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Expanding Phenotype of Poirier–Bienvenu Syndrome: New Evidence from an Italian Multicentrical Cohort of Patients

Title: Expanding Phenotype of Poirier–Bienvenu Syndrome: New Evidence from an Italian Multicentrical Cohort of Patients
Authors: Alessandro Orsini; Andrea Santangelo; Francesca Bravin; Alice Bonuccelli; Diego Peroni; Roberta Battini; Thomas Foiadelli; Veronica Bertini; Angelo Valetto; Michele Iacomino; Vincenzo Nigro; Anna Laura Torella; Marcello Scala; Valeria Capra; Maria Stella Vari; Anna Fetta; Veronica Di Pisa; Francesca Montanari; Roberta Epifanio; Paolo Bonanni; Roberto Giorda; Francesca Operto; Grazia Pastorino; Esra Sarigecili; Esra Sardaroglu; Cetin Okuyaz; Sevgan Bozdogan; Luciana Musante; Flavio Faletra; Caterina Zanus; Alessandro Ferretti; Federico Vigevano; Pasquale Striano; Duccio Maria Cordelli
Source: Genes ; Volume 13 ; Issue 2 ; Pages: 276
Publisher Information: Multidisciplinary Digital Publishing Institute
Publication Year: 2022
Collection: MDPI Open Access Publishing
Subject Terms: Pobinds; neurodevelopment; epilepsy; seizure; CSNK2B
Description: Background: Poirier–Bienvenu Neurodevelopmental Syndrome (POBINDS) is a rare disease linked to mutations of the CSNK2B gene, which encodes for a subunit of caseinkinase CK2 involved in neuronal growth and synaptic transmission. Its main features include early-onset epilepsy and intellectual disability. Despite the lack of cases described, it appears that POBINDS could manifest with a wide range of phenotypes, possibly related to the different mutations of CSNK2B. Methods: Our multicentric, retrospective study recruited nine patients with POBINDS, detected using next-generation sequencing panels and whole-exome sequencing. Clinical, laboratory, and neuroimaging data were reported for each patient in order to assess the severity of phenotype, and eventually, a correlation with the type of CSNK2B mutation. Results: We reported nine unrelated patients with heterozygous de novo mutations of the CSNK2B gene. All cases presented epilepsy, and eight patients were associated with a different degree of intellectual disability. Other features detected included endocrinological and vascular abnormalities and dysmorphisms. Genetic analysis revealed six new variants of CSNK2B that have not been reported previously. Conclusion: Although it was not possible to assess a genotype–phenotype correlation in our patients, our research further expands the phenotype spectrum of POBINDS patients, identifying new mutations occurring in the CSNK2B gene.
Document Type: text
File Description: application/pdf
Language: English
Relation: Human Genomics and Genetic Diseases; https://dx.doi.org/10.3390/genes13020276
DOI: 10.3390/genes13020276
Availability: https://doi.org/10.3390/genes13020276
Rights: https://creativecommons.org/licenses/by/4.0/
Accession Number: edsbas.8359BECE
Database: BASE