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隔离饲养引起的情境性恐惧学习缺陷不需要 CRF(2)受体。

Isolation rearing-induced deficits in contextual fear learning do not require CRF(2) receptors.

机构信息

Department of Psychiatry, University of California, San Diego, MC0804, La Jolla, CA 92093-0804, USA.

出版信息

Behav Brain Res. 2010 May 1;209(1):80-4. doi: 10.1016/j.bbr.2010.01.018. Epub 2010 Jan 25.

Abstract

Post-weaning social isolation of rodents is used to model developmental stressors linked to neuropsychiatric disorders including schizophrenia as well as anxiety and mood disorders. Isolation rearing produces alterations in emotional memory and hippocampal neuropathology. Corticotropin releasing factor (CRF) signaling has recently been shown to be involved in behavioral effects of isolation rearing. Activation of the CRF(2) receptor is linked to stress-induced alterations in fear learning and may also be involved in long-term adaptation to stress. Here we tested the hypothesis that CRF(2) contributes to isolation rearing effects on emotional memory. At weaning, mice were housed either in groups of three or individually in standard mouse cages. In adulthood, isolation-reared mice exhibited significant reductions in context-specific, but not cue-specific, freezing. Isolation-reared mice exhibited no significant changes in locomotor exploration during brief exposure to a novel environment, suggesting that the reduced freezing in response to context cues was not due to activity confounds. Isolation rearing also disrupted context fear memory in mice with a CRF(2) gene null mutation, indicating that the CRF(2) receptor is not required for isolation effects on fear memory. Thus, isolation rearing disrupts hippocampal-dependent fear learning as indicated by consistent reductions in context-conditioned freezing in two separate cohorts of mice, and these effects are via a CRF(2)-independent mechanism. These findings may be clinically relevant because they suggest that isolation rearing in mice may be a useful model of developmental perturbations linked to disruptions in emotional memory in a variety of neuropsychiatric disorders.

摘要

啮齿动物的断乳后社交隔离被用于模拟与神经精神疾病相关的发育应激源,包括精神分裂症以及焦虑和情绪障碍。隔离饲养会导致情绪记忆和海马神经病理学的改变。最近的研究表明,促肾上腺皮质素释放因子(CRF)信号参与了隔离饲养的行为效应。CRF(2)受体的激活与应激诱导的恐惧学习改变有关,也可能与应激的长期适应有关。在这里,我们测试了这样一个假设,即 CRF(2)有助于解释隔离饲养对情绪记忆的影响。在断奶时,将小鼠饲养在三组或标准小鼠笼中。在成年期,隔离饲养的小鼠在特定环境但非特定线索的冻结中表现出显著减少。隔离饲养的小鼠在短暂暴露于新环境中的运动探索中没有表现出明显的变化,这表明对环境线索的冻结减少不是由于活动混淆。在 CRF(2)基因缺失突变的小鼠中,隔离饲养也破坏了情景恐惧记忆,这表明 CRF(2)受体不是隔离对恐惧记忆影响所必需的。因此,隔离饲养破坏了海马依赖的恐惧学习,这表现在两个独立的小鼠队列中,环境条件性冻结持续减少,而这些影响是通过 CRF(2)独立的机制。这些发现可能具有临床相关性,因为它们表明,在小鼠中进行隔离饲养可能是一种有用的模型,可以模拟与各种神经精神疾病中的情绪记忆障碍相关的发育干扰。

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