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1. Correction to: Assessment of gene–disease associations and recommendations for genetic testing for somatic variants in vascular anomalies by VASCERN-VASCA

Author

Revencu, Nicole, Eijkelenboom, Astrid, Bracquemart, Claire, Alhopuro, Pia, Armstrong, Judith, Baselga, Eulalia, Cesario, Claudia, Dentici, Maria Lisa, Eyries, Melanie, Frisk, Sofia, Karstensen, Helena Gásdal, Gene‑Olaciregui, Nagore, Kivirikko, Sirpa, Lavarino, Cinzia, Mero, Inger‑Lise, Michiels, Rodolphe, Pisaneschi, Elisa, Schönewolf‑Greulich, Bitten, Wieland, Ilse, Zenker, Martin, and Vikkula, Miikka

Published
2024
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2. Assessment of gene–disease associations and recommendations for genetic testing for somatic variants in vascular anomalies by VASCERN-VASCA

Author

Revencu, Nicole, Eijkelenboom, Astrid, Bracquemart, Claire, Alhopuro, Pia, Armstrong, Judith, Baselga, Eulalia, Cesario, Claudia, Dentici, Maria Lisa, Eyries, Melanie, Frisk, Sofia, Karstensen, Helena Gásdal, Gene-Olaciregui, Nagore, Kivirikko, Sirpa, Lavarino, Cinzia, Mero, Inger-Lise, Michiels, Rodolphe, Pisaneschi, Elisa, Schönewolf-Greulich, Bitten, Wieland, Ilse, Zenker, Martin, and Vikkula, Miikka

Published
2024
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3. DLG4-related synaptopathy: a new rare brain disorder

Author

Rodríguez-Palmero, Agustí, Boerrigter, Melissa Maria, Gómez-Andrés, David, Aldinger, Kimberly A., Marcos-Alcalde, Íñigo, Popp, Bernt, Everman, David B., Lovgren, Alysia Kern, Arpin, Stephanie, Bahrambeigi, Vahid, Beunders, Gea, Bisgaard, Anne-Marie, Bjerregaard, V. A., Bruel, Ange-Line, Challman, Thomas D., Cogné, Benjamin, Coubes, Christine, de Man, Stella A., Denommé-Pichon, Anne-Sophie, Dye, Thomas J., Elmslie, Frances, Feuk, Lars, García-Miñaúr, Sixto, Gertler, Tracy, Giorgio, Elisa, Gruchy, Nicolas, Haack, Tobias B., Haldeman-Englert, Chad R., Haukanes, Bjørn Ivar, Hoyer, Juliane, Hurst, Anna C. E., Isidor, Bertrand, Soller, Maria Johansson, Kushary, Sulagna, Kvarnung, Malin, Landau, Yuval E., Leppig, Kathleen A., Lindstrand, Anna, Kleinendorst, Lotte, MacKenzie, Alex, Mandrile, Giorgia, Mendelsohn, Bryce A., Moghadasi, Setareh, Morton, Jenny E., Moutton, Sebastien, Müller, Amelie J., O’Leary, Melanie, Pacio-Míguez, Marta, Palomares-Bralo, Maria, Parikh, Sumit, Pfundt, Rolph, Pode-Shakked, Ben, Rauch, Anita, Repnikova, Elena, Revah-Politi, Anya, Ross, Meredith J., Ruivenkamp, Claudia A. L., Sarrazin, Elisabeth, Savatt, Juliann M., Schlüter, Agatha, Schönewolf-Greulich, Bitten, Shad, Zohra, Shaw-Smith, Charles, Shieh, Joseph T., Shohat, Motti, Spranger, Stephanie, Thiese, Heidi, Mau-Them, Frederic Tran, van Bon, Bregje, van de Burgt, Ineke, van de Laar, Ingrid M. B. H., van Drie, Esmée, van Haelst, Mieke M., van Ravenswaaij-Arts, Conny M., Verdura, Edgard, Vitobello, Antonio, Waldmüller, Stephan, Whiting, Sharon, Zweier, Christiane, Prada, Carlos E., de Vries, Bert B. A., Dobyns, William B., Reiter, Simone F., Gómez-Puertas, Paulino, Pujol, Aurora, and Tümer, Zeynep

Published
2021
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4. Mandibulofacial Dysostosis with Microcephaly: Mutation and Database Update

Author

Huang, Lijia, Vanstone, Megan R, Hartley, Taila, Osmond, Matthew, Barrowman, Nick, Allanson, Judith, Baker, Laura, Dabir, Tabib A, Dipple, Katrina M, Dobyns, William B, Estrella, Jane, Faghfoury, Hanna, Favaro, Francine P, Goel, Himanshu, Gregersen, Pernille A, Gripp, Karen W, Grix, Art, Guion‐Almeida, Maria‐Leine, Harr, Margaret H, Hudson, Cindy, Hunter, Alasdair GW, Johnson, John, Joss, Shelagh K, Kimball, Amy, Kini, Usha, Kline, Antonie D, Lauzon, Julie, Lildballe, Dorte L, López‐González, Vanesa, Martinezmoles, Johanna, Meldrum, Cliff, Mirzaa, Ghayda M, Morel, Chantal F, Morton, Jenny EV, Pyle, Louise C, Quintero‐Rivera, Fabiola, Richer, Julie, Scheuerle, Angela E, Schönewolf‐Greulich, Bitten, Shears, Deborah J, Silver, Josh, Smith, Amanda C, Temple, I Karen, Center, UCLA Clinical Genomics, de Kamp, Jiddeke M, Dijk, Fleur S, Vandersteen, Anthony M, White, Sue M, Zackai, Elaine H, Zou, Ruobing, Consortium, Care4Rare Canada, Bulman, Dennis E, Boycott, Kym M, and Lines, Matthew A

Subjects
Pediatric, Congenital Structural Anomalies, Rare Diseases, Genetics, Prevention, Human Genome, Neurosciences, Clinical Research, Dental/Oral and Craniofacial Disease, 2.1 Biological and endogenous factors, Aetiology, Congenital, Abnormalities, Multiple, Amino Acid Motifs, Databases, Genetic, Gene Expression, Haploinsufficiency, Hearing Loss, Humans, Intellectual Disability, Mandibulofacial Dysostosis, Microcephaly, Models, Molecular, Molecular Sequence Data, Mutation, Penetrance, Peptide Elongation Factors, Phenotype, Protein Structure, Secondary, Protein Structure, Tertiary, RNA Splicing, Ribonucleoprotein, U5 Small Nuclear, Spliceosomes, EFTUD2, mandibulofacial dysostosis with microcephaly, MFDM, mandibulofacial dysostosis Guion-Almeida type, mandibulofacial dysostosis, microcephaly, UCLA Clinical Genomics Center, Care4Rare Canada Consortium, Clinical Sciences, Genetics & Heredity
Abstract

