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243 results on '"Hennekam, R.C.M."'

3. Distinctive pattern of temporal atrophy in patients with frontotemporal dementia and the I383V variant in TARDBP

Author

Mol, M.O., Nijmeijer, S.W.R. (Sebastiaan W.R.), Rooij, J.G.J. (Jeroen) van, Van Spaendonk, R.M.L. (Resie M. L.), Pijnenburg, Y.A.L. (Yolande), Lee, S.J. (Sven) van der, Thornton, A.S. (Andrew), Donker Kaat, L. (Laura), Rozemuller, A.J.M. (Annemieke), Janse Van Mantgem, M.R. (Mark R.), Rheenen, W. (Wouter) van, Estrada Gil, K. (Karol), Veldink, J.H. (Jan), Hennekam, R.C.M. (Raoul), Vernooij, M.W. (Meike), Swieten, J.C. (John) van, Cohn-Hokke, P.E. (P.), Seelaar, H. (Harro), Dopper, E.G.P. (Elise), Mol, M.O., Nijmeijer, S.W.R. (Sebastiaan W.R.), Rooij, J.G.J. (Jeroen) van, Van Spaendonk, R.M.L. (Resie M. L.), Pijnenburg, Y.A.L. (Yolande), Lee, S.J. (Sven) van der, Thornton, A.S. (Andrew), Donker Kaat, L. (Laura), Rozemuller, A.J.M. (Annemieke), Janse Van Mantgem, M.R. (Mark R.), Rheenen, W. (Wouter) van, Estrada Gil, K. (Karol), Veldink, J.H. (Jan), Hennekam, R.C.M. (Raoul), Vernooij, M.W. (Meike), Swieten, J.C. (John) van, Cohn-Hokke, P.E. (P.), Seelaar, H. (Harro), and Dopper, E.G.P. (Elise)

Abstract

Introduction Frontotemporal dementia (FTD) and amyotrophic lateral sclerosis (ALS) are closely related disorders, linked pathologically and ge

Published
2020
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4. Primrose syndrome: Characterization of the phenotype in 42 patients

Author

Melis, D.A.M. (Danielle), Carvalho, D. (Daniel), Barbaro-Dieber, T. (Tina), Espay, A.J. (Alberto J.), Gambello, M.J. (Michael J.), Gener, B. (Blanca), Gerkes, E.H. (Erica H), Hitzert, M.M. (Marrit M.), Hove, H.B. (Hanne B.), Jansen, S. (Sandra), Jira, P.E. (Petr), Lachlan, K. (Katherine), Menke, L.A. (Leonie), Narayanan, V. (Vinodh), Ortiz, D. (Damara), Overwater, E. (Eline), Posmyk, R. (Renata), Ramsey, K. (Keri), Rossi, A. (Alessandro), Sandoval, R.L. (Renata Lazari), Stumpel, C. (Connie), Stuurman, K.E. (Kyra), Cordeddu, V. (Viviana), Turnpenny, P. (Peter), Strisciuglio, P. (Pietro), Tartaglia, M. (Marco), Unger, S. (Sheela), Waters, T. (Todd), Turnbull, C. (Clare), Hennekam, R.C.M. (Raoul), Melis, D.A.M. (Danielle), Carvalho, D. (Daniel), Barbaro-Dieber, T. (Tina), Espay, A.J. (Alberto J.), Gambello, M.J. (Michael J.), Gener, B. (Blanca), Gerkes, E.H. (Erica H), Hitzert, M.M. (Marrit M.), Hove, H.B. (Hanne B.), Jansen, S. (Sandra), Jira, P.E. (Petr), Lachlan, K. (Katherine), Menke, L.A. (Leonie), Narayanan, V. (Vinodh), Ortiz, D. (Damara), Overwater, E. (Eline), Posmyk, R. (Renata), Ramsey, K. (Keri), Rossi, A. (Alessandro), Sandoval, R.L. (Renata Lazari), Stumpel, C. (Connie), Stuurman, K.E. (Kyra), Cordeddu, V. (Viviana), Turnpenny, P. (Peter), Strisciuglio, P. (Pietro), Tartaglia, M. (Marco), Unger, S. (Sheela), Waters, T. (Todd), Turnbull, C. (Clare), and Hennekam, R.C.M. (Raoul)

Abstract

Primrose syndrome (PS; MIM# 259050) is characterized by intellectual disability (ID), macrocephaly, unusual facial features (frontal bossing, deeply set eyes, down-slanting palpebral fissures), calcified external ears, sparse body hair and distal muscle wasting. The syndrome is caused by de novo heterozygous missense variants in ZBTB20. Most of the 29 published patients are adults as characteristics appear more recognizable with age. We present 13 hitherto unpublished individuals and summarize the clinical and molecular findings in all 42 patients. Several signs and symptoms of PS develop during childhood, but the cardinal features, such as calcification of the external ears, cystic bone lesions

Published
2020
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7. Novel and recurrent TRPV4 mutations and their association with distinct phenotypes within the TRPV4 dysplasia family

Author

Dai, J., Kim, O.-H., Cho, T.-J., Schmidt-Rimpler, M., Tonoki, H., Takikawa, K., Haga, N., Miyoshi, K., Kitoh, H., Yoo, W.-J., Choi, I.-H., Song, H.-R., Jin, D.-K., Kim, H.-T., Kamasaki, H., Bianchi, P., Grigelioniene, G., Nampoothiri, S., Minagawa, M., Miyagawa, S.-i., Fukao, T., Marcelis, C., Jansweijer, M.C.E., Hennekam, R.C.M., Bedeschi, F., Mustonen, A., Jiang, Q., Ohashi, H., Furuichi, T., Unger, S., Zabel, B., Lausch, E., Superti-Furga, A., Nishimura, G., and Ikegawa, S.

Subjects
Gene mutations -- Research, Dysplasia -- Genetic aspects, Dysplasia -- Development and progression, Dysplasia -- Research, Bones -- Abnormalities, Bones -- Genetic aspects, Bones -- Development and progression, Bones -- Research, Health
Published
2010

8. Phenotypic variability in 49 cases of ESCO2 mutations, including novel missense and codon deletion in the acetyltransferase domain, correlates with ESCO2 expression and establishes the clinical criteria for Roberts syndrome

Author

Vega, H., Trainer, A.H., Gordillo, M., Crosier, M., Kayserili, H., Skovby, F., Giovannucci Uzielli, M.L., Schnur, R.E., Manouvrier, S., Blair, E., Hurst, J.A., Forzano, F., Meins, M., Simola, K.O.J., Raas-Rothschild, A., Hennekam, R.C.M., and Jabs, E. Wang

Subjects
Gene mutations -- Research, Chromosome deletion -- Research, Ectromelia -- Genetic aspects, Ectromelia -- Research, Health
Published
2010

9. Clinical spectrum of SIX3-associated mutations in holoprosencephaly: correlation between genotype, phenotype and function

Author

Lacbawan, F., Solomon, B.D., Roessler, E., El-Jaick, K., Domene, S., Velez, J.I., Zhou, N., Hadley, D., Balog, J.Z., Long, R., Fryer, A., Smith, W., Omar, S., McLean, S.D., Clarkson, K., Lichty, A., Clegg, N.J., Delgado, M.R., Levey, E., Stashinko, E., Potocki, L., VanAllen, M.I., Clayton-Smith, J., Donnai, D., Bianchi, D.W., Juliusson, P.B., Njolstad, P.R., Brunner, H.G., Carey, J.C., Hehr, U., Musebeck, J., Wieacker, P.F., Postra, A., Hennekam, R.C.M., van den Boogaard, M.-J.H., van Haeringen, A., Paulussen, A., Herbergs, J., Schrander-Stumpel, C.T.R.M., Janecke, A.R., Chitayat, D., Hahn, J., McDonald-McGinn, D.M., Zackai, E.H., Dobyns, W.B., and Muenke, M.

