Expanding the genetic and phenotypic relevance of
            <i>KCNB1</i>
            variants in developmental and epileptic encephalopathies: 27 new patients and overview of the literature

Bar, Claire; Barcia, Giulia; Jennesson, Mélanie; Guyader, Gwenaël Le; Schneider, Amy; Mignot, Cyril; Lesca, Gaëtan; Breuillard, Delphine; Montomoli, Martino; Keren, Boris; Doummar, Diane; Villemeur, Thierry Billette de; Afenjar, Alexandra; Marey, Isabelle; Gérard, Marion; Isnard, Hervé; Poisson, Alice; Dupont, Sophie; Berquin, Patrick; Meyer, Pierre; Geneviève, David; Saint‐Martin, Anne de; Chehadeh, Salima El; Chelly, Jamel; Guët, Agnès; Scalais, Emmanuel; Dorison, Nathalie; Myers, Candace T.; Mefford, Heather C; Howell, Katherine; Marini, Carla; Freeman, Jeremy L.; Nica, Anca; Terrone, Gaetano; Sekhara, Tayeb; Lèbre, Anne-Sophie; Odent, Sylvie; Sadleir, Lynette G.; Münnich, Arnold; Guerrini, Renzo; Scheffer, Ingrid E.; Kabashi, Edor; Nabbout, Rima

doi:10.1002/humu.23915

Cited by 38 publications

(58 citation statements)

References 58 publications

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“…Neurobehavioral abnormalities were prominent in the Kcnb1 G379R mice and overlap with features reported in children with KCNB1 encephalopathy (Bar et al, 2019;Calhoun et al, 2017;de Kovel et al, 2017;Marini et al, 2017;Srivastava et al, 2018;Thiffault et al, 2015;Torkamani et al, 2014). Attention-deficit/hyperactivity disorder or hyperactivity with inattention has been reported in numerous cases of KCNB1 encephalopathy.…”

Section: Discussionsupporting

confidence: 53%

“…Previous work has identified heterozygous de novo KCNB1 pathogenic variants in individuals with DEE (Allen et al, 2016;Bar et al, 2019;Calhoun et al, 2017;de Kovel et al, 2017;Latypova et al, 2017;Marini et al, 2017;Miao et al, 2017;Saitsu et al, 2015;Thiffault et al, 2015;Torkamani et al, 2014). In addition to seizures, individuals with KCNB1 variants display comorbidities that include developmental delay, intellectual disability, features of autism spectrum disorder, ADHD and aggression (Bar et al, 2019;Calhoun et al, 2017;de Kovel et al, 2017;Marini et al, 2017). Since the initial reports of KCNB1 variants in early infantile epileptic encephalopathy type 26 (EIEE26), the phenotype has expanded to include cases with less severe and/or later onset epilepsy or no discrete seizures, and thus the term KCNB1 encephalopathy encompasses this broader phenotype spectrum.…”

Section: Introductionmentioning

confidence: 99%

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Epilepsy and neurobehavioral abnormalities in mice with aKCNB1pathogenic variant that alters conducting and non-conducting functions of K_V2.1

Hawkins¹,

Misra

Jurado³

et al. 2019

Preprint

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Developmental and epileptic encephalopathies (DEE) are a group of severe epilepsies that usually present with intractable seizures, developmental delay and are at a higher risk for premature mortality. Numerous genes have been identified as a monogenic cause of DEE, including KCNB1. The voltage-gated potassium channel K V 2.1, encoded by KCNB1, is primarily responsible for delayed rectifier potassium currents that are important regulators of excitability in electrically excitable cells, including neurons and cardiomyocytes. The de novo pathogenic variant KCNB1-p.G379R was identified in an infant with epileptic spasms, atonic, focal and tonic-clonic seizures that were refractory to treatment with standard antiepileptic drugs. Previous work demonstrated deficits in potassium conductance, but did not assess non-conducting functions. To determine if the G379R variant affected clustering at endoplasmic reticulum-plasma membrane junctions K V 2.1-G379R was expressed in HEK293T cells. K V 2.1-G379R expression did not induce formation of endoplasmic reticulum-plasma membrane junctions, and coexpression of K V 2.1-G379R with K V 2.1-WT lowered induction of these structures relative to K V 2.1-WT alone, suggesting a dominant negative effect. To model this variant in vivo, we introduced Kcnb1 G379R into mice using CRISPR/Cas9 genome editing. We characterized neurological and neurobehavioral phenotypes of Kcnb1 G379R/+ (Kcnb1 R/+ ) and Kcnb1 G379R/G379R (Kcnb1 R/R ) mice, and screened for cardiac abnormalities. Immunohistochemistry studies on brains from Kcnb1 +/+ (WT), Kcnb1 R/+ and Kcnb1 R/R mice revealed genotype-dependent differences in the levels and subcellular localization of K V 2.1, with reduced plasma membrane expression of the K V 2.1-G379R protein, consistent with in vitro data. Kcnb1 R/+ and Kcnb1 R/R mice displayed profound hyperactivity, repetitive behaviors, impulsivity and reduced anxiety. In addition, both Kcnb1 R/+ and Kcnb1 R/R mice exhibited abnormal interictal EEG abnormalities, including isolated spike and slow waves. Spontaneous seizure events were observed in Kcnb1 R/R mice during exposure to novel environments and/or handling, while both Kcnb1 R/+ and Kcnb1 R/R mutants were more susceptible to induced seizures. Kcnb1 R/+ and Kcnb1 R/R mice exhibited prolonged rate-corrected QT interval on surface ECG recording. Overall, the Kcnb1 G379R mice recapitulate many features observed in individuals with DEE due to pathogenic variants in KCNB1. This new mouse model of KCNB1 associated DEE will be valuable for improving the understanding of the underlying pathophysiology and will provide a valuable tool for the development of therapies to treat this pharmacoresistant DEE.

