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细胞培养实验表明,高S100B和簇集素水平可能赋予冠海豹(Cystophora cristata)大脑耐缺氧能力。

Cell Culture Experiments Reveal that High S100B and Clusterin Levels may Convey Hypoxia-tolerance to the Hooded Seal (Cystophora cristata) Brain.

作者信息

Geßner Cornelia, Stillger Maren Nicole, Mölders Naomi, Fabrizius Andrej, Folkow Lars P, Burmester Thorsten

机构信息

Institute of Zoology, University of Hamburg, 20146 Hamburg, Germany.

Institute of Zoology, University of Hamburg, 20146 Hamburg, Germany.

出版信息

Neuroscience. 2020 Dec 15;451:226-239. doi: 10.1016/j.neuroscience.2020.09.039. Epub 2020 Sep 28.

Abstract

While the brain of most mammals suffers from irreversible damage after only short periods of low oxygen levels (hypoxia), marine mammals are excellent breath-hold divers that have adapted to hypoxia. In addition to physiological adaptations, such as large oxygen storing capacity and strict oxygen economy during diving, the neurons of the deep-diving hooded seal (Cystophora cristata) have an intrinsic tolerance to hypoxia. We aim to understand the molecular basis of this neuronal hypoxia tolerance. Previously, transcriptomics of the cortex of the hooded seal have revealed remarkably high expression levels of S100B and clusterin (apolipoprotein J) when compared to the ferret, a non-diving carnivore. Both genes have much-debated roles in hypoxia and oxidative stress. Here, we evaluated the effects of S100B and of two isoforms of clusterin (soluble and nucleus clusterin) on the survival, metabolic activity and the amount of reactive oxygen species (ROS) in HN33 neuronal mouse cells exposed to hypoxia and oxidative stress. S100B and soluble clusterin had neuroprotective effects, with reduced ROS-levels and retention of normoxic energy status of cells during both stress conditions. The protective effects of nucleus clusterin were restricted to hypoxia. S100B and clusterin showed purifying selection in marine and terrestrial mammals, indicating a functional conservation across species. Immunofluorescence revealed identical cellular distributions of S100B and clusterin in mice, ferrets and hooded seals, further supporting the functional conservation. Taken together, our data suggest that the neuroprotective effects of all three proteins are exclusively facilitated by their increased expression in the brain of the hooded seal.

摘要

虽然大多数哺乳动物的大脑在经历短时间的低氧水平(缺氧)后就会遭受不可逆的损伤,但海洋哺乳动物却是适应了缺氧环境的出色屏气潜水者。除了生理适应性,如潜水时具有较大的氧气储存能力和严格的氧气节约机制外,深海冠海豹(Cystophora cristata)的神经元对缺氧具有内在耐受性。我们旨在了解这种神经元缺氧耐受性的分子基础。此前,与非潜水食肉动物雪貂相比,冠海豹皮质的转录组学研究显示,S100B和簇集蛋白(载脂蛋白J)的表达水平显著较高。这两个基因在缺氧和氧化应激中的作用备受争议。在此,我们评估了S100B以及簇集蛋白的两种异构体(可溶性簇集蛋白和核簇集蛋白)对暴露于缺氧和氧化应激的HN33神经元小鼠细胞的存活、代谢活性和活性氧(ROS)量的影响。S100B和可溶性簇集蛋白具有神经保护作用,在两种应激条件下,细胞内的ROS水平降低,且维持了常氧能量状态。核簇集蛋白的保护作用仅限于缺氧情况。S100B和簇集蛋白在海洋和陆地哺乳动物中表现出纯化选择,表明跨物种存在功能保守性。免疫荧光显示,S100B和簇集蛋白在小鼠、雪貂和冠海豹中的细胞分布相同,进一步支持了功能保守性。综上所述,我们的数据表明所有这三种蛋白质的神经保护作用完全是由它们在冠海豹大脑中表达增加所促成的。

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