Subjects
Holoprosencephaly -- Genetic aspects, Holoprosencephaly -- Research, Holoprosencephaly -- Development and progression, Gene mutations -- Research, Animal models in research -- Usage, Health
Published
2009

11. Multiple tumors due to mosaic genome-wide paternal uniparental disomy

Author

Postema, FAM, Bliek, J, van Noesel, C.J.M., van Zutven, L., Oosterwijk, J.C. (Jan), Hopman, S.M.J. (Saskia), Merks, J.H.M. (Johannes), Hennekam, R.C.M. (Raoul), Postema, FAM, Bliek, J, van Noesel, C.J.M., van Zutven, L., Oosterwijk, J.C. (Jan), Hopman, S.M.J. (Saskia), Merks, J.H.M. (Johannes), and Hennekam, R.C.M. (Raoul)

Abstract

Mosaic genome-wide paternal uniparental disomy is an infrequently described disorder in which affected individuals have signs and symptoms that may resemble Beckwith–Wiedemann syndrome. In addition, they can develop multiple benign and malignant tumors throughout life. Routine molecular diagnostics may not detect the (characteristic) low level of mosaicism, and the diagnosis is likely to be missed. Genetic counseling and a life-long alertness for the development of tumors is indicated. We describe the long diagnostic process of a patient who already had a tumor at birth and developed multiple tumors in childhood and adulthood. Furthermore, we offer clues to recognize the entity

Published
2019
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12. Diagnosis and management in Pitt-Hopkins syndrome: First international consensus statement

Author

Zollino, M., Zweier, C., Balkom, I.D.C. van, Sweetser, D.A., Alaimo, J., Bijlsma, E.K., Deckers, S.R.J.M., Balkom, L.J.M. van, Whalen, S., Hennekam, R.C.M., Zollino, M., Zweier, C., Balkom, I.D.C. van, Sweetser, D.A., Alaimo, J., Bijlsma, E.K., Deckers, S.R.J.M., Balkom, L.J.M. van, Whalen, S., and Hennekam, R.C.M.

Abstract

Item does not contain fulltext, Pitt-Hopkins syndrome (PTHS) is a neurodevelopmental disorder characterized by intellectual disability, specific facial features, and marked autonomic nervous system dysfunction, especially with disturbances of regulating respiration and intestinal mobility. It is caused by variants in the transcription factor TCF4. Heterogeneity in the clinical and molecular diagnostic criteria and care practices have prompted a group of international experts to establish guidelines for diagnostics and care. For issues, for which there was limited information available in international literature, we collaborated with national support groups and the participants of a syndrome specific international conference to obtain further information. Here, we discuss the resultant consensus, including the clinical definition of PTHS and a molecular diagnostic pathway. Recommendations for managing particular health problems such as dysregulated respiration are provided. We emphasize the need for integration of care for physical and behavioral issues. The recommendations as presented here will need to be evaluated for improvements to allow for continued optimization of diagnostics and care.

Published
2019

14. Congenital abnormalities reported in Pelger-Huet homozygosity as compared to Greenberg/HEM dysplasia: highly variable expression of allelic phenotypes

Author

Oosterwijk, J.C., Mansour, S., van Noort, G., Waterham, H.R., Hall, C.M., and Hennekam, R.C.M.

Subjects
Leukocytes -- Abnormalities -- Research, Health, Research, Abnormalities
Abstract

In 1928 the Dutch physician Pelger described two patients with a morphological abnormality of leukocytes that consisted of hypolobulation of the nuclei: there were two lobes instead of the usual [...]

Published
2003

15. Short-limbed dwarfism with bowing, combined immune deficiency, and late onset aplastic anaemia caused by novel mutations in the RMPR gene

Author

Kuijpers, T.W., Ridanpaa, M., Peters, M., De Boer, I., Vossen, J.M.J.J., Pals, S.T., Kaitila, I., and Hennekam, R.C.M.

Subjects
Gene mutations -- Physiological aspects -- Health aspects -- Research -- Analysis -- Genetic aspects, Genetic research -- Analysis -- Physiological aspects -- Genetic aspects -- Health aspects, Dysplasia -- Health aspects -- Genetic aspects -- Complications and side effects -- Research, Medical genetics -- Research -- Health aspects -- Analysis -- Physiological aspects, Dwarfism -- Genetic aspects -- Health aspects -- Causes of -- Research -- Complications and side effects, Health
Abstract

J Med Genet 2003;40:761-766 Kyphomelic dysplasia has been described as a generalised skeletal dysplasia characterised by a disproportionate growth, bowing of long bones, mild facial dysmorphia, and normal intelligence, with [...]

Published
2003

16. Prospective screening for subtelomeric rearrangements in children with mental retardation of unknown aetiology: the Amsterdam experience. (Original Article)

Author

Karnebeek, C.D.M. van, Koevoets, C., Sluijter, S., Bijlsma, E.K., Smeets, D.F.M.C., Redeker, E.J., Hennekam, R.C.M., and Hoovers, J.M.N.

Subjects
Genetic disorders -- Research, Mental retardation -- Causes of -- Research, Health, Research, Causes of
Abstract

Objective: The frequency of subtelomeric rearrangements in patients with unexplained mental retardation (MR) is uncertain, as most studies have been retrospective and case retrieval may have been biased towards cases [...]

Published
2002

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

Author

Karnebeek, C.D.M. van, Gelderen, I. van, Nijhof, G.J., Abeling, N.G., Vreken, P., Redeker, E.J., Eeghen, A.M. van, Hoovers, J.M.N., and Hennekam, R.C.M.

Subjects
Health
Abstract

Autism is a chronic and severe neuropsychiatric disorder with an early onset, characterised by qualitative impairments of social interaction, deviant development of language and other communicative skills, delayed cognitive development, [...]

Published
2002

21. Mutations in IRS4 are associated with central hypothyroidism

Author

Heinen, C.A. (Charlotte A.), De Vries, E.M. (Emmely M.), Alders, M. (Mariëlle), Bikker, H. (Hennie), Zwaveling-Soonawala, N. (Nitash), Akker, E.L.T. (Erica) van den, Bakker, B. (Boudewijn), Hoorweg-Nijman, J.J.G. (Gera), Roelfsema, F. (Ferdinand), Hennekam, R.C.M. (Raoul), Boelen, A. (Anita), Trotsenburg, A.S.P. (Paul) van, Fliers, E. (Eric), Heinen, C.A. (Charlotte A.), De Vries, E.M. (Emmely M.), Alders, M. (Mariëlle), Bikker, H. (Hennie), Zwaveling-Soonawala, N. (Nitash), Akker, E.L.T. (Erica) van den, Bakker, B. (Boudewijn), Hoorweg-Nijman, J.J.G. (Gera), Roelfsema, F. (Ferdinand), Hennekam, R.C.M. (Raoul), Boelen, A. (Anita), Trotsenburg, A.S.P. (Paul) van, and Fliers, E. (Eric)

Abstract

Background: Four genetic causes of isolated congenital central hypothyroidism (CeH) have been identified, but many cases remain unexplained. We hypothesised the existence of other genetic causes of CeH with a Mendelian inheritance pattern. Methods: We performed exome sequencing in two families with unexplained isolated CeH and subsequently Sanger sequenced unrelated idiopathic CeH cases. We performed clinical and biochemical characterisation of the probands and carriers identified by family screening. We investigated IRS4 mRNA expression in human hypothalamus and pituitary tissue, and measured serum thyroid hormones and Trh and Tshb mRNA expression in hypothalamus and pituitary tissue of Irs4 knockout mice. Results: We found mutations in the insulin receptor substrate 4 (IRS4) gene in two pairs of brothers with CeH (one nonsense, one frameshift). Sequencing of IRS4 in 12 unrelated CeH cases negative for variants in known genes yielded three frameshift mutation

Published
2018
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24. Phenotypes and genotypes in individuals with SMC1A variants