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Section: Discussionsupporting

confidence: 53%

Section: Introductionmentioning

confidence: 99%

Epilepsy and neurobehavioral abnormalities in mice with aKCNB1pathogenic variant that alters conducting and non-conducting functions of K_V2.1

Hawkins¹,

Misra

Jurado³

et al. 2019

Preprint

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“…Both variants were predicted to be damaging and thus considered pathogenic and contributing to the individual's phenotype. 16…”

Section: Variantsmentioning

confidence: 99%

“…[8][9][10][11][12][13][14][15] A few individuals had developmental delay without seizures. 11,16 Outcome data are sified as having developmental and epileptic encephalopathy (DEE) or developmental encephalopathy (DE). In addition, we reviewed published cases and provided the longterm outcome in patients older than 12 years from our series and from literature.…”

Section: Introductionmentioning

confidence: 99%

“…It has been suggested that truncating variants in the C-terminal domain correlate with less severe epilepsy outcome. 11,16 Here, we analyze a series of 36 individuals with pathogenic KCNB1 variants to delineate the phenotypic spectrum of KCNB1 encephalopathy. We explore genotype-phenotype correlations and long-term outcome to guide patient management and inform genetic and prognostic counseling.…”

Section: Introductionmentioning

confidence: 99%

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Developmental and epilepsy spectrum of KCNB1 encephalopathy with long‐term outcome

et al. 2020

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Genomics of severe and treatment‐resistant obsessive–compulsive disorder treated with deep brain stimulation: A preliminary investigation

Chen,

Naesström,

Halvorsen

et al. 2024

American J of Med Genetics Pt B

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Individuals with severe and treatment‐resistant obsessive‐compulsive disorder (trOCD) represent a small but severely disabled group of patients. Since trOCD cases eligible for deep brain stimulation (DBS) probably comprise the most severe end of the OCD spectrum, we hypothesize that they may be more likely to have a strong genetic contribution to their disorder. Therefore, while the worldwide population of DBS‐treated cases may be small (~300), screening these individuals with modern genomic methods may accelerate gene discovery in OCD. As such, we have begun to collect DNA from trOCD cases who qualify for DBS, and here we report results from whole exome sequencing and microarray genotyping of our first five cases. All participants had previously received DBS in the bed nucleus of stria terminalis (BNST), with two patients responding to the surgery and one showing a partial response. Our analyses focused on gene‐disruptive rare variants (GDRVs; rare, predicted‐deleterious single‐nucleotide variants or copy number variants overlapping protein‐coding genes). Three of the five cases carried a GDRV, including a missense variant in the ion transporter domain of KCNB1, a deletion at 15q11.2, and a duplication at 15q26.1. The KCNB1 variant (hg19 chr20‐47991077‐C‐T, NM_004975.3:c.1020G>A, p.Met340Ile) causes substitution of methionine for isoleucine in the trans‐membrane region of neuronal potassium voltage‐gated ion channel KV2.1. This KCNB1 substitution (Met340Ile) is located in a highly constrained region of the protein where other rare missense variants have previously been associated with neurodevelopmental disorders. The patient carrying the Met340Ile variant responded to DBS, which suggests that genetic factors could potentially be predictors of treatment response in DBS for OCD. In sum, we have established a protocol for recruiting and genomically characterizing trOCD cases. Preliminary results suggest that this will be an informative strategy for finding risk genes in OCD.

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Expanding the genetic and phenotypic relevance of KCNB1 variants in developmental and epileptic encephalopathies: 27 new patients and overview of the literature

Cited by 38 publications

References 58 publications

Epilepsy and neurobehavioral abnormalities in mice with aKCNB1pathogenic variant that alters conducting and non-conducting functions of K_V2.1

Epilepsy and neurobehavioral abnormalities in mice with aKCNB1pathogenic variant that alters conducting and non-conducting functions of K_V2.1

Developmental and epilepsy spectrum of KCNB1 encephalopathy with long‐term outcome

Genomics of severe and treatment‐resistant obsessive–compulsive disorder treated with deep brain stimulation: A preliminary investigation

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Expanding the genetic and phenotypic relevance of KCNB1 variants in developmental and epileptic encephalopathies: 27 new patients and overview of the literature

Cited by 38 publications

References 58 publications

Epilepsy and neurobehavioral abnormalities in mice with aKCNB1pathogenic variant that alters conducting and non-conducting functions of KV2.1

Epilepsy and neurobehavioral abnormalities in mice with aKCNB1pathogenic variant that alters conducting and non-conducting functions of KV2.1

Developmental and epilepsy spectrum of KCNB1 encephalopathy with long‐term outcome

Genomics of severe and treatment‐resistant obsessive–compulsive disorder treated with deep brain stimulation: A preliminary investigation

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Product

Resources

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Epilepsy and neurobehavioral abnormalities in mice with aKCNB1pathogenic variant that alters conducting and non-conducting functions of K_V2.1

Epilepsy and neurobehavioral abnormalities in mice with aKCNB1pathogenic variant that alters conducting and non-conducting functions of K_V2.1