Your search keyword '"Trine Bjørg Hammer"' showing total 23 results

1. An O-GlcNAc transferase pathogenic variant linked to intellectual disability affects pluripotent stem cell self-renewal

Author

Michaela Omelková, Christina Dühring Fenger, Marta Murray, Trine Bjørg Hammer, Veronica M. Pravata, Sergio Galan Bartual, Ignacy Czajewski, Allan Bayat, Andrew T. Ferenbach, Marios P. Stavridis, and Daan M. F. van Aalten

Subjects

ogt, o-glcnac, congenital disorders of glycosylation, intellectual disability, stem cells, self-renewal, Medicine, Pathology, RB1-214

Published

2023

2. The Phenotypic Spectrum of PRRT2-Associated Paroxysmal Neurologic Disorders in Childhood

Author

Jan Henje Döring, Afshin Saffari, Thomas Bast, Knut Brockmann, Laura Ehrhardt, Walid Fazeli, Wibke G. Janzarik, Gerhard Kluger, Hiltrud Muhle, Rikke S. Møller, Konrad Platzer, Joana Larupa Santos, Iben Bache, Astrid Bertsche, Michaela Bonfert, Ingo Borggräfe, Philip J. Broser, Alexandre N. Datta, Trine Bjørg Hammer, Hans Hartmann, Anette Hasse-Wittmer, Marco Henneke, Hermann Kühne, Johannes R. Lemke, Oliver Maier, Eva Matzker, Andreas Merkenschlager, Joachim Opp, Steffi Patzer, Kevin Rostasy, Birgit Stark, Adam Strzelczyk, Celina von Stülpnagel, Yvonne Weber, Markus Wolff, Birgit Zirn, Georg Friedrich Hoffmann, Stefan Kölker, and Steffen Syrbe

Subjects

PRRT2, BFIS, PKD, PKD/IC, hemiplegic migraine, familial infantile epilepsy, Biology (General), QH301-705.5

Abstract

Pathogenic variants in PRRT2, encoding the proline-rich transmembrane protein 2, have been associated with an evolving spectrum of paroxysmal neurologic disorders. Based on a cohort of children with PRRT2-related infantile epilepsy, this study aimed at delineating the broad clinical spectrum of PRRT2-associated phenotypes in these children and their relatives. Only a few recent larger cohort studies are on record and findings from single reports were not confirmed so far. We collected detailed genetic and phenotypic data of 40 previously unreported patients from 36 families. All patients had benign infantile epilepsy and harbored pathogenic variants in PRRT2 (core cohort). Clinical data of 62 family members were included, comprising a cohort of 102 individuals (extended cohort) with PRRT2-associated neurological disease. Additional phenotypes in the cohort of patients with benign sporadic and familial infantile epilepsy consist of movement disorders with paroxysmal kinesigenic dyskinesia in six patients, infantile-onset movement disorders in 2 of 40 individuals, and episodic ataxia after mild head trauma in one girl with bi-allelic variants in PRRT2. The same girl displayed a focal cortical dysplasia upon brain imaging. Familial hemiplegic migraine and migraine with aura were reported in nine families. A single individual developed epilepsy with continuous spikes and waves during sleep. In addition to known variants, we report the novel variant c.843G>T, p.(Trp281Cys) that co-segregated with benign infantile epilepsy and migraine in one family. Our study highlights the variability of clinical presentations of patients harboring pathogenic PRRT2 variants and expands the associated phenotypic spectrum.

Published

2020

3. An O-GlcNAc transferase pathogenic variant that affects pluripotent stem cell self-renewal

Author

Michaela Omelková, Christina Dühring Fenger, Marta Murray, Trine Bjørg Hammer, Veronica M. Pravata, Sergio Galan Bartual, Ignacy Czajewski, Allan Bayat, Andrew T. Ferenbach, Marios P. Stavridis, and Daan M. F. van Aalten

Abstract

O-linked β-N-acetylglucosamine (O-GlcNAc) transferase (OGT) is an essential enzyme that modifies proteins with O-GlcNAc. InbornOGTgenetic variants were recently shown to mediate a novel type of Congenital Disorder of Glycosylation (OGT-CDG) which is characterized by X-linked intellectual disability (XLID) and developmental delay. Here, we report an OGTC921Yvariant which co-segregates with XLID and epileptic seizures, and results in loss of catalytic activity. Colonies formed by mouse embryonic stem cells carrying OGTC921Yshow decreased levels of protein O-GlcNAcylation accompanied by decreased levels of Oct4, Sox2 and extracellular alkaline phosphatase (ALP), implying reduced self-renewal capacity. These data establish a link between OGT-CDG and embryonic stem cell self-renewal, providing a foundation for examining the developmental aetiology of this syndrome.Summary statementWe show that the C921Y O-GlcNAc transferase variant found in patients with intellectual disability leads to a defect in pluripotent stem cell self-renewal and decreased levels of stem cell markers.

Published

2023

4. [Genetic testing in autism spectrum disorder]

Author

Janni Majgaard, Jensen, Ulla Schierup, Nielsen, Allan, Bayat, Malene Bøgehus, Rasmussen, Rikke Steensbjerre, Møller, Anne Marie, Bisgaard, and Trine Bjørg, Hammer

Subjects

Autism Spectrum Disorder, Humans, Genetic Predisposition to Disease, Genetic Testing, Genomics

Abstract

Autism spectrum disorders (ASD) have a complex genetic component comprising both frequent polygenic and rare monogenic factors. Research is conducted in methods used to calculate polygenic risk scores, which are not applicable in clinical practice. Advances in genomic technology have identified several monogenic causes, and genetic testing may be offered to persons with ASD where a monogenic etiology is suspected. Herein, we provide an overview of the current knowledge and present the first national recommendation regarding genetic testing in ASD.

Published

2022

5. [Genetic factors provide individualised targeted treatment of epilepsy]

Author

Katrine M, Johannesen, Allan, Bayat, Trine Bjørg, Hammer, and Rikke S, Møller

Subjects

Epilepsy, Risk Factors, Seizures, Humans

Abstract

Epilepsy is a common neurological disorder characterized by recurrent and unprovoked seizures. Genetic factors are thought to play a major role, either as multiple risk factors in common epilepsies or as single gene variants in rare monogenic epilepsies. The latter are more often found in individuals with early seizure onset and comorbidities. This review finds that, as technology has accelerated our knowledge on monogenic epilepsies, we slowly move from diagnostics to the clinical application of a genetic diagnosis to optimize treatment. Thus, sometimes a genetic diagnosis provides a targeted treatment strategy.

