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Sleep terrors are characterized by marked CNS arousal and typically occur during stage 3-4 sleep within the first NREM cycle. Studies of the EEG during sleep terrors suggest that delta power and synchrony in the EEG may be important physiological markers of sleep terror presence and intensity. An EEG mapping study was undertaken with a single participant who experienced three sleep terror episodes in the laboratory. A one-minute section of EEG was sampled immediately prior to the onset of each of the three sleep terrors. Similar EEG sections were taken from 10 healthy sex- and age-matched controls. The sleep tenors and control (normative) data were then compared topographically with z-scores (z-mapping). The z-maps indicated that all three sleep terrors contained more total and delta power in central and frontal areas than the control EEG sections. Moreover, relative delta power in these areas for the three sleep terrors was proportional to the subjective intensity of the episode. Although this pre-arousal EEG pattern may be related to ongoing slow-wave sleep mentation that may sometimes trigger sleep terror episodes, its functional significance remains an open question. The results demonstrate the utility of EEG mapping for the quantification of brain activation during sleep terror attacks and suggest that discrete activity profiles are identifiable for different types of dreaming-related arousal. 相似文献
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《Current biology : CB》2020,30(6):1077-1091.e5
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Lucy A.L. Tainton-Heap Leonie C. Kirszenblat Eleni T. Notaras Martyna J. Grabowska Rhiannon Jeans Kai Feng Paul J. Shaw Bruno van Swinderen 《Current biology : CB》2021,31(3):578-590.e6
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《Current biology : CB》2020,30(22):4373-4383.e7
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Susan C. P. Renn J. Douglas Armstrong Mingyao Yang Zongsheng Wang Xin An Kim Kaiser Paul H. Taghert 《Developmental neurobiology》1999,41(2):189-207
The central complex is an important center for higher‐order brain function in insects. It is an intricate neuropil composed of four substructures. Each substructure contains repeated neuronal elements which are connected by processes such that topography is maintained. Although the neuronal architecture has been described in several insects and the behavioral role investigated in various experiments, the exact function of this neuropil has proven elusive. To describe the architecture of the central complex, we study 15 enhancer‐trap lines that label various ellipsoid body neuron types. We find evidence for restriction of gene expression that is correlated with specific neuronal types: such correlations suggest functional classifications as well. We show that some enhancer‐trap patterns reveal a single ellipsoid body neuron type, while others label multiple types. We describe the development of the ellipsoid body neuropil in wild‐type animals and propose developmental mechanisms based on animals displaying structural mutations of this neuropil. The experiments performed here demonstrate the degree of resolution possible from the analysis of enhancer‐trap lines and form a useful library of tools for future structure/function studies of the ellipsoid body. © 1999 John Wiley & Sons, Inc. J Neurobiol 41: 189–207, 1999 相似文献
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ABSTRACT The well-known Two-Process Model of Sleep Regulation describes the integration of the circadian rhythm of arousal and sleep – Process C, and the homeostatic pressure to sleep – Process S. Presently, the known biological markers for Process C are melatonin and core body temperature; whereas, for Process S, there is no biological marker except that of aspects of the electroencephalogram (EEG). Endozepines are a class of endogenous compounds that act like benzodiazepines (BZ), i.e., serving as ligands for the BZ binding sites on GABAA receptors. Not much is known about the role of endozepines, in particular non-peptide endozepines, in the sleep field except very few reports about high concentrations observed in endozepine stupor, a rare phenomenon of idiopathic recurring stupor. We focused on hypoxanthine and thromboxane A2, which are considered to have endozepine function. This study aimed to examine the effect of 24 h of acute sleep deprivation on blood levels of hypoxanthine and thromboxane A2 of healthy subjects without sleep problems or disorders. The results showed a significant decrease of both compounds in the morning after sleep deprivation in comparison to the unrestricted normal sleep condition, thereby suggesting that these endozepines are secreted regularly while asleep, and, thus, are necessary for the sleep process. This study is the first to suggest a connection between specific biological markers – endozepines and Process S – in the Two-Process Model of Sleep Regulation and, furthermore, it sheds light on the possible role of endozepines in sleepiness and fatigue. 相似文献
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《Chronobiology international》2013,30(10):930-941
Cloistered monks and nuns adhere to a 10-century-old strict schedule with a common zeitgeber of a night split by a 2- to 3-h-long Office (Matins). The authors evaluated how the circadian core body temperature rhythm and sleep adapt in cloistered monks and nuns in two monasteries. Five monks and five nuns following the split-sleep night schedule for 5 to 46 yrs without interruption and 10 controls underwent interviews, sleep scales, and physical examination and produced a week-long sleep diary and actigraphy, plus 48-h recordings of core body temperature. The circadian rhythm of temperature was described by partial Fourier time-series analysis (with 12- and 24-h harmonics). The temperature peak and trough values and clock times did not differ between groups. However, the temperature rhythm was biphasic in monks and nuns, with an early decrease at 19:39?±?4:30?h (median?±?95% interval), plateau or rise of temperature at 22:35?±?00:23?h (while asleep) lasting 296?±?39?min, followed by a second decrease after the Matins Office, and a classical morning rise. Although they required alarm clocks to wake-up for Matins at midnight, the body temperature rise anticipated the nocturnal awakening by 85?±?15?min. Compared to the controls, the monks and nuns had an earlier sleep onset (20:05?±?00:59?h vs. 00:00?±?00:54?h, median?±?95% confidence interval, p?=?.0001) and offset (06:27?±?0:22?h, vs. 07:37?±?0:33?h, p?=?.0001), as well as a shorter sleep time (6.5?±?0.6 vs. 7.6?±?0.7?h, p?=?.05). They reported difficulties with sleep latency, sleep duration, and daytime function, and more frequent hypnagogic hallucinations. In contrast to their daytime silence, they experienced conversations (and occasionally prayers) in dreams. The biphasic temperature profile in monks and nuns suggests the human clock adapts to and even anticipates nocturnal awakenings. It resembles the biphasic sleep and rhythm of healthy volunteers transferred to a short (10-h) photoperiod and provides a living glance into the sleep pattern of medieval time. (Author correspondence: isabelle.
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《Current biology : CB》2023,33(13):2702-2716.e3
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