信号转导和转录激活因子3（STAT3）的抗氧化作用与细胞对异氟烷的易损性有关。

The antioxidative effect of STAT3 involved in cellular vulnerability to isoflurane.

作者信息

Yang Yan, Song Shiyu, Wang Hongwei, Ma Zhengliang, Gao Qian

机构信息

Department of Anesthesiology, Nanjing Drum Tower Hospital, Affiliated Hospital of Medical School, Nanjing University, Nanjing, Jiangsu Province, 210008, China.

Center for Translational Medicine and Jiangsu Key Laboratory of Molecular Medicine, Medical School of Nanjing University, Nanjing, Jiangsu Province, 210093, China.

出版信息

BMC Neurosci. 2024 Dec 4;25(1):75. doi: 10.1186/s12868-024-00911-x.

DOI:10.1186/s12868-024-00911-x

PMID:39633283

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11619428/

Abstract

BACKGROUND

The vulnerable period to neurotoxicity of isoflurane overlaps with a developmental stage characterized by programmed neuronal death. STAT3 has been identified as a crucial molecule involved in survival pathways during this period. We aimed to investigate the role of STAT3 in cellular vulnerability to isoflurane.

METHODS

C57/BL6 mice on postnatal day 7 or 21, primary neurons derived from mice embryos at gestational days 14-16 and cultured for 5 or 14 days, as well as human neuroglioma U251 cells were treated with isoflurane. A plasmid containing human wild-type STAT3, STAT3 anti-sense oligonucleotide, STAT3 specific inhibitor STA21, proteasome inhibitor MG-132 and calcineurin inhibitor FK506 were utilized to evaluate the influence of STAT3 levels on isoflurane-induced cytotoxicity. The levels of Western blot results, mRNA, intracellular ROS, apoptotic rate, and calcineurin activity were analyzed using unpaired Student's t-test or one-way ANOVA followed by Bonferroni post hoc test, as appropriate.

RESULTS

Elevated levels of STAT3, reduced activity of calcineurin, as well as a diminished response to isoflurane-induced calcineurin activation and neuroapoptosis were observed in more mature brain or neurons. Isoflurane accelerated the degradation of ubiquitin-conjugated proteins but did not facilitate ubiquitin conjugation to proteins. STAT3 was of particular importance in the all ubiquitin-conjugated proteins degraded by isoflurane. Knockdown or inhibition of STAT3 nuclear translocation exacerbated isoflurane-induced oxidative injury and apoptosis, while STAT3 overexpression mitigated these effects. Finally, this study demonstrated that FK506 pretreatment mitigated the apoptosis, ROS accumulation, and the impairment of neurite growth in primary neurons after exposed to isoflurane.

CONCLUSIONS

These findings indicate that specific regulation of STAT3 was closely related with the cellular vulnerability to isoflurane via an antioxidative pathway.

摘要

背景

异氟烷神经毒性的易损期与以程序性神经元死亡为特征的发育阶段重叠。信号转导和转录激活因子3（STAT3）已被确定为这一时期参与生存途径的关键分子。我们旨在研究STAT3在细胞对异氟烷易感性中的作用。

方法

对出生后第7天或第21天的C57/BL6小鼠、妊娠第14 - 16天小鼠胚胎来源并培养5天或14天的原代神经元以及人神经胶质瘤U251细胞进行异氟烷处理。使用含人野生型STAT3的质粒、STAT3反义寡核苷酸、STAT3特异性抑制剂STA21、蛋白酶体抑制剂MG - 132和钙调神经磷酸酶抑制剂FK506来评估STAT3水平对异氟烷诱导的细胞毒性的影响。根据情况，使用非配对学生t检验或单因素方差分析及Bonferroni事后检验分析蛋白质印迹结果、mRNA、细胞内活性氧（ROS）水平、凋亡率和钙调神经磷酸酶活性。

结果

在更成熟的脑或神经元中观察到STAT3水平升高、钙调神经磷酸酶活性降低，以及对异氟烷诱导的钙调神经磷酸酶激活和神经细胞凋亡的反应减弱。异氟烷加速了泛素结合蛋白的降解，但未促进泛素与蛋白质的结合。STAT3在异氟烷降解的所有泛素结合蛋白中尤为重要。敲低或抑制STAT3核转位会加剧异氟烷诱导的氧化损伤和细胞凋亡，而STAT3过表达则减轻这些效应。最后，本研究表明FK506预处理减轻了原代神经元暴露于异氟烷后的细胞凋亡、ROS积累和神经突生长损伤。