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1. Polygenic risk score-based phenome-wide association study identifies novel associations for Tourette syndrome

Author

Jain, P., Miller-Fleming, T., Topaloudi, A., Yu, D., Drineas, P., Georgitsi, M., Yang, Z, Rizzo, R., Müller-Vahl, K.R., Tumer, Z., Debes, N. Mol, Hartmann, A., Depienne, C., Worbe, Y., Mir, P., Cath, D.C., Boomsma, D.I., Roessner, V., Wolanczyk, T., Janik, P., Szejko, N., Zekanowski, C., Barta, C., Nemoda, Z., Tarnok, Z., Buxbaum, J.D., Grice, D., Glennon, J., Stefansson, H., Hengerer, B., Benaroya-Milshtein, N., Cardona, F., Hedderly, T., Heyman, I., Huyser, C., Morer, A., Mueller, N., Munchau, A., Plessen, K.J., Porcelli, C., Walitza, S., Schrag, A., Martino, D. de, Dietrich, A., Mathews, Carol A., Scharf, J.M., Hoekstra, P.J., Buitelaar, J.K., Davis, L.K., Paschou, P., Jain, P., Miller-Fleming, T., Topaloudi, A., Yu, D., Drineas, P., Georgitsi, M., Yang, Z, Rizzo, R., Müller-Vahl, K.R., Tumer, Z., Debes, N. Mol, Hartmann, A., Depienne, C., Worbe, Y., Mir, P., Cath, D.C., Boomsma, D.I., Roessner, V., Wolanczyk, T., Janik, P., Szejko, N., Zekanowski, C., Barta, C., Nemoda, Z., Tarnok, Z., Buxbaum, J.D., Grice, D., Glennon, J., Stefansson, H., Hengerer, B., Benaroya-Milshtein, N., Cardona, F., Hedderly, T., Heyman, I., Huyser, C., Morer, A., Mueller, N., Munchau, A., Plessen, K.J., Porcelli, C., Walitza, S., Schrag, A., Martino, D. de, Dietrich, A., Mathews, Carol A., Scharf, J.M., Hoekstra, P.J., Buitelaar, J.K., Davis, L.K., and Paschou, P.

Abstract

Contains fulltext : 291641.pdf (Publisher’s version ) (Open Access), Tourette Syndrome (TS) is a complex neurodevelopmental disorder characterized by vocal and motor tics lasting more than a year. It is highly polygenic in nature with both rare and common previously associated variants. Epidemiological studies have shown TS to be correlated with other phenotypes, but large-scale phenome wide analyses in biobank level data have not been performed to date. In this study, we used the summary statistics from the latest meta-analysis of TS to calculate the polygenic risk score (PRS) of individuals in the UK Biobank data and applied a Phenome Wide Association Study (PheWAS) approach to determine the association of disease risk with a wide range of phenotypes. A total of 57 traits were found to be significantly associated with TS polygenic risk, including multiple psychosocial factors and mental health conditions such as anxiety disorder and depression. Additional associations were observed with complex non-psychiatric disorders such as Type 2 diabetes, heart palpitations, and respiratory conditions. Cross-disorder comparisons of phenotypic associations with genetic risk for other childhood-onset disorders (e.g.: attention deficit hyperactivity disorder [ADHD], autism spectrum disorder [ASD], and obsessive-compulsive disorder [OCD]) indicated an overlap in associations between TS and these disorders. ADHD and ASD had a similar direction of effect with TS while OCD had an opposite direction of effect for all traits except mental health factors. Sex-specific PheWAS analysis identified differences in the associations with TS genetic risk between males and females. Type 2 diabetes and heart palpitations were significantly associated with TS risk in males but not in females, whereas diseases of the respiratory system were associated with TS risk in females but not in males. This analysis provides further evidence of shared genetic and phenotypic architecture of different complex disorders.

Published
2023

2. The clinical and molecular spectrum of QRICH1 associated neurodevelopmental disorder

Author

Kumble, S, Levy, AM, Punetha, J, Gao, H, Ah Mew, N, Anyane-Yeboa, K, Benke, PJ, Berger, SM, Bjerglund, L, Campos-Xavier, B, Ciliberto, M, Cohen, JS, Comi, AM, Curry, C, Damaj, L, Denomme-Pichon, A-S, Emrick, L, Faivre, L, Fasano, MB, Fievet, A, Finkel, RS, Garcia-Minaur, S, Gerard, A, Gomez-Puertas, P, Guillen Sacoto, MJ, Hoffman, TL, Howard, L, Iglesias, AD, Izumi, K, Larson, A, Leiber, A, Lozano, R, Marcos-Alcalde, I, Mintz, CS, Mullegama, SV, Moller, RS, Odent, S, Oppermann, H, Ostergaard, E, Pacio-Miguez, M, Palomares-Bralo, M, Parikh, S, Paulson, AM, Platzer, K, Posey, JE, Potocki, L, Revah-Politi, A, Rio, M, Ritter, AL, Robinson, S, Rosenfeld, JA, Santos-Simarro, F, Sousa, SB, Weber, M, Xie, Y, Chung, WK, Brown, NJ, Tumer, Z, Kumble, S, Levy, AM, Punetha, J, Gao, H, Ah Mew, N, Anyane-Yeboa, K, Benke, PJ, Berger, SM, Bjerglund, L, Campos-Xavier, B, Ciliberto, M, Cohen, JS, Comi, AM, Curry, C, Damaj, L, Denomme-Pichon, A-S, Emrick, L, Faivre, L, Fasano, MB, Fievet, A, Finkel, RS, Garcia-Minaur, S, Gerard, A, Gomez-Puertas, P, Guillen Sacoto, MJ, Hoffman, TL, Howard, L, Iglesias, AD, Izumi, K, Larson, A, Leiber, A, Lozano, R, Marcos-Alcalde, I, Mintz, CS, Mullegama, SV, Moller, RS, Odent, S, Oppermann, H, Ostergaard, E, Pacio-Miguez, M, Palomares-Bralo, M, Parikh, S, Paulson, AM, Platzer, K, Posey, JE, Potocki, L, Revah-Politi, A, Rio, M, Ritter, AL, Robinson, S, Rosenfeld, JA, Santos-Simarro, F, Sousa, SB, Weber, M, Xie, Y, Chung, WK, Brown, NJ, and Tumer, Z

Abstract

De novo variants in QRICH1 (Glutamine-rich protein 1) has recently been reported in 11 individuals with intellectual disability (ID). The function of QRICH1 is largely unknown but it is likely to play a key role in the unfolded response of endoplasmic reticulum stress through transcriptional control of proteostasis. In this study, we present 27 additional individuals and delineate the clinical and molecular spectrum of the individuals (n = 38) with QRICH1 variants. The main clinical features were mild to moderate developmental delay/ID (71%), nonspecific facial dysmorphism (92%) and hypotonia (39%). Additional findings included poor weight gain (29%), short stature (29%), autism spectrum disorder (29%), seizures (24%) and scoliosis (18%). Minor structural brain abnormalities were reported in 52% of the individuals with brain imaging. Truncating or splice variants were found in 28 individuals and 10 had missense variants. Four variants were inherited from mildly affected parents. This study confirms that heterozygous QRICH1 variants cause a neurodevelopmental disorder including short stature and expands the phenotypic spectrum to include poor weight gain, scoliosis, hypotonia, minor structural brain anomalies, and seizures. Inherited variants from mildly affected parents are reported for the first time, suggesting variable expressivity.

Published
2022

3. Enhancing neuroimaging genetics through meta-analysis for Tourette syndrome (ENIGMA-TS): A worldwide platform for collaboration

Author

Paschou, P., Jin, Y., Müller-Vahl, K., Möller, H.E., Rizzo, R., Hoekstra, P.J., Roessner, V., Debes, N. Mol, Worbe, Y., Hartmann, A., Mir, P., Cath, D., Neuner, I., Eichele, H., Zhang, C, Lewandowska, K., Munchau, A., Verrel, J., Musil, R., Silk, T.J., Hanlon, C.A., Bihun, E.D., Brandt, V., Dietrich, A., Forde, N., Ganos, C., Greene, D.J., Chu, C., Grothe, M.J., Hershey, T., Janik, P., Koller, J.M., Martin-Rodriguez, J.F., Müller, K., Palmucci, S., Prato, A., Ramkiran, S., Saia, F., Szejko, N., Torrecuso, R., Tumer, Z., Uhlmann, A., Veselinovic, T., Wolańczyk, T., Zouki, J.J., Jain, P., Topaloudi, A., Kaka, M., Yang, Z, Drineas, P., Thomopoulos, S.I., White, T., Veltman, D.J., Schmaal, L., Stein, D.J., Buitelaar, J.K., Franke, B., Heuvel, O. van den, Jahanshad, N., Thompson, P.M., Black, K.J., Paschou, P., Jin, Y., Müller-Vahl, K., Möller, H.E., Rizzo, R., Hoekstra, P.J., Roessner, V., Debes, N. Mol, Worbe, Y., Hartmann, A., Mir, P., Cath, D., Neuner, I., Eichele, H., Zhang, C, Lewandowska, K., Munchau, A., Verrel, J., Musil, R., Silk, T.J., Hanlon, C.A., Bihun, E.D., Brandt, V., Dietrich, A., Forde, N., Ganos, C., Greene, D.J., Chu, C., Grothe, M.J., Hershey, T., Janik, P., Koller, J.M., Martin-Rodriguez, J.F., Müller, K., Palmucci, S., Prato, A., Ramkiran, S., Saia, F., Szejko, N., Torrecuso, R., Tumer, Z., Uhlmann, A., Veselinovic, T., Wolańczyk, T., Zouki, J.J., Jain, P., Topaloudi, A., Kaka, M., Yang, Z, Drineas, P., Thomopoulos, S.I., White, T., Veltman, D.J., Schmaal, L., Stein, D.J., Buitelaar, J.K., Franke, B., Heuvel, O. van den, Jahanshad, N., Thompson, P.M., and Black, K.J.

