Publications by authors named "Louisiane Lemaire"
Slow brain rhythms, for example during slow-wave sleep or pathological conditions like seizures and spreading depolarization, can be accompanied by oscillations in extracellular potassium concentration. Such slow brain rhythms typically have a lower frequency than tonic action-potential firing. They are assumed to arise from network-level mechanisms, involving synaptic interactions and delays, or from intrinsically bursting neurons.
View Article and Find Full Text PDFNa1.1 (SCN1A) is a voltage-gated sodium channel mainly expressed in GABAergic neurons. Loss of function mutations of Na1.
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- Spreading depolarizations (SDs) play a role in various neurological conditions like migraines, epilepsy, and strokes, but the exact mechanisms behind them are not well understood.
- Research shows that activating the NaV1.1 sodium channel in interneurons or stimulating GABAergic interneurons can trigger cortical spreading depression (CSD) in the neocortex, indicating a specific mechanism for CSD initiation in this brain region.
- Gain-of-function mutations in NaV1.1 are linked to familial hemiplegic migraine type-3 (FHM3), and the study highlights the importance of GABAergic interneuron hyperactivity in initiating CSD, which may be relevant to other types of migraines and similar disorders.
Loss of function mutations of SCN1A, the gene coding for the voltage-gated sodium channel NaV1.1, cause different types of epilepsy, whereas gain of function mutations cause sporadic and familial hemiplegic migraine type 3 (FHM-3). However, it is not clear yet how these opposite effects can induce paroxysmal pathological activities involving neuronal networks' hyperexcitability that are specific of epilepsy (seizures) or migraine (cortical spreading depolarization, CSD).
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