Mandibulofacial dysostosis with microcephaly (MFDM) is a multiple malformation syndrome comprising microcephaly, craniofacial anomalies, hearing loss, dysmorphic features, and, in some cases, esophageal atresia. Haploinsufficiency of a spliceosomal GTPase, U5-116 kDa/EFTUD2, is responsible. Here, we review the molecular basis of MFDM in the 69 individuals described to date, and report mutations in 38 new individuals, bringing the total number of reported individuals to 107 individuals from 94 kindreds. Pathogenic EFTUD2 variants comprise 76 distinct mutations and seven microdeletions. Among point mutations, missense substitutions are infrequent (14 out of 76; 18%) relative to stop-gain (29 out of 76; 38%), and splicing (33 out of 76; 43%) mutations. Where known, mutation origin was de novo in 48 out of 64 individuals (75%), dominantly inherited in 12 out of 64 (19%), and due to proven germline mosaicism in four out of 64 (6%). Highly penetrant clinical features include, microcephaly, first and second arch craniofacial malformations, and hearing loss; esophageal atresia is present in an estimated ∼27%. Microcephaly is virtually universal in childhood, with some adults exhibiting late "catch-up" growth and normocephaly at maturity. Occasionally reported anomalies, include vestibular and ossicular malformations, reduced mouth opening, atrophy of cerebral white matter, structural brain malformations, and epibulbar dermoid. All reported EFTUD2 mutations can be found in the EFTUD2 mutation database (http://databases.lovd.nl/shared/genes/EFTUD2).

Published
2016

5. National clinical Genetic Networks - GENets - Establishment of expert collaborations in Denmark

Author

Lildballe, Dorte L., primary, Frederiksen, Anja Lisbeth, additional, Schönewolf-Greulich, Bitten, additional, Brasch-Andersen, Charlotte, additional, Lautrup, Charlotte Kvist, additional, Karstensen, Helena Gásdal, additional, Pedersen, Inge Søkilde, additional, Sunde, Lone, additional, Risom, Lotte, additional, Rasmussen, Maria, additional, Bertelsen, Mette, additional, Andersen, Mette Klarskov, additional, Rendtorff, Nanna Dahl, additional, Gregersen, Pernille Axél, additional, Tørring, Pernille M., additional, Hammer-Hansen, Sophia, additional, Boonen, Susanne E., additional, Lindquist, Suzanne Granhøj, additional, Hammer, Trine Bjørg, additional, and Diness, Birgitte R., additional

Published
2023
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7. National clinical Genetic Networks - GENets - Establishment of expert collaborations in Denmark

Author

Lildballe, Dorte L., Frederiksen, Anja Lisbeth, Schönewolf-Greulich, Bitten, Brasch-Andersen, Charlotte, Lautrup, Charlotte Kvist, Karstensen, Helena Gásdal, Pedersen, Inge Søkilde, Sunde, Lone, Risom, Lotte, Rasmussen, Maria, Bertelsen, Mette, Andersen, Mette Klarskov, Rendtorff, Nanna Dahl, Gregersen, Pernille Axél, Tørring, Pernille M., Hammer-Hansen, Sophia, Boonen, Susanne E., Lindquist, Suzanne Granhøj, Hammer, Trine Bjørg, Diness, Birgitte R., Lildballe, Dorte L., Frederiksen, Anja Lisbeth, Schönewolf-Greulich, Bitten, Brasch-Andersen, Charlotte, Lautrup, Charlotte Kvist, Karstensen, Helena Gásdal, Pedersen, Inge Søkilde, Sunde, Lone, Risom, Lotte, Rasmussen, Maria, Bertelsen, Mette, Andersen, Mette Klarskov, Rendtorff, Nanna Dahl, Gregersen, Pernille Axél, Tørring, Pernille M., Hammer-Hansen, Sophia, Boonen, Susanne E., Lindquist, Suzanne Granhøj, Hammer, Trine Bjørg, and Diness, Birgitte R.

Abstract

Genetic conditions are often familial, but not all relatives receive counseling from the same institution. It is therefore necessary to ensure consistency in variant interpretation, counseling practices, and clinical follow up across health care providers. Furthermore, as new possibilities for gene-specific treatments emerge and whole genome sequencing becomes more widely available, efficient data handling and knowledge sharing between clinical laboratory geneticists and medical specialists in clinical genetics are increasingly important. In Denmark, these needs have been addressed through the establishment of collaborative national networks called Genetic Expert Networks or "GENets". These networks have enhanced patient and family care significantly by bringing together groups of experts in national collaborations. This promotes coordinated clinical care, the dissemination of best clinical practices, and facilitates the exchange of new knowledge., Genetic conditions are often familial, but not all relatives receive counseling from the same institution. It is therefore necessary to ensure consistency in variant interpretation, counseling practices, and clinical follow up across health care providers. Furthermore, as new possibilities for gene-specific treatments emerge and whole genome sequencing becomes more widely available, efficient data handling and knowledge sharing between clinical laboratory geneticists and medical specialists in clinical genetics are increasingly important. In Denmark, these needs have been addressed through the establishment of collaborative national networks called Genetic Expert Networks or "GENets". These networks have enhanced patient and family care significantly by bringing together groups of experts in national collaborations. This promotes coordinated clinical care, the dissemination of best clinical practices, and facilitates the exchange of new knowledge.

Published
2023

9. Early diagnosis enabling precision medicine treatment in a young boy with PIK3R1-related overgrowth

Author

Schönewolf-Greulich, Bitten, Karstensen, Helena Gásdal, Hjortshøj, Tina D., Jørgensen, Finn Stener, Harder, Katja M., Frevert, Susanne, Hove, Hanne, Diness, Birgitte R., Schönewolf-Greulich, Bitten, Karstensen, Helena Gásdal, Hjortshøj, Tina D., Jørgensen, Finn Stener, Harder, Katja M., Frevert, Susanne, Hove, Hanne, and Diness, Birgitte R.

