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Net synaptic drive of fast-spiking interneurons is inverted towards inhibition in human FCD I epilepsy.


ABSTRACT: Focal cortical dysplasia type I (FCD I) is the most common cause of pharmaco-resistant epilepsy with the poorest prognosis. To understand the epileptogenic mechanisms of FCD I, we obtained tissue resected from patients with FCD I epilepsy, and from tumor patients as control. Using whole-cell patch clamp in acute human brain slices, we investigated the cellular properties of fast-spiking interneurons (FSINs) and pyramidal neurons (PNs) within the ictal onset zone. In FCD I epilepsy, FSINs exhibited lower firing rates from slower repolarization and action potential broadening, while PNs had increased firing. Importantly, excitatory synaptic drive of FSINs increased progressively with the scale of cortical activation as a general property across species, but this relationship was inverted towards net inhibition in FCD I epilepsy. Further comparison with intracranial electroencephalography (iEEG) from the same patients revealed that the spatial extent of pathological high-frequency oscillations (pHFO) was associated with synaptic events at FSINs.

SUBMITTER: Cho E 

PROVIDER: S-EPMC11303528 | biostudies-literature | 2024 Aug

REPOSITORIES: biostudies-literature

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Net synaptic drive of fast-spiking interneurons is inverted towards inhibition in human FCD I epilepsy.

Cho Eunhye E   Kwon Jii J   Lee Gyuwon G   Shin Jiwoo J   Lee Hyunsu H   Lee Suk-Ho SH   Chung Chun Kee CK   Yoon Jaeyoung J   Ho Won-Kyung WK  

Nature communications 20240806 1


Focal cortical dysplasia type I (FCD I) is the most common cause of pharmaco-resistant epilepsy with the poorest prognosis. To understand the epileptogenic mechanisms of FCD I, we obtained tissue resected from patients with FCD I epilepsy, and from tumor patients as control. Using whole-cell patch clamp in acute human brain slices, we investigated the cellular properties of fast-spiking interneurons (FSINs) and pyramidal neurons (PNs) within the ictal onset zone. In FCD I epilepsy, FSINs exhibit  ...[more]

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