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HUMAN NEURONAL NETWORKS ON MICRO-ELECTRODE ARRAYS AS A TOOL TO ASSESS GENOTYPE-PHENOTYPE CORRELATION IN <EM>CACNA1A</EM>-RELATED DISORDERS

Marina Hommersomand 9 co-authors

Radboud University Medical Center, Donders Institute for Brain, Cognition and Behaviour

FENS Forum 2026 (2026)
Barcelona, Spain
Board PS05-09AM-379

Presentation

Date TBA

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Board: PS05-09AM-379

Poster preview

HUMAN NEURONAL NETWORKS ON MICRO-ELECTRODE ARRAYS AS A TOOL TO ASSESS GENOTYPE-PHENOTYPE CORRELATION IN <EM>CACNA1A</EM>-RELATED DISORDERS poster preview

Event Information

Poster Board

PS05-09AM-379

Abstract

CACNA1A-related disorders constitute a diverse group of neurological conditions, including ataxia, migraine, and epilepsy. Despite extensive genetic studies, clear genotype-phenotype correlations remain elusive. Moreover, next generation sequencing has identified many variants of uncertain significance (VUS). Here, we leveraged patient-derived and CRISPR/Cas9-engineered human neuronal networks to explore relationships between CACNA1A variants and neurophysiological activity. CACNA1A haploinsufficiency induced subtle alterations in glutamatergic network activity, whereas missense variants had a more pronounced effect on overall network function. Network fingerprints were most affected from patients where ataxia co-occurred with migraine or epilepsy. Furthermore, we analysed the impact of CRISPR/Cas9-induced VUS on network developmental trajectories. Although functional changes could not be directly linked to clinical phenotypes, all tested variants induced measurable alterations in neuronal network function, supporting their classification as likely pathogenic. These findings highlight the potential of human neuronal networks as a translational model for evaluating CACNA1A variant effects and improving clinical variant interpretation.

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