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在情景性恐惧记忆的巩固和再巩固过程中,CA1 中涉及到数量和质量不同的细胞过程。

Quantitatively and qualitatively different cellular processes are engaged in CA1 during the consolidation and reconsolidation of contextual fear memory.

机构信息

Cardiff School of Biosciences, Cardiff University, Museum Avenue, Cardiff, United Kingdom.

出版信息

Hippocampus. 2012 Feb;22(2):149-71. doi: 10.1002/hipo.20879. Epub 2010 Nov 15.

DOI:10.1002/hipo.20879
PMID:21080409
Abstract

Whether the consolidation and reconsolidation long-term memory relies on qualitatively different molecular and cellular processes is controversial. Using a novel experimental strategy of combining intrahippocampal antisense oligodeoxynucleotides targeting BDNF or zif268 to the block consolidation or reconsolidation of contextual fear memory respectively, and Affymetrix microarray technology, we identified a comprehensive list of nonoverlapping candidate genes regulated in CA1 during the initial stages consolidation and reconsolidation. Using RT-qPCR in subsequent validation experiments, we estimated that over 80% of the candidates reflect gene transcripts truly regulated following the acquisition or retrieval of contextual fear memory. Statistical and over-representation bioinformatics analyses revealed that cellular processes and signaling mechanisms were differentially regulated during consolidation and reconsolidation, particularly those associated with pro-inflammatory cytokine signaling. This predicts that the two mnemonic processes are qualitatively as well as quantitatively distinct. This experimental strategy was further validated because the cytokine interleukin 1 (IL-1) was reciprocally regulated in CA1 after contextual fear conditioning and fear memory retrieval, and we showed for the first time that that IL-1 receptor mediated signaling in the hippocampus was necessary for reconsolidation.

摘要

巩固和再巩固长期记忆是否依赖于性质不同的分子和细胞过程是有争议的。我们采用了一种新的实验策略,即分别使用针对 BDNF 或 zif268 的海马内反义寡核苷酸来阻断情景恐惧记忆的巩固或再巩固,同时结合 Affymetrix 微阵列技术,我们确定了在 CA1 中在初始巩固和再巩固阶段受调控的非重叠候选基因的综合列表。在随后的验证实验中使用 RT-qPCR,我们估计超过 80%的候选基因反映了在获得或检索情景恐惧记忆后真正受调控的基因转录本。统计和过表达生物信息学分析表明,细胞过程和信号转导机制在巩固和再巩固期间受到不同的调控,特别是与促炎细胞因子信号有关的机制。这表明这两个记忆过程在质量和数量上都是不同的。由于细胞因子白细胞介素 1(IL-1)在情景恐惧条件作用和恐惧记忆检索后在 CA1 中呈反向调节,我们进一步验证了这种实验策略,并且我们首次表明,海马中的 IL-1 受体介导的信号转导对于再巩固是必要的。

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