Anxiogenic Potential of Experimental Sleep Fragmentation Is Duration-Dependent and Mediated via Oxidative Stress State | Zendy

Željko Grubač | Zendy; Nikola Šutulović | Zendy; Sonja Šuvakov | Zendy; Djurdja Jerotić | Zendy; Nela Puškaš | Zendy; Djuro Macut | Zendy; Aleksandra Rašić-Marković | Zendy; Tatjana Simić | Zendy; Olivera Stanojlović | Zendy; Dragan Hrnčić | Zendy

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Anxiogenic Potential of Experimental Sleep Fragmentation Is Duration-Dependent and Mediated via Oxidative Stress State

Author(s) -

Željko Grubač,

Nikola Šutulović,

Sonja Šuvakov,

Djurdja Jerotić,

Nela Puškaš,

Djuro Macut,

Aleksandra Rašić-Marković,

Tatjana Simić,

Olivera Stanojlović,

Dragan Hrnčić

Publication year - 2021

Publication title -

oxidative medicine and cellular longevity

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 1.494

H-Index - 93

eISSN - 1942-0900

pISSN - 1942-0994

DOI - 10.1155/2021/2262913

Subject(s) - oxidative stress , anxiogenic , anxiety , medicine , endocrinology , fragmentation (computing) , hippocampus , hippocampal formation , psychology , neuroscience , anxiolytic , biology , psychiatry , ecology

Sleep architecture alterations, among which sleep fragmentation is highly prevalent, represent risk factors for a variety of diseases, ranging from cardiovascular to brain disorders, including anxiety. What mediates anxiety occurrence upon sleep fragmentation is still a matter of debate. We hypothesized that the sleep fragmentation effects on anxiety are dependent on its duration and mediated by increased oxidative stress and alterations in the number of parvalbumin (PV+) interneurons in the hippocampus. Sleep was fragmented in rats by the treadmill method during a period of 14 days (SF group). Rats with undisturbed sleep in the treadmill (TC group) and those receiving equal amounts of treadmill belt motion (EC group) served as controls. To assess anxiety, we subjected rats to the open field, elevated plus maze, and light-dark tests on the 0, 7 th , and 14 th day. Upon the last test, brain structures were sampled for oxidative stress assessment and PV+ interneuron immunohistochemistry. The results of ethological tests of anxiety-linked behavior suggested duration-dependent anxiogenic potential of sleep fragmentation. Rats' anxiety-linked behavior upon sleep fragmentation significantly correlated with oxidative stress. The rats with fragmented sleep (SF) showed significantly higher oxidative stress in the hippocampus, thalamus, and cortex, compared to controls (TC and EC), while the antioxidant enzymes' activity was significantly decreased. No significant differences were observed in hippocampal PV+ interneurons among these groups. Our results showed that duration of sleep fragmentation is a significant determinant of anxiety-linked behavior, and these effects are mediated through oxidative distress in the brain. Herein, it is revealed that the sleep fragmentation-oxidative stress-anxiety axis contributes to our better understanding of pathophysiological processes, occurring due to disrupted sleep patterns.

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