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暴露于化学接触性变应原硫酸镍的CD34⁺祖细胞来源的树突状细胞中的基因表达特征

Gene expression signatures in CD34+-progenitor-derived dendritic cells exposed to the chemical contact allergen nickel sulfate.

作者信息

Schoeters Elke, Nuijten Jean-Marie, Van Den Heuvel Rosette L, Nelissen Inge, Witters Hilda, Schoeters Greet E R, Van Tendeloo Vigor F I, Berneman Zwi N, Verheyen Geert R

机构信息

Centre of Expertise in Environmental Toxicology, Flemish Institute for Technological Research (VITO), Boeretang 200, 2400 Mol, Belgium.

出版信息

Toxicol Appl Pharmacol. 2006 Oct 1;216(1):131-49. doi: 10.1016/j.taap.2006.04.009. Epub 2006 Jun 14.

Abstract

The detection of the sensitizing potential of chemicals is of great importance to industry. A promising in vitro alternative to the currently applied animal assays for sensitization testing makes use of dendritic cells (DCs) that have the capability to process and present antigens to naive T cells and induce their proliferation. Here, we studied changes in gene expression profiles after exposing DCs to the contact allergen nickel sulfate. CD34+-progenitor-derived DCs, initiated from 3 different donors, were exposed to 60 microM nickel sulfate, during 0.5, 1, 3, 6, 12 and 24 h. cDNA microarrays were used to assess the transcriptional activity of about 11,000 genes. Significant changes in the expression of 283 genes were observed; 178 genes were up-regulated and 93 down-regulated. These genes were involved in metabolism, cell structure, immune response, transcription, signal transduction, transport, and apoptosis. No functional information was found for 74 genes. Real-time RT-PCR was used to confirm the microarray results of 12 genes. In addition, 3 DC maturation markers not present on the microarrays (DEC205, DC LAMP and CCR7) were analyzed using real-time RT-PCR and found to be up-regulated at several time points. Our data indicate that a broad range of biological processes is influenced by nickel. Some processes are clearly linked to the immune response and DC maturation, others may indicate a toxic effect of nickel.

摘要

化学物质致敏潜力的检测对工业而言至关重要。一种有望替代当前用于致敏测试的动物试验的体外方法利用了树突状细胞(DCs),这种细胞能够处理抗原并将其呈递给未致敏的T细胞,进而诱导其增殖。在此,我们研究了将DCs暴露于接触性变应原硫酸镍后基因表达谱的变化。从3名不同供体分离出的CD34⁺祖细胞来源的DCs,在0.5、1、3、6、12和24小时期间暴露于60微摩尔的硫酸镍。利用cDNA微阵列评估约11,000个基因的转录活性。观察到283个基因的表达有显著变化;178个基因上调,93个基因下调。这些基因涉及代谢、细胞结构、免疫反应、转录、信号转导、转运和凋亡。74个基因未发现功能信息。采用实时RT-PCR对12个基因的微阵列结果进行了验证。此外,利用实时RT-PCR分析了微阵列上未出现的3个DC成熟标志物(DEC205、DC LAMP和CCR7),发现它们在多个时间点上调。我们的数据表明,镍会影响广泛的生物学过程。一些过程与免疫反应和DC成熟明显相关,其他过程可能表明镍具有毒性作用。

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