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An in silico and in vitro human neuronal network model reveals cellular mechanisms beyond NaV1.1 underlying Dravet syndrome

Nina Doorn, Eline van Hugte, Ummi Ciptasari, Annika Mordelt, Hil G. E. Meijer, Dirk Schubert, Monica Frega, Nael Nadif Kasri, Michel J. A. M. van Putten

2023Stem Cell Reports21 citationsDOIOpen Access PDF

Abstract

Human induced pluripotent stem cell (hiPSC)-derived neuronal networks on multi-electrode arrays (MEAs) provide a unique phenotyping tool to study neurological disorders. However, it is difficult to infer cellular mechanisms underlying these phenotypes. Computational modeling can utilize the rich dataset generated by MEAs, and advance understanding of disease mechanisms. However, existing models lack biophysical detail, or validation and calibration to relevant experimental data. We developed a biophysical in silico model that accurately simulates healthy neuronal networks on MEAs. To demonstrate the potential of our model, we studied neuronal networks derived from a Dravet syndrome (DS) patient with a missense mutation in SCN1A , encoding sodium channel Na V 1.1. Our in silico model revealed that sodium channel dysfunctions were insufficient to replicate the in vitro DS phenotype, and predicted decreased slow afterhyperpolarization and synaptic strengths. We verified these changes in DS patient-derived neurons, demonstrating the utility of our in silico model to predict disease mechanisms.

Topics & Concepts

In silicoBiologySodium channelDravet syndromeComputational biologyNeurosciencePhenotypeInteractomeBioinformaticsGeneticsGeneEpilepsyChemistrySodiumOrganic chemistryNeuroscience and Neural EngineeringNeuroscience and Neuropharmacology ResearchAdvanced Memory and Neural Computing
An in silico and in vitro human neuronal network model reveals cellular mechanisms beyond NaV1.1 underlying Dravet syndrome | Litcius