Author

Huisman, S.A. (Sylvia), Mulder, P.A. (Paul A.), Redeker, E.J.W. (Egbert), Bader, I. (Ingrid), Bisgaard, A.-M. (Anne-Marie), Brooks, A.S. (Alice), Cereda, A., Cinca, C. (Constanza), Clark, D. (Dinah), Cormier-Daire, V. (Valerie), Deardorff, M.A. (Matthew), Diderich, K.E.M. (Karin), Elting, M. (Mariet), Essen, J.A. (Anthonie) van, Fitzpatrick, D.R. (David R.), Gervasini, C., Gillessen-Kaesbach, G. (Gabriele), Girisha, K.M. (Katta M), Hilhorst-Hofstee, Y. (Yvonne), Hopman, S.M.J. (Saskia), Horn, D. (Denise), Isrie, M. (Mala), Jansen, S. (Sandra), Jespersgaard, C. (Cathrine), Kaiser, F.J. (Frank), Kaur, M. (Maninder), Kleefstra, T. (Tjitske), Krantz, D.H. (David), Lakeman, P. (Phillis), Landlust, A. (Annemiek), Lessel, D. (Davor), Michot, C. (Caroline), Moss, J. (Jo), Noon, S.E. (Sarah E.), Oliver, C. (Chris), Parenti, I., Pie, J. (Juan), Ramos, F.J., Rieubland, C. (Claudine), Russo, S. (Sascha), Selicorni, A. (Angelo), Tümer, Z., Vorstenbosch, R. (Rieneke), Wenger, T.L. (Tara L.), van Balkom, I. (Ingrid), Piening, S. (Sigrid), Wierzba, J. (Jolanta), Hennekam, R.C.M. (Raoul), Huisman, S.A. (Sylvia), Mulder, P.A. (Paul A.), Redeker, E.J.W. (Egbert), Bader, I. (Ingrid), Bisgaard, A.-M. (Anne-Marie), Brooks, A.S. (Alice), Cereda, A., Cinca, C. (Constanza), Clark, D. (Dinah), Cormier-Daire, V. (Valerie), Deardorff, M.A. (Matthew), Diderich, K.E.M. (Karin), Elting, M. (Mariet), Essen, J.A. (Anthonie) van, Fitzpatrick, D.R. (David R.), Gervasini, C., Gillessen-Kaesbach, G. (Gabriele), Girisha, K.M. (Katta M), Hilhorst-Hofstee, Y. (Yvonne), Hopman, S.M.J. (Saskia), Horn, D. (Denise), Isrie, M. (Mala), Jansen, S. (Sandra), Jespersgaard, C. (Cathrine), Kaiser, F.J. (Frank), Kaur, M. (Maninder), Kleefstra, T. (Tjitske), Krantz, D.H. (David), Lakeman, P. (Phillis), Landlust, A. (Annemiek), Lessel, D. (Davor), Michot, C. (Caroline), Moss, J. (Jo), Noon, S.E. (Sarah E.), Oliver, C. (Chris), Parenti, I., Pie, J. (Juan), Ramos, F.J., Rieubland, C. (Claudine), Russo, S. (Sascha), Selicorni, A. (Angelo), Tümer, Z., Vorstenbosch, R. (Rieneke), Wenger, T.L. (Tara L.), van Balkom, I. (Ingrid), Piening, S. (Sigrid), Wierzba, J. (Jolanta), and Hennekam, R.C.M. (Raoul)

Abstract

SMC1A encodes one of the proteins of the cohesin complex. SMC1A variants are known to cause a phenotype resembling Cornelia de Lange syndrome (CdLS). Exome sequencing has allowed recognizing SMC1A variants in individuals with encephalopathy with epilepsy who do not resemble CdLS. We performed an international, interdisciplinary study on 51 individuals with SMC1A variants for physical and behavioral characteristics, and compare results to those in 67 individuals with NIPBL variants. For the Netherlands all known individuals with SMC1A variants were studied, both with and without CdLS phenotype. Individuals with SMC1A variants can resemble CdLS, but manifestations are less marked compared to individuals with NIPBL variants: growth is less disturbed, facial signs are less marked (except for periocular signs and thin upper vermillion), there are no major limb anomalies, and they have a higher level of cognitive and adaptive functioning. Self-injurious behavior is more frequent and more severe in the NIPBL group. In the Dutch group 5 of 13 individuals (all females) had a phenotype that shows a remarkable resemblance to Rett syndrome: epileptic encephalopathy, severe or profound intellectual disability, stereotypic movements, and (in some) regression. Their missense, nonsense, and frameshift mutations are evenly spread over the gene. We conclude that SMC1A variants can result in a phenotype resembling CdLS and a phenotype resembling Rett syndrome. Resemblances between the SMC1A group and the NIPBL group suggest that a disturbed cohesin function contributes to the phenotype, but differences between these groups may also be explained by other underlying mechanisms such as moonlighting of the cohesin genes.

Published
2017
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25. Validation of a clinical screening instrument for tumour predisposition syndromes in patients with childhood cancer (TuPS): Protocol for a prospective, observational, multicentre study

Author

Postema, F.A.M. (Floor A. M.), Hopman, S.M.J. (Saskia), Borgie, C.A. (Corianne) de, Hammond, P. (Peter), Hennekam, R.C.M. (Raoul), Merks, J.H.M. (Johannes), Aalfs, C.M. (Cora), Anninga, J.K. (Jakob K.), Berger, L.P.V. (Lieke P.V.), Bleeker, F.E. (Fonnet), Bont, E.S.J.M. (Eveline) de, Dommering, C.J. (Charlotte), Van Eijkelenburg, N.K.A. (Natasha K.A.), Heuvel-Eibrink, M.M. (Marry) van den, Jongmans, M.C.J. (Marjolijn), Kors, W.A. (W.), Letteboer, T.G.W. (Tom), Loeffen, J. (Jan), Olderode-Berends, M. (Maran), Wagner, A. (Anja), Postema, F.A.M. (Floor A. M.), Hopman, S.M.J. (Saskia), Borgie, C.A. (Corianne) de, Hammond, P. (Peter), Hennekam, R.C.M. (Raoul), Merks, J.H.M. (Johannes), Aalfs, C.M. (Cora), Anninga, J.K. (Jakob K.), Berger, L.P.V. (Lieke P.V.), Bleeker, F.E. (Fonnet), Bont, E.S.J.M. (Eveline) de, Dommering, C.J. (Charlotte), Van Eijkelenburg, N.K.A. (Natasha K.A.), Heuvel-Eibrink, M.M. (Marry) van den, Jongmans, M.C.J. (Marjolijn), Kors, W.A. (W.), Letteboer, T.G.W. (Tom), Loeffen, J. (Jan), Olderode-Berends, M. (Maran), and Wagner, A. (Anja)

Abstract

Introduction: Recognising a tumour predisposition syndrome (TPS) in patients with childhood cancer is of significant clinical relevance, as it affects treatment, prognosis and facilitates genetic counselling. Previous studies revealed that only half of the known TPSs are recognised during standard paediatric cancer care. In current medical practice it is impossible to refer every patient with childhood cancer to a clinical geneticist, due to limited capacity for routine genetic consultation. Therefore, we have developed a screening instrument to identify patients with childhood cancer with a high probability of having a TPS. The aim of this study is to validate the clinical screening instrument for TPS in patients with childhood cancer. Methods and analysis: This study is a prospective nationwide cohort study including all newly diagnosed patients with childhood cancer in the Netherlands. The screening instrument consists of a checklist, two- and three-dimensional photographic series of the patient. 2 independent clinical geneticists will assess the content of the screening instrument. If a TPS is suspected based on the instrument data and thus further evaluation is indicated, the patient will be invited for full genetic consultation. A negative control group consists of 20% of the patients in whom a TPS is not suspected based on the instrument; they will be randomly invited for full genetic consultation. Primary outcome measurement will be sensitivity of the instrument. Ethics and dissemination: The Medical Ethical Committee of the Academic Medical Centre stated that the Medical Research Involving Human Subjects Act does not apply to this study and that official approval of this study by the Committee was not required. The results will be offered for publication in peer-reviewed journals and presented at International Conferences on Oncology and Clinical Genetics. The clinical data gathered in this study will be available for all participating centres.

