首页> 外文期刊>Toxicology: An International Journal Concerned with the Effects of Chemicals on Living Systems >Indomethacin reverts sleep disorders produced by ozone exposure in rats.
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Indomethacin reverts sleep disorders produced by ozone exposure in rats.

机译:消炎痛可逆转大鼠因臭氧暴露引起的睡眠障碍。

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摘要

Ozone (O(3)) exposure causes pulmonary biochemical changes both in humans and experimental animals, inducing the release of inflammatory mediators such as cytokines and eicosanoids. Some of these reaction products have been characterized as endogenous sleep-promoting substances and have been implicated in the development of sleepiness in patients with inflammatory disease. Furthermore, sleep alterations are known to occur in O(3)-exposed humans and experimental animals. In order to test the probable involvement of such inflammatory mediators in O(3)-induced sleep disorders, we blocked prostaglandin synthesis administrating the cyclooxygenase inhibitor indomethacin (IM) and compared conventional electrographic sleep parameters in rats under four different experimental conditions: treatment with IM alone, O(3)-exposure, pre-treatment with IM plus O(3) exposure, and control conditions. We found that O(3) exposure increased slow wave sleep (SWS) and decreased rapid eye movement sleep (REMs) significantly, while IM pre-treatment reduced these O(3)-induced sleep disorders. IM treatment alone did not affect sleep. These findings strongly support a role for inflammatory mediators in O(3) exposure-induced neurological alterations.
机译:臭氧(O(3))暴露会导致人类和实验动物的肺生化变化,从而诱导炎症介质(如细胞因子和类花生酸)的释放。这些反应产物中的一些已被表征为促进内源性睡眠的物质,并与炎症性疾病患者的嗜睡发展有关。此外,睡眠改变已知发生在O(3)暴露的人和实验动物中。为了测试这种炎性介质在O(3)诱发的睡眠障碍中的可能参与,我们阻断了前列腺素的合成,使用环加氧酶抑制剂吲哚美辛(IM),并在四种不同的实验条件下比较了大鼠的常规电描记睡眠参数:IM的治疗单独使用O(3)暴露,IM加O(3)暴露进行预处理以及控制条件。我们发现O(3)暴露可显着增加慢波睡眠(SWS)并减少快速眼动睡眠(REMs),而IM预处理可减少这些O(3)诱导的睡眠障碍。单独的IM治疗并不会影响睡眠。这些发现强烈支持炎症介质在O(3)暴露诱导的神经系统改变中的作用。

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