Abstract
The electrographic hallmark of childhood absence epilepsy (CAE) and other idiopathic forms of epilepsy are 2.5–4 Hz spike and wave discharges (SWDs) originating from abnormal electrical oscillations of the cortico-thalamo-cortical network. SWDs are generally associated with sudden and brief non-convulsive epileptic events mostly generating impairment of consciousness and correlating with attention and learning as well as cognitive deficits. To date, SWDs are known to arise from locally restricted imbalances of excitation and inhibition in the deep layers of the primary somatosensory cortex. SWDs propagate to the mostly GABAergic nucleus reticularis thalami (NRT) and the somatosensory thalamic nuclei that project back to the cortex, leading to the typical generalized spike and wave oscillations. Given their shared anatomical basis, SWDs have been originally considered the pathological transition of 11–16 Hz bursts of neural oscillatory activity (the so-called sleep spindles) occurring during Non-Rapid Eye Movement (NREM) sleep, but more recent research revealed fundamental functional differences between sleep spindles and SWDs, suggesting the latter could be more closely related to the slow (<1 Hz) oscillations alternating active (Up) and silent (Down) cortical activity and concomitantly occurring during NREM. Indeed, several lines of evidence support the fact that SWDs impair sleep architecture as well as sleep/wake cycles and sleep pressure, which, in turn, affect seizure circadian frequency and distribution. Given the accumulating evidence on the role of astroglia in the field of epilepsy in the modulation of excitation and inhibition in the brain as well as on the development of aberrant synchronous network activity, we aim at pointing at putative contributions of astrocytes to the physiology of slow-wave sleep and to the pathology of SWDs. Particularly, we will address the astroglial functions known to be involved in the control of network excitability and synchronicity and so far mainly addressed in the context of convulsive seizures, namely (i) interstitial fluid homeostasis, (ii) K+ clearance and neurotransmitter uptake from the extracellular space and the synaptic cleft, (iii) gap junction mechanical and functional coupling as well as hemichannel function, (iv) gliotransmission, (v) astroglial Ca2+ signaling and downstream effectors, (vi) reactive astrogliosis and cytokine release.
Highlights
Epilepsy is a highly heterogeneous neurological condition characterized by enduring predisposition to unpredictable pathological discharge of rhythmic activity in the brain networks, which is commonly referred as seizure activity [1]
We focus on the evidence that links to observations coming from the clinics as well as genetic and pharmacological models of spike and wave discharges (SWDs), aiming to point at specific topics which may be worth further research in the field of SWDs
Social and human point of view, epilepsy is probably one of the most heterogeneous neurological diseases. This variability partially relies on the fact that epilepsy may originate from a plethora of different conditions, among others traumatic injury, stroke, CNS infections or inflammation, brain tumor, genetic predisposition, and drug or alcohol abuse
Summary
Epilepsy is a highly heterogeneous neurological condition characterized by enduring predisposition to unpredictable pathological discharge of rhythmic activity in the brain networks, which is commonly referred as seizure activity [1]. Specific studies addressing the impact of OLE in absence epilepsy are still required, OLE has a sleep-inducing effect and enhances GABAA receptor-mediated responses, possibly affecting the physiological, temporal-spatial pattern of cortico-thalamo-cortical oscillations [146, 147].
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