Abstract

Mosaic PIK3R1 variants have recently been demonstrated in patients with complex vascular malformations and overgrowth in a syndrome resembling PIK3CA-related overgrowth syndrome (PROS). The PIK3CA-inhibitor, alpelisib, seems to be a promising treatment option for PROS patients. We describe a young boy with overgrowth and a pathogenic mosaic variant in PIK3R1; c.1699A > G, p.(Lys567Glu). He was prenatally suspected of a syndrome on the presence of unusual transient fluctuating subcutaneous edemas and lymphedema of his left shoulder. The pathogenic variant, later found to be causative, was below detection threshold in whole-genome sequencing (WGS) analysis of amniotic fluid. Upon delivery a mosaic pathogenic PIK3R1 variant, was identified by whole-exome sequencing (WES) of a skin biopsy. With no proven treatment options available, and based on the theoretical disease mechanism, alpelisib therapy was initiated at nine months of age. In the first year of treatment growth normalized and the affected vascular and lymphatic tissue regressed. No side effects have been observed. This report underlines the importance of early variant detection in children suspected of having severe mosaic overgrowth, and proves that prenatal diagnosis is possible, enabling prompt treatment. Furthermore, it demonstrates the promising effects of alpelisib in this patient group.

Published
2022

10. Clinical and molecular delineation of PUS3‐associated neurodevelopmental disorders

Author

Nøstvik, Miriam, primary, Kateta, Sarah M., additional, Schönewolf‐Greulich, Bitten, additional, Afenjar, Alexandra, additional, Barth, Magalie, additional, Boschann, Felix, additional, Doummar, Diane, additional, Haack, Tobias B., additional, Keren, Boris, additional, Livshits, Ludmila A., additional, Mei, Davide, additional, Park, Joohyun, additional, Pisano, Tiziana, additional, Prouteau, Clement, additional, Umair, Muhammad, additional, Waqas, Ahmed, additional, Ziegler, Alban, additional, Guerrini, Renzo, additional, Møller, Rikke S., additional, and Tümer, Zeynep, additional

Published
2021
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12. ZMYND11 variants are a novel cause of centrotemporal and generalised epilepsies with neurodevelopmental disorder

Author

Oates, Stephanie, primary, Absoud, Michael, additional, Goyal, Sushma, additional, Bayley, Sophie, additional, Baulcomb, Jennifer, additional, Sims, Annemarie, additional, Riddett, Amy, additional, Allis, Katrina, additional, Brasch‐Andersen, Charlotte, additional, Balasubramanian, Meena, additional, Bai, Renkui, additional, Callewaert, Bert, additional, Hüffmeier, Ulrike, additional, Le Duc, Diana, additional, Radtke, Maximilian, additional, Korff, Christian, additional, Kennedy, Joanna, additional, Low, Karen, additional, Møller, Rikke S., additional, Nielsen, Jens Erik Klint, additional, Popp, Bernt, additional, Quteineh, Lina, additional, Rønde, Gitte, additional, Schönewolf‐Greulich, Bitten, additional, Shillington, Amelle, additional, Taylor, Matthew RG, additional, Todd, Emily, additional, Torring, Pernille M., additional, Tümer, Zeynep, additional, Vasileiou, Georgia, additional, Yates, T. Michael, additional, Zweier, Christiane, additional, Rosch, Richard, additional, Basson, M. Albert, additional, and Pal, Deb K., additional

Published
2021
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13. ZMYND11 variants are a novel cause of centrotemporal and generalised epilepsies with neurodevelopmental disorder

Author

Oates, Stephanie, Absoud, Michael, Goyal, Sushma, Bayley, Sophie, Baulcomb, Jennifer, Sims, Annemarie, Riddett, Amy, Allis, Katrina, Brasch-Andersen, Charlotte, Balasubramanian, Meena, Bai, Renkui, Callewaert, Bert, Hüffmeier, Ulrike, Le Duc, Diana, Radtke, Maximilian, Korff, Christian, Kennedy, Joanna, Low, Karen, Møller, Rikke S., Nielsen, Jens Erik Klint, Popp, Bernt, Quteineh, Lina, Rønde, Gitte, Schönewolf-Greulich, Bitten, Shillington, Amelle, Taylor, Matthew R.G., Todd, Emily, Torring, Pernille M., DMSc, Zeynep Tümer M.D.Ph D., Vasileiou, Georgia, Yates, T. Michael, Zweier, Christiane, Rosch, Richard, Basson, M. Albert, Pal, Deb K., Oates, Stephanie, Absoud, Michael, Goyal, Sushma, Bayley, Sophie, Baulcomb, Jennifer, Sims, Annemarie, Riddett, Amy, Allis, Katrina, Brasch-Andersen, Charlotte, Balasubramanian, Meena, Bai, Renkui, Callewaert, Bert, Hüffmeier, Ulrike, Le Duc, Diana, Radtke, Maximilian, Korff, Christian, Kennedy, Joanna, Low, Karen, Møller, Rikke S., Nielsen, Jens Erik Klint, Popp, Bernt, Quteineh, Lina, Rønde, Gitte, Schönewolf-Greulich, Bitten, Shillington, Amelle, Taylor, Matthew R.G., Todd, Emily, Torring, Pernille M., DMSc, Zeynep Tümer M.D.Ph D., Vasileiou, Georgia, Yates, T. Michael, Zweier, Christiane, Rosch, Richard, Basson, M. Albert, and Pal, Deb K.

Abstract

ZMYND11 is the critical gene in chromosome 10p15.3 microdeletion syndrome, a syndromic cause of intellectual disability. The phenotype of ZMYND11 variants has recently been extended to autism and seizures. We expand on the epilepsy phenotype of 20 individuals with pathogenic variants in ZMYND11. We obtained clinical descriptions of 16 new and nine published individuals, plus detailed case history of two children. New individuals were identified through GeneMatcher, ClinVar and the European Network for Therapies in Rare Epilepsy (NETRE). Genetic evaluation was performed using gene panels or exome sequencing; variants were classified using American College of Medical Genetics (ACMG) criteria. Individuals with ZMYND11 associated epilepsy fell into three groups: (i) atypical benign partial epilepsy or idiopathic focal epilepsy (n = 8); (ii) generalised epilepsies/infantile epileptic encephalopathy (n = 4); (iii) unclassified (n = 8). Seizure prognosis ranged from spontaneous remission to drug resistant. Neurodevelopmental deficits were invariable. Dysmorphic features were variable. Variants were distributed across the gene and mostly de novo with no precise genotype–phenotype correlation. ZMYND11 is one of a small group of chromatin reader genes associated in the pathogenesis of epilepsy, and specifically ABPE. More detailed epilepsy descriptions of larger cohorts and functional studies might reveal genotype–phenotype correlation. The epileptogenic mechanism may be linked to interaction with histone H3.3.

