TY - JOUR
T1 - Neurodevelopmental Disorders Caused by De Novo Variants in KCNB1 Genotypes and Phenotypes
AU - de Kovel, Carolien G F
AU - Syrbe, Steffen
AU - Brilstra, Eva H
AU - Verbeek, Nienke
AU - Kerr, Bronwyn
AU - Dubbs, Holly
AU - Bayat, Allan
AU - Desai, Sonal
AU - Naidu, Sakkubai
AU - Srivastava, Siddharth
AU - Cagaylan, Hande
AU - Yis, Uluc
AU - Saunders, Carol
AU - Rook, Martin
AU - Plugge, Susanna
AU - Muhle, Hiltrud
AU - Afawi, Zaid
AU - Klein, Karl-Martin
AU - Jayaraman, Vijayakumar
AU - Rajagopalan, Ramakrishnan
AU - Goldberg, Ethan
AU - Marsh, Eric
AU - Kessler, Sudha
AU - Bergqvist, Christina
AU - Conlin, Laura K
AU - Krok, Bryan L
AU - Thiffault, Isabelle
AU - Pendziwiat, Manuela
AU - Helbig, Ingo
AU - Polster, Tilman
AU - Borggraefe, Ingo
AU - Lemke, Johannes R
AU - van den Boogaardt, Marie-José
AU - Møller, Rikke S
AU - Koeleman, Bobby P C
PY - 2017/10/1
Y1 - 2017/10/1
N2 - 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.
AB - 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.
KW - Adolescent
KW - Adult
KW - Brain/diagnostic imaging
KW - Child
KW - Child, Preschool
KW - Electroencephalography
KW - Female
KW - Genome-Wide Association Study
KW - Genotype
KW - Humans
KW - Magnetic Resonance Imaging
KW - Male
KW - Mutation, Missense/genetics
KW - Neurodevelopmental Disorders/diagnostic imaging
KW - Phenotype
KW - Shab Potassium Channels/genetics
KW - Young Adult
U2 - 10.1001/jamaneurol.2017.1714
DO - 10.1001/jamaneurol.2017.1714
M3 - Article
C2 - 28806457
SN - 2168-6149
VL - 74
SP - 1228
EP - 1236
JO - JAMA Neurology
JF - JAMA Neurology
IS - 10
ER -