Published

2022

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

Author

Zaid Afawi, Shekeeb S. Mohammad, Geoffrey Wallace, Ayelet Zerem, Amy L Schneider, Kyra E. Stuurman, Deepak Gill, Alison M. Muir, Russell C. Dale, Gali Heimer, Martino Montomoli, Elena Gardella, Emmanuelle Ranza, Simone Mandelstam, Peter Procopis, Øyvind L. Busk, Christian Korff, Arjan Bouman, Boudewijn Gunning, Connie T.R.M. Stumpel, Yunus Balcik, Christa de Geus, Philipp S. Reif, Yue-Hua Zhang, Sameer M. Zuberi, Volodymyr Kharytonov, Sébastien Küry, Patrick Edery, Sebastien Moutton, Trine Bjørg Hammer, Hannah Stamberger, Joseph D. Symonds, Gaetan Lesca, Samuel F. Berkovic, Massimiliano Rossi, Danique R.M. Vlaskamp, Eric W. Klee, Mark T Mackay, Felix Rosenow, Erica L. Macke, Chirag Patel, Jacob Bie Granild-Jensen, Helenius J. Schelhaas, Danielle M. Andrade, Lynette G. Sadleir, Iris M de Lange, Roseline Caumes, Eva Morava, Frédéric Tran Mau-Them, Anita Cairns, Keren Yosovich, Jing Zhang, Bruria Ben Zeev, Nicolas Chatron, Dorit Lev, Laura Reed, Pauline Monin, Eva H. Brilstra, Birgitte Bertelsen, Georgie Hollingsworth, Nienke E. Verbeek, Heather C Mefford, Rikke S. Møller, Johan R. Helle, Christina Fenger, Meriel McEntagart, Thomas Smol, Mark F. Bennett, Yuri A. Zarate, Renzo Guerrini, Elena Parrini, Candace T. Myers, Judith S. Verhoeven, Bertrand Isidor, Ruth Shalev, David A. Koolen, Ingrid E. Scheffer, Bobby P. C. Koeleman, Lauren Gunderson, Michael S. Hildebrand, Tara Sadoway, Richard J. Leventer, Sanjay M. Sisodiya, Krati Shah, Edith P. Almanza Fuerte, RS: GROW - R4 - Reproductive and Perinatal Medicine, MUMC+: DA KG Polikliniek (9), Klinische Genetica, and Clinical Genetics

Subjects

Male, Pediatrics, medicine.medical_specialty, INTELLECTUAL DISABILITY, Autism Spectrum Disorder, Encephalopathy, Nerve Tissue Proteins, ILAE COMMISSION, MOSAICISM, Epilepsy/genetics, CLASSIFICATION, Epilepsy, Brain Diseases/genetics, Genes, X-Linked, Seizures, Intellectual disability, Genotype, medicine, Humans, developmental and epileptic encephalopathy, MYOCLONIA, Atonic seizure, Genetics (clinical), Brain Diseases, ddc:618, Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7], KIAA2022, business.industry, MUTATIONS, medicine.disease, Phenotype, Autism Spectrum Disorder/genetics, Genes, X-Linked/genetics, Autism spectrum disorder, intellectual disability, NEXMIF, Autism, epilepsy, Female, INACTIVATION, Human medicine, Seizures/genetics, business, POSITION PAPER

Abstract

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

Published

2021

7. Neonatal developmental and epileptic encephalopathy due to autosomal recessive variants in SLC13A5 gene

Author

Tiziana Granata, Elena Freri, Nina Barišić, Paola Costa, Stefania Magri, Paola De Liso, Rami Abou Jamra, Barbara Castellotti, Luciana Musante, Trine Bjørg Hammer, Carla Marini, Gaetan Lesca, Federico Vigevano, Sara Matricardi, Tilman Polster, Cinzia Gellera, Rikke S. Møller, Dana Craiu, and Julie Oertel

Subjects

Male, 0301 basic medicine, Proband, Phenytoin, Pediatrics, medicine.medical_specialty, Adolescent, Developmental Disabilities, Genetic counseling, Status epilepticus, neonatal, Young Adult, 03 medical and health sciences, 0302 clinical medicine, tooth hypoplasia, medicine, Humans, Genetic Predisposition to Disease, Child, development, Brain Diseases, Epilepsy, Symporters, business.industry, Genetic Variation, Electroencephalography, autosomal recessive, SLC13A5 gene, Carbamazepine, medicine.disease, Hypodontia, epileptic encephalopathy, 030104 developmental biology, Neurology, Child, Preschool, Developmental Milestone, Female, Phenobarbital, Neurology (clinical), medicine.symptom, business, 030217 neurology & neurosurgery, Follow-Up Studies, medicine.drug

Abstract

Objective: Autosomal recessive pathogenic variants of the SLC13A5 gene are associated with severe neonatal epilepsy, developmental delay, and tooth hypoplasia/hypodontia. We report on 14 additional patients and compare their phenotypic features to previously published patients to identify the clinical hallmarks of this disorder. Methods: We collected clinical features of 14 patients carrying biallelic variants in SLC13A5 and performed a PubMed search to identify previously published patients. Results: All patients presented clonic or tonic seizures in the first days of life, evolving into status epilepticus in 57%. Analysis of seizure frequency and developmental milestones divided into five epochs showed an evolutionary trajectory of both items. In the first 3 years of life, 72% of patients had weekly/monthly seizures, often triggered by fever; 14% were seizure-free. Between the ages of 3 and 12 years, 60% become seizure-free; in the following years, up to age 18 years, 57% were seizure-free. After the age of 18 years, all three patients reaching this age were seizure-free. Similarly, 86% of patients at onset presented mild to moderate developmental impairment and diffuse hypotonia. In late childhood, all had developmental delay that was severe in most. Benzodiazepines, phenobarbital, phenytoin, and carbamazepine were the most effective drugs. Eight probands carried heterozygous compound variants, and homozygous pathogenic variants occurred in six. Literature review identified 45 patients carrying SLC13A5 gene pathogenic variants whose clinical features overlapped with our cohort. A peculiar and distinguishing sign is the presence of tooth hypoplasia and/or hypodontia in most patients. Significance: Autosomal recessive pathogenic variants in SLC13A5 are associated with a distinct neonatal epileptic encephalopathy evolving into severe cognitive and motor impairment, yet with seizures that settle down in late childhood. Tooth hypoplasia or hypodontia remains the peculiar feature. The SLC13A5 gene should be screened in neonatal epileptic encephalopathies; its recessive inheritance has relevance for genetic counseling.