Published
2021

14. Decline in gross motor skills in adult Rett syndrome; results from a Danish longitudinal study

Author

Bisgaard, Anne Marie, Wong, Kingsley, Højfeldt, Anne Katrine, Larsen, Jane Lunding, Schönewolf-Greulich, Bitten, Rønde, Gitte, Downs, Jenny, Stahlhut, Michelle, Bisgaard, Anne Marie, Wong, Kingsley, Højfeldt, Anne Katrine, Larsen, Jane Lunding, Schönewolf-Greulich, Bitten, Rønde, Gitte, Downs, Jenny, and Stahlhut, Michelle

Abstract

Longevity of individuals with neurodevelopmental diseases as Rett syndrome (RTT) has increased and many reach adulthood and old age. There is therefore a need to increase knowledge about the course of RTT in adults in order to improve medical care management and quality of life. We did a longitudinal study to address if a possible decline in motor skills in adults with RTT can be explained by the presence of common medical conditions as epilepsy, breathing disturbance, and scoliosis. Data from the Danish RTT database, medical files, and videos from visits at the national Center for Rett syndrome were reviewed. The study included 24 individuals aged 30–66 years at last visit after a follow-up period of 6–12 years. Results showed a clinically observable and significant decline in gross motor skills using the Rett syndrome Gross Motor Scale (RSGMS) with a tendency of less decline in the individuals with the best motor abilities. The frequencies of comorbidities were high. Decline in RSGMS score was associated with the presence of epilepsy and severe scoliosis that had been conservatively managed. The results emphasize that epilepsy plays a significant role in the adult RTT life and management of severe scoliosis in the younger years has impact on the motor abilities in adulthood.

Published
2021

15. Clinical and molecular delineation of PUS3-associated neurodevelopmental disorders

Author

Nøstvik, Miriam, Kateta, Sarah M., Schönewolf-Greulich, Bitten, Afenjar, Alexandra, Barth, Magalie, Boschann, Felix, Doummar, Diane, Haack, Tobias B., Keren, Boris, Livshits, Ludmilla A., Mei, Davide, Park, Joohyun, Pisano, Tiziana, Prouteau, Clement, Umair, Muhammad, Waqas, Ahmed, Ziegler, Alban, Guerrini, Renzo, Møller, Rikke S., Tümer, Zeynep, Nøstvik, Miriam, Kateta, Sarah M., Schönewolf-Greulich, Bitten, Afenjar, Alexandra, Barth, Magalie, Boschann, Felix, Doummar, Diane, Haack, Tobias B., Keren, Boris, Livshits, Ludmilla A., Mei, Davide, Park, Joohyun, Pisano, Tiziana, Prouteau, Clement, Umair, Muhammad, Waqas, Ahmed, Ziegler, Alban, Guerrini, Renzo, Møller, Rikke S., and Tümer, Zeynep

Abstract

Biallelic variants in PUS3 have recently been recognized as a rare cause of neurodevelopmental disorders. Pseudouridine synthase-3 encoded by PUS3 is an enzyme important for modification of various RNAs, including transfer RNA (tRNA). Here we present the clinical and genetic features of 21 individuals with biallelic PUS3 variants: seven new and 14 previously reported individuals, where clinical features of two were updated. The clinical and genetic information were collected through collaborations or by literature search. All individuals were characterized by the local clinicians and the gene variants were identified by next generation sequencing (NGS) based methodologies. The clinical picture was dominated by global developmental delay, epilepsy, hypotonia and microcephaly. Gray sclera, which has previously been suggested to be a characteristic feature of PUS3-associated phenotypes, was reported in only seven individuals. The patients had some dysmorphic facial features, but a recognizable gestalt was not observed. In conclusion, homozygous and compound heterozygous PUS3 variants lead to a rare neurodevelopmental disorder. Further functional studies are necessary to understand involvement of PUS3 and tRNA biogenesis in normal and abnormal brain development.

