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NF-κB抑制因子缺陷小鼠的天然免疫反应

Innate immune responses in NF-kappaB-repressing factor-deficient mice.

作者信息

Froese Natali, Schwarzer Michael, Niedick Ina, Frischmann Ursula, Köster Mario, Kröger Andrea, Mueller Peter P, Nourbakhsh Mahtab, Pasche Bastian, Reimann Jörg, Staeheli Peter, Hauser Hansjörg

机构信息

Department of Gene Regulation and Differentiation, German Research Centre for Biotechnolofy, Braunschweig, Germany.

出版信息

Mol Cell Biol. 2006 Jan;26(1):293-302. doi: 10.1128/MCB.26.1.293-302.2006.

Abstract

NF-kappaB-repressing factor (NRF) is a transcriptional silencer protein that specifically counteracts the basal activity of several NF-kappaB-dependent promoters by direct binding to specific neighboring DNA sequences. In cell culture experiments, the reduction of NRF mRNA leads to a derepression of beta interferon, interleukin-8, and inducible nitric oxide synthase transcription. The X chromosome-located single-copy NRF gene is ubiquitously expressed and encodes a protein of 690 amino acids. The N-terminal part contains a nuclear localization signal, the DNA-binding domain, and the NF-kappaB-repressing domain, while the C-terminal part is responsible for double-stranded RNA binding and nucleolar localization. To study the function of NRF in a systemic context, transgenic mice lacking the NRF gene were created. Against predictions from in vitro experiments, mice with a deletion of the NRF gene are viable and have a phenotype that is indistinguishable from wild-type mice, even after challenge with different pathogens. The data hint towards an unexpected functional redundancy of NRF.

摘要

核因子κB抑制因子(NRF)是一种转录沉默蛋白,它通过直接结合特定的相邻DNA序列,特异性地对抗几种依赖核因子κB的启动子的基础活性。在细胞培养实验中,NRF mRNA的减少导致β干扰素、白细胞介素-8和诱导型一氧化氮合酶转录的去抑制。位于X染色体上的单拷贝NRF基因在全身广泛表达,编码一个由690个氨基酸组成的蛋白质。N端部分包含一个核定位信号、DNA结合结构域和核因子κB抑制结构域,而C端部分负责双链RNA结合和核仁定位。为了在整体背景下研究NRF的功能,构建了缺失NRF基因的转基因小鼠。与体外实验的预测相反,缺失NRF基因的小鼠是存活的,并且即使在受到不同病原体攻击后,其表型与野生型小鼠也没有区别。这些数据表明NRF存在意想不到的功能冗余。

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