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Commonalities and Differences in the Substrates Underlying Consolidation of First- and Second-Order Conditioned Fear

机译:整合一阶和二阶条件性恐惧的基础之间的共性和差异

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摘要

Consolidation of newly formed fear memories requires a series of molecular events within the basolateral complex of the amygdala (BLA). Once consolidated, new information can be assimilated into these established associative networks to form higher-order associations. Much is known about the molecular events involved in consolidating newly acquired fear memories but little is known about the events that consolidate a secondary fear memory. Here, we show that, within the male rat BLA, DNA methylation and gene transcription are crucial for consolidating both the primary and secondary fear memories. We also show that consolidation of the primary, but not the secondary, fear memory requires de novo protein synthesis in the BLA. These findings show that consolidation of a fear memory and its updating to incorporate new information recruit distinct processes in the BLA, and suggest that DNA methylation in the BLA is fundamental to consolidation of both types of conditioned fear.>SIGNIFICANCE STATEMENT Our data provide clear evidence that a different set of mechanisms mediate consolidation of learning about cues that signal learned sources of danger (i.e., second-order conditioned fear) compared with those involved in consolidation of learning about cues that signal innate sources of danger (i.e., first-order conditioned fear). These findings carry important implications because second-order learning could underlie aberrant fear-related behaviors (e.g., in anxiety disorders) as a consequence of neutral secondary cues being integrated into associative fear networks established through first-order pairings, and thereby becoming potent conditioned reinforcers and predictors of fear. Therefore, our data suggest that targeting such second-order conditioned triggers of fear may require pharmacological intervention different to that typically used for first-order conditioned cues.
机译:新形成的恐惧记忆的巩固需要杏仁核(BLA)的基底外侧复合物中的一系列分子事件。一旦合并,新信息就可以被同化为这些已建立的关联网络,从而形成更高级别的关联。关于巩固新获得的恐惧记忆涉及的分子事件知之甚少,但有关巩固次要恐惧记忆的事件知之甚少。在这里,我们表明,在雄性大鼠BLA中,DNA甲基化和基因转录对于巩固主要和次要的恐惧记忆至关重要。我们还显示,巩固而不是次要的恐惧记忆需要在BLA中从头合成蛋白质。这些发现表明,恐惧记忆的合并及其更新以合并新信息会在BLA中招募不同的过程,并表明BLA中的DNA甲基化对于巩固两种条件性恐惧至关重要。>意义声明 >我们的数据提供了明确的证据,表明,与参与巩固表明先天危险源的线索的学习相比,采用不同的机制来协调对暗示已发现危险源的线索的学习(即,二级条件恐惧)(即一阶条件恐惧)。这些发现具有重要的意义,因为由于中性次要线索被整合到通过一阶配对建立的联想恐惧网络中,因此二阶学习可能成为异常的恐惧相关行为(例如,焦虑症)的基础,从而成为有条件的增强器和恐惧的预测因素。因此,我们的数据表明,针对此类二级条件性恐惧触发者可能需要不同于通常用于一级条件性暗示的药理干预。

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