Published

2020

8. DNA methylation episignature in Gabriele-de Vries syndrome

Author

Florian Cherik, Jack Reilly, Jennifer Kerkhof, Michael Levy, Haley McConkey, Mouna Barat-Houari, Kameryn M. Butler, Christine Coubes, Jennifer A. Lee, Gwenael Le Guyader, Raymond J. Louie, Wesley G. Patterson, Matthew L. Tedder, Mads Bak, Trine Bjørg Hammer, William Craigen, Florence Démurger, Christèle Dubourg, Mélanie Fradin, Rachel Franciskovich, Eirik Frengen, Jennifer Friedman, Nathalie Ruiz Palares, Maria Iascone, Doriana Misceo, Pauline Monin, Sylvie Odent, Christophe Philippe, Flavien Rouxel, Veronica Saletti, Petter Strømme, Perla Cassayre Thulin, Bekim Sadikovic, David Genevieve, CHU Clermont-Ferrand, University of Western Ontario (UWO), London Health Sciences Center (LHSC), CHU Montpellier, Centre Hospitalier Régional Universitaire [Montpellier] (CHRU Montpellier), The Greenwood Genetic Center, Centre hospitalier universitaire de Poitiers (CHU Poitiers), Rigshospitalet [Copenhagen], Copenhagen University Hospital, Baylor College of Medicine (BCM), Baylor University, Centre hospitalier Bretagne Atlantique (Morbihan) (CHBA), Institut de Génétique et Développement de Rennes (IGDR), Université de Rennes (UR)-Centre National de la Recherche Scientifique (CNRS)-Structure Fédérative de Recherche en Biologie et Santé de Rennes ( Biosit : Biologie - Santé - Innovation Technologique ), CHU Pontchaillou [Rennes], Centre de référence Maladies Rares CLAD-Ouest [Rennes], Oslo University Hospital [Oslo], University of California [San Diego] (UC San Diego), University of California (UC), Hospital Papa Giovanni XXIII (Hosp P Giovanni XXIII), Hôpital Femme Mère Enfant [CHU - HCL] (HFME), Hospices Civils de Lyon (HCL), Centre Hospitalier Universitaire de Dijon - Hôpital François Mitterrand (CHU Dijon), Fondazione IRCCS Istituto Neurologico 'Carlo Besta', and University of Utah

Subjects

Male, Gabriele-de Vries syndrome, Genome, Phenotype, Neurodevelopmental Disorders, [SDV]Life Sciences [q-bio], Intellectual Disability, Humans, Epigenetics, Syndrome, DNA Methylation, YY1, Genetics (clinical)

Abstract

International audience; PURPOSE: Gabriele-de Vries syndrome (GADEVS) is a rare genetic disorder characterized by developmental delay and/or intellectual disability, hypotonia, feeding difficulties, and distinct facial features. To refine the phenotype and to better understand the molecular basis of the syndrome, we analyzed clinical data and performed genome-wide DNA methylation analysis of a series of individuals carrying a YY1 variant. METHODS: Clinical data were collected for 13 individuals not yet reported through an international call for collaboration. DNA was collected for 11 of these individuals and 2 previously reported individuals in an attempt to delineate a specific DNA methylation signature in GADEVS. RESULTS: Phenotype in most individuals overlapped with the previously described features. We described 1 individual with atypical phenotype, heterozygous for a missense variant in a domain usually not involved in individuals with YY1 pathogenic missense variations. We also described a specific peripheral blood DNA methylation profile associated with YY1 variants. CONCLUSION: We reported a distinct DNA methylation episignature in GADEVS. We expanded the clinical profile of GADEVS to include thin/sparse hair and cryptorchidism. We also highlighted the utility of DNA methylation episignature analysis for classification of variants of unknown clinical significance.

Published

2021

9. SLC7A3: In Silico Prediction of a Potential New Cause of Childhood Epilepsy

Author

Jo Sourbron, Katrien Jansen, Davide Mei, Trine Bjørg Hammer, Rikke S. Møller, Nina B. Gold, Lauren O'Grady, Renzo Guerrini, and Lieven Lagae

Subjects

Male, Epilepsy, General Medicine, Microarray Analysis, SLC7A3, whole exome sequencing, gene panel, Seizures, case reports, Pediatrics, Perinatology and Child Health, Exome Sequencing, epilepsy, Amino Acid Transport Systems, Basic, Humans, Neurology (clinical), Genetic Testing, Child

Abstract

We report an in-depth genetic analysis in an 11-year-old boy with drug-resistant, generalized seizures and developmental disability. Three distinct variants of unknown clinical significance (VUS) were detected by whole exome sequencing (WES) but not by initial genetic analyses (microarray and epilepsy gene panel). These variants involve the SLC7A3, CACNA1H, and IGLON5 genes, which were subsequently evaluated by computational analyses using the InterVar tool and MutationTaster. While future functional studies are necessary to prove the pathogenicity of a certain VUS, segregation analyses over three generations and in silico predictions suggest the X-linked gene SLC7A3 (transmembrane solute carrier transporter) as the likely culprit gene in this patient. In addition, a search via GeneMatcher unveiled two additional patients with a VUS in SLC7A3. We propose SLC7A3 as a likely candidate gene for epilepsy and/or developmental/cognitive delay and provide an overview of the 27 SLC genes related to epilepsy by other preclinical and/or clinical studies.

