Abstract
Understanding the interaction between the nervous system and cerebral vasculature is fundamental to forming a complete picture of the neurophysiology of sleep and its role in maintaining physiological homeostasis. However, the intrinsic hemodynamics of slow-wave sleep (SWS) are still poorly known. We carried out 30 all-night sleep measurements with combined near-infrared spectroscopy (NIRS) and polysomnography to investigate spontaneous hemodynamic behavior in SWS compared to light (LS) and rapid-eye-movement sleep (REM). In particular, we concentrated on slow oscillations (3–150 mHz) in oxy- and deoxyhemoglobin concentrations, heart rate, arterial oxygen saturation, and the pulsation amplitude of the photoplethysmographic signal. We also analyzed the behavior of these variables during sleep stage transitions. The results indicate that slow spontaneous cortical and systemic hemodynamic activity is reduced in SWS compared to LS, REM, and wakefulness. This behavior may be explained by neuronal synchronization observed in electrophysiological studies of SWS and a reduction in autonomic nervous system activity. Also, sleep stage transitions are asymmetric, so that the SWS-to-LS and LS-to-REM transitions, which are associated with an increase in the complexity of cortical electrophysiological activity, are characterized by more dramatic hemodynamic changes than the opposite transitions. Thus, it appears that while the onset of SWS and termination of REM occur only as gradual processes over time, the termination of SWS and onset of REM may be triggered more abruptly by a particular physiological event or condition. The results suggest that scalp hemodynamic changes should be considered alongside cortical hemodynamic changes in NIRS sleep studies to assess the interaction between the autonomic and central nervous systems.
Highlights
Sleep is a part of constantly ongoing homeostatic regulation between neurons, glial cells, and vasculature of the brain to maintain health, adaptability, and cognitive performance [1]
We examine spontaneous hemodynamic oscillations measured with near-infrared spectroscopy (NIRS) in different sleep stages
Spontaneous hemodynamic oscillations Spectral analysis of the NIRS and systemic signals showed that the VLFO and LFO powers in Slow-wave sleep (SWS) mostly differed statistically significantly from the powers in the other stages, in the VLFO band (Fig. 2)
Summary
Sleep is a part of constantly ongoing homeostatic regulation between neurons, glial cells, and vasculature of the brain to maintain health, adaptability, and cognitive performance [1]. Slow-wave sleep (SWS), known as deep sleep, differs from the physiologically distinct light sleep (LS) and rapid-eye-movement sleep (REM) stages by a dramatic increase in synchronized neuronal activity and loss of information integration across cortical areas [2,3]. This activity plays a crucial role in cortical plasticity and is seen in electroencephalographic (EEG) recordings as largeamplitude delta waves (0.5–2 Hz) [3,4]. To form a comprehensive understanding of the neurophysiologic interactions related to sleep, bioelectric signals must be supplemented with hemodynamic and metabolic data [6,7,8,9,10]
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