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The Regulation of Cytokine Networks in Hippocampal CA1 Differentiates Extinction from Those Required for the Maintenance of Contextual Fear Memory after Recall

机译:海马CA1细胞因子网络的调节使灭绝与回忆后维持上下文恐惧记忆所需的灭绝区别开来

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We investigated the distinctiveness of gene regulatory networks in CA1 associated with the extinction of contextual fear memory (CFM) after recall using Affymetrix GeneChip Rat Genome 230 2.0 Arrays. These data were compared to previously published retrieval and reconsolidation-attributed, and consolidation datasets. A stringent dual normalization and pareto-scaled orthogonal partial least-square discriminant multivariate analysis together with a jack-knifing-based cross-validation approach was used on all datasets to reduce false positives. Consolidation, retrieval and extinction were correlated with distinct patterns of gene expression 2 hours later. Extinction-related gene expression was most distinct from the profile accompanying consolidation. A highly specific feature was the discrete regulation of neuroimmunological gene expression associated with retrieval and extinction. Immunity-associated genes of the tyrosine kinase receptor TGF beta and PDGF, and TNF families' characterized extinction. Cytokines and proinflammatory interleukins of the IL-1 and IL-6 families were enriched with the no-extinction retrieval condition. We used comparative genomics to predict transcription factor binding sites in proximal promoter regions of the retrieval-regulated genes. Retrieval that does not lead to extinction was associated with NF-kappa B-mediated gene expression. We confirmed differential NF-kappa Bp65 expression, and activity in all of a representative sample of our candidate genes in the no-extinction condition. The differential regulation of cytokine networks after the acquisition and retrieval of CFM identifies the important contribution that neuroimmune signalling plays in normal hippocampal function. Further, targeting cytokine signalling upon retrieval offers a therapeutic strategy to promote extinction mechanisms in human disorders characterised by dysregulation of associative memory.
机译:在使用Affymetrix GeneChip Rat Genome 230 2.0阵列召回后,我们调查了与背景恐惧记忆(CFM)灭绝相关的CA1基因调控网络的独特性。将这些数据与以前发布的检索和重新合并属性以及合并数据集进行比较。对所有数据集使用严格的对偶归一化和按比例缩放的正交偏最小二乘判别多元分析以及基于千斤顶刀的交叉验证方法,以减少误报。 2小时后,巩固,恢复和灭绝与基因表达的不同模式相关。灭绝相关的基因表达与巩固相关的特征最不同。一个高度特定的特征是与恢复和灭绝有关的神经免疫基因表达的离散调节。酪氨酸激酶受体TGFβ和PDGF的免疫相关基因以及TNF家族的灭绝特征。 IL-1和IL-6家族的细胞因子和促炎性白介素富含无灭绝恢复条件。我们使用比较基因组学来预测检索调控基因的近端启动子区域中的转录因子结合位点。不会导致灭绝的检索与NF-κB介导的基因表达有关。我们在无消光条件下证实了差异表达的NF-κBp65表达和所有候选基因代表性样品的活性。 CFM的获取和检索后,细胞因子网络的差异调节确定了神经免疫信号在正常海马功能中的重要作用。此外,在恢复时靶向细胞因子信号传导提供了一种治疗策略,以促进以关联记忆失调为特征的人类疾病的灭绝机制。

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