Weiss G, Goossen B, Doppler W, Fuchs D, Pantopoulos K, Werner-Felmayer G, Wachter H, Hentze M W
Gene Expression Programme, European Molecular Biology Laboratory, Heidelberg, Germany.
EMBO J. 1993 Sep;12(9):3651-7. doi: 10.1002/j.1460-2075.1993.tb06039.x.
Nitric oxide (NO) produced from L-arginine by NO synthases (NOS) is a transmitter known to be involved in diverse biological processes, including immunomodulation, neurotransmission and blood vessel dilatation. We describe a novel role of NO as a signaling molecule in post-transcriptional gene regulation. We demonstrate that induction of NOS in macrophage and non-macrophage cell lines activates RNA binding by iron regulatory factor (IRFs), the central trans regulator of mRNAs involved in cellular iron metabolism. NO-induced binding of IRF to iron-responsive elements (IRE) specifically represses the translation of transfected IRE-containing indicator mRNAs as well as the biosynthesis of the cellular iron storage protein ferritin. These findings define a new biological function of NO and identify a regulatory connection between the NO/NOS pathway and cellular iron metabolism.
一氧化氮合酶(NOS)将L-精氨酸转化生成的一氧化氮(NO)是一种已知参与多种生物学过程的递质,这些过程包括免疫调节、神经传递和血管舒张。我们描述了NO作为一种信号分子在转录后基因调控中的新作用。我们证明,在巨噬细胞和非巨噬细胞系中诱导NOS可激活铁调节因子(IRF)的RNA结合,IRF是参与细胞铁代谢的mRNA的核心反式调节因子。NO诱导IRF与铁反应元件(IRE)结合,特异性抑制转染的含IRE指示mRNA的翻译以及细胞铁储存蛋白铁蛋白的生物合成。这些发现定义了NO的一种新生物学功能,并确定了NO/NOS途径与细胞铁代谢之间的调节联系。
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