Published
2017
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26. CREBBP mutations in individuals without Rubinstein-Taybi syndrome phenotype

Author

Menke, L.A., Belzen, M.J. van, Alders, M., Cristofoli, F., Ehmke, N., Fergelot, P., Foster, A., Gerkes, E.H., Hoffer, M.J.V., Horn, D., Kant, S.G., Lacombe, D., Leon, E., Maas, S.M., Melis, D., Muto, V., Park, S.M., Peeters, H., Peters, D.J.M., Pfundt, R., Ravenswaaij-Arts, C.M.A. van, Tartaglia, M., Hennekam, R.C.M., DDD Study, Clinical Cognitive Neuropsychiatry Research Program (CCNP), ANS - Complex Trait Genetics, Paediatric Genetics, ACS - Amsterdam Cardiovascular Sciences, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, Other Research, Human Genetics, and APH - Amsterdam Public Health

Subjects
0301 basic medicine, Male, Microcephaly, clinical features, medicine.disease_cause, Bioinformatics, DISEASE, whole exome sequencing, Exon, DOMAIN, Missense mutation, Exome, Child, Genetics (clinical), Exome sequencing, Genetics, Mutation, MISSENSE, case series, High-Throughput Nucleotide Sequencing, genotype–phenotype correlation, Exons, CREBBP, syndrome, CREB-Binding Protein, Phenotype, intellectual disability, Child, Preschool, exon 30, exon 31, mutation, RSTS, Rubinstein–Taybi syndrome, Adolescent, Adult, Alleles, Amino Acid Sequence, Facies, Female, Genotype, Humans, Infant, Mutation, Missense, Rubinstein-Taybi Syndrome, Young Adult, Genetic Association Studies, medicine.symptom, genotype-phenotype correlation, CBP, ZZ, Short stature, 03 medical and health sciences, medicine, otorhinolaryngologic diseases, Preschool, Rubinstein-Taybi syndrome, SPECTRUM, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], business.industry, medicine.disease, 030104 developmental biology, business
Abstract

Item does not contain fulltext Mutations in CREBBP cause Rubinstein-Taybi syndrome. By using exome sequencing, and by using Sanger in one patient, CREBBP mutations were detected in 11 patients who did not, or only in a very limited manner, resemble Rubinstein-Taybi syndrome. The combined facial signs typical for Rubinstein-Taybi syndrome were absent, none had broad thumbs, and three had only somewhat broad halluces. All had apparent developmental delay (being the reason for molecular analysis); five had short stature and seven had microcephaly. The facial characteristics were variable; main characteristics were short palpebral fissures, telecanthi, depressed nasal ridge, short nose, anteverted nares, short columella, and long philtrum. Six patients had autistic behavior, and two had self-injurious behavior. Other symptoms were recurrent upper airway infections (n = 5), feeding problems (n = 7) and impaired hearing (n = 7). Major malformations occurred infrequently. All patients had a de novo missense mutation in the last part of exon 30 or beginning of exon 31 of CREBBP, between base pairs 5,128 and 5,614 (codons 1,710 and 1,872). No missense or truncating mutations in this region have been described to be associated with the classical Rubinstein-Taybi syndrome phenotype. No functional studies have (yet) been performed, but we hypothesize that the mutations disturb protein-protein interactions by altering zinc finger function. We conclude that patients with missense mutations in this specific CREBBP region show a phenotype that differs substantially from that in patients with Rubinstein-Taybi syndrome, and may prove to constitute one (or more) separate entities. (c) 2016 Wiley Periodicals, Inc.

Published
2016

27. Application of the Dutch, Finnish and British Screening Guidelines in a Cohort of Children with Growth Failure

Author

Stalman, S.E., Hellinga, I., Dommelen, P. van, Hennekam, R.C.M., Saari, A., Sankilampi, U., Dunkel, L., Wit, J.M., Kamp, G.A., and Plötz, F.B.

Subjects
Male, Practice guideline, Height standard deviation score, Child growth, Screening test, Growth disorders, Major clinical study, Height deflection, Life, CH - Child Health, Pediatric hospital, Clinical evaluation, Child, Diagnostic procedure, Finland, Netherlands, Patient referral, United Kingdom, Algorithm, Body height, Short stature, Sensitivity and specificity, Health, Parent, Target height, Assessment of humans, Medical history, Growth monitoring, Female, ELSS - Earth, Life and Social Sciences, Cohort analysis, Healthy for Life, Healthy Living
Abstract

Aims: To evaluate three guidelines for selecting short children for diagnostic workup in a general pediatric clinic. Methods: All patients (n = 131) aged 3.00-9.99 years who were referred for growth failure to a general pediatric clinic were evaluated for their medical history and growth and examined. All of them underwent the same standardized diagnostic workup. Retrospectively, the criteria for the diagnostic workup from three guidelines (proposed in the Netherlands, Finland and the UK) were applied, and their sensitivity was assessed. A Dutch reference sample (n = 958) was used for calculating population specificity. Results: In 23 patients (17.6%), a pathological cause of their growth failure was found. The sensitivity of the original Dutch, Finnish and British guidelines was 73.9, 78.3 and 56.5% and their specificity 98.5, 83.7 and 95.8%, respectively. When adding recent growth deflection to the Dutch guideline, sensitivity increased to 87%, but specificity decreased markedly (to 87%). Conclusion: The proposed cutoff values for height standard deviation score and distance to target height/mid-parental height, as used in the Netherlands and Finland, are effective for population growth monitoring, and superior to the monitoring algorithm in the UK. Growth deflection irrespective of height is an important sign of acquired growth disorders, but its specificity is too low for population screening.

Published
2015

28. Mutations in TBL1X are associated with central hypothyroidism

Author

Heinen, C.A. (Charlotte A.), Losekoot, M. (Monique), Sun, Y. (Yu), Watson, P.J. (Peter J.), Fairall, L. (Louise), Joustra, S.D. (Sjoerd), Zwaveling-Soonawala, N. (Nitash), Oostdijk, W. (Wilma), Akker, E.L.T. (Erica) van den, Alders, M. (Mariëlle), Santen, G.W.E. (Gijs), Rijn, R.R. (Rick) van, Dreschler, W.A. (Wouter), Surovtseva, O.V. (Olga V.), Biermasz, N.R., Hennekam, R.C.M. (Raoul), Wit, J.M. (Jan), Schwabe, J.W.R. (John W.R.), Boelen, A. (Anita), Fliers, E. (Eric), Trotsenburg, A.S.P. (Paul) van, Heinen, C.A. (Charlotte A.), Losekoot, M. (Monique), Sun, Y. (Yu), Watson, P.J. (Peter J.), Fairall, L. (Louise), Joustra, S.D. (Sjoerd), Zwaveling-Soonawala, N. (Nitash), Oostdijk, W. (Wilma), Akker, E.L.T. (Erica) van den, Alders, M. (Mariëlle), Santen, G.W.E. (Gijs), Rijn, R.R. (Rick) van, Dreschler, W.A. (Wouter), Surovtseva, O.V. (Olga V.), Biermasz, N.R., Hennekam, R.C.M. (Raoul), Wit, J.M. (Jan), Schwabe, J.W.R. (John W.R.), Boelen, A. (Anita), Fliers, E. (Eric), and Trotsenburg, A.S.P. (Paul) van

Abstract

Context: Isolated congenital central hypothyroidism (CeH) can result from mutations in TRHR, TSHB, and IGSF1, but its etiology often remains unexplained. We identified a missense mutation in the transducin X-like protein 1, X-linked (TBL1X) gene in three relatives diagnosed with isolated CeH. TBL1X is part of the thyroid hormone receptor-corepressor complex. Objective: The objectives of the study were the identification of TBL1X mutations in patients with unexplained isolated CeH, Sanger sequencing of relatives of affected individuals, and clinical and biochemical characterization; in vitro investigation of functional consequences of mutations; and mRNA expression in, and immunostaining of, human hypothalami and pituitary glands. Design: This was an observational study. Setting: The study was conducted at university medical centers. Patients: Nineteen individuals with and seven without a mutation participated in the study. Main Outcome Measures: Outcome measures included sequencing results, clinical and biochemical characteristics of mutation carriers, and results of in vitro functional and expression studies. Results: Sanger sequencing yielded five additional mutations. All patients (n = 8; six males) were previously diagnosed with CeH (free T4 [FT4] concentration below the reference interval, normal thyrotropin). Eleven relatives (two males) also carried mutations. One female had CeH, whereas 10 others had low-normal FT4 concentrations. As a group, adult mutation carriers had 20%-25% lower FT4 concentrations than controls. Twelve of 19 evaluated carriers had hearing loss. Mutations are located in the highly conserved WD40-repeat domain of the protein, influencing its expression and thermal stability. TBL1X mRNA and protein are expressed in the human hypothalamus and pituitary. Conclusions: TBL1X mutations are associated with CeH and hearing loss. FT4 concentrations in mutation carriers vary from low-normal to values compatible with CeH.