Abstract

Contains fulltext : 281802.pdf (Publisher’s version ) (Open Access), Tourette syndrome (TS) is characterized by multiple motor and vocal tics, and high-comorbidity rates with other neuropsychiatric disorders. Obsessive compulsive disorder (OCD), attention deficit hyperactivity disorder (ADHD), autism spectrum disorders (ASDs), major depressive disorder (MDD), and anxiety disorders (AXDs) are among the most prevalent TS comorbidities. To date, studies on TS brain structure and function have been limited in size with efforts mostly fragmented. This leads to low-statistical power, discordant results due to differences in approaches, and hinders the ability to stratify patients according to clinical parameters and investigate comorbidity patterns. Here, we present the scientific premise, perspectives, and key goals that have motivated the establishment of the Enhancing Neuroimaging Genetics through Meta-Analysis for TS (ENIGMA-TS) working group. The ENIGMA-TS working group is an international collaborative effort bringing together a large network of investigators who aim to understand brain structure and function in TS and dissect the underlying neurobiology that leads to observed comorbidity patterns and clinical heterogeneity. Previously collected TS neuroimaging data will be analyzed jointly and integrated with TS genomic data, as well as equivalently large and already existing studies of highly comorbid OCD, ADHD, ASD, MDD, and AXD. Our work highlights the power of collaborative efforts and transdiagnostic approaches, and points to the existence of different TS subtypes. ENIGMA-TS will offer large-scale, high-powered studies that will lead to important insights toward understanding brain structure and function and genetic effects in TS and related disorders, and the identification of biomarkers that could help inform improved clinical practice.

Published
2022

4. Enhancing neuroimaging genetics through meta-analysis for Tourette syndrome (ENIGMA-TS): A worldwide platform for collaboration

Author

Paschou, P, Jin, Y, Mueller-Vahl, K, Moeller, HE, Rizzo, R, Hoekstra, PJ, Roessner, V, Debes, NM, Worbe, Y, Hartmann, A, Mir, P, Cath, D, Neuner, I, Eichele, H, Zhang, C, Lewandowska, K, Munchau, A, Verrel, J, Musil, R, Silk, TJ, Hanlon, CA, Bihun, ED, Brandt, V, Dietrich, A, Forde, N, Ganos, C, Greene, DJ, Chu, C, Grothe, MJ, Hershey, T, Janik, P, Koller, JM, Francisco Martin-Rodriguez, J, Mueller, K, Palmucci, S, Prato, A, Ramkiran, S, Saia, F, Szejko, N, Torrecuso, R, Tumer, Z, Uhlmann, A, Veselinovic, T, Wolanczyk, T, Zouki, J-J, Jain, P, Topaloudi, A, Kaka, M, Yang, Z, Drineas, P, Thomopoulos, S, White, T, Veltman, DJ, Schmaal, L, Stein, DJ, Buitelaar, J, Franke, B, van den Heuvel, O, Jahanshad, N, Thompson, PM, Black, KJ, Paschou, P, Jin, Y, Mueller-Vahl, K, Moeller, HE, Rizzo, R, Hoekstra, PJ, Roessner, V, Debes, NM, Worbe, Y, Hartmann, A, Mir, P, Cath, D, Neuner, I, Eichele, H, Zhang, C, Lewandowska, K, Munchau, A, Verrel, J, Musil, R, Silk, TJ, Hanlon, CA, Bihun, ED, Brandt, V, Dietrich, A, Forde, N, Ganos, C, Greene, DJ, Chu, C, Grothe, MJ, Hershey, T, Janik, P, Koller, JM, Francisco Martin-Rodriguez, J, Mueller, K, Palmucci, S, Prato, A, Ramkiran, S, Saia, F, Szejko, N, Torrecuso, R, Tumer, Z, Uhlmann, A, Veselinovic, T, Wolanczyk, T, Zouki, J-J, Jain, P, Topaloudi, A, Kaka, M, Yang, Z, Drineas, P, Thomopoulos, S, White, T, Veltman, DJ, Schmaal, L, Stein, DJ, Buitelaar, J, Franke, B, van den Heuvel, O, Jahanshad, N, Thompson, PM, and Black, KJ

Abstract

Tourette syndrome (TS) is characterized by multiple motor and vocal tics, and high-comorbidity rates with other neuropsychiatric disorders. Obsessive compulsive disorder (OCD), attention deficit hyperactivity disorder (ADHD), autism spectrum disorders (ASDs), major depressive disorder (MDD), and anxiety disorders (AXDs) are among the most prevalent TS comorbidities. To date, studies on TS brain structure and function have been limited in size with efforts mostly fragmented. This leads to low-statistical power, discordant results due to differences in approaches, and hinders the ability to stratify patients according to clinical parameters and investigate comorbidity patterns. Here, we present the scientific premise, perspectives, and key goals that have motivated the establishment of the Enhancing Neuroimaging Genetics through Meta-Analysis for TS (ENIGMA-TS) working group. The ENIGMA-TS working group is an international collaborative effort bringing together a large network of investigators who aim to understand brain structure and function in TS and dissect the underlying neurobiology that leads to observed comorbidity patterns and clinical heterogeneity. Previously collected TS neuroimaging data will be analyzed jointly and integrated with TS genomic data, as well as equivalently large and already existing studies of highly comorbid OCD, ADHD, ASD, MDD, and AXD. Our work highlights the power of collaborative efforts and transdiagnostic approaches, and points to the existence of different TS subtypes. ENIGMA-TS will offer large-scale, high-powered studies that will lead to important insights toward understanding brain structure and function and genetic effects in TS and related disorders, and the identification of biomarkers that could help inform improved clinical practice.

Published
2022

5. Development, behaviour and autism in individuals with SMC1A variants

Author

Mulder, P.A., Huisman, S., Landlust, A.M., Moss, J., Bader, I., Balkom, I.D.C. van, Bisgaard, A.M., Brooks, A., Cereda, A., Cinca, C., Clark, D., Cormier-Daire, V., Deardorff, M.A., Diderich, K., Elting, M., Essen, A. van, FitzPatrick, D., Gervasini, C., Gillessen-Kaesbach, G., Girisha, K.M., Hennekam, R.C., Hilhorst-Hofstee, Y., Hopman, S., Horn, D., Isrie, M., Jansen, S., Jespersgaard, C., Kaiser, F.J., Kaur, M., Kleefstra, T., Krantz, I.D., Lakeman, P., Lessel, D., Michot, C., Noon, S.E., Oliver, C., Parenti, I., Pie, J., Piening, S., Puisac, B., Ramos, F.J., Redeker, E., Rieubland, C., Russo, S., Selicorni, A., Tumer, Z., Vorstenbosch, R., Vries, I.M., Wenger, T.L., Wierzba, J., SMC1A Consortium, Clinical Genetics, Pediatric surgery, APH - Quality of Care, Human genetics, Amsterdam Reproduction & Development (AR&D), Graduate School, ANS - Cellular & Molecular Mechanisms, and Paediatric Genetics

Subjects
cognition, Male, Autism Spectrum Disorder, Chromosomal Proteins, Non-Histone, CHILDREN, Cell Cycle Proteins, COMMUNICATION, Pediatrics, 0302 clinical medicine, De Lange Syndrome, Intellectual disability, Developmental and Educational Psychology, Spectrum disorder, Child, self-injurious behaviour, 05 social sciences, SELF-INJURIOUS-BEHAVIOR, Perinatology, PREVALENCE, and Child Health, Psychiatry and Mental health, Phenotype, DE-LANGE-SYNDROME, Autism spectrum disorder, Child, Preschool, Female, Psychology, 050104 developmental & child psychology, Clinical psychology, Behavioural phenotype, Adult, Down syndrome, cornelia de lange syndrome, Cornelia de Lange Syndrome, Adolescent, autism, Rett syndrome, 03 medical and health sciences, Young Adult, All institutes and research themes of the Radboud University Medical Center, Journal Article, medicine, Humans, 0501 psychology and cognitive sciences, Cognitive Dysfunction, Pediatrics, Perinatology, and Child Health, rett syndrome, SPECTRUM DISORDER, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], MUTATIONS, Infant, NIPBL, medicine.disease, Cross-Sectional Studies, Pediatrics, Perinatology and Child Health, Autism, Down Syndrome, Self-Injurious Behavior, 030217 neurology & neurosurgery
Abstract

