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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Glutamate receptor activation regulates mRNA at both transcriptional and posttranscriptional levels.
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Glutamate receptor activation regulates mRNA at both transcriptional and posttranscriptional levels.

机译:谷氨酸受体激活在转录和转录后水平上调节mRNA。

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Previous studies from this laboratory have demonstrated that extracellular calcium entry through the NMDA subtype of glutamate receptors in hippocampal neurons selectively down-regulated ligatin gene expression in a rapid and long-lasting manner. Here we investigated the molecular mechanism that underlies this phenomenon. We demonstrate that glutamate receptor activation transiently increased the transcriptional activity of the ligatin gene and simultaneously shortened the half-life of its message. Using nuclear run-on assays and northern analyses of total RNA from alpha-amanitin-treated cells, we measured the effects of glutamate on the transcriptional activity and mRNA stability of the ligatin gene. The transcriptional activity of ligatin was found to be transiently increased (1.4-fold) 20 min after the addition of glutamate, with a return to basal levels by 60 min. Thus, the glutamate-dependent decrease in ligatin message could not be explained by a decline in its synthesis. Instead, concurrent withtranscriptional up-regulation, glutamate shortened the half-life of the ligatin message from 10 h to 58 min, leading to a net decrease (0.7-fold) in its steady-state levels by 60 min. This posttranscriptional destablization of ligatin mRNA was mimicked by the translation inhibitor, cycloheximide, but not by puromycin. This finding indicated that the stability of ligatin mRNA was translation independent and distinguished this posttranscriptional regulatory mechanism from those previously described. Moreover, using in situ hybridization and confocal microscopy, we showed that control of message stability occurred both in the cell body and in the dendritic regions distant from the nucleus.(ABSTRACT TRUNCATED AT 250 WORDS)
机译:该实验室的先前研究表明,海马神经元中通过谷氨酸受体NMDA亚型的细胞外钙进入以快速和持久的方式选择性下调了ligatin基因的表达。在这里,我们研究了这种现象的分子机制。我们证明,谷氨酸受体激活暂时增加了木质素基因的转录活性,同时缩短了其信息的半衰期。使用核试穿法和经alpha-amanitin处理的细胞的总RNA的Northern分析,我们测量了谷氨酸对木质素基因转录活性和mRNA稳定性的影响。发现添加谷氨酸后20分钟,配体的转录活性瞬时增加(1.4倍),并在60分钟后恢复到基础水平。因此,不能通过合成的下降来解释谷氨酸依赖的木质素信息的下降。相反,在转录上调的同时,谷氨酸将木质素信息的半衰期从10小时缩短至58分钟,导致稳态水平净降低60分钟(0.7倍)。连接蛋白mRNA的这种转录后去稳定由翻译抑制剂环己酰亚胺模拟,但不由嘌呤霉素模拟。这一发现表明,连接素mRNA的稳定性与翻译无关,并将这种转录后调控机制与先前所述的机制区分开。此外,使用原位杂交和共聚焦显微镜,我们发现对信息稳定性的控制发生在细胞体和远离核的树突区域中。(摘要截断为250个字)

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