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斑马鱼胚胎固有免疫反应中 Traf6 功能的转录组分析。

Transcriptome analysis of Traf6 function in the innate immune response of zebrafish embryos.

机构信息

Institute of Biology, Leiden University, Einsteinweg 55, 2333 CC Leiden, The Netherlands.

出版信息

Mol Immunol. 2010 Nov-Dec;48(1-3):179-90. doi: 10.1016/j.molimm.2010.08.011. Epub 2010 Sep 18.

Abstract

TRAF6 is a key player at the cross-roads of development and immunity. The analysis of its in vivo molecular function is a great challenge since severe developmental defects and early lethality caused by Traf6 deficiency in knock-out mice interfere with analyses of the immune response. In this study we have used a new strategy to analyze the function of Traf6 in a zebrafish-Salmonella infectious disease model. In our approach the effect of a Traf6 translation-blocking morpholino was titrated down to avoid developmental defects and the response to infection under these conditions was studied using the combination of microarray analysis and whole transcriptome deep sequencing. Transcriptome profiling of the traf6 knock-down allowed the identification of a gene set whose responsiveness during infection is highly dependent on Traf6. Expression trend analysis based on the resulting datasets identified nine clusters of genes with characteristic transcription response profiles, demonstrating Traf6 has a dynamic role as a positive and negative regulator. Among the Traf6-dependent genes was a large set of well known anti-microbial and inflammatory genes. Additionally, we identified several genes which were not previously linked to a response to microbial infection, such as the fertility hormone gene gnrh2 and the DNA-damage regulated autophagy modulator 1 gene dram1. With the use of the zebrafish embryo model we have now analyzed the in vivo function of Traf6 in the innate immune response without interference of adaptive immunity.

摘要

TRAF6 是发育和免疫交汇点的关键参与者。由于 TRAF6 敲除小鼠中严重的发育缺陷和早期致死性,其体内分子功能的分析是一个巨大的挑战,这干扰了对免疫反应的分析。在这项研究中,我们使用了一种新策略来分析 TRAF6 在斑马鱼-沙门氏菌感染疾病模型中的功能。在我们的方法中,我们将 TRAF6 翻译阻断型 morpholino 的作用滴定降低,以避免发育缺陷,并在这些条件下研究感染的反应,使用微阵列分析和全转录组深度测序相结合的方法。 traf6 敲低的转录组分析允许鉴定出一组基因,其在感染过程中的反应高度依赖于 TRAF6。基于所得数据集的表达趋势分析确定了具有特征转录反应谱的 9 个基因簇,表明 TRAF6 作为正调节剂和负调节剂具有动态作用。在依赖 TRAF6 的基因中,有一大组众所周知的抗微生物和炎症基因。此外,我们还鉴定了几个以前与微生物感染反应无关的基因,例如生育激素基因 gnrh2 和 DNA 损伤调节自噬调节剂 1 基因 dram1。使用斑马鱼胚胎模型,我们现在在没有适应性免疫干扰的情况下分析了 TRAF6 在先天免疫反应中的体内功能。

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