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首页> 外文期刊>Neuroimmunomodulation >Imbalance between Th17 and Treg Cells May Play an Important Role in the Development of Chronic Unpredictable Mild Stress-Induced Depression in Mice.
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Imbalance between Th17 and Treg Cells May Play an Important Role in the Development of Chronic Unpredictable Mild Stress-Induced Depression in Mice.

机译:Th17和Treg细胞之间的失衡可能在小鼠慢性不可预测的轻度应激诱导的抑郁症的发生中起重要作用。

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Background: Recent data suggest that major depression is potentially associated with dysregulated cytokine production. However, the roles of T helper (Th) cells and their subsets in the development of depression still remain to be determined. The present study assessed changes in Th cell subsets and cytokines during the development of depression in a mouse model. Methods: Chronic unpredictable mild stress (CUMS) was used to simulate depression behavior in mice. The open field test, sucrose preference, and ingestion were used as evaluative indicators of depressive behavior. During the CUMS protocol, on days 3, 7, 14, and 21, we assessed behavioral changes, cytokine levels in serum or stimulated (CD3/CD28) cell culture medium, and mRNA expression (ELISA, RT-PCR), regulatory T (Treg) and Th17 subsets in spleen (ex vivo, flow cytometry, RT-PCR), and CD3/rIL-23-stimulated Th17 cell proliferation (MTT assay). Results: The results showed that in the depression model mice, IL-4 mRNA expression and serum levels increased on day 7, while no detectable change was observed in IFN-γ. Notably, a reduced proportion of Th17 cells with decreased proliferation capacity was observed at later stages, in parallel with a decline in serum IL-23 levels. In contrast, an increased Treg cell proportion and increased Foxp3 mRNA expression were observed in the mid-stages. Correlation analysis showed that the proportion of Tregs was correlated negatively with sucrose preference, while the proliferation of Th17 cells was notably correlated positively with sucrose preference. Also, an increased TGF-β level was detected in serum and was believed to be a key factor responsible for the imbalance between Th17 and Treg cells. Furthermore, the sucrose preference in TGF-β type I receptor blockade mice increased considerably, compared with CUMS mice. Conclusion: These results indicate that in CUMS-induced depression, behavioral changes may closely correlate with the imbalance between Th17 and Treg cell subsets, and TGF-β may be a key regulatory cytokine.
机译:背景:最新数据表明,严重的抑郁症可能与细胞因子产生失调有关。然而,T辅助细胞(Th)及其亚群在抑郁症发展中的作用仍有待确定。本研究评估了小鼠模型中抑郁症发展过程中Th细胞亚群和细胞因子的变化。方法:使用慢性不可预测的轻度应激(CUMS)模拟小鼠的抑郁行为。露天试验,蔗糖偏爱和摄取被用作抑郁行为的评估指标。在CUMS方案中,在第3、7、14和21天,我们评估了行为变化,血清或刺激的(CD3 / CD28)细胞培养基中的细胞因子水平,以及mRNA表达(ELISA,RT-PCR),调节性T( Treg)和脾脏中Th17亚群(离体,流式细胞仪,RT-PCR)和CD3 / rIL-23刺激的Th17细胞增殖(MTT分析)。结果:结果显示,在抑郁模型小鼠中,IL-4 mRNA表达和血清水平在第7天升高,而IFN-γ则未检测到变化。值得注意的是,在后期观察到具有降低的增殖能力的Th17细胞比例降低,同时血清IL-23水平下降。相反,在中期观察到Treg细胞比例增加和Foxp3 mRNA表达增加。相关分析表明,Tregs的比例与蔗糖偏爱呈负相关,而Th17细胞的增殖与蔗糖偏爱呈显着正相关。另外,在血清中检测到TGF-β水平升高,并且被认为是导致Th17和Treg细胞之间失衡的关键因素。此外,与CUMS小鼠相比,TGF-βI型受体阻断小鼠的蔗糖偏爱显着增加。结论:这些结果表明,在CUMS诱发的抑郁症中,行为改变可能与Th17和Treg细胞亚群之间的失衡密切相关,而TGF-β可能是关键的调节细胞因子。

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