Identification of epilepsy-associated neuronal subtypes and gene expression underlying epileptogenesis

Author:

Pfisterer Ulrich,Petukhov Viktor,Demharter Samuel,Meichsner JohannaORCID,Thompson Jonatan J.,Batiuk Mykhailo Y.ORCID,Asenjo-Martinez Andrea,Vasistha Navneet A.ORCID,Thakur Ashish,Mikkelsen Jens,Adorjan Istvan,Pinborg Lars H.,Pers Tune H.ORCID,von Engelhardt Jakob,Kharchenko Peter V.ORCID,Khodosevich KonstantinORCID

Abstract

AbstractEpilepsy is one of the most common neurological disorders, yet its pathophysiology is poorly understood due to the high complexity of affected neuronal circuits. To identify dysfunctional neuronal subtypes underlying seizure activity in the human brain, we have performed single-nucleus transcriptomics analysis of >110,000 neuronal transcriptomes derived from temporal cortex samples of multiple temporal lobe epilepsy and non-epileptic subjects. We found that the largest transcriptomic changes occur in distinct neuronal subtypes from several families of principal neurons (L5-6_Fezf2 and L2-3_Cux2) and GABAergic interneurons (Sst and Pvalb), whereas other subtypes in the same families were less affected. Furthermore, the subtypes with the largest epilepsy-related transcriptomic changes may belong to the same circuit, since we observed coordinated transcriptomic shifts across these subtypes. Glutamate signaling exhibited one of the strongest dysregulations in epilepsy, highlighted by layer-wise transcriptional changes in multiple glutamate receptor genes and strong upregulation of genes coding for AMPA receptor auxiliary subunits. Overall, our data reveal a neuronal subtype-specific molecular phenotype of epilepsy.

Funder

Institutional Excellence in Higher Education Grant

Lundbeckfonden

Novo Nordisk Fonden

Det Frie Forskningsråd

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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