Published
2021

16. DLG4-related synaptopathy:a new rare brain disorder

Author

Rodríguez-Palmero, Agustí, Boerrigter, Melissa Maria, Gómez-Andrés, David, Aldinger, Kimberly A., Marcos-Alcalde, Íñigo, Popp, Bernt, Everman, David B., Lovgren, Alysia Kern, Arpin, Stephanie, Bahrambeigi, Vahid, Beunders, Gea, Bisgaard, Anne Marie, Bjerregaard, V. A., Bruel, Ange Line, Challman, Thomas D., Cogné, Benjamin, Coubes, Christine, de Man, Stella A., Denommé-Pichon, Anne Sophie, Dye, Thomas J., Elmslie, Frances, Feuk, Lars, García-Miñaúr, Sixto, Gertler, Tracy, Giorgio, Elisa, Gruchy, Nicolas, Haack, Tobias B., Haldeman-Englert, Chad R., Haukanes, Bjørn Ivar, Hoyer, Juliane, Hurst, Anna C.E., Isidor, Bertrand, Soller, Maria Johansson, Kushary, Sulagna, Kvarnung, Malin, Landau, Yuval E., Leppig, Kathleen A., Lindstrand, Anna, Kleinendorst, Lotte, MacKenzie, Alex, Mandrile, Giorgia, Mendelsohn, Bryce A., Moghadasi, Setareh, Morton, Jenny E., Moutton, Sebastien, Müller, Amelie J., O’Leary, Melanie, Pacio-Míguez, Marta, Palomares-Bralo, Maria, Parikh, Sumit, Pfundt, Rolph, Pode-Shakked, Ben, Rauch, Anita, Repnikova, Elena, Revah-Politi, Anya, Ross, Meredith J., Ruivenkamp, Claudia A.L., Sarrazin, Elisabeth, Savatt, Juliann M., Schlüter, Agatha, Schönewolf-Greulich, Bitten, Shad, Zohra, Shaw-Smith, Charles, Shieh, Joseph T., Shohat, Motti, Spranger, Stephanie, Thiese, Heidi, Mau-Them, Frederic Tran, van Bon, Bregje, van de Burgt, Ineke, van de Laar, Ingrid M.B.H., van Drie, Esmée, van Haelst, Mieke M., van Ravenswaaij-Arts, Conny M., Verdura, Edgard, Vitobello, Antonio, Waldmüller, Stephan, Whiting, Sharon, Zweier, Christiane, Prada, Carlos E., de Vries, Bert B.A., Dobyns, William B., Reiter, Simone F., Gómez-Puertas, Paulino, Pujol, Aurora, Tümer, Zeynep, Rodríguez-Palmero, Agustí, Boerrigter, Melissa Maria, Gómez-Andrés, David, Aldinger, Kimberly A., Marcos-Alcalde, Íñigo, Popp, Bernt, Everman, David B., Lovgren, Alysia Kern, Arpin, Stephanie, Bahrambeigi, Vahid, Beunders, Gea, Bisgaard, Anne Marie, Bjerregaard, V. A., Bruel, Ange Line, Challman, Thomas D., Cogné, Benjamin, Coubes, Christine, de Man, Stella A., Denommé-Pichon, Anne Sophie, Dye, Thomas J., Elmslie, Frances, Feuk, Lars, García-Miñaúr, Sixto, Gertler, Tracy, Giorgio, Elisa, Gruchy, Nicolas, Haack, Tobias B., Haldeman-Englert, Chad R., Haukanes, Bjørn Ivar, Hoyer, Juliane, Hurst, Anna C.E., Isidor, Bertrand, Soller, Maria Johansson, Kushary, Sulagna, Kvarnung, Malin, Landau, Yuval E., Leppig, Kathleen A., Lindstrand, Anna, Kleinendorst, Lotte, MacKenzie, Alex, Mandrile, Giorgia, Mendelsohn, Bryce A., Moghadasi, Setareh, Morton, Jenny E., Moutton, Sebastien, Müller, Amelie J., O’Leary, Melanie, Pacio-Míguez, Marta, Palomares-Bralo, Maria, Parikh, Sumit, Pfundt, Rolph, Pode-Shakked, Ben, Rauch, Anita, Repnikova, Elena, Revah-Politi, Anya, Ross, Meredith J., Ruivenkamp, Claudia A.L., Sarrazin, Elisabeth, Savatt, Juliann M., Schlüter, Agatha, Schönewolf-Greulich, Bitten, Shad, Zohra, Shaw-Smith, Charles, Shieh, Joseph T., Shohat, Motti, Spranger, Stephanie, Thiese, Heidi, Mau-Them, Frederic Tran, van Bon, Bregje, van de Burgt, Ineke, van de Laar, Ingrid M.B.H., van Drie, Esmée, van Haelst, Mieke M., van Ravenswaaij-Arts, Conny M., Verdura, Edgard, Vitobello, Antonio, Waldmüller, Stephan, Whiting, Sharon, Zweier, Christiane, Prada, Carlos E., de Vries, Bert B.A., Dobyns, William B., Reiter, Simone F., Gómez-Puertas, Paulino, Pujol, Aurora, and Tümer, Zeynep

Abstract

Purpose: Postsynaptic density protein-95 (PSD-95), encoded by DLG4, regulates excitatory synaptic function in the brain. Here we present the clinical and genetic features of 53 patients (42 previously unpublished) with DLG4 variants. Methods: The clinical and genetic information were collected through GeneMatcher collaboration. All the individuals were investigated by local clinicians and the gene variants were identified by clinical exome/genome sequencing. Results: The clinical picture was predominated by early onset global developmental delay, intellectual disability, autism spectrum disorder, and attention deficit–hyperactivity disorder, all of which point to a brain disorder. Marfanoid habitus, which was previously suggested to be a characteristic feature of DLG4-related phenotypes, was found in only nine individuals and despite some overlapping features, a distinct facial dysmorphism could not be established. Of the 45 different DLG4 variants, 39 were predicted to lead to loss of protein function and the majority occurred de novo (four with unknown origin). The six missense variants identified were suggested to lead to structural or functional changes by protein modeling studies. Conclusion: The present study shows that clinical manifestations associated with DLG4 overlap with those found in other neurodevelopmental disorders of synaptic dysfunction; thus, we designate this group of disorders as DLG4-related synaptopathy. [Figure not available: see fulltext.]

Published
2021

17. Mitochondrial Function in Gilles de la Tourette Syndrome Patients With and Without Intragenic IMMP2L Deletions

Author

Bjerregaard, Victoria A., Schönewolf-Greulich, Bitten, Juel Rasmussen, Lene, Desler, Claus, Tümer, Zeynep, Bjerregaard, Victoria A., Schönewolf-Greulich, Bitten, Juel Rasmussen, Lene, Desler, Claus, and Tümer, Zeynep

Abstract

Background: Gilles de la Tourette syndrome (GTS) is a neurodevelopmental condition characterized by motor and vocal tics. The underlying etiology remains largely unknown, and GTS is considered as a complex multifactorial disorder associated with effects of several genes in combination with environmental factors. The inner mitochondrial membrane peptidase, subunit 2 (IMMP2L) has been suggested as one of the susceptibility genes for GTS, and IMMP2L-deficient mouse and human cells show increased levels of mitochondrial oxidative stress and altered cell fate programming. Hence, a potential involvement of IMMP2L-induced mitochondrial dysfunction in GTS pathology is yet to be elucidated. To address this, we investigated mitochondrial function in a group of GTS patients with intragenic IMMP2L deletions and compared with GTS without IMMP2L deletions and healthy controls. Methods: Mitochondrial function in fibroblasts from GTS patients and non-GTS parents (with and without IMMP2L deletions) compared to healthy controls were evaluated by measuring mitochondrial superoxide production, mitochondrial membrane potential, mitochondrial mass, and mitochondrial respiration. In addition, we evaluated apoptosis and senescence. Results: None of the mitochondrial parameters assessed in this study were significantly distinctive when comparing GTS patients with and without IMMP2L deletions against healthy controls or parents with or without IMMP2L deletions, and we did not observe altered cell programming. Conclusion: This study suggests that IMMP2L deletions do not lead to a substantial general mitochondrial dysfunction in GTS fibroblasts. Assessing a large cohort of controls and patients of similar age and gender would possibly reveal small differences in mitochondrial function. However, it is possible that IMMP2L variants affect mitochondrial function during specific instances of stress stimuli or in brain regions suggested to be affected in GTS.