Published

2021

10. Phenotypic heterogeneity and mosaicism in Xia-Gibbs syndrome:Five Danish patients with novel variants in AHDC1

Author

Brian Nauheimer Andersen, Trine Bjørg Hammer, Niels Ove Illum, Dorte L Lildballe, Naja Becher, Lotte Andreasen, Mikkel Ø Andersen, Pernille Axel Gregersen, Jens Erik K Nielsen, Mette B Thorup, Christina Fagerberg, Emilie Erbs, Anders Bojesen, Charlotte Brasch-Andersen, Monica Zilmer, Soren L Faergeman, and Maria Rasmussen

Subjects

Adult, Foot Deformities, Male, AHDC1, Adolescent, Developmental Disabilities, Biology, Frameshift mutation, Craniofacial Abnormalities, Loss of heterozygosity, Young Adult, Neurodevelopmental disorder, Intellectual disability, Genetics, medicine, Humans, Frameshift Mutation, Genetics (clinical), Exome sequencing, Genetic heterogeneity, Whole exome sequencing, Syndrome, General Medicine, medicine.disease, Phenotype, Hypotonia, DNA-Binding Proteins, Dysmorphism, Muscle Hypotonia, Female, medicine.symptom, Xia-gibbs syndrome, Reverse phenotyping

Abstract

Xia-Gibbs syndrome (XGS) is a neurodevelopmental disorder characterized by intellectual disability, developmental delay, seizures, hypotonia, obstructive sleep apnoea and mild facial dysmorphism. Heterozygosity for loss-of-function variants in AHDC1, encoding the AT-hook DNA binding motif containing protein 1, were discovered in 2014 as the likely genetic cause of Xia-Gibbs syndrome. We present five patients with Xia-Gibbs syndrome caused by previously unreported variants in AHDC1. Two of the patients share a frameshift variant: c.2849del (p.(Pro950Argfs*192)) in AHDC1. Despite sharing this variant, the two patients show remarkable phenotypic differences underscoring the clinical heterogeneity of Xia-Gibbs syndrome. In addition, we present a case of Xia-Gibbs syndrome caused by mosaicism for an AHDC1 variant.

Published

2021

11. A Recurrent Missense Variant in AP2M1 Impairs Clathrin-Mediated Endocytosis and Causes Developmental and Epileptic Encephalopathy

Author

Batsal Devkota, José M. Serratosa, Joel N. Hirschhorn, Renzo Guerrini, Patrick May, Johanna A. Jähn, Paul Avillach, Yvonne G. Weber, Sha Tang, Kaja Kristine Selmer, Joseph J. Shen, Annika Rademacher, Joseph Peeden, Ulrich Stephani, Judson Kilbourn, Niklas Schwarz, Deb K. Pal, Lacey Smith, Trine Bjørg Hammer, Carla Marini, Deanne Taylor, Ingo Helbig, Rudi Balling, Arvid Suls, Holger Lerche, Karl Martin Klein, Simone Seiffert, Annapurna Poduri, Bobby P. C. Koeleman, Tania López-Hernández, Deepali N. Shinde, Stéphanie Baulac, Sawona Biswas, Eric LeGuern, Peter D. Galer, Volker Haucke, Katherine L. Helbig, Ian D. Krantz, Aarno Palotie, Sarah Weckhuysen, Nadja Hümpfer, Tiina Talvik, Rikke S. Møller, Roland Krause, Allison Heath, Dorota Hoffman-Zacharska, Nina Barišić, Peter De Jonghe, Hiltrud Muhle, In-Hee Lee, Kenneth D. Mandl, Felix Benninger, Dana Craiu, Florence T. Bourgeois, Colin A Ellis, Sanjay M. Sisodiya, Christel Depienne, Barbara Hallinan, Eric D. Marsh, Susanne Schubert-Bast, Manuela Pendziwiat, Kristen L. Sund, Federico Zara, Tracy A. Glauser, Katalin Štěrbová, Johannes R. Lemke, Oded Shor, Anna-Elina Lehesjoki, Helle Hjalgrim, Anna Bartels, Vladimir Komarek, Peter White, Tarja Linnankivi, Hande Caglayan, Sarah von Spiczak, Shiva Ganesan, Felix Rosenow, Sek Won Kong, Pasquale Striano, EuroEPINOMICS-RES Consortium, GRIN Consortium, Department of Medical and Clinical Genetics, Centre of Excellence in Complex Disease Genetics, Aarno Palotie / Principal Investigator, Genomics of Neurological and Neuropsychiatric Disorders, Institute for Molecular Medicine Finland, HUS Children and Adolescents, and Children's Hospital

Subjects

0301 basic medicine, PROTEIN, ILAE COMMISSION, clathrin-mediated endocytosis, 3124 Neurology and psychiatry, Mice, Epilepsy, 0302 clinical medicine, BINDING, Conditional gene knockout, Missense mutation, Child, Genetics (clinical), Mice, Knockout, Genetics, Brain Diseases, neurodevelopmental disorders, Phenotype, Endocytosis, Adaptor Protein Complex mu Subunits, Child, Preschool, Female, POSITION PAPER, RECRUITMENT, Adolescent, computational phenotypes, developmental and epileptic encephalopathy, Human Phenotype Ontology, synaptic transmission, Adaptor Protein Complex 2, Mutation, Missense, Biology, CLASSIFICATION, Article, 03 medical and health sciences, Exome Sequencing, medicine, Animals, Humans, Synaptic vesicle recycling, ADAPTER AP-2, Generalized epilepsy, 3112 Neurosciences, Infant, Receptor-mediated endocytosis, medicine.disease, Clathrin, 030104 developmental biology, DE-NOVO MUTATIONS, 3111 Biomedicine, Human medicine, 030217 neurology & neurosurgery