Introduction: Development and behaviour in Cornelia de Lange Syndrome (CdLS), including autism characteristics, have been described infrequently stratified to genetic cause and only a few studies have considered behavioural characteristics in relation to developmental level. Here, we describe the behavioural phenotype in individuals with CdLS with SMC1A variants. Methods: We performed an international, interdisciplinary study on 51 individuals with SMC1A variants. Results of questionnaire studies are compared to those in individuals with Down Syndrome and with Autism Spectrum Disorder. Results on cognition and self-injurious behaviour (SIB) are compared to those in individuals with CdLS caused by NIPBL variants. For Dutch participants with SMC1A variants we performed direct in-person assessments of cognition, autism, and added an interview and questionnaire on adaptive behaviour and sensory processing. Results: Individuals with SMC1A variants show a higher cognitive level and less SIB than individuals with NIPBL variants. Individuals with SMC1A variants without classic CdLS phenotype but with a Rett-like phenotype show more severe intellectual disability and more SIB compared to those with a CdLS phenotype. Autism is less present if outcomes in direct in-person assessments are evaluated taking developmental level into account compared to results based on a questionnaire. Conclusions: Behaviour in individuals with CdLS should be evaluated taking genetic cause into account. Detailed interdisciplinary approaches are of clinical importance to inform tailored care and may eventually improve quality of life of patients and families.

Published
2019

6. Phenotypic and genotypic description of 44 patients with variants in DLG4 encoding the post-synaptic density protein PSD-95

Author

Rodriguez-Palmero Seuma, A., Boerrigter, M., Mandrile, G., Pelle, A., Giorgio, E., Lindstrand, A., Johansson, M., Kvarnung, M., Everman, D., Bahrambeigi, V., MacKenzie, A., Morton, J., Ruivenkamp, C., Challman, T., Hurst, A., Hoyer, J., Elmslie, F., Dye, T., Isidor, B., Haldeman-Englert, C., Gomez-Andres, D., Schluter, A., de Man, S., Shieh, J., Prada, C., Moutton, S., Denomme-Pichon, A., Motti, S., Bruel, A., Mau-Them, F. Tran, Reiter, S., van Ravenswaaij-Arts, C., Shaw-Smith, C., Parikh, S., Aldinger, K., Lovgren, A., Rauch, A., Ross, M., Gomez-Puertas, P., de Vries, B., Pujol, A., Tumer, Z., and Clinical Cognitive Neuropsychiatry Research Program (CCNP)

Published
2020

7. Expansion of the phenotypic spectrum of de novo missense variants in kinesin family member 1A (KIF1A)

Author

Kaur, S, Van Bergen, NJ, Verhey, KJ, Nowell, CJ, Budaitis, B, Yue, Y, Ellaway, C, Brunetti-Pierri, N, Cappuccio, G, Bruno, I, Boyle, L, Nigro, V, Torella, A, Roscioli, T, Cowley, MJ, Massey, S, Sonawane, R, Burton, MD, Schonewolf-Greulich, B, Tumer, Z, Chung, WK, Gold, WA, Christodoulou, J, Kaur, S, Van Bergen, NJ, Verhey, KJ, Nowell, CJ, Budaitis, B, Yue, Y, Ellaway, C, Brunetti-Pierri, N, Cappuccio, G, Bruno, I, Boyle, L, Nigro, V, Torella, A, Roscioli, T, Cowley, MJ, Massey, S, Sonawane, R, Burton, MD, Schonewolf-Greulich, B, Tumer, Z, Chung, WK, Gold, WA, and Christodoulou, J

Abstract

Defects in the motor domain of kinesin family member 1A (KIF1A), a neuron-specific ATP-dependent anterograde axonal transporter of synaptic cargo, are well-recognized to cause a spectrum of neurological conditions, commonly known as KIF1A-associated neurological disorders (KAND). Here, we report one mutation-negative female with classic Rett syndrome (RTT) harboring a de novo heterozygous novel variant [NP_001230937.1:p.(Asp248Glu)] in the highly conserved motor domain of KIF1A. In addition, three individuals with severe neurodevelopmental disorder along with clinical features overlapping with KAND are also reported carrying de novo heterozygous novel [NP_001230937.1:p.(Cys92Arg) and p.(Pro305Leu)] or previously reported [NP_001230937.1:p.(Thr99Met)] variants in KIF1A. In silico tools predicted these variants to be likely pathogenic, and 3D molecular modeling predicted defective ATP hydrolysis and/or microtubule binding. Using the neurite tip accumulation assay, we demonstrated that all novel KIF1A variants significantly reduced the ability of the motor domain of KIF1A to accumulate along the neurite lengths of differentiated SH-SY5Y cells. In vitro microtubule gliding assays showed significantly reduced velocities for the variant p.(Asp248Glu) and reduced microtubule binding for the p.(Cys92Arg) and p.(Pro305Leu) variants, suggesting a decreased ability of KIF1A to move along microtubules. Thus, this study further expanded the phenotypic characteristics of KAND individuals with pathogenic variants in the KIF1A motor domain to include clinical features commonly seen in RTT individuals.

Published
2020

8. Recommendations for a nomenclature system for reporting methylation aberrations in imprinted domains

Author

Monk, D., Morales, J., Dunnen, J.T. den, Russo, S., Court, F., Prawitt, D., Eggermann, T., Beygo, J., Buiting, K., Tumer, Z., and European Network Human Congenital

Subjects
Epigenomics, 0301 basic medicine, Cancer Research, ADN, Medizin, Biology, Bioinformatics, Methylation, Genomic Imprinting, 03 medical and health sciences, 0302 clinical medicine, Terminology as Topic, Health care, Journal Article, imprinting disorders, Animals, Humans, Point of View, Molecular Biology, Nomenclature, Polymorphism, Genetic, Aberrant methylation, business.industry, Imprinting, DNA, DNA Methylation, 3. Good health, 030104 developmental biology, Differentially methylated regions, 030220 oncology & carcinogenesis, Practice Guidelines as Topic, DNA methylation, nomenclature, Human genome, methylation, Special care, Metilació, business
Abstract

The analysis of DNA methylation has become routine in the pipeline for diagnosis of imprinting disorders, with many publications reporting aberrant methylation associated with imprinted differentially methylated regions (DMRs). However, comparisons between these studies are routinely hampered by the lack of consistency in reporting sites of methylation evaluated. To avoid confusion surrounding nomenclature, special care is needed to communicate results accurately, especially between scientists and other health care professionals. Within the European Network for Human Congenital Imprinting Disorders we have discussed these issues and designed a nomenclature for naming imprinted DMRs as well as for reporting methylation values. We apply these recommendations for imprinted DMRs that are commonly assayed in clinical laboratories and show how they support standardized database submission. The recommendations are in line with existing recommendations, most importantly the Human Genome Variation Society nomenclature, and should facilitate accurate reporting and data exchange among laboratories and thereby help to avoid future confusion.

Published
2018

9. High frequency of submicroscopic genomic aberrations detected by tiling path array comparative genome hybridisation in patients with isolated congenital heart disease

Author

Erdogan, F., Larsen, L.A., Zhang, L., Tumer, Z., Tommerup, N., Chen, W., Jacobsen, J.R., Schubert, M., Jurkatis, J., Tzschach, A., Ropers, H.-H., and Ullmann, R.

Subjects
Hybridization -- Research, Hybridization -- Genetic aspects, Congenital heart disease -- Research, Congenital heart disease -- Genetic aspects, Congenital heart disease -- Risk factors, Genomes -- Research, Genomes -- Physiological aspects, Health
Published
2008

11. Breakpoints around the HOXD cluster result in various limb malformations

Author

Dlugaszewska, B., Silahtaroglu, A., Menzel, C., Kubart, S., Cohen, M., Mundlos, S., Tumer, Z., Kjaer, K., Friedrich, U., Ropers, H.-H., Tommerup, N., Neitzel, H., and Kalscheuer, V.M.

