在人SK-N-SH神经元中，通过rna结合蛋白RBM3表达的神经保护受低温调节，而不受缺氧调节。

Hypoxia (Auckland, N.Z.) Pub Date : 2017-05-23 eCollection Date: 2017-01-01 DOI:10.2147/HP.S132462

Lisa-Maria Rosenthal, Giang Tong, Christoph Walker, Sylvia J Wowro, Jana Krech, Constanze Pfitzer, Georgia Justus, Felix Berger, Katharina Rose Luise Schmitt

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引用次数: 5

摘要

目的:治疗性低温是围产期窒息的常用治疗方法。然而，许多足月婴儿继续死亡或患有神经发育障碍。几项实验研究表明，在缺氧损伤后，轻度至中度低温有有益的作用，但对低温诱导的神经保护的理解仍然不完整。一般来说，低温会减弱整体蛋白质合成，但一小部分rna结合蛋白，包括rna结合基序3 (RBM3)，在低温下会上调。本研究的目的是建立体外模型，研究缺氧和低温对神经元细胞存活的影响，并检测并发冷休克蛋白RBM3基因表达的动力学。方法:将人SK-N-SH神经元暴露在不同氧浓度(21%，8%或0.2% O2)中24小时，然后进行中低温(33.5°C)或常温24,48或72小时的实验。通过乳酸脱氢酶和神经元特异性烯醇化酶释放到细胞培养液中定量测定细胞死亡，并通过免疫荧光染色评估细胞形态。采用逆转录-定量聚合酶链反应和Western blot分析RBM3基因表达的调控。结果:暴露于缺氧(0.2% O2) 24小时可显著增加SK-N-SH神经元的细胞死亡，而暴露于8% O2对细胞活力无显著影响。在缺氧后进行48或72小时的中等低温治疗可使神经元免于缺氧诱导的细胞死亡。此外，暴露于严重缺氧导致可观察到的细胞肿胀，中等低温也会减弱。最后，适度低温而非缺氧诱导RBM3在转录和翻译水平上的表达。结论:适度低温可保护缺氧诱导的神经元细胞死亡。低温诱导冷休克蛋白RBM3的表达，可能是低温诱导神经保护的一种可能介质。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Neuroprotection via RNA-binding protein RBM3 expression is regulated by hypothermia but not by hypoxia in human SK-N-SH neurons.

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Neuroprotection via RNA-binding protein RBM3 expression is regulated by hypothermia but not by hypoxia in human SK-N-SH neurons.

Objective: Therapeutic hypothermia is an established treatment for perinatal asphyxia. Yet, many term infants continue to die or suffer from neurodevelopmental disability. Several experimental studies have demonstrated a beneficial effect of mild-to-moderate hypothermia after hypoxic injury, but the understanding of hypothermia-induced neuroprotection remains incomplete. In general, global protein synthesis is attenuated by hypothermia, but a small group of RNA-binding proteins including the RNA-binding motif 3 (RBM3) is upregulated in response to cooling. The aim of this study was to establish an in vitro model to investigate the effects of hypoxia and hypothermia on neuronal cell survival, as well as to examine the kinetics of concurrent cold-shock protein RBM3 gene expression.

Methods: Experiments were performed by using human SK-N-SH neurons exposed to different oxygen concentrations (21%, 8%, or 0.2% O₂) for 24 hours followed by moderate hypothermia (33.5°C) or normothermia for 24, 48, or 72 hours. Cell death was determined by quantification of lactate dehydrogenase and neuron-specific enolase releases into the cell cultured medium, and cell morphology was assessed by using immunofluorescence staining. The regulation of RBM3 gene expression was assessed by reverse transcriptase-quantitative polymerase chain reaction and Western blot analysis.

Results: Exposure to hypoxia (0.2% O₂) for 24 hours resulted in significantly increased cell death in SK-N-SH neurons, whereas exposure to 8% O₂ had no significant impact on cell viability. Post-hypoxia treatment with moderate hypothermia for 48 or 72 hours rescued the neurons from hypoxia-induced cell death. Moreover, exposure to severe hypoxia led to observable cell swelling, which was also attenuated by moderate hypothermia. Finally, moderate hypothermia but not hypoxia led to the induction of RBM3 expression on both transcriptional and translational levels.

Conclusion: Moderate hypothermia protects neurons from hypoxia-induced cell death. The expression of the cold-shock protein RBM3 is induced by moderate hypothermia and could be one possible mediator of hypothermia-induced neuroprotection.

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Hypoxia (Auckland, N.Z.)

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16 weeks