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Distinct effects of acute and chronic sleep loss on DNA damage in rats.

机译:急性和慢性睡眠丧失对大鼠DNA损伤的不同影响。

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摘要

The aim of this investigation was to evaluate genetic damage induced in male rats by experimental sleep loss for short-term (24 and 96 h) and long-term (21 days) intervals, as well as their respective recovery periods in peripheral blood, brain, liver and heart tissue by the single cell gel (comet) assay. Rats were paradoxically deprived of sleep (PSD) by the platform technique for 24 or 96 h, or chronically sleep-restricted (SR) for 21 days. We also sought to verify the time course of their recovery after 24 h of rebound sleep. The results showed DNA damage in blood cells of rats submitted to PSD for 96 h. Brain tissue showed extensive genotoxic damage in PSD rats (both 24 and 96 h), though the effect was more pronounced in the 96 h group. Rats allowed to recover from the PSD-96 h and SR-21 days treatments showed DNA damage as compared to negative controls. Liver and heart did not display any genotoxicity activity. Corticosterone concentrations were increased after PSD (24 and 96 h) relative to control rats, whereas these levels were unaffected in the SR group. Collectively, these findings reveal that sleep loss was able to induce genetic damage in blood and brain cells, especially following acute exposure. Since DNA damage is an important step in events leading to genomic instability, this study represents a relevant contribution to the understanding of the potential health risks associated with sleep deprivation.
机译:这项研究的目的是评估短期(24和96 h)和长期(21天)间隔的实验性睡眠丧失对雄性大鼠诱发的遗传损伤,以及它们各自在外周血,脑中的恢复期,肝和心脏组织通过单细胞凝胶(彗星)测定。通过平台技术自相矛盾地剥夺了大鼠的睡眠(PSD)24或96 h,或使长期限制睡眠(SR)的大鼠失去了21天。我们还试图验证其在反弹睡眠24小时后恢复的时间过程。结果显示,接受PSD 96 h的大鼠血细胞DNA损伤。脑组织在PSD大鼠中均表现出广泛的遗传毒性损害(24和96 h),尽管在96 h组中这种作用更为明显。与阴性对照相比,从PSD-96 h和SR-21天治疗中恢复的大鼠显示出DNA损伤。肝和心脏未显示任何遗传毒性活动。相对于对照大鼠,PSD后(24和96 h)皮质类固醇浓度增加,而SR组这些水平未受影响。这些发现共同表明,睡眠不足能够引起血液和脑细胞的遗传损伤,尤其是在急性暴露后。由于DNA损伤是导致基因组不稳定的重要一步,因此这项研究为理解与睡眠剥夺相关的潜在健康风险做出了重要贡献。

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