Published
2016
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29. Molecular basis of autosomal recessive desmosterolosis

Author

Waterham, R., Koster, J., Romeijn, G.J., Vreken, P., Hennekam, R.C.M., Andersson, H.C., FitzPatrick, D., Kelley, R.I., and Wanders, R.J.A.

Subjects
Human genetics -- Research, Genetic disorders -- Research, Biological sciences
Published
2001

30. Next-generation sequencing-based genome diagnostics across clinical genetics centers: Implementation choices and their effects

Author

Vrijenhoek, T. (T.), Kraaijeveld, K. (Ken), Elferink, M.G. (Martin), Ligt, J. (Joep) de, Kranendonk, E. (Elcke), Santen, G.W.E. (Gijs), Nijman, I.J. (Isaac ), Butler, D. (Derek), Claes, G. (Godelieve), Costessi, A. (Adalberto), Dorlijn, W. (Wim), Van Eyndhoven, W. (Winfried), Halley, D.J.J. (Dicky), Van Den Hout, M.C.G.N. (Mirjam C.G.N.), Van Hove, S. (Steven), Johansson, L.F. (Lennart F.), Jongbloed, J.D.H. (Jan), Kamps, R. (Rick), Kockx, C. (Christel), De Koning, B. (Bart), Kriek, N. (Nadia), Lekanne Dit Deprez, R.H., Lunstroo, H. (Hans), Mannens, M.M.A.M. (Marcel), Mook, O. (Olaf), Nelen, M.R. (Marcel), Ploem, C. (Corrette), Rijnen, M. (Marco), Saris, J.J. (Jasper), Sinke, R.J. (Richard J), Sistermans, E. (Erik), Slegtenhorst, M.A. (Marjon) van, Sleutels, F. (Frank), Stoep, N. (Nienke) van der, Tienhoven, M. (Marianne) van, Vermaat, M. (Martijn), Vogel, M.J. (Maartje), Waisfisz, Q. (Quinten), Weiss, J.M. (Janneke), Wijngaard, A. (Arthur) van den, Workum, W. (W) van, Ijntema, H. (Helger), Zwaag, B. (Bert) van der, IJcken, W.F.J. (Wilfred) van, Dunnen, J.T. (Johan) den, Veltman, J.A. (Joris), Hennekam, R.C.M. (Raoul), Cuppen, E. (Edwin), Vrijenhoek, T. (T.), Kraaijeveld, K. (Ken), Elferink, M.G. (Martin), Ligt, J. (Joep) de, Kranendonk, E. (Elcke), Santen, G.W.E. (Gijs), Nijman, I.J. (Isaac ), Butler, D. (Derek), Claes, G. (Godelieve), Costessi, A. (Adalberto), Dorlijn, W. (Wim), Van Eyndhoven, W. (Winfried), Halley, D.J.J. (Dicky), Van Den Hout, M.C.G.N. (Mirjam C.G.N.), Van Hove, S. (Steven), Johansson, L.F. (Lennart F.), Jongbloed, J.D.H. (Jan), Kamps, R. (Rick), Kockx, C. (Christel), De Koning, B. (Bart), Kriek, N. (Nadia), Lekanne Dit Deprez, R.H., Lunstroo, H. (Hans), Mannens, M.M.A.M. (Marcel), Mook, O. (Olaf), Nelen, M.R. (Marcel), Ploem, C. (Corrette), Rijnen, M. (Marco), Saris, J.J. (Jasper), Sinke, R.J. (Richard J), Sistermans, E. (Erik), Slegtenhorst, M.A. (Marjon) van, Sleutels, F. (Frank), Stoep, N. (Nienke) van der, Tienhoven, M. (Marianne) van, Vermaat, M. (Martijn), Vogel, M.J. (Maartje), Waisfisz, Q. (Quinten), Weiss, J.M. (Janneke), Wijngaard, A. (Arthur) van den, Workum, W. (W) van, Ijntema, H. (Helger), Zwaag, B. (Bert) van der, IJcken, W.F.J. (Wilfred) van, Dunnen, J.T. (Johan) den, Veltman, J.A. (Joris), Hennekam, R.C.M. (Raoul), and Cuppen, E. (Edwin)

Abstract

Implementation of next-generation DNA sequencing (NGS) technology into routine diagnostic genome care requires strategic choices. Instead of theoretical discussions on the consequences of such choices, we compared NGS-based diagnostic practices in eight clinical genetic centers in the Netherlands, based on genetic testing of nine pre-selected patients with cardiomyopathy. We highlight critical implementation choices, including the specific contributions of laboratory and medical specialists, bioinformaticians and researchers to diagnostic genome care, and how these affect interpretation and reporting of variants. Reported pathogenic mutations were consistent for all but one patient. Of the two centers that were inconsistent in their diagnosis, one reported to have found 'no causal variant', thereby underdiagnosing this patient. The other provided an alternative diagnosis, identifying another variant as causal than the other centers. Ethical and legal analysis showed that informed consent procedures in all centers were generally adequate for diagnostic NGS applications that target a limited set of genes, but not for exome- and genome-based diagnosis. We propose changes to further improve and align these procedures, taking into account the blurring boundary between diagnostics and research, and specific counseling options for exome- and genome-based diagnostics. We conclude that alternative diagnoses may infer a certain level of 'greediness' to come to a positive diagnosis in interpreting sequencing results. Moreover, there is an increasing interdependence of clinic, diagnostics and research departments for comprehensive diagnostic genome care. Therefore, we invite clinical geneticists, physicians, researchers, bioinformatics experts and patients to reconsider their role and position in future diagnostic genome care.

Published
2015
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31. A de novo mutation in ZMYND11, a candidate gene for 10p15.3 deletion syndrome, is associated with syndromic intellectual disability

Author

Cobben, J.M., Weiss, M.M., Dijk, F.S. Van, Reuver, R. de, Kruiff, C. de, Pondaag, W., Hennekam, R.C.M., Yntema, H.G., Cobben, J.M., Weiss, M.M., Dijk, F.S. Van, Reuver, R. de, Kruiff, C. de, Pondaag, W., Hennekam, R.C.M., and Yntema, H.G.

Abstract

Item does not contain fulltext, We report a boy with severe syndromic intellectual disability who has a de novo mutation in the ZMYND11 gene. Arguments for pathogenicity of this mutation are found in cases from the literature, especially several with 10p15.3 deletions, harbouring ZMYND11. Additional reports of ZMYND11 mutations in cases with syndromic intellectual disability are needed before the ZMYND11 mutation identified in our case can be considered as definitely pathogenic.

Published
2014

32. Is Marfan syndrome associated with symptomatic intracranial aneurysms?

Author

Berg, J.S.P. van den, Limburg, M., and Hennekam, R.C.M.

