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创伤应激时雌激素受体调控对创伤应激诱导的情绪记忆改变的作用。

The role of estrogen receptor manipulation during traumatic stress on changes in emotional memory induced by traumatic stress.

机构信息

Department of Psychological and Brain Sciences, University of Delaware, Newark, DE, USA.

出版信息

Psychopharmacology (Berl). 2023 May;240(5):1049-1061. doi: 10.1007/s00213-023-06342-6. Epub 2023 Mar 6.

Abstract

RATIONALE

Traumatic stress leads to persistent fear, which is a core feature of post-traumatic stress disorder (PTSD). Women are more likely than men to develop PTSD after trauma exposure, which suggests women are differentially sensitive to traumatic stress. However, it is unclear how this differential sensitivity manifests. Cyclical changes in vascular estrogen release could be a contributing factor where levels of vascular estrogens (and activation of estrogen receptors) at the time of traumatic stress alter the impact of traumatic stress.

METHODS

To examine this, we manipulated estrogen receptors at the time of stress and observed the effect this had on fear and extinction memory (within the single prolonged stress (SPS) paradigm) in female rats. In all experiments, freezing and darting were used to measure fear and extinction memory.

RESULTS

In Experiment 1, SPS enhanced freezing during extinction testing, and this effect was blocked by nuclear estrogen receptor antagonism prior to SPS. In Experiment 2, SPS decreased conditioned freezing during the acquisition and testing of extinction. Administration of 17β-estradiol altered freezing in control and SPS animals during the acquisition of extinction, but this treatment had no effect on freezing during the testing of extinction memory. In all experiments, darting was only observed to footshock onset during fear conditioning.

CONCLUSION

The results suggest multiple behaviors (or different behavioral paradigms) are needed to characterize the nature of traumatic stress effects on emotional memory in female rats and that nuclear estrogen receptor antagonism prior to SPS blocks SPS effects on emotional memory in female rats.

摘要

理由

创伤后应激会导致持续的恐惧,这是创伤后应激障碍(PTSD)的核心特征。女性在创伤后比男性更容易患上 PTSD,这表明女性对创伤后应激的敏感性不同。然而,这种差异的敏感性如何表现尚不清楚。血管雌激素释放的周期性变化可能是一个促成因素,即在创伤应激时血管雌激素的水平(和雌激素受体的激活)改变了创伤应激的影响。

方法

为了研究这一点,我们在应激时操纵雌激素受体,并观察这对雌性大鼠的恐惧和消退记忆(在单一延长应激(SPS)范式内)的影响。在所有实验中,使用冻结和 darting 来测量恐惧和消退记忆。

结果

在实验 1 中,SPS 在消退测试中增强了冻结,而这种效应在 SPS 之前被核雌激素受体拮抗剂阻断。在实验 2 中,SPS 降低了在获得和测试消退期间的条件性冻结。17β-雌二醇的给药改变了对照组和 SPS 动物在消退获得期间的冻结,但这种处理对消退记忆测试期间的冻结没有影响。在所有实验中,只有在恐惧条件反射期间观察到 darting 对足电击的起始。

结论

结果表明,需要多种行为(或不同的行为范式)来描述创伤后应激对雌性大鼠情绪记忆的影响的性质,并且 SPS 之前的核雌激素受体拮抗剂阻断了 SPS 对雌性大鼠情绪记忆的影响。

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