Altered functional connectome hierarchy with gene expression signatures in newly-diagnosed focal epilepsy

Author:

de Bézenac Christophe EORCID,Caciagli LorenzoORCID,Alonazi Batil K,Bernhardt Boris CORCID,Marson Anthony G,Keller Simon SORCID

Abstract

AbstractObjectiveNeuroimaging research is providing insights into epilepsy as a disorder of brain connectivity linked to functional impairments which may have an identifiable genetic component. This case-control study aims to identify imbalances in a functional connectome dimension spanning from unimodal to transmodal networks and explore the potential genetic basis of such alterations in patients with newly diagnosed focal epilepsy (NDfE).MethodsWe used gradient-based analysis of resting-sate fMRI data comparing cortical gradient maps in patients with NDfE (n = 27) to age and sex-matched controls (n = 36). Using a brain-wide gene expression dataset, gene combinations associated with altered brain regions were then entered into an enrichment analysis.ResultsWe found an increased differentiation of connectivity profiles between unimodal and transmodal networks in NDfE, which was particularly pronounced in the patients with persistent seizures at 12-months follow-up (n=10). Differences corresponded to gradient score reductions in a visual network and increases in limbic and default mode systems which subserve higher-level cognition. Cortical difference maps were spatially correlated with regional expression of a weighted gene combination. These genes were enriched for disease and ontology terms and pathways previously associated with epilepsy and seizure susceptibility.InterpretationsLarge-scale functional hierarchy may be altered from in focal epilepsy from diagnosis and correlate with response to treatment. Combining functional neuroimaging and transcriptional data analysis may provide a framework for understanding the wide-ranging impairments associated with the disorder and mechanistic insight into how gene processes may drive alterations in brain function mediating the genetic risk of epilepsy.

Publisher

Cold Spring Harbor Laboratory

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