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Th1、单核细胞/巨噬细胞和Th2细胞因子混合物对中枢神经系统混合神经胶质细胞培养物中与代谢、信号传导和调节相关分子的早期基因表达的差异影响。

Differential effects of Th1, monocyte/macrophage and Th2 cytokine mixtures on early gene expression for molecules associated with metabolism, signaling and regulation in central nervous system mixed glial cell cultures.

作者信息

Lisak Robert P, Benjamins Joyce A, Bealmear Beverly, Nedelkoska Liljana, Studzinski Diane, Retland Ernest, Yao Bin, Land Susan

机构信息

Department of Neurology, 8D University Health Center, Wayne State University School of Medicine, 4201 St Antoine, Detroit, MI, 48210, USA.

出版信息

J Neuroinflammation. 2009 Jan 21;6:4. doi: 10.1186/1742-2094-6-4.

Abstract

BACKGROUND

Cytokines secreted by immune cells and activated glia play central roles in both the pathogenesis of and protection from damage to the central nervous system (CNS) in multiple sclerosis (MS).

METHODS

We have used gene array analysis to identify the initial direct effects of cytokines on CNS glia by comparing changes in early gene expression in CNS glial cultures treated for 6 hours with cytokines typical of those secreted by Th1 and Th2 lymphocytes and monocyte/macrophages (M/M).

RESULTS

In two previous papers, we summarized effects of these cytokines on immune-related molecules, and on neural and glial related proteins, including neurotrophins, growth factors and structural proteins. In this paper, we present the effects of the cytokines on molecules involved in metabolism, signaling and regulatory mechanisms in CNS glia. Many of the changes in gene expression were similar to those seen in ischemic preconditioning and in early inflammatory lesions in experimental autoimmune encephalomyelitis (EAE), related to ion homeostasis, mitochondrial function, neurotransmission, vitamin D metabolism and a variety of transcription factors and signaling pathways. Among the most prominent changes, all three cytokine mixtures markedly downregulated the dopamine D3 receptor, while Th1 and Th2 cytokines downregulated neuropeptide Y receptor 5. An unexpected finding was the large number of changes related to lipid metabolism, including several suggesting a switch from diacylglycerol to phosphatidyl inositol mediated signaling pathways. Using QRT-PCR we validated the results for regulation of genes for iNOS, arginase and P glycoprotein/multi-drug resistance protein 1 (MDR1) seen at 6 hours with microarray.

CONCLUSION

Each of the three cytokine mixtures differentially regulated gene expression related to metabolism and signaling that may play roles in the pathogenesis of MS, most notably with regard to mitochondrial function and neurotransmitter signaling in glia.

摘要

背景

免疫细胞和活化神经胶质细胞分泌的细胞因子在多发性硬化症(MS)中枢神经系统(CNS)的发病机制和损伤保护中均发挥核心作用。

方法

我们通过比较中枢神经系统神经胶质细胞培养物中早期基因表达的变化,利用基因阵列分析来确定细胞因子对中枢神经系统神经胶质细胞的初始直接影响。这些细胞因子是典型的由Th1和Th2淋巴细胞以及单核细胞/巨噬细胞(M/M)分泌的。

结果

在之前的两篇论文中,我们总结了这些细胞因子对免疫相关分子以及神经和神经胶质相关蛋白的影响,这些蛋白包括神经营养因子、生长因子和结构蛋白。在本文中,我们展示了细胞因子对中枢神经系统神经胶质细胞中参与代谢、信号传导和调节机制的分子的影响。许多基因表达的变化与缺血预处理以及实验性自身免疫性脑脊髓炎(EAE)早期炎症病变中观察到的变化相似,这些变化与离子稳态、线粒体功能、神经传递、维生素D代谢以及多种转录因子和信号通路有关。在最显著的变化中,所有三种细胞因子混合物均显著下调多巴胺D3受体,而Th1和Th2细胞因子下调神经肽Y受体5。一个意外发现是大量与脂质代谢相关的变化,其中一些表明从二酰基甘油介导的信号通路转向磷脂酰肌醇介导的信号通路。我们使用定量逆转录聚合酶链反应(QRT-PCR)验证了在6小时时通过微阵列观察到的诱导型一氧化氮合酶(iNOS)、精氨酸酶和P糖蛋白/多药耐药蛋白1(MDR1)基因调控的结果。

结论

三种细胞因子混合物中的每一种都对与代谢和信号传导相关的基因表达进行了差异调节,这些调节可能在MS的发病机制中发挥作用,最显著的是在神经胶质细胞的线粒体功能和神经递质信号传导方面。

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