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miR-7b, a microRNA up-regulated in the hypothalamus after chronic hyperosmolar stimulation, inhibits Fos translation

机译:miR-7b是慢性高渗性刺激后下丘脑中上调的microRNA,可抑制Fos翻译

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摘要

The transcription factor activator protein 1 (AP-1) is formed through the dimerization of immediate–early genes Fos and Jun family members. Activator protein 1 is known as a pivotal regulator of major biological events such as cell proliferation, differentiation, organogenesis, memory formation, and apoptosis. During a search for microRNAs (miRNAs; small, endogenous, noncoding RNAs that repress gene expression of target mRNAs in animals posttranscriptionally) that are differentially expressed in the mouse paraventricular and supraoptic nuclei after 10 days of drinking 2% saline, one candidate microRNA that is relatively highly expressed, mmu-miR-7b (miR-7b), was studied further because sequence analysis suggested a likely interaction with the 3′ untranslated region of Fos mRNA. We show that miR-7b expression inhibits Fos translation in vitro and that it and its host gene are prominently expressed in the PVN and other brain areas, including the suprachiasmatic nucleus. No effect on Fos mRNA levels was observed. Normally, Fos is expressed at low to undetectable levels in cells, but it shows rapid induction and decay after acute stimuli. Various pathways have been identified through which Fos family proteins are degraded; our results indicate a significant additional mechanism by which Fos protein and activity may be regulated.
机译:转录因子激活蛋白1(AP-1)通过立即早期基因Fos和Jun家族成员的二聚作用形成。活化蛋白1被称为主要生物学事件的关键调节剂,例如细胞增殖,分化,器官发生,记忆形成和凋亡。在搜寻microRNA(miRNA;转录后抑制动物中目标mRNA的基因表达的小的内源性非编码RNA)在饮用2%盐水10天后在小鼠心室旁和视上核中差异表达的一种候选microRNA,即进一步研究了相对较高表达的mmu-miR-7b(miR-7b),因为序列分析表明可能与Fos mRNA的3'非翻译区相互作用。我们表明,miR-7b的表达在体外抑制Fos的翻译,并且它及其宿主基因在PVN和其他大脑区域(包括视交叉上核)中明显表达。没有观察到对Fos mRNA水平的影响。正常情况下,Fos在细胞中以低至无法检测的水平表达,但在急性刺激后显示迅速诱导和衰变。已经确定了降解Fos家族蛋白的各种途径。我们的结果表明,Fos蛋白和活性可能受到调控的重要机制。

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