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从太空的BION-M1任务返回的小鼠免疫细胞信号传导、细胞凋亡和应激反应功能的变化。

Changes in immune cell signalling, apoptosis and stress response functions in mice returned from the BION-M1 mission in space.

作者信息

Novoselova E G, Lunin S M, Khrenov M O, Parfenyuk S B, Novoselova T V, Shenkman B S, Fesenko E E

机构信息

Institute of Cell Biophysics, Pushchino, Moscow Region, Russia.

Institute of Cell Biophysics, Pushchino, Moscow Region, Russia.

出版信息

Immunobiology. 2015 Apr;220(4):500-9. doi: 10.1016/j.imbio.2014.10.021. Epub 2014 Oct 30.

Abstract

To explore the effect of the spaceflight environment on immunity in animals, C57/BL6 mice flown on a 30-day space high-orbit satellite mission (BION-M1) were analyzed. Cytokine response in mice was measured in tandem with the following parameters: the synthesis of inducible forms of the heat shock proteins HSP72 and HSP90α; activity of the NF-κB, IFR3, and SAPK/JNK signalling pathways; and TLR4 expression. In addition, apoptosis in the thymus was measured by caspase-3 and ph-p53/p53 ratio testing. In response to flight environment exposure, mice had a reduction in spleen and thymus masses and decreased splenic and thymic lymphocyte counts. Plasma concentration of IL-6 and IFN-γ but not TNF-α was decreased in C57BL6 mice. The NF-κB activity in splenic lymphocytes through the canonical pathway involving IκB degradation was significantly increased at 12h after landing. One week after landing, however, the activity of NF-κB was markedly decreased below even the control values. Non-canonical NF-κB activity increased during the whole observation period. The activities of SAPK/JNK and IRF-3 were invariable at 12h but significantly increased 7 days after landing. The expression of Hsp72 and Hsp90α was somewhat increased 12h (Hsp72) and 7 days (Hsp90α). TLR4 expression in splenic cells was significantly increased only at 12h, returning to normal 7 days after landing. To assess the apoptosis in thymus lymphocytes, caspase-3 and levels of p53 protein along with its phosphorylated form were measured in thymic lymphocytes. The results indicated that the high-orbit spaceflight environment caused an increase in the level of p53 but more notably in the activated, phosphorylated form of the p53 protein. The calculated ratio of the active to inactive forms of the protein (ph-53/p53) 12h after landing increased by more than twofold, indicating the apparent induction of apoptosis in thymus cells. Interestingly, 7 days after the landing, this ratio was not restored, but rather increased: the specified ratio was four times higher compared to the ground-based control. Measurements of caspase-3 in thymic cells indicated more expressive increase in apoptosis. Taken together, the results of the present study indicate that spaceflight induces an imbalance in the immunity of mice, showing variation in signalling, apoptosis and stress response that are not restored by 7 days after landing. These changes are distinguished from classic stress-related alterations usually caused by conventional stressors.

摘要

为探究太空飞行环境对动物免疫力的影响,对搭乘30天太空高轨道卫星任务(BION-M1)的C57/BL6小鼠进行了分析。同时测量了小鼠体内细胞因子反应以及以下参数:热休克蛋白HSP72和HSP90α诱导型的合成;NF-κB、IFR3和SAPK/JNK信号通路的活性;以及TLR4表达。此外,通过检测caspase-3和ph-p53/p53比值来测量胸腺中的细胞凋亡情况。暴露于飞行环境后,小鼠的脾脏和胸腺重量减轻,脾脏和胸腺淋巴细胞数量减少。C57BL6小鼠血浆中IL-6和IFN-γ的浓度降低,但TNF-α浓度未降低。着陆后12小时,通过涉及IκB降解的经典途径,脾淋巴细胞中的NF-κB活性显著增加。然而,着陆一周后,NF-κB的活性明显降低,甚至低于对照值。在整个观察期内,非经典NF-κB活性增加。SAPK/JNK和IRF-3的活性在着陆后12小时无变化,但在着陆7天后显著增加。Hsp72的表达在着陆后12小时有所增加,Hsp90α的表达在着陆7天后有所增加。脾细胞中TLR4的表达仅在着陆后12小时显著增加,着陆7天后恢复正常。为评估胸腺淋巴细胞中的细胞凋亡情况,在胸腺淋巴细胞中测量了caspase-3以及p53蛋白及其磷酸化形式的水平。结果表明,高轨道太空飞行环境导致p53水平升高,但更显著的是p53蛋白的活化、磷酸化形式升高。着陆后12小时计算得出的蛋白活性与非活性形式的比值(ph-53/p53)增加了两倍多,表明胸腺细胞中明显诱导了细胞凋亡。有趣的是,着陆7天后,该比值并未恢复,反而升高:与地面对照组相比,该特定比值高出四倍。胸腺细胞中caspase-3的测量结果表明细胞凋亡有更明显的增加。综上所述,本研究结果表明太空飞行会导致小鼠免疫力失衡,在信号传导、细胞凋亡和应激反应方面出现变化,且着陆7天后这些变化并未恢复。这些变化与通常由传统应激源引起的经典应激相关改变不同。

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