Subjects
Genetic regulation -- Research, Gene expression -- Research, Bones -- Abnormalities, Bones -- Genetic aspects, Bones -- Development and progression, Health
Published
2006

12. Autism and developmental disability caused by KCNQ3 gain-of-function variants

Author

Sands, TT, Miceli, F, Lesca, G, Beck, AE, Sadleir, LG, Arrington, DK, Schonewolf-Greulich, B, Moutton, S, Lauritano, A, Nappi, P, Soldovieri, MV, Scheffer, IE, Mefford, HC, Stong, N, Heinzen, EL, Goldstein, DB, Perez, AG, Kossoff, EH, Stocco, A, Sullivan, JA, Shashi, V, Gerard, B, Francannet, C, Bisgaard, A-M, Tumer, Z, Willems, M, Rivier, F, Vitobello, A, Thakkar, K, Rajan, DS, Barkovich, AJ, Weckhuysen, S, Cooper, EC, Taglialatela, M, Cilio, MR, Sands, TT, Miceli, F, Lesca, G, Beck, AE, Sadleir, LG, Arrington, DK, Schonewolf-Greulich, B, Moutton, S, Lauritano, A, Nappi, P, Soldovieri, MV, Scheffer, IE, Mefford, HC, Stong, N, Heinzen, EL, Goldstein, DB, Perez, AG, Kossoff, EH, Stocco, A, Sullivan, JA, Shashi, V, Gerard, B, Francannet, C, Bisgaard, A-M, Tumer, Z, Willems, M, Rivier, F, Vitobello, A, Thakkar, K, Rajan, DS, Barkovich, AJ, Weckhuysen, S, Cooper, EC, Taglialatela, M, and Cilio, MR

Abstract

OBJECTIVE: Recent reports have described single individuals with neurodevelopmental disability (NDD) harboring heterozygous KCNQ3 de novo variants (DNVs). We sought to assess whether pathogenic variants in KCNQ3 cause NDD and to elucidate the associated phenotype and molecular mechanisms. METHODS: Patients with NDD and KCNQ3 DNVs were identified through an international collaboration. Phenotypes were characterized by clinical assessment, review of charts, electroencephalographic (EEG) recordings, and parental interview. Functional consequences of variants were analyzed in vitro by patch-clamp recording. RESULTS: Eleven patients were assessed. They had recurrent heterozygous DNVs in KCNQ3 affecting residues R230 (R230C, R230H, R230S) and R227 (R227Q). All patients exhibited global developmental delay within the first 2 years of life. Most (8/11, 73%) were nonverbal or had a few words only. All patients had autistic features, and autism spectrum disorder (ASD) was diagnosed in 5 of 11 (45%). EEGs performed before 10 years of age revealed frequent sleep-activated multifocal epileptiform discharges in 8 of 11 (73%). For 6 of 9 (67%) recorded between 1.5 and 6 years of age, spikes became near-continuous during sleep. Interestingly, most patients (9/11, 82%) did not have seizures, and no patient had seizures in the neonatal period. Voltage-clamp recordings of the mutant KCNQ3 channels revealed gain-of-function (GoF) effects. INTERPRETATION: Specific GoF variants in KCNQ3 cause NDD, ASD, and abundant sleep-activated spikes. This new phenotype contrasts both with self-limited neonatal epilepsy due to KCNQ3 partial loss of function, and with the neonatal or infantile onset epileptic encephalopathies due to KCNQ2 GoF. ANN NEUROL 2019;86:181-192.

Published
2019

13. Clinician's guide to genes associated with Rett-like phenotypes-Investigation of a Danish cohort and review of the literature

Author

Schonewolf-Greulich, B, Bisgaard, A-M, Moller, RS, Duno, M, Brondum-Nielsen, K, Kaur, S, Van Bergen, NJ, Lunke, S, Eggers, S, Jespersgaard, C, Christodoulou, J, Tumer, Z, Schonewolf-Greulich, B, Bisgaard, A-M, Moller, RS, Duno, M, Brondum-Nielsen, K, Kaur, S, Van Bergen, NJ, Lunke, S, Eggers, S, Jespersgaard, C, Christodoulou, J, and Tumer, Z

Abstract

The differential diagnostics in Rett syndrome has evolved with the development of next generation sequencing-based techniques and many patients have been diagnosed with other syndromes or variants in newly described genes where the associated phenotype(s) is yet to be fully explored. The term Rett-like refers to phenotypes with distinct overlapping features of Rett syndrome where the clinical criteria are not completely fulfilled. In this study we have combined a review of Rett-like disorders with data from a Danish cohort of 35 patients with Rett-like phenotypes emphasizing the diagnostic overlap with Pitt-Hopkins syndrome, Cornelia de Lange syndrome with SMC1A variants, and epileptic encephalopathies, for example, due to STXBP1 variants. We also found a patient with a pathogenic variant in KCNB1, which has not been previously linked to a Rett-like phenotype. This study underlines the clinical and genetic heterogeneity of a Rett syndrome spectrum, and provides an overview of the Rett syndrome-related genes described to date, and hence serves as a guide for diagnosing patients with Rett-like phenotypes.

Published
2019

14. Mosaic MECP2 variants in males with classical Rett syndrome features, including stereotypical hand movements

Author

Schonewolf-Greulich, B, Bisgaard, A-M, Duno, M, Jespersgaard, C, Rokkjaer, M, Hansen, LK, Tsoutsou, E, Sofokleous, C, Topcu, M, Kaur, S, Van Bergen, NJ, Brondum-Nielsen, K, Larsen, MJ, Sorensen, KP, Christodoulou, J, Fagerberg, CR, Tumer, Z, Schonewolf-Greulich, B, Bisgaard, A-M, Duno, M, Jespersgaard, C, Rokkjaer, M, Hansen, LK, Tsoutsou, E, Sofokleous, C, Topcu, M, Kaur, S, Van Bergen, NJ, Brondum-Nielsen, K, Larsen, MJ, Sorensen, KP, Christodoulou, J, Fagerberg, CR, and Tumer, Z

Abstract

Rett syndrome is rarely suspected in males because of the X-linked dominant inheritance. In the literature, only six male patients have been reported with methyl-CpG-binding protein 2 (MECP2) mosaicism. Next-generation sequencing (NGS) methods have enabled better detection of somatic mosaicism compared to conventional Sanger sequencing; however, mosaics can still be difficult to detect. We present clinical and molecular findings in two males mosaic for a pathogenic MECP2 variant. Both have been reexamined using deep sequencing of DNA isolated from four different cell tissues (blood, muscle, fibroblasts and oral mucosa). Deep sequencing of the different tissues revealed that the variants were present in all tissues. In one patient, the molecular diagnosis could only be established by reexamination after a normal whole exome sequencing, and the other case is an example of reverse genetic diagnostics. Rett syndrome should be considered in males with neurodevelopmental delay and stereotypical hand movements. Subsequent to clinical diagnosis males should be investigated with NGS-based technologies of MECP2 with high read depth and a low threshold for variant calls. If the initial analysis on full blood derived DNA fails to confirm the suspicion, we recommend repeating the analysis on another tissue, preferentially fibroblasts to increase the diagnostic yield.

Published
2019

15. The MECP2 variant c.925C>T (p.Arg309Trp) causes intellectual disability in both males and females without classic features of Rett syndrome

Author

Schonewolf-Greulich, B., Tejada, M.I., Stephens, K., Hadzsiev, K., Gauthier, J., Brondum-Nielsen, K., Pfundt, R.P., Ravn, K., Maortua, H., Gener, B., Martinez-Bouzas, C., Piton, A., Rouleau, G., Clayton-Smith, J., Kleefstra, T., Bisgaard, A.M., and Tumer, Z.

Subjects
congenital, hereditary, and neonatal diseases and abnormalities, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7]
Abstract

Item does not contain fulltext Missense MECP2 variants can have various phenotypic effects ranging from a normal phenotype to typical Rett syndrome (RTT). In females, the phenotype can also be influenced by the X-inactivation pattern. In this study, we present detailed clinical descriptions of six patients with a rare base-pair substitution affecting Arg309 at the C-terminal end of the transcriptional repression domain (TRD). All patients have intellectual disability and present with some RTT features, but they do not fulfill the clinical criteria for typical or atypical RTT. Most of the patients also have mild facial dysmorphism. Intriguingly, the mother of an affected male patient is an asymptomatic carrier of this variant. It is therefore likely that the p.(Arg309Trp) variation does not necessarily lead to male lethality, and it results in a wide range of clinical features in females, probably influenced by different X-inactivation patterns in target tissues.

Published
2016

17. Whole genome characterization of array defined clustered CNVs reveals two distinct complex rearrangement subclasses generated through either non-homologous repair or template switching

Author

Nazaryan-Petersen, L., Eisfeldt, J., Lundin, J., Pettersson, M., Nilsson, D., Wincent, J., Lieden, A., Vezzi, F., Wirta, Valtteri, Käller, Max, Duelund, T., Houssari, R., Pignata, L., Bak, M., Tommerup, N., Lundberg, E. S., Tumer, Z., Lindstrand, A., Nazaryan-Petersen, L., Eisfeldt, J., Lundin, J., Pettersson, M., Nilsson, D., Wincent, J., Lieden, A., Vezzi, F., Wirta, Valtteri, Käller, Max, Duelund, T., Houssari, R., Pignata, L., Bak, M., Tommerup, N., Lundberg, E. S., Tumer, Z., and Lindstrand, A.

