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首页> 外文期刊>Frontiers in Psychiatry >Effects of Xiaoyaosan on the Hippocampal Gene Expression Profile in Rats Subjected to Chronic Immobilization Stress
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Effects of Xiaoyaosan on the Hippocampal Gene Expression Profile in Rats Subjected to Chronic Immobilization Stress

机译:逍遥散对慢性束缚应激大鼠海马基因表达的影响。

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Objective: This study examined the effect of Xiaoyaosan and its anti-stress mechanism in rats subjected to chronic immobilization stress at the whole genome level. Methods: Rat whole genome expression chips (Illumina) were used to detect differences in hippocampal gene expression in rats from the control group (CN group), model group (M group) and Xiaoyaosan group (XYS group) that were subjected to chronic immobilization stress. The Gene Ontology terms and signaling pathways that were altered in the hippocampus gene expression profile were analyzed. The network regulating the transcription of the differentially expressed genes was also established. To verify the results from the gene chips, real-time quantitative polymerase chain reaction was used to determine the expression of the GABRA1, FADD, CRHR2, and CDK6 genes in hippocampal tissues. In situ hybridization (ISH) and immunohistochemistry were used to determine the expression of the GABRA1 and CRHR2 genes and proteins, respectively. Results: Compared with the CN group, 566 differentially expressed genes were identified in the M group. Compared with the M group, 544 differentially expressed genes were identified in the XYS group. In the M and XYS groups, multiple significantly upregulated or downregulated genes functioned in various biological processes. The cytokine receptor interaction pathway was significantly inhibited in the hippocampus of the model group. The actin cytoskeleton regulation pathway was significantly increased in the hippocampus of the XYS group. The inhibition of hippocampal cell growth was the core molecular event of network regulating the transcription of the differentially expressed genes in the model group. Promotion of the regeneration of hippocampal neurons was the core molecular event of the transcriptional regulatory network in the XYS group. The levels of the GABRA1, FADD, CRHR2 and CDK6 mRNAs, and proteins were basically consistent with the results obtained from the gene chip. Conclusion: XYS may have the ability of resistance to stress, enhancement immunity and promotion nerve cell regeneration by regulating the expression of multiple genes in numerous pathways and repaired the stress-induced impairments in hippocampal structure and function by inducing cytoskeletal reorganization. These results may provide the possible target spots in the treatment of stress in rats with XYS.
机译:目的:研究逍遥散在全基因组水平上对慢性固定应激大鼠的作用及其抗应激机制。方法:采用大鼠全基因组表达芯片(Illumina)检测慢性固定应激对照组(CN组),模型组(M组)和逍遥散组(XYS组)大鼠海马基因表达的差异。 。分析了海马基因表达谱中改变的基因本体论术语和信号传导途径。还建立了调节差异表达基因转录的网络。为了验证基因芯片的结果,实时定量聚合酶链反应用于确定海马组织中GABRA1,FADD,CRHR2和CDK6基因的表达。原位杂交(ISH)和免疫组化分别用于确定GABRA1和CRHR2基因和蛋白质的表达。结果:与CN组相比,M组中鉴定出566个差异表达基因。与M组相比,XYS组中鉴定出544个差异表达基因。在M和XYS组中,多个显着上调或下调的基因在各种生物学过程中起作用。在模型组的海马中,细胞因子受体的相互作用途径被显着抑制。 XYS组海马中的肌动蛋白细胞骨架调节途径显着增加。海马细胞生长的抑制是网络调节模型组中差异表达基因转录的核心分子事件。促进海马神经元再生是XYS组转录调控网络的核心分子事件。 GABRA1,FADD,CRHR2和CDK6 mRNA和蛋白质的水平与从基因芯片获得的结果基本一致。结论:XYS可能通过调节多种途径中多个基因的表达,具有抗应激,增强免疫力和促进神经细胞再生的能力,并通过诱导细胞骨架重组来修复应激诱导的海马结构和功能障碍。这些结果可能为治疗XYS大鼠的应激提供可能的靶点。

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