Subjects
Muscle, Peripheral Nervous System Diseases, Skeletal, Neuromuscular Diseases, Peripheral Nerves, Muscle, Skeletal, GeneralLiterature_REFERENCE(e.g.,dictionaries,encyclopedias,glossaries)
Abstract

Contains fulltext : 24182___.PDF (Publisher’s version ) (Open Access)

Published
1996

34. Exome sequencing identifies DYNC2H1 mutations as a common cause of asphyxiating thoracic dystrophy (Jeune syndrome) without major polydactyly, renal or retinal involvement

Author

Schmidts, M., Arts, H.H., Bongers, E.M.H.F., Yap, Z., Oud, M.M., Antony, D., Duijkers, L.E.M., Emes, R.D., Stalker, J., Yntema, J.L., Plagnol, V., Hoischen, A., Gilissen, C.F.H.A., Forsythe, E., Lausch, E., Veltman, J.A., Roeleveld, N., Superti-Furga, A., Kutkowska-Kazmierczak, A., Kamsteeg, E.J., Elcioglu, N., Maarle, M.C. van, Graul-Neumann, L.M., Devriendt, K., Smithson, S.F., Wellesley, D., Verbeek, N.E., Hennekam, R.C.M., Kayserili, H., Scambler, P.J., Beales, P.L., Knoers, N.V.A.M., Roepman, R., Mitchison, H.M., et al., Schmidts, M., Arts, H.H., Bongers, E.M.H.F., Yap, Z., Oud, M.M., Antony, D., Duijkers, L.E.M., Emes, R.D., Stalker, J., Yntema, J.L., Plagnol, V., Hoischen, A., Gilissen, C.F.H.A., Forsythe, E., Lausch, E., Veltman, J.A., Roeleveld, N., Superti-Furga, A., Kutkowska-Kazmierczak, A., Kamsteeg, E.J., Elcioglu, N., Maarle, M.C. van, Graul-Neumann, L.M., Devriendt, K., Smithson, S.F., Wellesley, D., Verbeek, N.E., Hennekam, R.C.M., Kayserili, H., Scambler, P.J., Beales, P.L., Knoers, N.V.A.M., Roepman, R., Mitchison, H.M., and et al.

Abstract

Contains fulltext : 116495.pdf (publisher's version ) (Open Access), BACKGROUND: Jeune asphyxiating thoracic dystrophy (JATD) is a rare, often lethal, recessively inherited chondrodysplasia characterised by shortened ribs and long bones, sometimes accompanied by polydactyly, and renal, liver and retinal disease. Mutations in intraflagellar transport (IFT) genes cause JATD, including the IFT dynein-2 motor subunit gene DYNC2H1. Genetic heterogeneity and the large DYNC2H1 gene size have hindered JATD genetic diagnosis. AIMS AND METHODS: To determine the contribution to JATD we screened DYNC2H1 in 71 JATD patients JATD patients combining SNP mapping, Sanger sequencing and exome sequencing. RESULTS AND CONCLUSIONS: We detected 34 DYNC2H1 mutations in 29/71 (41%) patients from 19/57 families (33%), showing it as a major cause of JATD especially in Northern European patients. This included 13 early protein termination mutations (nonsense/frameshift, deletion, splice site) but no patients carried these in combination, suggesting the human phenotype is at least partly hypomorphic. In addition, 21 missense mutations were distributed across DYNC2H1 and these showed some clustering to functional domains, especially the ATP motor domain. DYNC2H1 patients largely lacked significant extra-skeletal involvement, demonstrating an important genotype-phenotype correlation in JATD. Significant variability exists in the course and severity of the thoracic phenotype, both between affected siblings with identical DYNC2H1 alleles and among individuals with different alleles, which suggests the DYNC2H1 phenotype might be subject to modifier alleles, non-genetic or epigenetic factors. Assessment of fibroblasts from patients showed accumulation of anterograde IFT proteins in the ciliary tips, confirming defects similar to patients with other retrograde IFT machinery mutations, which may be of undervalued potential for diagnostic purposes.

Published
2013

35. MSX1 in relation to clefting. hypodontia and hydrocephaly in humans

Author

Lindhout, D., Ploos van Amstel, Hans Kristian, Koole, R, Cune, M.S., Hennekam, R.C.M., van Bokhoven, J.H.L.M., van den Boogaard, M.J.H., Lindhout, D., Ploos van Amstel, Hans Kristian, Koole, R, Cune, M.S., Hennekam, R.C.M., van Bokhoven, J.H.L.M., and van den Boogaard, M.J.H.

Published
2013

36. The IGSF1 deficiency syndrome: Characteristics of male and female patients

Author

Joustra, S.D. (Sjoerd), Schoenmakers, N. (Nadia), Persani, L. (Luca), Campi, I. (Irene), Bonomi, E. (Elisa), Radetti, G. (Giorgio), Beck-Peccoz, P. (Paolo), Zhu, H. (H.), Davis, T.M.E. (Timothy M.), Sun, Y. (Yu), Corssmit, E.P. (Eleonora), Appelman-Dijkstra, N.M. (Natasha), Heinen, C.A. (C.), Pereira, A.M. (Alberto), Varewijck, A.J. (Aimee), Janssen, J.A.M.J.L. (Joop), Endert, E. (Erik), Hennekam, R.C.M. (Raoul), Lombardi, M.P. (Paola), Mannens, M.M.A.M. (Marcel), Bak, B. (Beata), Bernard, D.J. (Daniel), Breuning, M.H. (Martijn), Chatterjee, K. (Krishna), Dattani, M.T. (Mehul), Oostdijk, W. (Wilma), Biermasz, N.R., Wit, J.M. (Jan), Trotsenburg, A.S.P. (Paul) van, Joustra, S.D. (Sjoerd), Schoenmakers, N. (Nadia), Persani, L. (Luca), Campi, I. (Irene), Bonomi, E. (Elisa), Radetti, G. (Giorgio), Beck-Peccoz, P. (Paolo), Zhu, H. (H.), Davis, T.M.E. (Timothy M.), Sun, Y. (Yu), Corssmit, E.P. (Eleonora), Appelman-Dijkstra, N.M. (Natasha), Heinen, C.A. (C.), Pereira, A.M. (Alberto), Varewijck, A.J. (Aimee), Janssen, J.A.M.J.L. (Joop), Endert, E. (Erik), Hennekam, R.C.M. (Raoul), Lombardi, M.P. (Paola), Mannens, M.M.A.M. (Marcel), Bak, B. (Beata), Bernard, D.J. (Daniel), Breuning, M.H. (Martijn), Chatterjee, K. (Krishna), Dattani, M.T. (Mehul), Oostdijk, W. (Wilma), Biermasz, N.R., Wit, J.M. (Jan), and Trotsenburg, A.S.P. (Paul) van

Abstract

Context: Ig superfamily member1 (IGSF1) deficiency was recently discovered as a novel X-linked cause of central hypothyroidism (CeH) and macro-orchidism. However, clinical and biochemical data regarding growth, puberty, and metabolic outcome, as well as features of female carriers, are scarce. Objective: Our objective was to investigate clinical and biochemical characteristics associated with IGSF1 deficiency in both sexes.Methods: All patients (n=42, 24 males) from 10 families examined in the university clinics of Leiden, Amsterdam, Cambridge, and Milan were included in this case series. Detailed clinical data were collected with an identical protocol, and biochemical measurements were performed in a central laboratory. Results: Male patients (age 0-87 years, 17 index cases and 7 from family studies) showed CeH (100%), hypoprolactinemia (n = 16, 67%), and transient partial GH deficiency (n = 3, 13%). Pubertal testosterone productionwasdelayed, aswerethe growth spurtandpubic hair development. However, testicular growth started at a normal age and attained macro-orchid size in all evaluable adults. Body mass index, percent fat, and waist circumference tended to be elevated. The metabolic syndrome was present in 4 of 5 patients over 55 years of age. Heterozygous female carriers (age 32-80 years) showed CeH in 6 of 18 cases (33%), hypoprolactinemia in 2 (11%), and GH deficiency in none. As in men, body mass index, percent fat, and waist circumference were relatively high, and the metabolic syndrome was present in 3 cases. Conclusion: In male patients, the X-linked IGSF1 deficiency syndrome is characterized by CeH, hypoprolactinemia, delayed puberty, macro-orchidism, and increased body weight. A subset of female carriers also exhibits CeH.