Abstract

QC 20200312

Published
2018

18. Phenotypes and genotypes in individuals with SMC1A variants

Author

Huisman, S., Mulder, P.A., Redeker, E., Bader, I., Bisgaard, A.M., Brooks, A., Cereda, A., Cinca, C., Clark, D., Cormier-Daire, V., Deardorff, M.A., Diderich, K., Elting, M., Essen, A. van, Fitzpatrick, D., Gervasini, C., Gillessen-Kaesbach, G., Girisha, K.M., Hilhorst-Hofstee, Y., Hopman, S., Horn, D., Isrie, M., Jansen, S, Jespersgaard, C., Kaiser, F.J., Kaur, M., Kleefstra, T., Krantz, I.D., Lakeman, P., Landlust, A., Lessel, D., Michot, C., Moss, J., Noon, S.E., Oliver, C., Parenti, I., Pie, J., Ramos, F.J., Rieubland, C., Russo, S., Selicorni, A., Tumer, Z., Vorstenbosch, R., Wenger, T.L., Balkom, I.D.C. van, Piening, S., Wierzba, J., Hennekam, R.C., Huisman, S., Mulder, P.A., Redeker, E., Bader, I., Bisgaard, A.M., Brooks, A., Cereda, A., Cinca, C., Clark, D., Cormier-Daire, V., Deardorff, M.A., Diderich, K., Elting, M., Essen, A. van, Fitzpatrick, D., Gervasini, C., Gillessen-Kaesbach, G., Girisha, K.M., Hilhorst-Hofstee, Y., Hopman, S., Horn, D., Isrie, M., Jansen, S, Jespersgaard, C., Kaiser, F.J., Kaur, M., Kleefstra, T., Krantz, I.D., Lakeman, P., Landlust, A., Lessel, D., Michot, C., Moss, J., Noon, S.E., Oliver, C., Parenti, I., Pie, J., Ramos, F.J., Rieubland, C., Russo, S., Selicorni, A., Tumer, Z., Vorstenbosch, R., Wenger, T.L., Balkom, I.D.C. van, Piening, S., Wierzba, J., and Hennekam, R.C.

Abstract

Item does not contain fulltext, 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

19. Phenotypes and genotypes in individuals with SMC1A variants

Author

Huisman, S, Mulder, PA, Redeker, E, Bader, I, Bisgaard, AM, Brooks, A, Cereda, A, Cinca, C, Clark, D, Cormier-Daire, V, Deardorff, MA, Diderich, K, Elting, M, van Essen, A, FitzPatrick, D, Gervasini, C, Gillessen-Kaesbach, G, Girisha, KM, Hilhorst-Hofstee, Y, Hopman, S, Horn, D, Isrie, M, Jansen, S (Silke), Jespersgaard, C, Kaiser, FJ, Kaur, M, Kleefstra, T, Krantz, ID, Lakeman, P, Landlust, A, Lessel, D, Michot, C, Moss, J, Noon, SE, Oliver, C, Parenti, I, Pie, J, Ramos, FJ, Rieubland, C, Russo, S, Selicorni, A, Tumer, Z, van de Vorstenbosch, R, Wenger, TL, van Balkom, I, Piening, S, Wierzba, J, Hennekam, RC, Huisman, S, Mulder, PA, Redeker, E, Bader, I, Bisgaard, AM, Brooks, A, Cereda, A, Cinca, C, Clark, D, Cormier-Daire, V, Deardorff, MA, Diderich, K, Elting, M, van Essen, A, FitzPatrick, D, Gervasini, C, Gillessen-Kaesbach, G, Girisha, KM, Hilhorst-Hofstee, Y, Hopman, S, Horn, D, Isrie, M, Jansen, S (Silke), Jespersgaard, C, Kaiser, FJ, Kaur, M, Kleefstra, T, Krantz, ID, Lakeman, P, Landlust, A, Lessel, D, Michot, C, Moss, J, Noon, SE, Oliver, C, Parenti, I, Pie, J, Ramos, FJ, Rieubland, C, Russo, S, Selicorni, A, Tumer, Z, van de Vorstenbosch, R, Wenger, TL, van Balkom, I, Piening, S, Wierzba, J, and Hennekam, RC

Published
2017

20. Diagnosis and management of Silver-Russell syndrome: first international consensus statement

Author

Wakeling, EL, Brioude, F, Lokulo-Sodipe, O, O'Connell, SM, Salem, J, Bliek, J, Canton, APM, Chrzanowska, KH, Davies, JH, Dias, RP, Dubern, B, Elbracht, M, Giabicani, E, Grimberg, A, Gronskov, K, Koelega, Anita, Jorge, AA, Kagami, M, Linglart, A, Maghnie, M, Mohnike, K, Monk, D, Moore, GE, Murray, PG, Ogata, T, Petit, IO, Russo, S, Said, E, Toumba, M, Tumer, Z, Binder, G, Eggermann, T, Harbison, MD, Temple, IK, Mackay, DJG, Netchine, I, Wakeling, EL, Brioude, F, Lokulo-Sodipe, O, O'Connell, SM, Salem, J, Bliek, J, Canton, APM, Chrzanowska, KH, Davies, JH, Dias, RP, Dubern, B, Elbracht, M, Giabicani, E, Grimberg, A, Gronskov, K, Koelega, Anita, Jorge, AA, Kagami, M, Linglart, A, Maghnie, M, Mohnike, K, Monk, D, Moore, GE, Murray, PG, Ogata, T, Petit, IO, Russo, S, Said, E, Toumba, M, Tumer, Z, Binder, G, Eggermann, T, Harbison, MD, Temple, IK, Mackay, DJG, and Netchine, I

Published
2017

21. TS-EUROTRAIN: A European-Wide Investigation and Training Network on the Etiology and Pathophysiology of Gilles de la Tourette Syndrome

Author

Forde, J.N., Kanaan, A.S., Widomska, J.M., Padmanabhuni, S.S., Nespoli, E., Alexander, J., Rodriguez Arranz, J.I., Fan, S., Houssari, R., Nawaz, M.S., Rizzo, F., Pagliaroli, L., Zilhao, N.R., Aranyi, T., Barta, C., Boeckers, T.M., Boomsma, D.I., Buisman, W.R., Buitelaar, J.K., Cath, D., Dietrich, A., Driessen, N., Drineas, P., Dunlap, M., Gerasch, S., Glennon, J.C., Hengerer, B., Heuvel, O.A. van den, Jespersgaard, C., Moller, H.E., Muller-Vahl, K.R., Openneer, T.J., Poelmans, G.J.V., Pouwels, P.J., Scharf, J.M., Stefansson, H., Tumer, Z., Veltman, D.J., Werf, Y.D. van der, Hoekstra, P.J., Ludolph, A., Paschou, P., Forde, J.N., Kanaan, A.S., Widomska, J.M., Padmanabhuni, S.S., Nespoli, E., Alexander, J., Rodriguez Arranz, J.I., Fan, S., Houssari, R., Nawaz, M.S., Rizzo, F., Pagliaroli, L., Zilhao, N.R., Aranyi, T., Barta, C., Boeckers, T.M., Boomsma, D.I., Buisman, W.R., Buitelaar, J.K., Cath, D., Dietrich, A., Driessen, N., Drineas, P., Dunlap, M., Gerasch, S., Glennon, J.C., Hengerer, B., Heuvel, O.A. van den, Jespersgaard, C., Moller, H.E., Muller-Vahl, K.R., Openneer, T.J., Poelmans, G.J.V., Pouwels, P.J., Scharf, J.M., Stefansson, H., Tumer, Z., Veltman, D.J., Werf, Y.D. van der, Hoekstra, P.J., Ludolph, A., and Paschou, P.

Abstract

Contains fulltext : 168171.pdf (publisher's version ) (Open Access), Gilles de la Tourette Syndrome (GTS) is characterized by the presence of multiple motor and phonic tics with a fluctuating course of intensity, frequency, and severity. Up to 90% of patients with GTS present with comorbid conditions, most commonly attention-deficit/hyperactivity disorder (ADHD), and obsessive-compulsive disorder (OCD), thus providing an excellent model for the exploration of shared etiology across disorders. TS-EUROTRAIN (FP7-PEOPLE-2012-ITN, Grant Agr.No. 316978) is a Marie Curie Initial Training Network (http://ts-eurotrain.eu) that aims to elucidate the complex etiology of the onset and clinical course of GTS, investigate the neurobiological underpinnings of GTS and related disorders, translate research findings into clinical applications, and establish a pan-European infrastructure for the study of GTS. This includes the challenges of (i) assembling a large genetic database for the evaluation of the genetic architecture with high statistical power; (ii) exploring the role of gene-environment interactions including the effects of epigenetic phenomena; (iii) employing endophenotype-based approaches to understand the shared etiology between GTS, OCD, and ADHD; (iv) establishing a developmental animal model for GTS; (v) gaining new insights into the neurobiological mechanisms of GTS via cross-sectional and longitudinal neuroimaging studies; and (vi) partaking in outreach activities including the dissemination of scientific knowledge about GTS to the public. Fifteen partners from academia and industry and 12 PhD candidates pursue the project. Here, we aim to share the design of an interdisciplinary project, showcasing the potential of large-scale collaborative efforts in the field of GTS. Our ultimate aims are to elucidate the complex etiology and neurobiological underpinnings of GTS, translate research findings into clinical applications, and establish Pan-European infrastructure for the study of GTS and associated disorders.

