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首页> 外文期刊>Hippocampus >Distinctive features of Egr transcription factor regulation and DNA binding activity in CA1 of the hippocampus in synaptic plasticity and consolidation and reconsolidation of fear memory
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Distinctive features of Egr transcription factor regulation and DNA binding activity in CA1 of the hippocampus in synaptic plasticity and consolidation and reconsolidation of fear memory

机译:海马CA1区Egr转录因子调控和DNA结合活性在突触可塑性和恐惧记忆的巩固与巩固方面的显着特征

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摘要

Activity-dependent regulation of Egr1/Zif268, a transcription factor (TF) of the Egr family, is essential for stabilization of dentate gyrus synaptic plasticity and consolidation and reconsolidation of several forms of memory. The gene can be rapidly induced in selective brain circuits after certain types of learning or after recall. Here, we focused on area CA1 and examined regulation of Egr1, Egr2, and Egr3 mRNA and protein, and their DNA binding activity to the Egr response element (ERE) at different times after LTP in vivo and after learning and recall of a fear memory. We found LTP in CA1 leads to rapid induction of the three Egrs, however only Egr1 protein was overexpressed without a co-ordinated change in binding activity, indicating a fundamental difference between CA1 and dentate gyrus LTP. Our investigations in fear memory reveal that both learning and retrieval lead to an increase in binding of constitutively expressed Egr1 and Egr3 to the ERE, but not Egr2. Memory recall was also associated with increased Egr1 protein translation. The nature and temporal dynamics of these changes and tests for interactions between TFs suggest that in addition to ERE-mediated transcription, Egr1 in CA1 may interact with the TF c-Fos to regulate genes via other DNA response elements.
机译:Egr1 / Zif268,Egr家族的一个转录因子(TF)的活动依赖调节,对于稳定齿状回突触可塑性以及巩固和巩固几种记忆形式至关重要。在某些类型的学习或回忆后,可以在选择性的脑回路中快速诱导该基因。在这里,我们专注于区域CA1,并检查了体内LTP后以及学习和回忆恐惧记忆后不同时间的Egr1,Egr2和Egr3 mRNA和蛋白质的调节及其与Egr反应元件(ERE)的DNA结合活性。 。我们发现CA1中的LTP导致了三个Egrs的快速诱导,但是只有Egr1蛋白过表达而没有结合活性的协调变化,表明CA1和齿状回LTP之间存在根本差异。我们对恐惧记忆的研究表明,学习和检索都导致组成型表达的Egr1和Egr3与ERE(而非Egr2)的结合增加。记忆记忆还与Egr1蛋白翻译增加有关。这些变化的性质和时间动态以及对TF之间相互作用的测试表明,除了ERE介导的转录外,CA1中的Egr1可能与TF c-Fos相互作用,以通过其他DNA响应元件调节基因。

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