Published
2013
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37. Coffin-Siris syndrome and the BAF complex: genotype-phenotype study in 63 patients

Author

Santen, G.W., Aten, E., Silfhout, A.T. van, Pottinger, C., Bon, B.W.M. van, Minderhout, I.J. van, Snowdowne, R., Lans, C.A. van der, Boogaard, M. van den, Linssen, M.M., Vijfhuizen, L., Wielen, M.J.R. van der, Vollebregt, M.J., Coffin-Siris, c., Breuning, M.H., Kriek, M., Haeringen, A. van, Dunnen, J.T. den, Hoischen, A., Clayton-Smith, J., Vries, L.B.A. de, Hennekam, R.C.M., Belzen, M.J van, Santen, G.W., Aten, E., Silfhout, A.T. van, Pottinger, C., Bon, B.W.M. van, Minderhout, I.J. van, Snowdowne, R., Lans, C.A. van der, Boogaard, M. van den, Linssen, M.M., Vijfhuizen, L., Wielen, M.J.R. van der, Vollebregt, M.J., Coffin-Siris, c., Breuning, M.H., Kriek, M., Haeringen, A. van, Dunnen, J.T. den, Hoischen, A., Clayton-Smith, J., Vries, L.B.A. de, Hennekam, R.C.M., and Belzen, M.J van

Abstract

Item does not contain fulltext, De novo germline variants in several components of the SWI/SNF-like BAF complex can cause Coffin-Siris syndrome (CSS), Nicolaides-Baraitser syndrome (NCBRS), and nonsyndromic intellectual disability. We screened 63 patients with a clinical diagnosis of CSS for these genes (ARID1A, ARID1B, SMARCA2, SMARCA4, SMARCB1, and SMARCE1) and identified pathogenic variants in 45 (71%) patients. We found a high proportion of variants in ARID1B (68%). All four pathogenic variants in ARID1A appeared to be mosaic. By using all variants from the Exome Variant Server as test data, we were able to classify variants in ARID1A, ARID1B, and SMARCB1 reliably as being pathogenic or nonpathogenic. For SMARCA2, SMARCA4, and SMARCE1 several variants in the EVS remained unclassified, underlining the importance of parental testing. We have entered all variant and clinical information in LOVD-powered databases to facilitate further genotype-phenotype correlations, as these will become increasingly important because of the uptake of targeted and untargeted next generation sequencing in diagnostics. The emerging phenotype-genotype correlation is that SMARCB1 patients have the most marked physical phenotype and severe cognitive and growth delay. The variability in phenotype seems most marked in ARID1A and ARID1B patients. Distal limbs anomalies are most marked in ARID1A patients and least in SMARCB1 patients. Numbers are small however, and larger series are needed to confirm this correlation.

Published
2013

38. The cardiac phenotype in patients with a CHD7 mutation.

Author

Corsten-Janssen, N., Kerstjens-Frederikse, W.S., Marchie Sarvaas, G.J. du, Baardman, M.E., Bakker, M.K., Bergman, J.E., Hove, H.D., Heimdal, K.R., Rustad, C.F., Hennekam, R.C.M., Hofstra, R.M., Hoefsloot, L.H., Ravenswaaij-Arts, C.M.A. van, Kapusta, L., Corsten-Janssen, N., Kerstjens-Frederikse, W.S., Marchie Sarvaas, G.J. du, Baardman, M.E., Bakker, M.K., Bergman, J.E., Hove, H.D., Heimdal, K.R., Rustad, C.F., Hennekam, R.C.M., Hofstra, R.M., Hoefsloot, L.H., Ravenswaaij-Arts, C.M.A. van, and Kapusta, L.

Abstract

01 juni 2013, Item does not contain fulltext, BACKGROUND: Loss-of-function mutations in CHD7 cause Coloboma, Heart Disease, Atresia of Choanae, Retardation of Growth and/or Development, Genital Hypoplasia, and Ear Abnormalities With or Without Deafness (CHARGE) syndrome, a variable combination of multiple congenital malformations including heart defects. Heart defects are reported in 70% to 92% of patients with a CHD7 mutation, but most studies are small and do not provide a detailed classification of the defects. We present the first, detailed, descriptive study on the cardiac phenotype of 299 patients with a CHD7 mutation and discuss the role of CHD7 in cardiac development. METHODS AND RESULTS: We collected information on congenital heart defects in 299 patients with a pathogenic CHD7 mutation, of whom 220 (74%) had a congenital heart defect. Detailed information on the heart defects was available for 202 of these patients. We classified the heart defects based on embryonic cardiac development and compared the distribution to 1007 equally classified nonsyndromic heart defects of patients registered by EUROCAT, a European Registry of Congenital Anomalies. Heart defects are highly variable in patients with CHD7 mutations, but atrioventricular septal defects and conotruncal heart defects are over-represented. Sex did not have an effect on the presence of heart defects, but truncating CHD7 mutations resulted in a heart defect significantly more often than missense or splice-site mutations (chi(2), P<0.001). CONCLUSIONS: CHD7 plays an important role in cardiac development, given that we found a wide range of heart defects in 74% of a large cohort of patients with a CHD7 mutation. Conotruncal defects and atrioventricular septal defects are over-represented in patients with CHD7 mutations compared with patients with nonsyndromic heart defects.

Published
2013

39. MSX1 in relation to clefting. hypodontia and hydrocephaly in humans

Author

Child Health, Genetica, Brain, Lindhout, D., Ploos van Amstel, Hans Kristian, van den Boogaard, M.J.H., Koole, R, Cune, M.S., Hennekam, R.C.M., van Bokhoven, J.H.L.M., Child Health, Genetica, Brain, Lindhout, D., Ploos van Amstel, Hans Kristian, van den Boogaard, M.J.H., Koole, R, Cune, M.S., Hennekam, R.C.M., and van Bokhoven, J.H.L.M.

Published
2013

42. Genotypic and phenotypic spectrum in the Tricho-Rhino-Phalangeal Syndromes Types I and III

Author

Lüdecke, H.-J., Schaper, J., Meinecke, P., Momeni, P., Gross, S., von Holtum, D., Hirsche, H., Abramowicz, M.J., Albrecht, B., Apacik, C., Christen, H.-J., Claussen, U., Devriendt, K., Fastnacht, E., Forderer, A., Friedrich, U., Goodship, T.H.J., Greiwe, M., Hamm, H., Hennekam, R.C.M., Hinkel, G.K., Hoeltzenbein, M., Kayserili, H., Majewski, F., Mathieu, M., McLeod, R., Midro, A.T., Moog, U., Nagai, T., Niikawa, N., Ørstavik, K.H., Plöchl, E., Seitz, C., Schmidtke, J., Tranebjærg, L., Tsukahara, M., Wittwer, B., Zabel, B., Gillessen-Kaesbach, G., and Horsthemke, B.

Published
2001

43. Meier-Gorlin syndrome: Growth and secondary sexual development of a microcephalic primordial dwarfism disorder

Author

de Munnik, S.A., Otten, B.J., Schoots, J., Bicknell, L.S., Aftimos, S., Al-Aama, J.Y., van Bever, Y., Bober, M.B., Borm, G.F., Clayton-Smith, J., Deal, C.L., Edrees, A.Y., Feingold, M., Fryer, A., van Hagen, J.M., Hennekam, R.C.M., Jansweijer, M.C.E., Johnson, D., Kant, S.G., Opitz, J.M., Ramadevi, A.R., Reardon, W., Ross, A., Sarda, P., Schrander-Stumpel, C.T.R.M., Sluiter, A.E., Temple, I.K., Terhal, P.A., Toutain, A., Wise, C.A., Wright, M., Skidmore, D.L., Samuels, M.E., Hoefsloot, L.H., Knoers, N.V.A.M., Brunner, H.G., Jackson, A.P., Bongers, M.H.F., de Munnik, S.A., Otten, B.J., Schoots, J., Bicknell, L.S., Aftimos, S., Al-Aama, J.Y., van Bever, Y., Bober, M.B., Borm, G.F., Clayton-Smith, J., Deal, C.L., Edrees, A.Y., Feingold, M., Fryer, A., van Hagen, J.M., Hennekam, R.C.M., Jansweijer, M.C.E., Johnson, D., Kant, S.G., Opitz, J.M., Ramadevi, A.R., Reardon, W., Ross, A., Sarda, P., Schrander-Stumpel, C.T.R.M., Sluiter, A.E., Temple, I.K., Terhal, P.A., Toutain, A., Wise, C.A., Wright, M., Skidmore, D.L., Samuels, M.E., Hoefsloot, L.H., Knoers, N.V.A.M., Brunner, H.G., Jackson, A.P., and Bongers, M.H.F.