Abstract

The developmental and epileptic encephalopathies (DEEs) are heterogeneous disorders with a strong genetic contribution, but the underlying genetic etiology remains unknown in a significant proportion of individuals. To explore whether statistical support for genetic etiologies can be generated on the basis of phenotypic features, we analyzed whole-exome sequencing data and phenotypic similarities by using Human Phenotype Ontology (HPO) in 314 individuals with DEEs. We identified a de novo c.508C>T (p.Arg170Trp) variant in AP2M1 in two individuals with a phenotypic similarity that was higher than expected by chance (p = 0.003) and a phenotype related to epilepsy with myoclonic-atonic seizures. We subsequently found the same de novo variant in two individuals with neurodevelopmental disorders and generalized epilepsy in a cohort of 2,310 individuals who underwent diagnostic whole-exome sequencing. AP2M1 encodes the mu-subunit of the adaptor protein complex 2 (AP-2), which is involved in clathrin-mediated endocytosis (CME) and synaptic vesicle recycling. Modeling of protein dynamics indicated that the p.Arg170Trp variant impairs the conformational activation and thermodynamic entropy of the AP-2 complex. Functional complementation of both the mu-subunit carrying the p.Arg170Trp variant in human cells and astrocytes derived from AP-2 mu conditional knockout mice revealed a significant impairment of CME of transferrin. In contrast, stability, expression levels, membrane recruitment, and localization were not impaired, suggesting a functional alteration of the AP-2 complex as the underlying disease mechanism. We establish a recurrent pathogenic variant in AP2M1 as a cause of DEEs with distinct phenotypic features, and we implicate dysfunction of the early steps of endocytosis as a disease mechanism in epilepsy.

Published

2019

12. Expansion of the CCDC22 associated ritscher-schinzel/3C syndrome and review of the literature:Should the minimal diagnostic criteria be revised?

Author

Christina Fenger, Trine Bjørg Hammer, Cathrine E. Gjerulfsen, Allan Bayat, and Rikke S. Møller

Subjects

0301 basic medicine, Proband, Male, Pediatrics, medicine.medical_specialty, RTSCS, Fossa, Adolescent, Mutation, Missense, Disease, 030105 genetics & heredity, Heart Septal Defects, Atrial, Craniofacial Abnormalities, Diagnosis, Differential, 03 medical and health sciences, Epilepsy, CCDC22, Genetics, medicine, Missense mutation, Humans, Abnormalities, Multiple, Craniofacial, Genetics (clinical), Genetic testing, medicine.diagnostic_test, biology, business.industry, Epileptic encephalopathy, Ritscher-schinzel syndrome, Proteins, General Medicine, medicine.disease, biology.organism_classification, 030104 developmental biology, Phenotype, 3C syndrome, business, Dandy-Walker Syndrome

Abstract

The Ritscher-Schinzel syndrome (RTSCS) is a rare condition with craniofacial, cardiac and fossa posterior abnormalities. RTSCS is subdivided into Ritscher-Schinzel syndrome 1 (RTSCS1) caused by pathogenic variants in coiled-coil domain-containing protein 22 (CCDC22), and Ritscher-Schinzel syndrome 2 (RTSCS2) caused by pathogenic variants in WASH complex subunit 5 (WASHC5). CCDC22 is inherited in an X-linked recessive manner while WASHC5 is inherited in an autosomal recessive manner. Only 17 individuals with a molecular diagnosis are reported. In the past, the diagnosis of RTSCS was solely based on the clinical findings, and minimal diagnostic criteria has been proposed for the syndrome: Cardiac malformations (other than isolated patent ductus arteriosis), fossa posterior malformations, and certain dysmorphic features. However, those criteria are not present in all patients. We aim to further delineate the spectrum of CDCC22 associated RTSCS and present a novel patient with epileptic encephalopathy due to a presumed disease causing CCDC22 missense variant inherited from a healthy mother and grandmother. An affected maternal uncle had passed away at the age of 12 months and was thus unavailable for genetic testing. The proband and the maternal uncle had the typical facial dysmorphism associated with RTSCS, and they closely resembled previously published RTSCS2 patients with a molecular diagnosis. This suggests that RTSCS1 and RTSCS2 patients have a similar facial gestalt. We also review the literature on RTSCS, we explore potential differences and similarities between CCDC22 and W ASHC5 associated RTSCS and discuss the minimal diagnostic criteria.

Published

2021

13. RHOBTB2 Mutations Expand the Phenotypic Spectrum of Alternating Hemiplegia of Childhood

Author

Nathalie Bednarek, Hannah Stamberger, Anna Basu, Diane Doummar, Walid Fazeli, Sara Zagaglia, Rikke S. Møller, F. Lucy Raymond, S. Krithika, Andrew A Mallick, Tobias Bartolomaeus, Trine Bjørg Hammer, Sarah Weckhuysen, Manju A. Kurian, J. Helen Cross, Bryan Lynch, Alba Sanchis-Juan, Laura Hernandez-Hernandez, Sanjay M. Sisodiya, Helena Martins Custodio, Anirban Majumdar, Cyril Mignot, Dora Steel, Robert Spaull, Mary D. King, Aikaterini Vezyroglou, Kathleen M. Gorman, Boris Keren, Centre de Recherche en Sciences et Technologies de l'Information et de la Communication - EA 3804 (CRESTIC), and Université de Reims Champagne-Ardenne (URCA)

Subjects

0301 basic medicine, Dystonia, Pediatrics, medicine.medical_specialty, Ataxia, business.industry, Alternating hemiplegia of childhood, medicine.disease, Article, 3. Good health, 03 medical and health sciences, Epilepsy, 030104 developmental biology, 0302 clinical medicine, ATP1A3, Intellectual disability, medicine, Missense mutation, Human medicine, Neurology (clinical), Young adult, medicine.symptom, business, [SDV.MHEP]Life Sciences [q-bio]/Human health and pathology, 030217 neurology & neurosurgery

Abstract

ObjectiveTo explore the phenotypic spectrum of RHOBTB2-related disorders and specifically to determine whether patients fulfill criteria for alternating hemiplegia of childhood (AHC), we report the clinical features of 11 affected individuals.MethodsIndividuals with RHOBTB2-related disorders were identified through a movement disorder clinic at a specialist pediatric center, with additional cases identified through collaboration with other centers internationally. Clinical data were acquired through retrospective case-note review.ResultsEleven affected patients were identified. All had heterozygous missense variants involving exon 9 of RHOBTB2, confirmed as de novo in 9 cases. All had a complex motor phenotype, including at least 2 different kinds of movement disorder, e.g., ataxia and dystonia. Many patients demonstrated several features fulfilling the criteria for AHC: 10 patients had a movement disorder including paroxysmal elements, and 8 experienced hemiplegic episodes. In contrast to classic AHC, commonly caused by mutations in ATP1A3, these events were reported later only in RHOBTB2 mutation–positive patients from 20 months of age. Seven patients had epilepsy, but of these, 4 patients achieved seizure freedom. All patients had intellectual disability, usually moderate to severe. Other features include episodes of marked skin color change and gastrointestinal symptoms, each in 4 patients.ConclusionAlthough heterozygous RHOBTB2 mutations were originally described in early infantile epileptic encephalopathy type 64, our study confirms that they account for a more expansive clinical phenotype, including a complex polymorphic movement disorder with paroxysmal elements resembling AHC. RHOBTB2 testing should therefore be considered in patients with an AHC-like phenotype, particularly those negative for ATPA1A3 mutations.

