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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免疫相关分子早期基因表达的不同影响。

Differential effects of Th1, monocyte/macrophage and Th2 cytokine mixtures on early gene expression for immune-related molecules by central nervous system mixed glial cell cultures.

作者信息

Lisak R P, Benjamins J A, Bealmear B, Yao B, Land S, Nedelkoska L, Skundric D

机构信息

Department of Neurology, Wayne State University, Detroit, MI 48201, USA.

出版信息

Mult Scler. 2006 Apr;12(2):149-68. doi: 10.1191/135248506ms1251oa.

Abstract

Cytokines secreted within the central nervous system (CNS) are important in the development of multiple sclerosis (MS) lesions. The balance between Th1, monocyte/macrophage (M/M) and Th2 cytokines in the CNS may be pivotal in determining the outcome of lesion development. We examined the effects of mixtures of cytokines on gene expression by CNS glial cells, as mixtures of cytokines are present in MS lesions, which in turn contain mixtures of glial cells. In this initial analysis by gene array, we examined changes at 6 hours to identify early changes in gene expression that represent primary responses to the cytokines. Rat glial cells were incubated with mixtures of Th1, M/M and Th2 cytokines for 6 hours and examined for changes in early gene expression employing microarray gene chip technology. A minimum of 814 genes were differentially regulated by one or more of the cytokine mixtures in comparison to controls, including changes in expression in a large number of genes for immune system-related proteins. Expression of the proteins for these genes likely influences development and inhibition of MS lesions as well as protective and regenerative processes. Analysing gene expression for the effects of various combinations of exogenous cytokines on glial cells in the absence of the confounding effects of inflammatory cells themselves should increase our understanding of cytokine-induced pathways in the CNS.

摘要

中枢神经系统(CNS)中分泌的细胞因子在多发性硬化症(MS)病变的发展中起重要作用。CNS中Th1、单核细胞/巨噬细胞(M/M)和Th2细胞因子之间的平衡可能对决定病变发展的结果至关重要。我们研究了细胞因子混合物对CNS神经胶质细胞基因表达的影响,因为MS病变中存在细胞因子混合物,而这些病变又包含神经胶质细胞混合物。在这项通过基因阵列进行的初步分析中,我们在6小时时检查变化,以识别代表对细胞因子的初级反应的基因表达早期变化。将大鼠神经胶质细胞与Th1、M/M和Th2细胞因子混合物孵育6小时,并采用微阵列基因芯片技术检查早期基因表达的变化。与对照组相比,至少814个基因受到一种或多种细胞因子混合物的差异调节,包括大量免疫系统相关蛋白质基因的表达变化。这些基因的蛋白质表达可能影响MS病变的发展和抑制以及保护和再生过程。在没有炎症细胞自身混杂效应的情况下,分析外源性细胞因子各种组合对神经胶质细胞的基因表达影响,应该会增加我们对CNS中细胞因子诱导途径的理解。

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