Published
2020

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

Author

UCL - (SLuc) Centre de génétique médicale UCL, UCL - (SLuc) Centre de référence neuromusculaire, UCL - (SLuc) Service d'oto-rhino-laryngologie, UCL - SSS/IREC/SLUC - Pôle St.-Luc, Westra, Dineke, Schouten, Meyke I., Stunnenberg, Bas C., Kusters, Benno, Saris, Christiaan G.J., Erasmus, Corrie E., van Engelen, Baziel G., Bulk, Saskia, Verschuuren-Bemelmans, Corien C., Gerkes, E.H., de Geus, Christa, van der Zwaag, P.A., Chan, Sophelia, Chung, Brian, Barge-Schaapveld, Daniela Q.C.M., Kriek, Marjolein, Sznajer, Yves, van Spaendonck-Zwarts, Karin, van der Kooi, Anneke J., Krause, Amanda, Schönewolf-Greulich, Bitten, de Die-Smulders, Christine, Sallevelt, Suzanne C.E.H., Krapels, Ingrid P.C., Rasmussen, Magnhild, Maystadt, Isabelle, Kievit, Anneke J.A., Witting, Nanna, Pennings, Maartje, Meijer, Rowdy, Gillissen, Christian, Kamsteeg, Erik-Jan, Voermans, Nicol C., UCL - (SLuc) Centre de génétique médicale UCL, UCL - (SLuc) Centre de référence neuromusculaire, UCL - (SLuc) Service d'oto-rhino-laryngologie, UCL - SSS/IREC/SLUC - Pôle St.-Luc, Westra, Dineke, Schouten, Meyke I., Stunnenberg, Bas C., Kusters, Benno, Saris, Christiaan G.J., Erasmus, Corrie E., van Engelen, Baziel G., Bulk, Saskia, Verschuuren-Bemelmans, Corien C., Gerkes, E.H., de Geus, Christa, van der Zwaag, P.A., Chan, Sophelia, Chung, Brian, Barge-Schaapveld, Daniela Q.C.M., Kriek, Marjolein, Sznajer, Yves, van Spaendonck-Zwarts, Karin, van der Kooi, Anneke J., Krause, Amanda, Schönewolf-Greulich, Bitten, de Die-Smulders, Christine, Sallevelt, Suzanne C.E.H., Krapels, Ingrid P.C., Rasmussen, Magnhild, Maystadt, Isabelle, Kievit, Anneke J.A., Witting, Nanna, Pennings, Maartje, Meijer, Rowdy, Gillissen, Christian, Kamsteeg, Erik-Jan, and Voermans, Nicol C.

Abstract

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

Published
2019

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

Author

Schönewolf-Greulich, Bitten, Bisgaard, Anne-Marie, Møller, Rikke S, Dunø, Morten, Brøndum-Nielsen, Karen, Kaur, Simran, Van Bergen, Nicole J, Lunke, Sebastian, Eggers, Stefanie, Jespersgaard, Cathrine, Christodoulou, John, Tümer, Zeynep, Schönewolf-Greulich, Bitten, Bisgaard, Anne-Marie, Møller, Rikke S, Dunø, Morten, Brøndum-Nielsen, Karen, Kaur, Simran, Van Bergen, Nicole J, Lunke, Sebastian, Eggers, Stefanie, Jespersgaard, Cathrine, Christodoulou, John, and Tümer, Zeynep

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

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

Author

Sands, Tristan T, Miceli, Francesco, Lesca, Gaetan, Beck, Anita E, Sadleir, Lynette G, Arrington, Daniel K, Schönewolf-Greulich, Bitten, Moutton, Sébastien, Lauritano, Anna, Nappi, Piera, Soldovieri, Maria Virginia, Scheffer, Ingrid E, Mefford, Heather C, Stong, Nicholas, Heinzen, Erin L, Goldstein, David B, Perez, Ana Grijalvo, Kossoff, Eric H, Stocco, Amber, Sullivan, Jennifer A, Shashi, Vandana, Gerard, Benedicte, Francannet, Christine, Bisgaard, Anne-Marie, Tümer, Zeynep, Willems, Marjolaine, Rivier, François, Vitobello, Antonio, Thakkar, Kavita, Rajan, Deepa S, Barkovich, A James, Weckhuysen, Sarah, Cooper, Edward C, Taglialatela, Maurizio, Cilio, M Roberta, Sands, Tristan T, Miceli, Francesco, Lesca, Gaetan, Beck, Anita E, Sadleir, Lynette G, Arrington, Daniel K, Schönewolf-Greulich, Bitten, Moutton, Sébastien, Lauritano, Anna, Nappi, Piera, Soldovieri, Maria Virginia, Scheffer, Ingrid E, Mefford, Heather C, Stong, Nicholas, Heinzen, Erin L, Goldstein, David B, Perez, Ana Grijalvo, Kossoff, Eric H, Stocco, Amber, Sullivan, Jennifer A, Shashi, Vandana, Gerard, Benedicte, Francannet, Christine, Bisgaard, Anne-Marie, Tümer, Zeynep, Willems, Marjolaine, Rivier, François, Vitobello, Antonio, Thakkar, Kavita, Rajan, Deepa S, Barkovich, A James, Weckhuysen, Sarah, Cooper, Edward C, Taglialatela, Maurizio, and Cilio, M Roberta

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

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

Author

Schönewolf-Greulich, Bitten, Bisgaard, Anne Marie, Dunø, Morten, Jespersgaard, Cathrine, Rokkjær, Mette, Hansen, Lars K., Tsoutsou, Eirini, Sofokleous, Christalena, Topcu, Meral, Kaur, Simran, Van Bergen, Nicole J., Brøndum-Nielsen, Karen, Larsen, Martin J., Sørensen, Kristina P., Christodoulou, John, Fagerberg, Christina R., Tümer, Zeynep, Schönewolf-Greulich, Bitten, Bisgaard, Anne Marie, Dunø, Morten, Jespersgaard, Cathrine, Rokkjær, Mette, Hansen, Lars K., Tsoutsou, Eirini, Sofokleous, Christalena, Topcu, Meral, Kaur, Simran, Van Bergen, Nicole J., Brøndum-Nielsen, Karen, Larsen, Martin J., Sørensen, Kristina P., Christodoulou, John, Fagerberg, Christina R., and Tümer, Zeynep