Abstract

Item does not contain fulltext, Meier-Gorlin syndrome (MGS) is a rare autosomal recessive disorder characterized by primordial dwarfism, microtia, and patellar aplasia/hypoplasia. Recently, mutations in the ORC1, ORC4, ORC6, CDT1, and CDC6 genes, encoding components of the pre-replication complex, have been identified. This complex is essential for DNA replication and therefore mutations are expected to impair cell proliferation and consequently could globally reduce growth. However, detailed growth characteristics of MGS patients have not been reported, and so this is addressed here through study of 45 MGS patients, the largest cohort worldwide. Here, we report that growth velocity (length) is impaired in MGS during pregnancy and first year of life, but, thereafter, height increases in paralleled normal reference centiles, resulting in a mean adult height of -4.5 standard deviations (SD). Height is dependent on ethnic background and underlying molecular cause, with ORC1 and ORC4 mutations causing more severe short stature and microcephaly. Growth hormone therapy (n = 9) was generally ineffective, though in two patients with significantly reduced IGF1 levels, growth was substantially improved by GH treatment, with 2SD and 3.8 SD improvement in height. Growth parameters for monitoring growth in future MGS patients are provided and as well we highlight that growth is disproportionately affected in certain structures, with growth related minor genital abnormalities (42%) and mammary hypoplasia (100%) frequently present, in addition to established effects on ears and patellar growth. (c) 2012 Wiley Periodicals, Inc.

Published
2012

44. Meier-Gorlin syndrome genotype-phenotype studies: 35 individuals with pre-replication complex gene mutations and 10 without molecular diagnosis.

Author

Munnik, S.A. de, Bicknell, L.S., Aftimos, S., Al-Aama, J.Y., Bever, Y. Van, Bober, M.B., Clayton-Smith, J., Edrees, A.Y., Feingold, M., Fryer, A., Hagen, J.M. van, Hennekam, R.C.M., Jansweijer, M.C.E., Johnson, D., Kant, S.G., Opitz, J.M., Ramadevi, A.R., Reardon, W., Ross, A., Sarda, P., Schrander-Stumpel, C.T.R.M., Schoots, J., Temple, I.K., Terhal, P.A., Toutain, A., Wise, C.A., Wright, M., Skidmore, D.L., Samuels, M.E., Hoefsloot, L.H., Knoers, N.V.A.M., Brunner, H.G., Jackson, A.P., Bongers, M.H.F., Munnik, S.A. de, Bicknell, L.S., Aftimos, S., Al-Aama, J.Y., Bever, Y. Van, Bober, M.B., Clayton-Smith, J., Edrees, A.Y., Feingold, M., Fryer, A., Hagen, J.M. van, Hennekam, R.C.M., Jansweijer, M.C.E., Johnson, D., Kant, S.G., Opitz, J.M., Ramadevi, A.R., Reardon, W., Ross, A., Sarda, P., Schrander-Stumpel, C.T.R.M., Schoots, J., Temple, I.K., Terhal, P.A., Toutain, A., Wise, C.A., Wright, M., Skidmore, D.L., Samuels, M.E., Hoefsloot, L.H., Knoers, N.V.A.M., Brunner, H.G., Jackson, A.P., and Bongers, M.H.F.

Abstract

01 juni 2012, Item does not contain fulltext, Meier-Gorlin syndrome (MGS) is an autosomal recessive disorder characterized by microtia, patellar aplasia/hypoplasia, and short stature. Recently, mutations in five genes from the pre-replication complex (ORC1, ORC4, ORC6, CDT1, and CDC6), crucial in cell-cycle progression and growth, were identified in individuals with MGS. Here, we report on genotype-phenotype studies in 45 individuals with MGS (27 females, 18 males; age 3 months-47 years). Thirty-five individuals had biallelic mutations in one of the five causative pre-replication genes. No homozygous or compound heterozygous null mutations were detected. In 10 individuals, no definitive molecular diagnosis was made. The triad of microtia, absent/hypoplastic patellae, and short stature was observed in 82% of individuals with MGS. Additional frequent clinical features were mammary hypoplasia (100%) and abnormal genitalia (42%; predominantly cryptorchidism and hypoplastic labia minora/majora). One individual with ORC1 mutations only had short stature, emphasizing the highly variable clinical spectrum of MGS. Individuals with ORC1 mutations had significantly shorter stature and smaller head circumferences than individuals from other gene categories. Furthermore, compared with homozygous missense mutations, compound heterozygous mutations appeared to have a more severe effect on phenotype, causing more severe growth retardation in ORC4 and more frequently pulmonary emphysema in CDT1. A lethal phenotype was seen in four individuals with compound heterozygous ORC1 and CDT1 mutations. No other clear genotype-phenotype association was observed. Growth hormone and estrogen treatment may be of some benefit, respectively, to growth retardation and breast hypoplasia, though further studies in this patient group are needed.

Published
2012

46. Familial syndromic esophegeal atresia maps to p23-p24

Author

Celli, J., Beusekom, E., Hennekam, R.C.M., Gallardo, M.E., Smeets, D.F.C.M., de Córdoba, S.R., Innis, J.W., Frydman, M., König, R., Kingston, H., Tolmie, J., Govaerts, L.C.P., van Bokhoven, H., Brunner, H.G., and Faculteit der Geneeskunde

Published
2000

48. Morphological features in children with autism spectrum disorders: a matched case-control study.

Author

Özgen, H., Hellemann, G.S., Stellato, R.K., Lahuis, B., Daalen, E. van, Staal, W.G., Rozendal, M., Hennekam, R.C.M., Beemer, F.A., Engeland, H.M. van, Özgen, H., Hellemann, G.S., Stellato, R.K., Lahuis, B., Daalen, E. van, Staal, W.G., Rozendal, M., Hennekam, R.C.M., Beemer, F.A., and Engeland, H.M. van

Abstract

01 januari 2011, Item does not contain fulltext, This study was designed to examine morphological features in a large group of children with autism spectrum disorder versus normal controls. Amongst 421 patients and 1,007 controls, 224 matched pairs were created. Prevalence rates and odds ratios were analyzed by conditional regression analysis, McNemar test or paired t-test matched pairs. Morphological abnormalities were significantly more prevalent in patients with autism than in the normal control group and 48 morphological features distinguished patients from controls. Our findings show that morphological features are associated with autism. Exploring potential underlying genetic mechanisms of this association might lead to a better understanding of autism.

Published
2011

49. Growth charts for children with Ellis-van Creveld syndrome

Author

Verbeek, S. (Sabine), Eilers, P.H.C. (Paul), Lawrence, K.A. (Karen), Hennekam, R.C.M. (Raoul), Versteegh, F.G. (Florens), Verbeek, S. (Sabine), Eilers, P.H.C. (Paul), Lawrence, K.A. (Karen), Hennekam, R.C.M. (Raoul), and Versteegh, F.G. (Florens)

Abstract

Ellis-van Creveld (EvC) syndrome is a congenital malformation syndrome with marked growth retardation. In this study, specific growth charts for EvC patients were derived to allow better follow-up of growth and earlier detection of growth patterns unusual for EvC. With the use of 235 observations of 101 EvC patients (49 males, 52 females), growth charts for males and females from 0 to 20 years of age were derived. Longitudinal and cross-sectional data were collected from an earlier review of growt

Published
2011
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50. Heterozygous germline mutations in the P53 homolog P63 are causes of the EEC syndrome

Author

Celli, J., Duijf, P.H., Hamel, B.C.J., Bamshad, M., Kramer, B.M., Smits, A.P.T., Newbury-Ecob, R., Hennekam, R.C.M., Buggenhout, G.J.C.M. van, Haeringen, A. van, Woods, C.G., Essen, A.J. van, Waal, R.M.W. de, Vriend, G., Haber, D.A., Yang, A., McKeon, F., Brunner, H.G., and Bokhoven, J.H.L.M. van

Subjects
Breuk-gevoelige plaatsen in chromosomen bij de mens, Bioinformatics, (Fragile) breakage-prone sites in human chromosomes, Clinical description and delineation of genetic syndromes, Tumor pathology, Tumor pathologie, Klinische beschrijving en moleculaire definiëring van genetische syndromen
Abstract

Item does not contain fulltext

Published
1999

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