首页> 外文期刊>The Journal of Neuroscience: The Official Journal of the Society for Neuroscience >Local protein synthesis mediates a rapid increase in dendritic elongation factor 1A after induction of late long-term potentiation.
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Local protein synthesis mediates a rapid increase in dendritic elongation factor 1A after induction of late long-term potentiation.

机译:诱导后期长期增强后,局部蛋白质合成介导了树突状伸长因子1A的快速增加。

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摘要

The maintenance of long-term potentiation (LTP) requires a brief period of accelerated protein synthesis soon after synaptic stimulation, suggesting that an early phase of enhanced translation contributes to stable LTP. The mechanism regulating protein synthesis and the location and identities of mRNAs translated are not well understood. Here, we show in acute brain slices that the induction of protein synthesis-dependent hippocampal LTP increases the expression of elongation factor 1A (eEF1A), the mRNA of which contains a 5' terminal oligopyrimidine tract. This effect is blocked by rapamycin, indicating that the increase in EF1A expression is mediated by the mammalian target of rapamycin (mTOR) pathway. We find that mRNA for eEF1A is present in pyramidal cell dendrites and that the LTP-associated increase in eEF1A expression was intact in dendrites that had been severed from their cell bodies before stimulation. eEF1A levels increased within 5 min after stimulation in a translation-dependent manner, and this effect remained stable for 3 h. These results suggest a mechanism whereby synaptic stimulation, by signaling through the mTOR pathway, produces an increase in dendritic translational capacity that contributes to LTP maintenance.
机译:维持长时程增强(LTP)需要在突触刺激后的短时间内加速蛋白质合成,这表明增强翻译的早期有助于稳定LTP。调节蛋白质合成的机制以及翻译的mRNA的位置和身份尚不十分清楚。在这里,我们在急性脑切片中显示,诱导依赖蛋白质合成的海马LTP可以增加延伸因子1A(eEF1A)的表达,其mRNA包含5'末端寡嘧啶束。雷帕霉素可阻断这种作用,表明EF1A表达的增加是由雷帕霉素(mTOR)途径的哺乳动物靶标介导的。我们发现,锥体细胞树突中存在eEF1A的mRNA,eEF1A表达的LTP相关增加在刺激之前已从其细胞体切断的树突中是完整的。 eEF1A水平在刺激后5分钟内以翻译依赖性方式增加,并且这种作用在3小时内保持稳定。这些结果提示了一种机制,通过该机制,突触刺激通过mTOR途径发出信号,导致树突状翻译能力增加,从而有助于LTP维持。

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