Neurodevelopmental Disorders Caused by De Novo Variants in KCNB1 Genotypes and 
Phenotypes

De Kovel, Carolien G. F.; Syrbe, S.; Brilstra, E. H.; Verbeek, N.; Kerr, B.; Dubbs, H.; Bayat, A.; Desai, S.; Naidu, S.; Srivastava, S.; Cagaylan, H.; Yis, U.; Saunders, C.; Rook, M.; Plugge, S.; Muhle, H.; Afawi, Z.; Klein, K. M.; Jayaraman, V.; Rajagopalan, R.; Goldberg, E.; Marsh, E.; Kessler, S.; Bergqvist, C.; Conlin, L. K.; Krok, B. L.; Thiffault, I.; Pendziwiat, M.; Helbig, I.; Polster, T.; Borggraefe, I.; Lemke, J. R.; Van den Boogaardt, M. J.; Moller, R. S.; Koeleman, B. P. C.

doi:10.1001/jamaneurol.2017.1714

Lokale TagsFreigabegeschichteDetailsÜbersicht

Neurodevelopmental Disorders Caused by De Novo Variants in KCNB1 Genotypes and Phenotypes

De Kovel, C. G. F., Syrbe, S., Brilstra, E. H., Verbeek, N., Kerr, B., Dubbs, H., et al. (2017). Neurodevelopmental Disorders Caused by De Novo Variants in KCNB1 Genotypes and Phenotypes. JAMA Neurology, 74(10), 1228-1236. doi:10.1001/jamaneurol.2017.1714.

Item is Freigegeben

einblenden: alle ausblenden: alle

Basisdaten

einblenden: ausblenden:

Datensatz-Permalink: https://hdl.handle.net/11858/00-001M-0000-002E-17A3-F Versions-Permalink: https://hdl.handle.net/11858/00-001M-0000-002E-17AC-E

Genre: Zeitschriftenartikel

Dateien

einblenden: Dateien

ausblenden: Dateien

:

DeKovel_etal_2017a.pdf (Verlagsversion), 2MB

Öffnen Speichern

Datei-Permalink:
https://hdl.handle.net/11858/00-001M-0000-002E-17AD-C

Name:
DeKovel_etal_2017a.pdf

Beschreibung:
-

OA-Status:

Sichtbarkeit:
Öffentlich

MIME-Typ / Prüfsumme:
application/pdf / [MD5]

Technische Metadaten:

Öffnen

Copyright Datum:
-

Copyright Info:
-

Lizenz:
-

Externe Referenzen

einblenden:

Urheber

einblenden:

ausblenden:

Urheber:
De Kovel, Carolien G. F.^{1, 2}, Autor
Syrbe, S.³, Autor
Brilstra, E. H.², Autor
Verbeek, N.², Autor
Kerr, B.^{4, 5, 6}, Autor
Dubbs, H.⁷, Autor
Bayat, A.⁸, Autor
Desai, S.⁹, Autor
Naidu, S.^{10, 11}, Autor
Srivastava, S.¹², Autor
Cagaylan, H.¹³, Autor
Yis, U.¹⁴, Autor
Saunders, C.^{15, 16, 17}, Autor
Rook, M.¹⁸, Autor
Plugge, S.¹⁹, Autor
Muhle, H.²⁰, Autor
Afawi, Z.²¹, Autor
Klein, K. M.²², Autor
Jayaraman, V.²³, Autor
Rajagopalan, R.²³, Autor
Goldberg, E.⁷, AutorMarsh, E.⁷, AutorKessler, S.⁷, AutorBergqvist, C.⁷, AutorConlin, L. K.²³, AutorKrok, B. L.²³, AutorThiffault, I.^{15, 16}, AutorPendziwiat, M.²⁰, AutorHelbig, I.^{7, 24}, AutorPolster, T.²⁵, AutorBorggraefe, I.²⁶, AutorLemke, J. R.²⁷, AutorVan den Boogaardt, M. J.², AutorMoller, R. S.^{28, 29}, AutorKoeleman, B. P. C.², Autor mehr..

