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学习和记忆的神经相关物会被早期生活压力改变。

Neural correlates of learning and memory are altered by early-life stress.

机构信息

Brain Plasticity Group, SILS-CNS, University of Amsterdam, Amsterdam, The Netherlands.

Brain Plasticity Group, SILS-CNS, University of Amsterdam, Amsterdam, The Netherlands.

出版信息

Neurobiol Learn Mem. 2024 Sep;213:107952. doi: 10.1016/j.nlm.2024.107952. Epub 2024 Jun 19.

DOI:10.1016/j.nlm.2024.107952
PMID:38906243
Abstract

The ability to learn and remember, which is fundamental for behavioral adaptation, is susceptible to stressful experiences during the early postnatal period, such as abnormal levels of maternal care. The exact mechanisms underlying these effects still remain elusive. This study examined whether early life stress (ELS) alters memory and brain activation patterns in male mice. Therefore, we examined the expression of the immediate early genes (IEGs) c-Fos and Arc in the dentate gyrus (DG) and basolateral amygdala (BLA) after training and memory retrieval in a fear conditioning task. Furthermore, we examined the potential of RU38486 (RU486), a glucocorticoid receptor antagonist, to mitigate ELS-induced memory deficits by blocking stress signalling during adolescence. Arc::dVenus reporter mice, which allow investigating experience-dependent expression of the immediate early gene Arc also at more remote time points, were exposed to ELS by housing dams and offspring with limited bedding and nesting material (LBN) between postnatal days (PND) 2-9 and trained in a fear conditioning task at adult age. We found that ELS reduced both fear acquisition and contextual memory retrieval. RU486 did not prevent these effects. ELS reduced the number of Arc::dVenus cells in DG and BLA after training, while the number of c-Fos cells were left unaffected. After memory retrieval, ELS decreased c-Fos cells in the ventral DG and BLA. ELS also altered the colocalization of c-Fos cells with Arc::dVenus cells in the ventral DG, possibly indicating impaired engram allocation in the ventral DG after memory retrieval. In conclusion, this study shows that ELS alters neuronal activation patterns after fear acquisition and retrieval, which may provide mechanistic insights into enduring impact of ELS on the processing of fear memories, possibly via changes in cell (co-) activation and engram cell allocation.

摘要

学习和记忆能力是行为适应的基础,易受产后早期应激体验的影响,如母性照顾异常。这些影响的确切机制仍不清楚。本研究旨在探讨早期生活应激(ELS)是否改变雄性小鼠的记忆和大脑激活模式。因此,我们在恐惧条件反射任务中训练和记忆检索后,检测了即刻早期基因(IEG)c-Fos 和 Arc 在齿状回(DG)和外侧杏仁核(BLA)中的表达。此外,我们还研究了 RU38486(RU486),一种糖皮质激素受体拮抗剂,通过阻断青春期应激信号,是否有能力减轻 ELS 引起的记忆缺陷。Arc::dVenus 报告小鼠允许在更遥远的时间点研究即时早期基因 Arc 的经验依赖性表达,在产后第 2-9 天通过限制垫料和筑巢材料(LBN)将母鼠和幼鼠关在笼子里,使其暴露于 ELS 中,并在成年时进行恐惧条件反射任务训练。我们发现 ELS 降低了恐惧获得和情境记忆检索。RU486 不能防止这些影响。ELS 减少了训练后 DG 和 BLA 中的 Arc::dVenus 细胞数量,而 c-Fos 细胞数量不受影响。记忆检索后,ELS 减少了 DG 和 BLA 腹侧的 c-Fos 细胞。ELS 还改变了 DG 腹侧 c-Fos 细胞与 Arc::dVenus 细胞的共定位,这可能表明记忆检索后 DG 腹侧的印迹分配受损。总之,这项研究表明,ELS 改变了恐惧获得和检索后的神经元激活模式,这可能为 ELS 对恐惧记忆处理的持久影响提供机制上的见解,可能是通过改变细胞(共)激活和印迹细胞分配。

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