Published

2021

14. SLC35A2-related congenital disorder of glycosylation: Defining the phenotype

Author

Meena Balasubramanian, Mohnish Suri, Gaetan Lesca, Archana Desurkar, Ann-Charlotte Thuresson, Carina Wallgren-Pettersson, Ashok Raghavan, Rikke S. Møller, T. Michael Yates, Anne Lise Poulat, Trine Bjørg Hammer, Medicum, and Department of Medical and Clinical Genetics

Subjects

Developmental and epileptic encephalopathy, 0301 basic medicine, medicine.medical_specialty, Glycosylation, Neurology, Monosaccharide Transport Proteins, Intellectual disability, Cortical visual impairment, Disease, Bioinformatics, 3124 Neurology and psychiatry, 03 medical and health sciences, medicine, Humans, Abnormalities, Multiple, Congenital disorders of glycosylation, Child, X chromosome, business.industry, 3112 Neurosciences, Infant, General Medicine, medicine.disease, Phenotype, Hypsarrhythmia, 3. Good health, 030104 developmental biology, Pediatrics, Perinatology and Child Health, GENETIC CAUSES, Female, Neurology (clinical), SLC35A2, medicine.symptom, business, Congenital disorder of glycosylation

Abstract

We aim to further delineate the phenotype associated with pathogenic variants in the SLC35A2 gene, and review all published literature to-date. This gene is located on the X chromosome and encodes a UDP-galactose transporter. Pathogenic variants in SLC35A2 cause a congenital disorder of glycosylation. The condition is rare, and less than twenty patients have been reported to-date. The phenotype is complex and has not been fully defined. Here, we present a series of five patients with de novo pathogenic variants in SLC35A2. The patients' phenotype includes developmental and epileptic encephalopathy with hypsarrhythmia, facial dysmorphism, severe intellectual disability, skeletal abnormalities, congenital cardiac disease and cortical visual impairment. Developmental and epileptic encephalopathy with hypsarrhythmia is present in most patients with SLC35A2 variants, and is drug-resistant in the majority of cases. Adrenocorticotropic hormone therapy may achieve partial or complete remission of seizures, but the effect is usually temporary. Isoelectric focusing of transferrins may be normal after infancy, therefore a congenital disorder of glycosylation should still be considered as a diagnosis in the presence of a suggestive phenotype. We also provide evidence that cortical visual impairment is part of the phenotypic spectrum. (C) 2018 European Paediatric Neurology Society. Published by Elsevier Ltd. All rights reserved.

Published

2018

15. Translation and Adaptation of the Genetic Counselling Outcome Scale (GCOS-24) for Use in Denmark

Author

Trine Bjørg Hammer, Birgitte Rode Diness, Gritt Overbeck, Tina Duelund Hjortshøj, Else Sørensen, Susanne Timshel, and Marion McAllister

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Psychometrics, Denmark, Genetic counseling, Genetic Counseling, 030105 genetics & heredity, Outcome (game theory), Danish, 03 medical and health sciences, 0302 clinical medicine, Cronbach's alpha, Surveys and Questionnaires, Outcome Assessment, Health Care, Health care, Humans, Medicine, Translations, 030212 general & internal medicine, Genetics (clinical), Descriptive statistics, business.industry, Reproducibility of Results, language.human_language, Family medicine, language, Ceiling effect, Female, Patient-reported outcome, business, Social psychology

Abstract

Outcome measurement in clinical genetics is challenging. Robust outcome measures are needed to provide evidence to support service development within genetic counseling. The Genetic Counselling Outcome Scale (GCOS-24), a Patient Reported Outcome Measure (PROM), was developed in English and validated with clinical genetics patients in the British NHS. This study reports the translation and adaptation of the GCOS-24 for use in Denmark. GCOS-24 was translated and back translated, supervised by an expert committee. Feedback on the first version was collected from genetic counseling patients in qualitative interviews focusing on instructions for use, response options and specific items considered semantically difficult. After further adjustment the adapted and translated version was administered to a second sample of patients, with responses analyzed using descriptive statistics. Eighteen interviews were conducted, and led to adjustment of item wording. Sixty-one patients completed the final version GCOS-24dk. Internal consistency is good (Cronbach's α =0.79), with an acceptable number of missing responses and no floor or ceiling effect observed. GCOS-24 has been successfully translated and adapted for use in a Danish setting. The study confirms the feasibility of local adaptation of patient reported outcome measures and stresses the importance of adaptation, even across quite similar populations and health care systems.

