of excitability in some neurological disorders. Brain modulation to reduce the over-excitability of the primary motor cortex in ALS is the subject of the chapter 2 and chapter 3 in which transcranial direct current stimulation (tDCS) and theta burst stimulation (TBS), the latter as a specific form of repetitive transcranial magnetic stimulation (TMS), are used respectively. The effect of TBS over the cerebellum on freezing in patients with Parkinson’s disease is described in chapter 4. Chapter 5 reviews the first studies in literature using TMS as a biomarker in epilepsy. Chapter 6 shows that, in a brain computer interface mediated neurofeedback study, TMS can give “hard proof” on the effectiveness in changing brain excitability. The connectivity between the motor cortex and the muscular system is essential for several neurological disorders like the prediction of recovery after stroke. Any muscle response in a paralyzed muscle group after TMS signals the presence of a connection that might be relevant for the change of functional recovery. A guideline in optimization specifically the recording of electric muscle responses after TMS in the lower arm muscles is the subject of chapter 7.

Published
2014

41. Genome-wide association study identifies 19p13.3 (UNC13A) and 9p21.2 as susceptibility loci for sporadic amyotrophic lateral sclerosis

Author

Es, M.A. van, Veldink, J.H., Saris, C.G.J., Blauw, H.M., Vught, P.W. van, Birve, A., Lemmens, R., Schelhaas, H.J., Groen, E.J., Huisman, M.H., Kooi, A.J. van der, Visser, M. de, Dahlberg, C., Estrada, K., Rivadeneira, F., Hofman, A., Zwarts, M.J., Doormaal, P.T. van, Rujescu, D., Strengman, E., Giegling, I., Muglia, P., Tomik, B., Slowik, A., Uitterlinden, A.G., Hendrich, C., Waibel, S., Meyer, T., Ludolph, A.C., Glass, J.D., Purcell, S., Cichon, S., Nothen, Markus, Wichmann, H.E., Schreiber, S., Vermeulen, S., Kiemeney, L.A.L.M., Wokke, J.H.J., Cronin, S., McLaughlin, R.L., Hardiman, O., Fumoto, K., Pasterkamp, R.J., Meininger, V., Melki, J., Leigh, P.N., Shaw, C.E., Landers, J.E., Al-Chalabi, A., Brown Jr., R.H., Robberecht, W., Andersen, P.M., Ophoff, R.A., and Berg, L.H. van den

Abstract

We conducted a genome-wide association study among 2,323 individuals with sporadic amyotrophic lateral sclerosis (ALS) and 9,013 control subjects and evaluated all SNPs with P < 1.0 x 10(-4) in a second, independent cohort of 2,532 affected individuals and 5,940 controls. Analysis of the genome-wide data revealed genome-wide significance for one SNP, rs12608932, with P = 1.30 x 10(-9). This SNP showed robust replication in the second cohort (P = 1.86 x 10(-6)), and a combined analysis over the two stages yielded P = 2.53 x 10(-14). The rs12608932 SNP is located at 19p13.3 and maps to a haplotype block within the boundaries of UNC13A, which regulates the release of neurotransmitters such as glutamate at neuromuscular synapses. Follow-up of additional SNPs showed genome-wide significance for two further SNPs (rs2814707, with P = 7.45 x 10(-9), and rs3849942, with P = 1.01 x 10(-8)) in the combined analysis of both stages. These SNPs are located at chromosome 9p21.2, in a linkage region for familial ALS with frontotemporal dementia found previously in several large pedigrees.

Published
2009

43. Differentiation of hereditary spastic paraparesis from primary lateral sclerosis in sporadic adult-onset upper motor neuron syndromes

Author

Brugman, F., Veldink, J.H., Franssen, H., Visser, M. de, Jong, J.M. de, Faber, C.G., Kremer, H.P.H., Schelhaas, H.J., Doorn, P.A. van, Verschuuren, J.J., Bruyn, R.P.M., Kuks, J.B.M., Robberecht, W., Wokke, J.H.J., and Berg, L.H. van den