Affiliations:
1Language and Genetics Department, MPI for Psycholinguistics, Max Planck Society, ou_792549
2Department of Genetics, University Medical Center Utrecht, Utrecht, The Netherlands, ou_persistent22
3Division of Child Neurology and Inherited Metabolic Diseases, Department of General Pediatrics, Center for Pediatrics and Adolescent Medicine, University Hospital Heidelberg, Heidelberg, Germany, ou_persistent22
4Institute of Evolution, Systems and Genomics, Faculty of Medical and Human Sciences, University of Manchester, Manchester, UK, ou_persistent22
5Manchester Centre For Genomic Medicine, Central Manchester University Hospitals National Health Service Foundation Trust, Manchester, UK, ou_persistent22
6Manchester Academic Health Science Centre, Manchester, UK, ou_persistent22
7Division of Neurology, The Children's Hospital of Philadelphia, Philadelphia, PA, USA, ou_persistent22
8Department of Pediatrics, University Hospital of Hvidovre, Copenhagen, Denmark, ou_persistent22
9Department of Neurogenetics, Kennedy Krieger Institute, Baltimore, MD, USA, ou_persistent22
10Department of Neurology and Pediatrics, Johns Hopkins School of Medicine, Baltimore, MD, USA, ou_persistent22
11Hugo Moser Research Institute, Kennedy Krieger Institute, Baltimore, MD, USA, ou_persistent22
12Department of Neurology, Boston Children's Hospital, Boson, MA, USA, ou_persistent22
13Department of Molecular Biology and Genetics, Bogaziçi University, Istanbul, Turkey, ou_persistent22
14Division of Child Neurology, Department of Pediatrics, School of Medicine, Dokuz Eylül University, İzmir, Turkey, ou_persistent22
15Center for Pediatric Genomic Medicine, Department of Pathology and Laboratory Medicine, Children's Mercy Hospital, Kansas City, MO, USA, ou_persistent22
16Department of Pediatrics, Children's Mercy Hospital, Kansas City, MO, USA, ou_persistent22
17Pediatric Pathology and Laboratory Medicine, University of Missouri–Kansas City School of Medicine, Kansas City, MO, USA, ou_persistent22
18Department of Medical Physiology, University Medical Center Utrecht, Utrecht, The Netherlands, ou_persistent22
19Department of Biomedical Sciences, University Medical Center Utrecht, Utrecht, The Netherlands, ou_persistent22
20Department of Neuropediatrics, University Medical Center Schleswig-Holstein, Christian Albrechts University, Kiel, Germany, ou_persistent22
21Department of Physiology and Pharmacology, Tel Aviv University Medical School, Ramat Aviv, Israel, ou_persistent22
22Department of Neurology, Epilepsy Center Frankfurt Rhine-Main, Center of Neurology and Neurosurgery, University Hospital, Goethe-University Frankfurt, Frankfurt, Germany, ou_persistent22
23Division of Genomic Diagnostics, Children’s Hospital of Philadelphia, Philadelphia, PA, USA, ou_persistent22
24University Medical Center Schleswig-Holstein, Christian Albrechts University, Kiel, Germany, ou_persistent22
25Epilepsiezentrum Bethel, Krankenhaus Mara, Kinderepileptologie, Bielefeld, Germany, ou_persistent22
26Department of Pediatric Neurology, Developmental Medicine and Social Pediatrics Dr. von Hauner’s Children’s Hospital, University of Munich, Munich, Germany, ou_persistent22
27Institute of Human Genetics, University of Leipzig Hospitals and Clinics, Leipzig, Germany, ou_persistent22
28Danish Epilepsy Centre, Dianalund, Denmark, ou_persistent22
29Institute for Regional Health Services, University of Southern Denmark, Odense, Denmark, ou_persistent22

Inhalt

einblenden:

ausblenden:

Schlagwörter: -

Zusammenfassung: Importance Knowing the range of symptoms seen in patients with a missense or loss-of-function variant in KCNB1 and how these symptoms correlate with the type of variant will help clinicians with diagnosis and prognosis when treating new patients. Objectives To investigate the clinical spectrum associated with KCNB1 variants and the genotype-phenotype correlations. Design, Setting, and Participants This study summarized the clinical and genetic information of patients with a presumed pathogenic variant in KCNB1.Patients were identified in research projects or during clinical testing. Information on patients from previously published articles was collected and authors contacted if feasible. All patients were seen at a clinic at one of the participating institutes because of presumed genetic disorder. They were tested in a clinical setting or included in a research project. Main Outcomes and Measures The genetic variant and its inheritance and information on the patient's symptoms and characteristics in a predefined format. All variants were identified with massive parallel sequencing and confirmed with Sanger sequencing in the patient. Absence of the variant in the parents could be confirmed with Sanger sequencing in all families except one. Results Of 26 patients (10 female, 15 male, 1 unknown; mean age at inclusion, 9.8 years; age range, 2-32 years) with developmental delay, 20 (77%) carried a missense variant in the ion channel domain of KCNB1, with a concentration of variants in region S5 to S6. Three variants that led to premature stops were located in the C-terminal and 3 in the ion channel domain. Twenty-one of 25 patients (84%) had seizures, with 9 patients (36%) starting with epileptic spasms between 3 and 18 months of age. All patients had developmental delay, with 17 (65%) experiencing severe developmental delay; 14 (82%) with severe delay had behavioral problems. The developmental delay was milder in 4 of 6 patients with stop variants and in a patient with a variant in the S2 transmembrane element rather than the S4 to S6 region. Conclusions and Relevance De novo KCNB1 missense variants in the ion channel domain and loss-of-function variants in this domain and the C-terminal likely cause neurodevelopmental disorders with or without seizures. Patients with presumed pathogenic variants in KCNB1 have a variable phenotype. However, the type and position of the variants in the protein are (imperfectly) correlated with the severity of the disorder.

Details

einblenden:

ausblenden:

Sprache(n): eng - English

Datum: Erschienen: 2017

Publikationsstatus: Erschienen

Seiten: -

Ort, Verlag, Ausgabe: -

Inhaltsverzeichnis: -

Art der Begutachtung: Expertenbegutachtung

Identifikatoren: DOI: 10.1001/jamaneurol.2017.1714

Art des Abschluß: -

ausblenden:

Titel: JAMA Neurology

Kurztitel : JAMA Neurol

Genre der Quelle: Zeitschrift

Urheber:

Affiliations:

Ort, Verlag, Ausgabe: Chicago, Ill. : American Medical Association

Seiten: - Band / Heft: 74 (10) Artikelnummer: - Start- / Endseite: 1228 - 1236 Identifikator: Anderer: 2168-6157
CoNE: https://pure.mpg.de/cone/journals/resource/2168-6157

Datensatz

Basisdaten

Dateien

Externe Referenzen

Urheber

Inhalt

Details

Veranstaltung

Entscheidung

Projektinformation

Quelle 1