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This study aims to understand the interactions between seizures and sleep in a mouse model of tuberous sclerosis complex, focusing on the role of orexin.

February 14, 2026

Bidirectional sleep‐seizure interactions and orexin in a mouse model of tuberous sclerosis complex‐related epilepsy

Key Points

This study aims to understand the interactions between seizures and sleep in a mouse model of tuberous sclerosis complex, focusing on the role of orexin.
Utilized Tsc1 GFAP CKO mice for experimentation.
Conducted video, EEG, and electromyographic analysis to investigate seizure and sleep relationships.
Assessed orexin expression in the hypothalamus through immunohistochemistry.
Examined the effects of orexin antagonists on sleep and seizures using video-EEG.
Seizures predominantly occurred during non-REM sleep but had the highest frequency during REM sleep.
Seizures disrupted the sleep-wake cycle, particularly reducing REM sleep.
Tsc1 GFAP CKO mice with seizures showed higher orexin expression compared to controls.
Orexin antagonist suvorexant reversed the reduction in REM sleep but did not significantly affect seizure frequency.

Abstract

Abstract Objective A strong bidirectional relationship exists between epilepsy and sleep, with seizures often occurring more frequently in sleep and, in turn, sleep being disrupted by seizures. However, the mechanistic basis of seizure–sleep interactions is poorly understood. In this study, we characterized the relationship between seizures and sleep in a mouse model of the genetic disorder tuberous sclerosis complex (TSC) and investigated potential mechanisms underlying seizure–sleep interactions related to hypothalamic orexin. Methods Tsc1 GFAP CKO mice were used to investigate the relationship between seizures and sleep with video, electroencephalographic (EEG), and electromyographic analysis, including the dependence of seizure frequency on vigilance state (awake, rapid eye movement REM, non‐REM) and the effect of seizures on the wake–sleep cycle. Orexin expression in hypothalamus was assessed by immunohistochemistry in relation to seizure frequency. The effect of orexin antagonists on sleep and seizures was tested by video‐EEG. Results Overall seizures occurred most commonly in non‐REM sleep in Tsc1 GFAP CKO mice but had the highest seizure frequency in REM sleep after normalizing for amount of time spent in each vigilance state. Conversely, seizures were associated with disruptions in the sleep–wake cycle, particularly a decrease in REM sleep. Tsc1 GFAP CKO mice with seizures had increased orexin expression compared with control mice or Tsc1 GFAP CKO mice without seizures. The orexin antagonist suvorexant reversed the decrease in REM sleep but had no significant effect on seizures in Tsc1 GFAP CKO mice. Significance A bidirectional relationship between seizures and sleep was demonstrated in a mouse model of TSC, with relative seizure frequency surprisingly being highest in REM sleep and seizures causing a disruption of REM sleep. Hypothalamic orexin may partly mediate these seizure–sleep interactions, and orexin antagonists may represent rational therapies for sleep disorders in TSC.

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Bidirectional sleep‐seizure interactions and orexin in a mouse model of tuberous sclerosis complex‐related epilepsy

Key Points

Abstract

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