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体内电穿孔诱导长时程增强诱导快速基因表达网络。

Rapidly induced gene networks following induction of long-term potentiation at perforant path synapses in vivo.

机构信息

Department of Anatomy and Structural Biology, Otago School of Medical Sciences, P.O. Box 913, Dunedin, New Zealand.

出版信息

Hippocampus. 2011 May;21(5):541-53. doi: 10.1002/hipo.20770.

DOI:10.1002/hipo.20770
PMID:20108223
Abstract

The canonical view of the maintenance of long-term potentiation (LTP), a widely accepted experimental model for memory processes, is that new gene transcription contributes to its consolidation; however, the gene networks involved are unknown. To address this issue, we have used high-density Rat 230.2 Affymetrix arrays to establish a set of genes induced 20-min post-LTP, and using Ingenuity Pathway network analysis tools we have investigated how these early responding genes are interrelated. This analysis identified LTP-induced regulatory networks in which the transcription factors (TFs) nuclear factor-KB and serum response factor, which, to date, have not been widely recognized as coordinating the early gene response, play a key role alongside the more well-known TFs cyclic AMP response element-binding protein, and early growth response 1. Analysis of gene-regulatory promoter sites and chromosomal locations of the genes within the dataset reinforced the importance of these molecules in the early gene response and predicted that the coordinated action might arise from gene clustering on particular chromosomes. We have also identified a transcription-based response that affects mitogen-activated protein kinase signaling pathways and protein synthesis during the stabilization of the LTP response. Furthermore, evidence from biological function, networks, and regulatory analyses showed convergence on genes related to development, proliferation, and neurogenesis, suggesting that these functions are regulated early following LTP induction. This raises the interesting possibility that LTP-related gene expression plays a role in both synaptic reorganization and neurogenesis.

摘要

长时程增强(LTP)的维持被认为是记忆过程的一个广泛接受的实验模型,其典型观点是新的基因转录有助于其巩固;然而,涉及的基因网络尚不清楚。为了解决这个问题,我们使用高密度 Rat 230.2 Affymetrix 芯片来确定一组在 LTP 后 20 分钟诱导的基因,并使用 Ingenuity Pathway 网络分析工具来研究这些早期反应基因是如何相互关联的。该分析确定了 LTP 诱导的调节网络,其中转录因子(TFs)核因子-KB 和血清反应因子,迄今为止,尚未被广泛认为是协调早期基因反应的因子,与更知名的 TFs 环腺苷酸反应元件结合蛋白和早期生长反应 1 一起发挥关键作用。对数据集内基因的基因调节启动子位点和染色体位置的分析增强了这些分子在早期基因反应中的重要性,并预测协调作用可能来自于特定染色体上基因的聚类。我们还确定了一种基于转录的反应,该反应在 LTP 反应稳定期间影响丝裂原激活蛋白激酶信号通路和蛋白质合成。此外,生物学功能、网络和调节分析的证据都集中在与发育、增殖和神经发生相关的基因上,这表明这些功能在 LTP 诱导后早期受到调节。这提出了一个有趣的可能性,即与 LTP 相关的基因表达可能在突触重组和神经发生中都发挥作用。

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