Published

2017

16. SLC35A2-CDG: Functional Characterization, Expanded Molecular, Clinical, and Biochemical Phenotypes of 30 Unreported Individuals

Author

Jesse M. Hunter, Mary S. Willis, Bryce A. Mendelsohn, Sha Tang, Carlos A. Bacino, Eric Vilain, Hane Lee, Jill A. Rosenfeld, Delphine Héron, Tyler Mark Pierson, Zöe Powis, Shenela Lakhani, Naghmeh Dorrani, Lorenzo D. Botto, Maria J. Guillen Sacoto, Jaclyn Haven, Julie S. Cohen, Trine Bjørg Hammer, Bobby G. Ng, Charles Marques Lourenço, Rita Barone, Jennifer Burton, Ingrid E. Scheffer, Wendy G. Mitchell, Pasquale Striano, Stephanie Grunewald, Stanley F. Nelson, Nicola Longo, Jane Juusola, Fernando Scaglia, Christopher C.Y. Mak, Hudson H. Freeze, Shoji Yano, Leon G. Epstein, Arthur Partikian, Domenico Garozzo, Mohammed Almannai, Joy Lee, Hui Yang, Dianalee McKnight, Abdallah F. Elias, William A. Gahl, Nilika S. Singhal, Christina G.S. Palmer, Devorah Segal, Andrew C. Edmondson, George E. Hoganson, Cyril Mignot, Brian H.Y. Chung, Colleen M. Carlston, Mahim Jain, M. Elizabeth Ross, Paulina Sosicka, David Coman, Sharon F. Suchy, Shane C. Quinonez, Ghayda M. Mirzaa, Katrina M. Dipple, Satish Agadi, Joseph D. Symonds, Lynne A. Wolfe, Marc C. Patterson, Brigid M. Regan, Luisa Sturiale, Mariusz Olczak, Hiltrud Muhle, Katherine Lewis, William B. Dobyns, and Matthew R. Herzog

Subjects

UDP-galactose, congenital disorders of glycosylation, glycoside, nucleotide sugar transporter, Male, Glycosylation, Monosaccharide Transport Proteins, Cells, Biopsy, Clinical Sciences, CHO Cells, Biology, medicine.disease_cause, Article, Uridine Diphosphate Galactose, 03 medical and health sciences, chemistry.chemical_compound, Congenital Disorders of Glycosylation, Cricetulus, Clinical Research, Genetics, medicine, 2.1 Biological and endogenous factors, Animals, Humans, Aetiology, Allele, Gene, Genetics (clinical), Cells, Cultured, 030304 developmental biology, Pediatric, Genetics & Heredity, 0303 health sciences, Mutation, Cultured, 030305 genetics & heredity, medicine.disease, Phenotype, Biomarker (cell), carbohydrates (lipids), chemistry, Female, Lipid glycosylation, Congenital disorder of glycosylation

Abstract

Pathogenic de novo variants in the X-linked gene SLC35A2 encoding the major Golgi-localized UDP-galactose transporter required for proper protein and lipid glycosylation cause a rare type of congenital disorder of glycosylation known as SLC35A2-congenital disorders of glycosylation (CDG; formerly CDG-IIm). To date, 29 unique de novo variants from 32 unrelated individuals have been described in the literature. The majority of affected individuals are primarily characterized by varying degrees of neurological impairments with or without skeletal abnormalities. Surprisingly, most affected individuals do not show abnormalities in serum transferrin N-glycosylation, a common biomarker for most types of CDG. Here we present data characterizing 30 individuals and add 26 new variants, the single largest study involving SLC35A2-CDG. The great majority of these individuals had normal transferrin glycosylation. In addition, expanding the molecular and clinical spectrum of this rare disorder, we developed a robust and reliable biochemical assay to assess SLC35A2-dependent UDP-galactose transport activity in primary fibroblasts. Finally, we show that transport activity is directly correlated to the ratio of wild-type to mutant alleles in fibroblasts from affected individuals.

Published

2019

17. Children and adolescents previously treated with glucocorticoids display lower verbal intellectual abilities

Author

Olaf B. Paulson, William F. C. Baaré, Hartwig R. Siebner, Kathrine Skak Madsen, Sara Krøis Holm, Martin D. Vestergaard, Peter Uldall, Alfred Peter Born, and Trine Bjørg Hammer

Subjects

Male, medicine.medical_specialty, Nephrotic Syndrome, Adolescent, Disease, Speech Disorders, Rheumatic Diseases, Cognitive development, Humans, Medicine, Child, Psychiatry, Glucocorticoids, Retrospective Studies, Wechsler Intelligence Scale for Children, Intelligence Tests, Perinatal Exposure, Intelligence quotient, business.industry, Cumulative dose, Retrospective cohort study, General Medicine, Pediatrics, Perinatology and Child Health, Prednisolone, Female, business, medicine.drug, Clinical psychology

Abstract

Aim Perinatal exposure to glucocorticoids has been associated with adverse cerebral effects, but little is known about their effect on cognitive development and exposure later in childhood. This study examined intellectual abilities, memory and behavioural problems in children previously treated with glucocorticoids. Methods We evaluated 38 children aged from seven to 16 years, who had been treated with glucocorticoids for rheumatic disease or nephrotic syndrome, together with 42 healthy controls matched for age, gender and parental education. The median cumulative dose of prednisolone equivalents was 158 mg/kg (range 21–723) and the mean time that had elapsed since treatment was three-and-a-half (standard deviation 2.2) years. Intellectual abilities were assessed with the Wechsler Intelligence Scale for Children and memory performance and behavioural problems with a pattern recognition memory task and the Child Behaviour Check List. Results There were no significant differences between the groups in pattern recognition memory, perceptual organisation index or behavioural problems, but patients had a significantly lower verbal comprehension index and this difference was present in both disease groups. There were no significant dose–response relationships regarding verbal intellectual abilities. Conclusion Children and adolescents previously treated with glucocorticoids seemed to have lower intellectual verbal abilities than healthy controls.

Published

2015

18. Structural brain correlates of sensorimotor gating in antipsychotic-naive men with first-episode schizophrenia

Author

B. Glenthøj, Bodil Aggernaes, William F. C. Baaré, Trine Bjørg Hammer, Arnold Skimminge, Bjørn H Ebdrup, and Bob Oranje

Subjects

Adult, Male, Reflex, Startle, Posterior parietal cortex, Grey matter, Brain mapping, Premotor cortex, Young Adult, medicine, Image Processing, Computer-Assisted, Humans, Pharmacology (medical), Biological Psychiatry, Prepulse inhibition, Cerebral Cortex, Brain Mapping, Sensory gating, Brain, Sensory Gating, Startle reaction, Research Papers, Magnetic Resonance Imaging, Psychiatry and Mental health, medicine.anatomical_structure, Superior frontal gyrus, Acoustic Stimulation, Case-Control Studies, Schizophrenia, Psychology, Neuroscience