Published
2016

22. Association of AADAC Deletion and Gilles de la Tourette Syndrome in a Large European Cohort

Author

Bertelsen, B., Stefansson, H., Jensen, L., Melchior, L., Debes, N. Mol, Groth, C., Skov, L., Werge, T., Karagiannidis, I., Tarnok, Z., Barta, C., Nagy, P., Farkas, L., Brondum-Nielsen, K., Rizzo, R., Gulisano, M., Rujescu, D., Kiemeney, L.A.L.M., Tosato, S., Nawaz, M.S., Ingason, A., Unnsteinsdottir, U., Steinberg, S., Ludvigsson, P., Stefansson, K., Kuss, A.W., Paschou, P., Cath, D., Hoekstra, P.J., Muller-Vahl, K., Stuhrmann, M., Silahtaroglu, A., Pfundt, R.P., Tumer, Z., Bertelsen, B., Stefansson, H., Jensen, L., Melchior, L., Debes, N. Mol, Groth, C., Skov, L., Werge, T., Karagiannidis, I., Tarnok, Z., Barta, C., Nagy, P., Farkas, L., Brondum-Nielsen, K., Rizzo, R., Gulisano, M., Rujescu, D., Kiemeney, L.A.L.M., Tosato, S., Nawaz, M.S., Ingason, A., Unnsteinsdottir, U., Steinberg, S., Ludvigsson, P., Stefansson, K., Kuss, A.W., Paschou, P., Cath, D., Hoekstra, P.J., Muller-Vahl, K., Stuhrmann, M., Silahtaroglu, A., Pfundt, R.P., and Tumer, Z.

Abstract

Item does not contain fulltext, BACKGROUND: Gilles de la Tourette syndrome (GTS) is a complex neuropsychiatric disorder with a strong genetic influence where copy number variations are suggested to play a role in disease pathogenesis. In a previous small-scale copy number variation study of a GTS cohort (n = 111), recurrent exon-affecting microdeletions of four genes, including the gene encoding arylacetamide deacetylase (AADAC), were observed and merited further investigations. METHODS: We screened a Danish cohort of 243 GTS patients and 1571 control subjects for submicroscopic deletions and duplications of these four genes. The most promising candidate gene, AADAC, identified in this Danish discovery sample was further investigated in cohorts from Iceland, the Netherlands, Hungary, Germany, and Italy, and a final meta-analysis, including a total of 1181 GTS patients and 118,730 control subjects from these six European countries, was performed. Subsequently, expression of the candidate gene in the central nervous system was investigated using human and mouse brain tissues. RESULTS: In the Danish cohort, we identified eight patients with overlapping deletions of AADAC. Investigation of the additional five countries showed a significant association between the AADAC deletion and GTS, and a final meta-analysis confirmed the significant association (p = 4.4 x 10(-4); odds ratio = 1.9; 95% confidence interval = 1.33-2.71). Furthermore, RNA in situ hybridization and reverse transcription-polymerase chain reaction studies revealed that AADAC is expressed in several brain regions previously implicated in GTS pathology. CONCLUSIONS: AADAC is a candidate susceptibility factor for GTS and the present findings warrant further genomic and functional studies to investigate the role of this gene in the pathogenesis of GTS.

Published
2016

23. Prenatal molecular testing for Beckwith-Wiedemann and Silver-Russell syndromes: A challenge for molecular analysis and genetic counseling.

Author

Prawitt D., Begemann M., Soellner L., Eggermann K., Tenorio J., Nevado J., Moore G.E., Mackay D.J.G., Temple K., Gillessen-Kaesbach G., Ogata T., Weksberg R., Algar E., Lapunzina P., Eggermann T., Brioude F., Russo S., Lombardi M.P., Bliek J., Maher E.R., Larizza L., Netchine I., Gonzales M., Gronskov K., Tumer Z., Monk D., Mannens M., Chrzanowska K., Walasek M.K., Prawitt D., Begemann M., Soellner L., Eggermann K., Tenorio J., Nevado J., Moore G.E., Mackay D.J.G., Temple K., Gillessen-Kaesbach G., Ogata T., Weksberg R., Algar E., Lapunzina P., Eggermann T., Brioude F., Russo S., Lombardi M.P., Bliek J., Maher E.R., Larizza L., Netchine I., Gonzales M., Gronskov K., Tumer Z., Monk D., Mannens M., Chrzanowska K., and Walasek M.K.

Abstract

Beckwith-Wiedemann and Silver-Russell syndromes (BWS/SRS) are two imprinting disorders (IDs) associated with disturbances of the 11p15.5 chromosomal region. In BWS, epimutations and genomic alterations within 11p15.5 are observed in >70% of patients, whereas in SRS they are observed in about 60% of the cases. In addition, 10% of the SRS patients carry a maternal uniparental disomy of chromosome 7 11p15.5. There is an increasing demand for prenatal testing of these disorders owing to family history, indicative prenatal ultrasound findings or aberrations involving chromosomes 7 and 11. The complex molecular findings underlying these disorders are a challenge not only for laboratories offering these tests but also for geneticists counseling affected families. The scope of counseling must consider the range of detectable disturbances and their origin, the lack of precise quantitative knowledge concerning the inheritance and recurrence risks for the epigenetic abnormalities, which are hallmarks of these developmental disorders. In this paper, experts in the field of BWS and SRS, including members of the European network of congenital IDs (EUCID.net; www.imprinting-disorders.eu), put together their experience and work in the field of 11p15.5-Associated IDs with a focus on prenatal testing. Altogether, prenatal tests of 160 fetuses (122 referred for BWS, 38 for SRS testing) from 5 centers were analyzed and reviewed. We summarize the current knowledge on BWS and SRS with respect to diagnostic testing, the consequences for prenatal genetic testing and counseling and our cumulative experience in dealing with these disorders.Copyright © 2016 Macmillan Publishers Limited.

Published
2016

24. EMQN best practice guidelines for the molecular genetic testing and reporting of chromosome 11p15 imprinting disorders: Silver-Russell and Beckwith-Wiedemann syndrome.

Author

MacKay D.J., Riccio A., Weksberg R., Lapunzina P., Gronskov K., Eggermann T., Eggermann K., Bliek J., Brioude F., Algar E., Buiting K., Russo S., Tumer Z., Monk D., Moore G., Antoniadi T., MacDonald F., Netchine I., Lombardi P., Soellner L., Begemann M., Prawitt D., Maher E.R., Mannens M., MacKay D.J., Riccio A., Weksberg R., Lapunzina P., Gronskov K., Eggermann T., Eggermann K., Bliek J., Brioude F., Algar E., Buiting K., Russo S., Tumer Z., Monk D., Moore G., Antoniadi T., MacDonald F., Netchine I., Lombardi P., Soellner L., Begemann M., Prawitt D., Maher E.R., and Mannens M.

Abstract

Molecular genetic testing for the 11p15-associated imprinting disorders Silver-Russell and Beckwith-Wiedemann syndrome (SRS, BWS) is challenging because of the molecular heterogeneity and complexity of the affected imprinted regions. With the growing knowledge on the molecular basis of these disorders and the demand for molecular testing, it turned out that there is an urgent need for a standardized molecular diagnostic testing and reporting strategy. Based on the results from the first external pilot quality assessment schemes organized by the European Molecular Quality Network (EMQN) in 2014 and in context with activities of the European Network of Imprinting Disorders (EUCID.net) towards a consensus in diagnostics and management of SRS and BWS, best practice guidelines have now been developed. Members of institutions working in the field of SRS and BWS diagnostics were invited to comment, and in the light of their feedback amendments were made. The final document was ratified in the course of an EMQN best practice guideline meeting and is in accordance with the general SRS and BWS consensus guidelines, which are in preparation. These guidelines are based on the knowledge acquired from peer-reviewed and published data, as well as observations of the authors in their practice. However, these guidelines can only provide a snapshot of current knowledge at the time of manuscript submission and readers are advised to keep up with the literature.Copyright © 2016 Macmillan Publishers Limited, part of Springer Nature. All rights reserved.