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

25. Autism and developmental disability caused by KCNQ3 gain‐of‐function variants

Author

Sands, Tristan T., primary, Miceli, Francesco, additional, Lesca, Gaetan, additional, Beck, Anita E., additional, Sadleir, Lynette G., additional, Arrington, Daniel K., additional, Schönewolf‐Greulich, Bitten, additional, Moutton, Sébastien, additional, Lauritano, Anna, additional, Nappi, Piera, additional, Soldovieri, Maria Virginia, additional, Scheffer, Ingrid E., additional, Mefford, Heather C., additional, Stong, Nicholas, additional, Heinzen, Erin L., additional, Goldstein, David B., additional, Perez, Ana Grijalvo, additional, Kossoff, Eric H., additional, Stocco, Amber, additional, Sullivan, Jennifer A., additional, Shashi, Vandana, additional, Gerard, Benedicte, additional, Francannet, Christine, additional, Bisgaard, Anne‐Marie, additional, Tümer, Zeynep, additional, Willems, Marjolaine, additional, Rivier, François, additional, Vitobello, Antonio, additional, Thakkar, Kavita, additional, Rajan, Deepa S., additional, Barkovich, A. James, additional, Weckhuysen, Sarah, additional, Cooper, Edward C., additional, Taglialatela, Maurizio, additional, and Cilio, M. Roberta, additional

Published
2019
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26. Panel-Based Exome Sequencing for Neuromuscular Disorders as a Diagnostic Service

Author

Westra, Dineke, primary, Schouten, Meyke I., additional, Stunnenberg, Bas C., additional, Kusters, Benno, additional, Saris, Christiaan G.J., additional, Erasmus, Corrie E., additional, van Engelen, Baziel G., additional, Bulk, Saskia, additional, Verschuuren-Bemelmans, Corien C., additional, Gerkes, E.H., additional, de Geus, Christa, additional, van der Zwaag, P.A., additional, Chan, Sophelia, additional, Chung, Brian, additional, Barge-Schaapveld, Daniela Q.C.M., additional, Kriek, Marjolein, additional, Sznajer, Yves, additional, van Spaendonck-Zwarts, Karin, additional, van der Kooi, Anneke J., additional, Krause, Amanda, additional, Schönewolf-Greulich, Bitten, additional, de Die-Smulders, Christine, additional, Sallevelt, Suzanne C.E.H., additional, Krapels, Ingrid P.C., additional, Rasmussen, Magnhild, additional, Maystadt, Isabelle, additional, Kievit, Anneke J.A., additional, Witting, Nanna, additional, Pennings, Maartje, additional, Meijer, Rowdy, additional, Gillissen, Christian, additional, Kamsteeg, Erik-Jan, additional, and Voermans, Nicol C., additional

Published
2019
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27. Mosaic MECP2 variants in males with classical Rett syndrome features, including stereotypical hand movements

Author

Schönewolf‐Greulich, Bitten, primary, Bisgaard, Anne‐Marie, additional, Dunø, Morten, additional, Jespersgaard, Cathrine, additional, Rokkjær, Mette, additional, Hansen, Lars K., additional, Tsoutsou, Eirini, additional, Sofokleous, Christalena, additional, Topcu, Meral, additional, Kaur, Simran, additional, Van Bergen, Nicole J., additional, Brøndum‐Nielsen, Karen, additional, Larsen, Martin J., additional, Sørensen, Kristina P., additional, Christodoulou, John, additional, Fagerberg, Christina R., additional, and Tümer, Zeynep, additional

Published
2018
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28. Development of hypomelanotic macules is associated with constitutive activated mTORC1 in tuberous sclerosis complex

Author

Møller, Lisbeth Birk, primary, Schönewolf-Greulich, Bitten, additional, Rosengren, Thomas, additional, Larsen, Lasse Jonsgaard, additional, Ostergaard, John R., additional, Sommerlund, Mette, additional, Ostenfeldt, Caroline, additional, Stausbøl-Grøn, Brian, additional, Linnet, Karen Markussen, additional, Gregersen, Pernille Axél, additional, and Jensen, Uffe Birk, additional

Published
2017
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29. Mosaic MECP2 variants in males with classical Rett syndrome features, including stereotypical hand movements.

Author

Bisgaard, Anne‐Marie, Schönewolf‐Greulich, Bitten, Jespersgaard, Cathrine, Tümer, Zeynep, Dunø, Morten, Brøndum‐Nielsen, Karen, Rokkjær, Mette, Hansen, Lars K., Tsoutsou, Eirini, Sofokleous, Christalena, Topcu, Meral, Kaur, Simran, Van Bergen, Nicole J., Christodoulou, John, Larsen, Martin J., Sørensen, Kristina P., and Fagerberg, Christina R.

Subjects
*MOSAICISM, *METHYL-CpG-binding protein 2, *RETT syndrome, *NUCLEOTIDE sequencing, *HAND, *HUMAN mechanics
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. Even very low‐grade mosaicim in methyl‐CPG‐binding protein 2 (MECP2) can cause Rett syndrome in males. The c.1308dupT variant of a male patient was present in 4.2% in blood and 23.8% in muscle tissue (encircled). Analysis of MECP2 in males should be carried out with very high read depth and variant call threshold should be low. A negative finding blood should be repeated using other tissues. [ABSTRACT FROM AUTHOR]

Published
2019
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30. The MECP2 variant c.925C>T (p.Arg309Trp) causes intellectual disability in both males and females without classic features of Rett syndrome

Author

Schönewolf-Greulich, Bitten, Tejada, Maria-Isabel, Stephens, K, Hadzsiev, K, Gauthier, J, Brøndum-Nielsen, Karen, Pfundt, R, Ravn, Kirstine Johanne Theresia, Maortua, H, Gener, B, Martínez-Bouzas, C, Piton, A, Rouleau, G, Clayton-Smith, J, Kleefstra, T, Bisgaard, Anne-Marie, Tümer, Zeynep, Schönewolf-Greulich, Bitten, Tejada, Maria-Isabel, Stephens, K, Hadzsiev, K, Gauthier, J, Brøndum-Nielsen, Karen, Pfundt, R, Ravn, Kirstine Johanne Theresia, Maortua, H, Gener, B, Martínez-Bouzas, C, Piton, A, Rouleau, G, Clayton-Smith, J, Kleefstra, T, Bisgaard, Anne-Marie, and Tümer, Zeynep

Abstract

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

32. Klinisk og molekylærgenetisk diagnostik af Retts syndrom i Danmark

Author

Schönewolf-Greulich, Bitten, Dunø, Morten, Ravn, Kirstine, Brøndum-Nielsen, Karen, Bisgaard, Anne-Marie, Schönewolf-Greulich, Bitten, Dunø, Morten, Ravn, Kirstine, Brøndum-Nielsen, Karen, and Bisgaard, Anne-Marie

Abstract

The neurodevelopmental disorder Rett syndrome was first described in 1966 by Andreas Rett, who described girls with loss of speech and hand use displaying characteristic hand stereotypies. Since then, the disease has been linked to mutations in the gene MECP2. However, the basis of the diagnosis is still clinical as defined by the latest clinical criteria as proposed by Neul and colleagues in 2010. This article presents a short clinical and molecular overview of the latest in Rett syndrome with emphasis on the Danish patients, headlines for making the diagnosis, differential diagnoses and molecular diagnostic possibilities.

