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首页> 外文期刊>International journal of hyperthermia: The official journal of European Society for Hyperthermic Oncology, North American Hyperthermia Group >Hyperthermia protects mice against chronic unpredictable stress-induced anxiety-like behaviour and hippocampal CA3 cell apoptosis.
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Hyperthermia protects mice against chronic unpredictable stress-induced anxiety-like behaviour and hippocampal CA3 cell apoptosis.

机译:热疗保护小鼠免受慢性不可预测的应激诱导的焦虑样行为和海马CA3细胞凋亡的影响。

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摘要

PURPOSE: It is widely accepted that chronic stress can induce anxiety; however, the cellular and molecular mechanisms of stress-induced anxiety are far from being elucidated. Hyperthermia has been shown to induce expression of heat shock proteins (HSPs) to provide protection against a variety of stresses. To our knowledge, the effect of hyperthermia on the development of chronic unpredictable stress (CUS)-induced anxiety has not been studied. This study was to determine the relationship between hyperthermia induced Hsp72 and CUS related anxiety. MATERIALS AND METHODS: Heat shock factor 1 knockout (hsf1(-/-)) and wild-type (hsf1(+/+)) mice were subjected to CUS with or without hyperthermia treatment. Anxiety-like behaviours were evaluated by elevated plus maze and open field tests. Apoptosis in the hippocampal CA3 area was detected by TUNEL staining. Hsp72 protein level in the hippocampus was measured by Western blot. RESULTS: CUS caused significant apoptosis in hippocampal CA3 cells in both hsf1(-/-) and hsf1(+/+) mice, which significantly correlated with anxiety-like behaviours. Hyperthermia induced Hsp72 expression in hsf1(+/+) mice, but not in hsf1(-/-) mice. Importantly, hyperthermia protected hsf1(+/+) mice against developing CUS-related anxiety-like behaviours and reduced CUS-induced apoptosis in hippocampal CA3 cells. In contrast, hyperthermia exhibited no protective role in hsf1(-/-) mice. CONCLUSIONS: Apoptosis of hippocampal CA3 cells is involved in the development of anxiety-like behaviours underlying CUS. Hsp72 protein is a crucial player in the protective effect of hyperthermia against CUS-induced apoptosis and development of anxiety-like behaviours. Our study suggests hyperthermia is an effective treatment for CUS-induced mood disorders.
机译:目的:人们普遍认为,慢性压力会引起焦虑。但是,还没有阐明应激引起焦虑的细胞和分子机制。热疗已显示可诱导热休克蛋白(HSP)的表达,从而提供针对各种压力的保护作用。据我们所知,尚未研究过高温对慢性不可预测压力(CUS)诱发的焦虑的影响。本研究旨在确定热疗诱导的Hsp72与CUS相关焦虑之间的关系。材料与方法:对热休克因子1基因敲除(hsf1(-/-))和野生型(hsf1(+ / +))小鼠进行CUS,不论是否进行热疗。焦虑样行为通过高架迷宫和野外试验进行评估。通过TUNEL染色检测海马CA3区的细胞凋亡。通过蛋白质印迹法测量海马中的Hsp72蛋白水平。结果:CUS引起hsf1(-/-)和hsf1(+ / +)小鼠海马CA3细胞明显凋亡,这与焦虑样行为显着相关。热疗诱导hsf1(+ / +)小鼠中的Hsp72表达,而不是hsf1(-/-)小鼠中的Hsp72表达。重要的是,热疗保护hsf1(+ / +)小鼠免于发展CUS相关的焦虑样行为,并减少CUS诱导的海马CA3细胞凋亡。相反,热疗在hsf1(-/-)小鼠中未显示保护作用。结论:海马CA3细胞的凋亡参与了CUS潜在的焦虑样行为的发展。 Hsp72蛋白在热疗对CUS诱导的细胞凋亡和焦虑样行为发展的保护作用中起着至关重要的作用。我们的研究表明,热疗是治疗CUS引起的情绪障碍的有效方法。

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