Published
2016

25. EMQN best practice guidelines for the molecular genetic testing and reporting of chromosome 11p15 imprinting disorders: Silver-Russell and Beckwith-Wiedemann syndrome

Author

Eggermann, K, Bliek, J, Brioude, F, Algar, E, Buiting, K, Russo, S, Tumer, Z, Monk, D, Moore, G, Antoniadi, T, Macdonald, F, Netchine, I, Lombardi, P, Soellner, L, Begemann, M, Prawitt, D, Maher, ER, Mannens, M, Riccio, A, Weksberg, R, Lapunzina, P, Gronskov, K, Mackay, DJG, Eggermann, T, Eggermann, K, Bliek, J, Brioude, F, Algar, E, Buiting, K, Russo, S, Tumer, Z, Monk, D, Moore, G, Antoniadi, T, Macdonald, F, Netchine, I, Lombardi, P, Soellner, L, Begemann, M, Prawitt, D, Maher, ER, Mannens, M, Riccio, A, Weksberg, R, Lapunzina, P, Gronskov, K, Mackay, DJG, and Eggermann, T

Abstract

Molecular genetic testing for the 11p15-associated imprinting disorders Silver-Russell and Beckwith-Wiedemann syndrome (SRS, BWS) is challenging because of the molecular heterogeneity and complexity of the affected imprinted regions. With the growing knowledge on the molecular basis of these disorders and the demand for molecular testing, it turned out that there is an urgent need for a standardized molecular diagnostic testing and reporting strategy. Based on the results from the first external pilot quality assessment schemes organized by the European Molecular Quality Network (EMQN) in 2014 and in context with activities of the European Network of Imprinting Disorders (EUCID.net) towards a consensus in diagnostics and management of SRS and BWS, best practice guidelines have now been developed. Members of institutions working in the field of SRS and BWS diagnostics were invited to comment, and in the light of their feedback amendments were made. The final document was ratified in the course of an EMQN best practice guideline meeting and is in accordance with the general SRS and BWS consensus guidelines, which are in preparation. These guidelines are based on the knowledge acquired from peer-reviewed and published data, as well as observations of the authors in their practice. However, these guidelines can only provide a snapshot of current knowledge at the time of manuscript submission and readers are advised to keep up with the literature.

Published
2016

26. Refinement of the critical 2p25.3 deletion region: the role of MYT1L in intellectual disability and obesity

Author

Rocker, N. de, Vergult, S., Koolen, D.A., Jacobs, E., Hoischen, A., Zeesman, S., Bang, B., Bena, F., Bockaert, N., Bongers, E.M.H.F., Ravel, T. de, Devriendt, K., Giglio, S., Faivre, L., Joss, S., Maas, S., Marle, N., Novara, F., Nowaczyk, M.J., Peeters, H., Polstra, A., Roelens, F., Rosenberg, C., Thevenon, J., Tumer, Z., Vanhauwaert, S., Varvagiannis, K., Willaert, A., Willemsen, M.H., Willems, M., Zuffardi, O., Coucke, P., Speleman, F., Eichler, E.E., Kleefstra, T., Menten, B., Rocker, N. de, Vergult, S., Koolen, D.A., Jacobs, E., Hoischen, A., Zeesman, S., Bang, B., Bena, F., Bockaert, N., Bongers, E.M.H.F., Ravel, T. de, Devriendt, K., Giglio, S., Faivre, L., Joss, S., Maas, S., Marle, N., Novara, F., Nowaczyk, M.J., Peeters, H., Polstra, A., Roelens, F., Rosenberg, C., Thevenon, J., Tumer, Z., Vanhauwaert, S., Varvagiannis, K., Willaert, A., Willemsen, M.H., Willems, M., Zuffardi, O., Coucke, P., Speleman, F., Eichler, E.E., Kleefstra, T., and Menten, B.

Abstract

Item does not contain fulltext, PURPOSE: Submicroscopic deletions of chromosome band 2p25.3 are associated with intellectual disability and/or central obesity. Although MYT1L is believed to be a critical gene responsible for intellectual disability, so far no unequivocal data have confirmed this hypothesis. METHODS: In this study we evaluated a cohort of 22 patients (15 sporadic patients and two families) with a 2p25.3 aberration to further refine the clinical phenotype and to delineate the role of MYT1L in intellectual disability and obesity. In addition, myt1l spatiotemporal expression in zebrafish embryos was analyzed by quantitative polymerase chain reaction and whole-mount in situ hybridization. RESULTS: Complete MYT1L deletion, intragenic deletion, or duplication was observed in all sporadic patients, in addition to two patients with a de novo point mutation in MYT1L. The familial cases comprise a 6-Mb deletion in a father and his three children and a 5' MYT1L overlapping duplication in a father and his two children. Expression analysis in zebrafish embryos shows specific myt1l expression in the developing brain. CONCLUSION: Our data strongly strengthen the hypothesis that MYT1L is the causal gene for the observed syndromal intellectual disability. Moreover, because 17 patients present with obesity/overweight, haploinsufficiency of MYT1L might predispose to weight problems with childhood onset.Genet Med 17 6, 460-466.

Published
2015

28. X-linked congenital ptosis and associated intellectual disability, short stature, microcephaly, cleft palate, digital and genital abnormalities define novel Xq25q26 duplication syndrome

Author

Moller, R.S., Jensen, L.R., Maas, S.M., Filmus, J., Capurro, M., Hansen, C., Marcelis, C.L.M., Ravn, K., Andrieux, J., Mathieu, M., Kirchhoff, M., Rodningen, O.K., Leeuw, N. de, Yntema, H.G., Froyen, G., Vandewalle, J., Ballon, K., Klopocki, E., Joss, S., Tolmie, J., Knegt, A.C., Lund, A.M., Hjalgrim, H., Kuss, A.W., Tommerup, N., Ullmann, R., Brouwer, A.P.M. de, Stromme, P., Kjaergaard, S., Tumer, Z., Kleefstra, T., Moller, R.S., Jensen, L.R., Maas, S.M., Filmus, J., Capurro, M., Hansen, C., Marcelis, C.L.M., Ravn, K., Andrieux, J., Mathieu, M., Kirchhoff, M., Rodningen, O.K., Leeuw, N. de, Yntema, H.G., Froyen, G., Vandewalle, J., Ballon, K., Klopocki, E., Joss, S., Tolmie, J., Knegt, A.C., Lund, A.M., Hjalgrim, H., Kuss, A.W., Tommerup, N., Ullmann, R., Brouwer, A.P.M. de, Stromme, P., Kjaergaard, S., Tumer, Z., and Kleefstra, T.

Abstract

Item does not contain fulltext, Submicroscopic duplications along the long arm of the X-chromosome with known phenotypic consequences are relatively rare events. The clinical features resulting from such duplications are various, though they often include intellectual disability, microcephaly, short stature, hypotonia, hypogonadism and feeding difficulties. Female carriers are often phenotypically normal or show a similar but milder phenotype, as in most cases the X-chromosome harbouring the duplication is subject to inactivation. Xq28, which includes MECP2 is the major locus for submicroscopic X-chromosome duplications, whereas duplications in Xq25 and Xq26 have been reported in only a few cases. Using genome-wide array platforms we identified overlapping interstitial Xq25q26 duplications ranging from 0.2 to 4.76 Mb in eight unrelated families with in total five affected males and seven affected females. All affected males shared a common phenotype with intrauterine- and postnatal growth retardation and feeding difficulties in childhood. Three had microcephaly and two out of five suffered from epilepsy. In addition, three males had a distinct facial appearance with congenital bilateral ptosis and large protruding ears and two of them showed a cleft palate. The affected females had various clinical symptoms similar to that of the males with congenital bilateral ptosis in three families as most remarkable feature. Comparison of the gene content of the individual duplications with the respective phenotypes suggested three critical regions with candidate genes (AIFM1, RAB33A, GPC3 and IGSF1) for the common phenotypes, including candidate loci for congenital bilateral ptosis, small head circumference, short stature, genital and digital defects.

Published
2014

29. Delineation of an interstitial 9q22 deletion in basal cell nevus syndrome

Author

Boonen, S., Stahl, D., Kreiborg, S., Rosenberg, T., Kalscheuer, V., Larsen, L., Tommerup, N., Brondum-Nielsen, K., and Tumer, Z.

Subjects
stomatognathic diseases
Abstract

Basal cell nevus syndrome (Gorlin syndrome) is an autosomal dominant disorder characterized by the presence of multiple basal cell carcinomas (BCC), odontogenic keratocysts, palmoplantar pits, and calcification in the falx cerebri caused by mutational inactivation of the PTCH gene. In few cases, the syndrome is due to a microdeletion at 9q22. Using high-resolution chromosome analysis we have identified a patient with the karyotype, 46,XY,del(9)(q21.3q31) de novo. He had typical clinical features consistent with basal cell nevus syndrome, but also additional features likely to be caused by loss of additional chromosomal material in this region. The deletion breakpoints were characterized with fluorescence in situ hybridization (FISH) analysis using BAC clones. The 15 Mb long deletion includes 87 RefSeq genes including PTCH. Hemizygosity of one or more genes might contribute to the additional symptoms observed in this patient.

