Abstract
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). To better understand differential mechanisms leading to the initiation of these pathological activities, we used a two-neuron conductance-based model of interconnected GABAergic and pyramidal glutamatergic neurons, in which we incorporated ionic concentration dynamics in both neurons. We modeled FHM-3 mutations by increasing the persistent sodium current in the interneuron and epileptogenic mutations by decreasing the sodium conductance in the interneuron. Therefore, we studied both FHM-3 and epileptogenic mutations within the same framework, modifying only two parameters. In our model, the key effect of gain of function FHM-3 mutations is ion fluxes modification at each action potential (in particular the larger activation of voltage-gated potassium channels induced by the NaV1.1 gain of function), and the resulting CSD-triggering extracellular potassium accumulation, which is not caused only by modifications of firing frequency. Loss of function epileptogenic mutations, on the other hand, increase GABAergic neurons’ susceptibility to depolarization block, without major modifications of firing frequency before it. Our modeling results connect qualitatively to experimental data: potassium accumulation in the case of FHM-3 mutations and facilitated depolarization block of the GABAergic neuron in the case of epileptogenic mutations. Both these effects can lead to pyramidal neuron hyperexcitability, inducing in the migraine condition depolarization block of both the GABAergic and the pyramidal neuron. Overall, our findings suggest different mechanisms of network hyperexcitability for migraine and epileptogenic NaV1.1 mutations, implying that the modifications of firing frequency may not be the only relevant pathological mechanism.
Highlights
NaV1.1 is a voltage-gated sodium channel mainly expressed in GABAergic neurons and it is crucial for their excitability
3.1 NaV1.1 familial hemiplegic migraine (FHM) type 3 (FHM-3) mutations can lead to cortical spreading depolarization (CSD) initiation via extracellular potassium build-up when neuronal input-output features are not modified
To better understand the enhanced transition from the firing regime to depolarization block of the GABAergic neuron when NaV1.1 carries an epileptogenic loss of function mutation, which we observed in Fig 10A1, we studied it as a dynamic bifurcation phenomenon [53]
Summary
NaV1.1 is a voltage-gated sodium channel mainly expressed in GABAergic neurons and it is crucial for their excitability. The link between FHM-3 mutations and the initiation of CSD is not well understood yet It is unclear how gain of function mutations in voltage-gated sodium channels of GABAergic neurons, which classically have an inhibitory role, can lead to the network hyperexcitability characterizing CSD. Studying this link can give a better understanding of FHM-3 pathophysiology, and of CSD and migraine aura in general, as well as stroke, traumatic brain injury and other pathologies in which spreading depolarizations are involved
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