Subjects
Perception and Action [DCN 1]
Abstract

Contains fulltext : 80492.pdf (Publisher’s version ) (Closed access) OBJECTIVE: To study whether clinical characteristics can differentiate sporadic presentations of hereditary spastic paraparesis (HSP) from primary lateral sclerosis (PLS). Differentiation between these diseases is important for genetic counseling and prognostication. DESIGN: Case series. SETTING: Tertiary referral center. PATIENTS: One hundred four Dutch patients with an adult-onset, sporadic upper motor neuron syndrome of at least 3 years' duration. Hereditary spastic paraparesis was genetically confirmed in 14 patients (7 with SPG4 and 7 with SPG7 mutations). RESULTS: All 14 patients with the SPG4 or SPG7 mutation had symptom onset in the legs, and 1 of the patients with the SPG7 mutation also developed symptoms in the arms. Of the other 90 patients, 78 (87%) had symptom onset in the legs. Thirty-six patients developed a PLS phenotype (bulbar region involvement), 15 had a phenotype that was difficult to classify as similar to HSP or PLS (involvement of legs and arms only), and 39 continued to have a phenotype similar to typical HSP (involvement of the legs only). Median age at onset was lower in patients with the SPG4 or SPG7 mutation (39 [range, 29-69] years), but there was considerable overlap with patients with the PLS phenotype (52 [range, 32-76] years). No differences were found in the features used by previous studies to distinguish HSP from PLS, including evidence of mild dorsal column impairment (decreased vibratory sense or abnormal leg somatosensory evoked potentials), symptoms of urinary urgency, or mild electromyographic abnormalities. CONCLUSIONS: In most patients with a sporadic adult-onset upper motor neuron syndrome, differentiation of sporadic presentations of HSP from PLS based on clinical characteristics is unreliable and therefore depends on results of genetic testing.

Published
2009

44. Hereditaire spatische paraparesen: stand van zaken en leidraad voor genetisch onderzoek

Author

Bot, S.T. de, Scheffer, H., Schelhaas, H.J., Knoers, N.V.A.M., Willemsen, M.A.A.P., Warrenburg, B.P.C. van de, and Kremer, H.P.H.

Subjects
Genomic disorders and inherited multi-system disorders [IGMD 3], Perception and Action [DCN 1], Membrane transport and intracellular motility [NCMLS 5], Neuroinformatics [DCN 3], GeneralLiterature_REFERENCE(e.g.,dictionaries,encyclopedias,glossaries)
Abstract

Contains fulltext : 80567.pdf (Publisher’s version ) (Open Access)

Published
2009

46. Rise and fall of skeletal muscle size over the entire life span

Author

Arts, I.M.P., Pillen, S., Overeem, S., Schelhaas, H.J., and Zwarts, M.J.

Subjects
Perception and Action [DCN 1], Functional Neurogenomics [DCN 2], Neuromuscular development and genetic disorders [UMCN 3.1]
Abstract

Contains fulltext : 51752.pdf (Publisher’s version ) (Closed access)

Published
2007

47. [Turning the head, an unusual mechanism to compensate for diplopia caused by abduction restriction of one eye]

Author

Kappelle, A.C., Schelhaas, H.J., Pasman, J.W., and Bloem, B.R.

Subjects
genetic structures, Cognitive neurosciences [UMCN 3.2], eye diseases
Abstract

Contains fulltext : 58909.pdf (Publisher’s version ) (Closed access) A 59-year-old-man visited the neurological outpatient clinic because of a leftward rotation of his head for the last 8 months. This head deviation turned out to represent a compensatory mechanism to alleviate diplopia that resulted from an abduction restriction of his left eye. By turning his head into the direction of the weak left lateral rectus muscle, the patient could fixate both eyes on target and maintain binocular vision.

Published
2004

48. Is the Frontal Assessment Battery reliable in ALS patients?

Author

Raaphorst, J., Beeldman, E., Jaeger, B., Schmand, B.A., Berg, L.H. van den, Weikamp, J.G., Schelhaas, H.J., Visser, M. de, Haan, R.J. de, Raaphorst, J., Beeldman, E., Jaeger, B., Schmand, B.A., Berg, L.H. van den, Weikamp, J.G., Schelhaas, H.J., Visser, M. de, and Haan, R.J. de