Published
2005

31. Transient Neonatal Diabetes, ZFP57, and Hypomethylation of Multiple Imprinted Loci A detailed follow-up

Author

Boonen, SE, Mackay, DJG, Hahnemann, JMD, Docherty, L, Gronskov, K, Lehmann, A, Larsen, LG, Haemers, AP, Kockaerts, Y, Dooms, L, Dung, CV, Ngoc, CTB, Phuong, BN, Kordonouri, O, Sundberg, F, Dayanikli, P, Puthi, V, Acerini, C, Massoud, AF, Tumer, Z, Temple, IK, Boonen, SE, Mackay, DJG, Hahnemann, JMD, Docherty, L, Gronskov, K, Lehmann, A, Larsen, LG, Haemers, AP, Kockaerts, Y, Dooms, L, Dung, CV, Ngoc, CTB, Phuong, BN, Kordonouri, O, Sundberg, F, Dayanikli, P, Puthi, V, Acerini, C, Massoud, AF, Tumer, Z, and Temple, IK

Abstract

OBJECTIVE: Transient neonatal diabetes mellitus 1 (TNDM1) is the most common cause of diabetes presenting at birth. Approximately 5% of the cases are due to recessive ZFP57 mutations, causing hypomethylation at the TNDM locus and other imprinted loci (HIL). This has consequences for patient care because it has impact on the phenotype and recurrence risk for families. We have determined the genotype, phenotype, and epigenotype of the first 10 families to alert health professionals to this newly described genetic subgroup of diabetes. RESEARCH DESIGN AND METHODS: The 10 families (14 homozygous/compound heterozygous individuals) with ZFP57 mutations were ascertained through TNDM1 diagnostic testing. ZFP57 was sequenced in probands and their relatives, and the methylation levels at multiple maternally and paternally imprinted loci were determined. Medical and family histories were obtained, and clinical examination was performed. RESULTS: The key clinical features in probands were transient neonatal diabetes, intrauterine growth retardation, macroglossia, heart defects, and developmental delay. However, the finding of two homozygous relatives without diabetes and normal intelligence showed that the phenotype could be very variable. The epigenotype always included total loss of methylation at the TNDM1 locus and reproducible combinations of differential hypomethylation at other maternally imprinted loci, including tissue mosaicism. CONCLUSIONS: There is yet no clear genotype-epigenotype-phenotype correlation to explain the variable clinical presentation, and this results in difficulties predicting the prognosis of affected individuals. However, many cases have a more severe phenotype than seen in other causes of TNDM1. Further cases and global epigenetic testing are needed to clarify this.

Published
2013

32. Human CCS gene: genomic organization and exclusion as a candidate for amyotrophic lateral sclerosis (ALS)

Author

Silahtaroglu, AN Brondum-Nielsen, K Gredal, O Werdelin, L and Panas, M Petersen, MB Tommerup, N Tumer, Z

Subjects
fungi
Abstract

Background: Amyotrophic lateral sclerosis (ALS) is a progressive lethal disorder of large motor neurons of the spinal cord and brain. In approximately 20% of the familial and 2% of sporadic cases the disease is due to a defect in the gene encoding the cytosolic antioxidant enzyme Cu, Zn-superoxide dismutase (SOD1). The underlying molecular defect is known only in a very small portion of the remaining cases and therefore involvement of other genes is likely. As SOD1 receives copper, essential for its normal function, by the copper chaperone, CCS (Copper Chaperone for SOD), we considered CCS as a potential candidate gene for ALS. Results: We have characterized the genomic organization of CCS and determined exon-intron boundaries. The 823 bp coding region of the CCS is organized in 8 exons. We have evaluated involvement of the CCS in ALS by sequencing the entire coding region for mutations in 20 sporadic ALS patients. Conclusions: No causative mutations for the ALS have been detected in the CCS gene in 20 sporadic ALS patients analyzed, but an intragenic single nucleotide polymorphism has been identified.

Published
2002

33. Metaphase FISH on a Chip: Miniaturized Microfluidic Device for Fluorescence in situ Hybridization

Author

Vedarethinam, Indumathi, Shah, Pranjul Jaykumar, Dimaki, Maria, Tumer, Z., Tommerup, N., Svendsen, Winnie Edith, Vedarethinam, Indumathi, Shah, Pranjul Jaykumar, Dimaki, Maria, Tumer, Z., Tommerup, N., and Svendsen, Winnie Edith

Abstract

Fluorescence in situ Hybridization (FISH) is a major cytogenetic technique for clinical genetic diagnosis of both inherited and acquired chromosomal abnormalities. Although FISH techniques have evolved and are often used together with other cytogenetic methods like CGH, PRINS and PNA-FISH, the process continues to be a manual, labour intensive, expensive and time consuming technique, often taking over 3-5 days, even in dedicated labs. We have developed a novel microFISH device to perform metaphase FISH on a chip which overcomes many shortcomings of the current laboratory protocols. This work also introduces a novel splashing device for preparing metaphase spreads on a microscope glass slide, followed by a rapid adhesive tape-based bonding protocol leading to rapid fabrication of the microFISH device. The microFISH device allows for an optimized metaphase FISH protocol on a chip with over a 20-fold reduction in the reagent volume. This is the first demonstration of metaphase FISH on a microfluidic device and offers a possibility of automation and significant cost reduction of many routine diagnostic tests of genetic anomalies.

Published
2010

34. Molecular characterization of two patients with de novo interstitial deletions in 4q22-q24.

Author

Algemeen Onderzoek DGK, Dep Infectieziekten Immunologie, Hilhorst-Hofstee, Y., Tumer, Z., Born, P., Knijnenburg, J., Hansson, K., Yatawara, V., Steensberg, J., Ullman, R., Arkesteijn, G., Tommerup, N., Larsen, L.A., Algemeen Onderzoek DGK, Dep Infectieziekten Immunologie, Hilhorst-Hofstee, Y., Tumer, Z., Born, P., Knijnenburg, J., Hansson, K., Yatawara, V., Steensberg, J., Ullman, R., Arkesteijn, G., Tommerup, N., and Larsen, L.A.

Published
2009

35. Investigation of 4q-deletion in two unrelated patients using array CGH

Author

Kaalund, Sanne Simone, Møller, Rikke Steensbjerre, Teszas, A., Miranda, M., Kosztolanyi, G., Ullmann, R., Tommerup, Niels, Tumer, Z., Kaalund, Sanne Simone, Møller, Rikke Steensbjerre, Teszas, A., Miranda, M., Kosztolanyi, G., Ullmann, R., Tommerup, Niels, and Tumer, Z.

Abstract

Udgivelsesdato: 2008-Sep-15

Published
2008

36. Multiple hypomethylation of maternally imprinted genes

Author

Tumer, Z., Temple, K., Mackay, D.J., Boonen, Susanne Eriksen, Olsen, B.S., Mortensen, H.B., Porksen, S., Bondrum-Nielsen, K., Tommerup, Niels, Hahnemann, J.M., Tumer, Z., Temple, K., Mackay, D.J., Boonen, Susanne Eriksen, Olsen, B.S., Mortensen, H.B., Porksen, S., Bondrum-Nielsen, K., Tommerup, Niels, and Hahnemann, J.M.

Abstract

Udgivelsesdato: 2008

Published
2008

38. Truncation of the Down syndrome candidate gene DYRK1A in two unrelated patients with microcephaly

Author

Møller, Rikke Steensbjerre, Kubart, S., Hoeltzenbein, M., Heye, B., Vogel, I., Hansen, C.P., Menzel, C, Ullmann, R., Tommerup, Niels, Ropers, H.H., Tumer, Z., Kalscheuer, V.M., Møller, Rikke Steensbjerre, Kubart, S., Hoeltzenbein, M., Heye, B., Vogel, I., Hansen, C.P., Menzel, C, Ullmann, R., Tommerup, Niels, Ropers, H.H., Tumer, Z., and Kalscheuer, V.M.

Abstract

Udgivelsesdato: 2008/5

Published
2008

40. Mowat-Wilson syndrome: an underdiagnosed syndrome?

Author

Engenheiro, E., Møller, Rikke Steensbjerre, Pinto, M., Soares, G., Nikanorova, M., Carreira, I.M., Ullmann, R., Tommerup, Niels, Tumer, Z., Engenheiro, E., Møller, Rikke Steensbjerre, Pinto, M., Soares, G., Nikanorova, M., Carreira, I.M., Ullmann, R., Tommerup, Niels, and Tumer, Z.

Abstract

Udgivelsesdato: 2008/6

Published
2008

41. Deletions and rearrangements of the H19/IGF2 enhancer region in patients with Silver-Russell syndrome and growth retardation

Author

Gronskov, K., primary, Poole, R. L., additional, Hahnemann, J. M. D., additional, Thomson, J., additional, Tumer, Z., additional, Brondum-Nielsen, K., additional, Murphy, R., additional, Ravn, K., additional, Melchior, L., additional, Dedic, A., additional, Dolmer, B., additional, Temple, I. K., additional, Boonen, S. E., additional, and Mackay, D. J. G., additional

Published
2011
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45. Molecular cytogenetic detection of 9q34 breakpoints associated with nail patella syndrome.

Author

Silahtaroglu, A., Hol, F.A., Jensen, P.K.A., Erdel, M., Duba, H.C., Geurds, M.P.A., Knoers, N.V.A.M., Mariman, E.C.M., Tumer, Z., Utermann, G., Wirth, J., Brugge, M., Tommerup, N., Silahtaroglu, A., Hol, F.A., Jensen, P.K.A., Erdel, M., Duba, H.C., Geurds, M.P.A., Knoers, N.V.A.M., Mariman, E.C.M., Tumer, Z., Utermann, G., Wirth, J., Brugge, M., and Tommerup, N.

Abstract

Item does not contain fulltext

Published
1999

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