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Sleep alterations following exposure to stress predict fear-associated memory impairments in a rodent model of PTSD
被引:0
|作者:
William M. Vanderheyden
Sophie A. George
Lea Urpa
Michaela Kehoe
Israel Liberzon
Gina R. Poe
机构:
[1] University of Michigan,Department of Anesthesiology
[2] University of Michigan,Department of Psychiatry
来源:
关键词:
PTSD;
Stress;
REM sleep;
Rat;
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暂无
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学科分类号:
摘要:
Sleep abnormalities, such as insomnia, nightmares, hyper-arousal, and difficulty initiating or maintaining sleep, are diagnostic criteria of posttraumatic stress disorder (PTSD). The vivid dream state, rapid eye movement (REM) sleep, has been implicated in processing emotional memories. We have hypothesized that REM sleep is maladaptive in those suffering from PTSD. However, the precise neurobiological mechanisms regulating sleep disturbances following trauma exposure are poorly understood. Using single prolonged stress (SPS), a well-validated rodent model of PTSD, we measured sleep alterations in response to stressor exposure and over a subsequent 7-day isolation period during which the PTSD-like phenotype develops. SPS resulted in acute increases in REM sleep and transition to REM sleep, and decreased waking in addition to alterations in sleep architecture. The severity of the PTSD-like phenotype was later assessed by measuring freezing levels on a fear-associated memory test. Interestingly, the change in REM sleep following SPS was significantly correlated with freezing behavior during extinction recall assessed more than a week later. Reductions in theta (4–10 Hz) and sigma (10–15 Hz) band power during transition to REM sleep also correlated with impaired fear-associated memory processing. These data reveal that changes in REM sleep, transition to REM sleep, waking, and theta and sigma power may serve as sleep biomarkers to identify individuals with increased susceptibility to PTSD following trauma exposure.
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页码:2335 / 2346
页数:11
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