Abstract

Background: Prepulse inhibition (PPI) of the startle reflex is modulated by a complex neural network. Prepulse inhibition impairments are found at all stages of schizophrenia. Previous magnetic resonance imaging (MRI) studies suggest that brain correlates of PPI differ between patients with schizophrenia and healthy controls; however, these studies included only patients with chronic illness and medi cated patients. Our aim was to examine the structural brain correlates of PPI in antipsychotic-naive patients with first-episode schizophrenia. Methods: We performed acoustic PPI assessment and structural MRI (1.5 and 3 T) in men with first-episode schizophrenia and age-matched controls. Voxel-based morphometry was used to investigate the association between PPI and grey matter volumes. Results: We included 27 patients and 38 controls in the study. Patients had lower PPI than controls. The brain areas in which PPI and grey matter volume correlated did not differ between the groups. Independent of group, PPI was significantly and positively associated with regional grey matter volume in the right superior parietal cortex. Prepulse inhibition and grey matter volume associations were also observed in the left rostral dorsal premotor cortex, the right presupplementary motor area and the anterior medial superior frontal gyrus bilaterally. Follow-up analyses suggested that the rostral dorsal premotor cortex and presupplementary motor area correlations were driven predominantly by the controls. Limitations: We used 2 different MRI scanners, which might have limited our ability to find subcortical associations since interscanner consistency is low for subcortical regions. Conclusion: The superior parietal cortex seems to be involved in the regulation of PPI in controls and antipsychotic-naive men with first-episode schizophrenia. Our observation that PPI deficits in schizophrenia may be related to the rostral dorsal premotor cortex and presupplementary motor area, brain areas involved in maintaining relevant sensory information and voluntary inhibition, warrants further study.

Published

2013

19. Stability of prepulse inhibition and habituation of the startle reflex in schizophrenia: a 6-year follow-up study of initially antipsychotic-naive, first-episode schizophrenia patients

Author

Bob Oranje, Hannah Bro, Birte Glenthøj, Birgitte Fagerlund, and Trine Bjørg Hammer

Subjects

Adult, Male, medicine.medical_specialty, Reflex, Startle, Time Factors, Audiology, Mental Processes, Moro reflex, medicine, Humans, Pharmacology (medical), Habituation, Habituation, Psychophysiologic, Prepulse inhibition, Pharmacology, Antipsychotic naive, Follow up studies, Stimulus onset asynchrony, Neural Inhibition, medicine.disease, Psychiatry and Mental health, Schizophrenia, Endophenotype, Case-Control Studies, Psychology, Clinical psychology, Antipsychotic Agents, Follow-Up Studies

Abstract

Deficits in information processing appear to be core features in the pathogenesis of schizophrenia. Prepulse inhibition (PPI) and habituation of the startle reflex are operational measures of early information processing. Impaired PPI in schizophrenia has been replicated in many studies and is regarded as an endophenotype for schizophrenia. However, reports on the stability of PPI over a longer period of time are lacking, both for patients with schizophrenia and for healthy subjects. The current study examined 25 initially drug-naive, first-episode schizophrenia patients and 23 healthy matched controls. Three PPI measures [stimulus onset asynchrony (SOA) 30, 60, 120 ms] and habituation were assessed at baseline, and again after 6 yr. Sixteen patients and 17 healthy controls completed the study, and 13 patients and 17 healthy controls were included in the final analysis. The schizophrenia patients had PPI deficits compared to controls at baseline. After 6 yr, no significant group differences were found. PPI had increased significantly in the patients and had decreased significantly in controls. In addition, patients showed significantly less habituation than controls while habituation did not change in patients or controls. The present results show that PPI in drug-naive, first-episode schizophrenia patients can improve significantly over time. As PPI increased in patients over the same period that it decreased in controls, it is likely that the increase was caused by disease-related factors such as disease process, clinical state, or medication.

Published

2011

20. Poster #256 STRUCTURAL BRAIN CORRELATES OF SENSORIMOTOR GATING IN SCHIZOPHRENIA PATIENTS AND HEALTHY CONTROLS: A 6 YEAR FOLLOW-UP STUDY OF INITIALLY ANTIPSYCHOTIC NAÍ

Author

Birte Glenthøj, William F. C. Baaré, Arnold Skimminge, Bob Oranje, and Trine Bjørg Hammer

Subjects

Psychiatry and Mental health, medicine.medical_specialty, Schizophrenia, medicine.medical_treatment, Sensorimotor Gating, medicine, Follow up studies, Psychology, Antipsychotic, medicine.disease, Psychiatry, Biological Psychiatry, Clinical psychology

Published

2012

21. THE STABILITY OF PREPULSE INHIBITION AND HABITUATION OF THE STARTLE REFLEX IN SCHIZOPHRENIA: - A 6 YEAR FOLLOW-UP STUDY OF ANTIPSYCHOTIC NAïVE, FIRST-EPISODE SCHIZOPHRENIA PATIENTS

Author

Trine Bjørg Hammer, Birte Glenthøj, and Bob Oranje

Subjects

medicine.medical_specialty, business.industry, Antipsychotic naive, Follow up studies, Audiology, First episode schizophrenia, medicine.disease, Psychiatry and Mental health, Schizophrenia, Moro reflex, medicine, Habituation, business, Biological Psychiatry, Prepulse inhibition

Published

2010

22. Genetic testing in autism spectrum disorder

Author

Janni Majgaard Jensen, Ulla Schierup Nielsen, Allan Bayat, Malene Bøgehus Rasmussen, Møller, Rikke S., Anne-Marie Bisgaard, and Trine Bjørg Hammer

Subjects

Autism Spectrum Disorder/diagnosis, Humans, Genetic Predisposition to Disease, Genetic Testing, Genomics

Abstract

Autism spectrum disorders (ASD) have a complex genetic component comprising both frequent polygenic and rare monogenic factors. Research is conducted in methods used to calculate polygenic risk scores, which are not applicable in clinical practice. Advances in genomic technology have identified several monogenic causes, and genetic testing may be offered to persons with ASD where a monogenic etiology is suspected. Herein, we provide an overview of the current knowledge and present the first national recommendation regarding genetic testing in ASD.

23. Genetikken fremmer individualiseret behandling af epilepsi

Author

Johannesen, Katrine M., Allan Bayat, Trine Bjørg Hammer, and Møller, Rikke S.