Abstract

Item does not contain fulltext, The assessment of frontal functions in ALS patients is important because of the overlap with the behavioural variant of frontotemporal dementia (bvFTD). We investigated the applicability and reliability of the Frontal Assessment Battery (FAB) within a cohort of predominantly prevalent ALS patients. The FAB was administered to 85 ALS patients and eight ALS-bvFTD patients. Original scores and the percentage of items that could be performed were recorded. Item-adjusted scores of the FAB were calculated. The ALS Functional Rating Scale-Revised version (ALSFRS-R) was used to assess disease severity. Eighty-seven patients (94%) had ALS symptoms of more than one year. Twenty patients (21.5%) were not able to perform one or more FAB items. The original FAB score correlated with the ALSFRS-R score (r = 0.30; p < 0.01), while the item-adjusted FAB score did not. In contrast to the original FAB scores, the item-adjusted FAB score was lower in ALS-bvFTD patients (66.7, range 33.3-100) compared to ALS patients without bvFTD (94.4, range 38.9-100; p < 0.01). In summary, 20% of prevalent ALS patients could not complete the FAB, which limits its use in ALS and emphasizes the importance of disease specific instruments and adjusting for motor impairment in cognitive and behavioural examinations of ALS patients.

Published
2013

49. Mutations in BICD2, which encodes a Golgin and Important Motor Adaptor, Cause Congenital Autosomal-Dominant Spinal Muscular Atrophy

Author

Neveling, K., Martinez-Carrera, L., Hölker, I., Heister, A., Verrips, A., Hosseini-Barkooie, S.M., Gilissen, C.F.H.A., Vermeer, S., Pennings, M.C.P., Meijer, R., Riele, M.G.E. te, Frijns, C.J., Suchowersky, O., MacLaren, L., Rudnik-Schöneborn, S., Sinke, R.J., Zerres, K., Lowry, R.B., Lemmink, H.H., Garbes, L., Veltman, J.A., Schelhaas, H.J., Scheffer, H., Wirth, B., Neveling, K., Martinez-Carrera, L., Hölker, I., Heister, A., Verrips, A., Hosseini-Barkooie, S.M., Gilissen, C.F.H.A., Vermeer, S., Pennings, M.C.P., Meijer, R., Riele, M.G.E. te, Frijns, C.J., Suchowersky, O., MacLaren, L., Rudnik-Schöneborn, S., Sinke, R.J., Zerres, K., Lowry, R.B., Lemmink, H.H., Garbes, L., Veltman, J.A., Schelhaas, H.J., Scheffer, H., and Wirth, B.

Abstract

Contains fulltext : 116576.pdf (publisher's version ) (Closed access)

Published
2013

50. Rapidly deteriorating course in Dutch hereditary spastic paraplegia type 11 patients

Author

Bot, S.T. de, Burggraaff, R.C., Herkert, J.C., Schelhaas, H.J., Post, B., Diekstra, A., Vliet, R.O. van, Knaap, M.S. van der, Kamsteeg, E.J., Scheffer, H., Warrenburg, B.P.C. van de, Verschuuren-Bemelmans, C.C., Kremer, H.P.H., Bot, S.T. de, Burggraaff, R.C., Herkert, J.C., Schelhaas, H.J., Post, B., Diekstra, A., Vliet, R.O. van, Knaap, M.S. van der, Kamsteeg, E.J., Scheffer, H., Warrenburg, B.P.C. van de, Verschuuren-Bemelmans, C.C., and Kremer, H.P.H.

Abstract

Item does not contain fulltext, Although SPG11 is the most common complicated hereditary spastic paraplegia, our knowledge of the long-term prognosis and life expectancy is limited. We therefore studied the disease course of all patients with a proven SPG11 mutation as tested in our laboratory, the single Dutch laboratory providing SPG11 mutation analysis, between 1 January 2009 and 1 January 2011. We identified nine different SPG11 mutations, four of which are novel, in nine index patients. Eighteen SPG11 patients from these nine families were studied by means of a retrospective chart analysis and additional interview/examination. Ages at onset were between 4 months and 14 years; 39% started with learning difficulties rather than gait impairment. Brain magnetic resonance imaging showed a thin corpus callosum and typical periventricular white matter changes in the frontal horn region (known as the 'ears-of the lynx'-sign) in all. Most patients became wheelchair bound after a disease duration of 1 to 2 decades. End-stage disease consisted of loss of spontaneous speech, severe dysphagia, spastic tetraplegia with peripheral nerve involvement and contractures. Several patients died of complications between ages 30 and 48 years, 3-4 decades after onset of gait impairment. Other relevant features during the disease were urinary and fecal incontinence, obesity and psychosis. Our study of 18 Dutch SPG11-patients shows the potential serious long-term consequences of SPG11 including a possibly restricted life span.

Published
2013

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