Published
2015

35. Functional abilities in aging women with Rett syndrome – the Danish cohort.

Author

Schönewolf-Greulich, Bitten, Stahlhut, Michelle, Larsen, Jane Lunding, Syhler, Birgit, and Bisgaard, Anne-Marie

Subjects
*PROTEIN analysis, *AGING, *CAREGIVERS, *COMMUNICATION, *COMMUNICATIVE competence, *INGESTION, *INTERVIEWING, *LIFE skills, *LONGITUDINAL method, *GENETIC mutation, *QUALITY of life, *RETT syndrome, *HEALTH self-care, *WALKING, *WOMEN'S health, *ACTIVITIES of daily living, *FEEDING tubes, *DESCRIPTIVE statistics, RESEARCH evaluation
Abstract

Rett syndrome (RTT) is a neurodevelopmental disorder, which mainly affects females and results in multiple disabilities. Many clinical descriptions of the symptoms and functional abilities have been made medically, though mainly in children with RTT. Previous reports have established that even though the syndrome causes severe psychomotor disability, women with RTT can live long into adulthood. Purpose: We aim to describe what to expect from aging women with RTT regarding some of the basic functional abilities that are used in daily activities and that could have an impact on quality of life in these women. Methods: A team of two medical doctors, a physiotherapist and an educational psychological adviser, performed clinical evaluations of 27 women with RTT in Denmark above 30 years of age and confirmed MECP2 mutation. Results: We found that 63% of the women were able to walk outside their homes and only 11% were not able to walk at all. However, 67% could not transfer from sitting to standing position without support. There was profound difficulties communicating, but 85.1% of the women could either consistently point with their hand or eyes to things of their interest. Conclusions: Women with RTT are very dependent on caregivers who maintain and rehabilitate their functional abilities. They can often walk short distances unassisted, but do have trouble transferring and thus getting up from a chair on their own. They have severe problems communicating and they often perform subtle signs that can be difficult to recognize. 3/4 of aging RTT women are household ambulators – daily training of motor functions and focus on assisting the initiation of movements are needed lifelong to maintain walking ability and participation in daily activities More than half of aging women with RTT can grab on to things – persons with hand function should be motivated to use this ability in the context of eating Communication is a difficult task especially for the aging RTT women – Communicative signs, their meaning and how to react to them should be written down for every woman in an easy accessible way to all caregivers The majority of aging RTT women can point out things of interest – they should be given the opportunity to participate in choice making [ABSTRACT FROM AUTHOR]

Published
2017
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36. Forstørret nakkefold kan ses ved osteogenesis imperfecta

Author

Schönewolf-Greulich, Bitten, Skibsted, Lillian, Maroun, Lisa Leth, Lund, Allan Meldgaard, Brøndum-Nielsen, Karen, Schönewolf-Greulich, Bitten, Skibsted, Lillian, Maroun, Lisa Leth, Lund, Allan Meldgaard, and Brøndum-Nielsen, Karen

Abstract

A limited number of reports published since 2001 have described an association between increased nuchal translucency (NT) and osteogenesis imperfecta (OI). We report a new case which underlines the frequency of this association as well as the importance of follow-up and genetic evaluation. In the present case, ultrasound scanning at 13 weeks of gestation showed a NT of 3.2 mm and no other pathological findings. At 20 weeks a severe skeletal dysplasia was diagnosed by ultrasound. The pathology report of the aborted foetus indicated OI, and DNA analysis confirmed a COL1A1 mutation.

Published
2011

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

Author

Schönewolf-Greulich B, Bisgaard AM, Dunø M, Jespersgaard C, Rokkjaer M, Hansen LK, Tsoutsou E, Sofokleous C, Topcu M, Kaur S, Van Bergen NJ, Brøndum-Nielsen K, Larsen MJ, Sørensen KP, Christodoulou J, Fagerberg CR, and Tümer Z

Subjects
Alleles, Biopsy, Child, Facies, Genetic Association Studies, Genetic Predisposition to Disease, Genetic Testing, Humans, Male, Methyl-CpG-Binding Protein 2 genetics, Mosaicism, Mutation, Phenotype, Rett Syndrome diagnosis, Rett Syndrome genetics
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., (© 2018 John Wiley & Sons A/S. Published by John Wiley & Sons Ltd.)

Published
2019
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38. [Clinical molecular genetics diagnostics of Rett syndrome in Denmark].

Author

Schönewolf-Greulich B, Dunø M, Ravn K, Brøndum-Nielsen K, and Bisgaard AM

Subjects
Denmark, Diagnosis, Differential, Disease Progression, Female, Humans, Rett Syndrome genetics, Rett Syndrome pathology, Rett Syndrome diagnosis
Abstract

The neurodevelopmental disorder Rett syndrome was first described in 1966 by Andreas Rett, who described girls with loss of speech and hand use displaying characteristic hand stereotypies. Since then, the disease has been linked to mutations in the gene MECP2. However, the basis of the diagnosis is still clinical as defined by the latest clinical criteria as proposed by Neul and colleagues in 2010. This article presents a short clinical and molecular overview of the latest in Rett syndrome with emphasis on the Danish patients, headlines for making the diagnosis, differential diagnoses and molecular diagnostic possibilities.

Published
2015

39. [Increased nuchal translucency in osteogenesis imperfecta].

Author

Schönewolf-Greulich B, Skibsted L, Maroun LL, Lund AM, and Brøndum-Nielsen K

Subjects
Collagen Type I genetics, Female, Gestational Age, Humans, Osteogenesis Imperfecta embryology, Osteogenesis Imperfecta genetics, Pregnancy, Nuchal Translucency Measurement, Osteogenesis Imperfecta diagnostic imaging
Abstract

A limited number of reports published since 2001 have described an association between increased nuchal translucency (NT) and osteogenesis imperfecta (OI). We report a new case which underlines the frequency of this association as well as the importance of follow-up and genetic evaluation. In the present case, ultrasound scanning at 13 weeks of gestation showed a NT of 3.2 mm and no other pathological findings. At 20 weeks a severe skeletal dysplasia was diagnosed by ultrasound. The pathology report of the aborted foetus indicated OI, and DNA analysis confirmed a COL1A1 mutation.

Published
2011

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