首页> 美国卫生研究院文献>The Journal of Neuroscience >The RNA-Binding Protein HuD Binds Acetylcholinesterase mRNA in Neurons and Regulates its Expression after Axotomy
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The RNA-Binding Protein HuD Binds Acetylcholinesterase mRNA in Neurons and Regulates its Expression after Axotomy

机译:RNA结合蛋白HuD结合神经元中的乙酰胆碱酯酶mRNA并调节其在轴突切开后的表达

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摘要

After axotomy, expression of acetylcholinesterase (AChE) is greatly reduced in the superior cervical ganglion (SCG); however, the molecular events involved in this response remain unknown. Here, we first examined AChE mRNA levels in the brain of transgenic mice that overexpress human HuD. Both in situ hybridization and reverse transcription-PCR demonstrated that AChE transcript levels were increased by more than twofold in the hippocampus of HuD transgenic mice. Additionally, direct interaction between the HuD transgene product and AChE mRNA was observed. Next, we examined the role of HuD in regulating AChE expression in intact and axotomized rat SCG neurons. After axotomy of the adult rat SCG neurons, AChE transcript levels decreased by 50 and 85% by the first and fourth day, respectively. In vitro mRNA decay assays indicated that the decrease in AChE mRNA levels resulted from changes in the stability of presynthesized transcripts. A combination of approaches performed using the region that directly encompasses an adenylate and uridylate (AU)-rich element within the AChE 3′-untranslated region demonstrated a decrease in RNA–protein complexes in response to axotomy of the SCG and, specifically, a decrease in HuD binding. After axotomy, HuD transcript and protein levels also decreased. Using a herpes simplex virus construct containing the human HuD sequence to infect SCG neurons in vivo, we found that AChE and GAP-43 mRNA levels were maintained in the SCG after axotomy. Together, the results of this study demonstrate that AChE expression in neurons of the rat SCG is regulated via post-transcriptional mechanisms that involve the AU-rich element and HuD.
机译:切开后,上颈神经节(SCG)中的乙酰胆碱酯酶(AChE)的表达大大降低。然而,该反应涉及的分子事件仍然未知。在这里,我们首先检查了过表达人类HuD的转基因小鼠大脑中的AChE mRNA水平。原位杂交和逆转录-PCR均表明,HuD转基因小鼠海马中的AChE转录水平增加了两倍以上。另外,观察到HuD转基因产物和AChE mRNA之间的直接相互作用。接下来,我们检查了HuD在调节完整的和切开的大鼠SCG神经元中AChE表达中的作用。在成年大鼠SCG神经元轴向切开后,第一天和第四天AChE转录水平分别下降了50%和85%。体外mRNA衰减分析表明,AChE mRNA水平的降低是由于预先合成的转录本的稳定性发生了变化。使用直接包含AChE 3'非翻译区域内富含腺苷酸和尿苷酸(AU)元素的区域进行的方法组合表明,响应SCG的轴突切开,RNA-蛋白质复合物减少,特别是减少在HuD绑定中。轴切后,HuD转录本和蛋白质水平也下降。使用包含人类HuD序列的单纯疱疹病毒构建体在体内感染SCG神经元,我们发现轴切术后SCG中的AChE和GAP-43 mRNA水平得以维持。总之,这项研究的结果表明,大鼠SCG神经元中AChE的表达受转录后机制的调控,该机制涉及富含AU的元素和HuD。

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