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间歇性低氧调节氧化还原稳态、与脂质代谢相关的炎症过程和氧化还原翻译后修饰:高海拔的益处。

Intermittent hypoxia modulates redox homeostasis, lipid metabolism associated inflammatory processes and redox post-translational modifications: Benefits at high altitude.

机构信息

Peptide and Proteomics Division, Defence Institute of Physiology and Allied Sciences, Defence Research and Development Organization, Lucknow Road, Timarpur, Delhi, 110054, India.

出版信息

Sci Rep. 2020 May 13;10(1):7899. doi: 10.1038/s41598-020-64848-x.

Abstract

Intermittent hypoxia, initially associated with adverse effects of sleep apnea, has now metamorphosed into a module for improved sports performance. The regimen followed for improved sports performance is milder intermittent hypoxic training (IHT) as compared to chronic and severe intermittent hypoxia observed in sleep apnea. Although several studies have indicated the mechanism and enough data on physiological parameters altered by IH is available, proteome perturbations remain largely unknown. Altitude induced hypobaric hypoxia is known to require acclimatization as it causes systemic redox stress and inflammation in humans. In the present study, a short IHT regimen consisting of previously reported physiologically beneficial FIO2 levels of 13.5% and 12% was administered to human subjects. These subjects were then airlifted to altitude of 3500 m and their plasma proteome along with associated redox parameters were analyzed on days 4 and 7 of high altitude stay. We observed that redox stress and associated post-translational modifications, perturbed lipid metabolism and inflammatory signaling were induced by IHT exposure at Baseline. However, this caused activation of antioxidants, energy homeostasis mechanisms and anti-inflammatory responses during subsequent high-altitude exposure. Thus, we propose IHT as a beneficial non-pharmacological intervention that benefits individuals venturing to high altitude areas.

摘要

间歇性低氧最初与睡眠呼吸暂停的不良影响有关,现在已经演变成提高运动表现的模块。与睡眠呼吸暂停中观察到的慢性和严重间歇性低氧相比,为提高运动表现而遵循的方案是轻度间歇性低氧训练 (IHT)。尽管有几项研究表明了 IH 改变生理参数的机制和足够的数据,但蛋白质组的改变在很大程度上仍不清楚。众所周知,高原诱导的低气压低氧需要适应,因为它会导致人体全身氧化应激和炎症。在本研究中,对人类受试者给予先前报道的生理有益的 FIO2 水平 13.5%和 12%的短 IHT 方案。然后将这些受试者空运到 3500 m 的海拔高度,并在高海拔停留的第 4 天和第 7 天分析他们的血浆蛋白质组及其相关的氧化还原参数。我们观察到,在基线时,IHT 暴露会引起氧化应激和相关的翻译后修饰、脂质代谢紊乱和炎症信号。然而,这会在随后的高海拔暴露期间激活抗氧化剂、能量稳态机制和抗炎反应。因此,我们提出 IHT 作为一种有益的非药物干预措施,有益于前往高海拔地区的个体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7bc1/7220935/6ae915fc8470/41598_2020_64848_Fig1_HTML.jpg

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