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恐惧消退过程中高水平的卵巢激素通过黑质纹状体多巴胺通路减少恐惧复发。

High ovarian hormones present during fear extinction reduce fear relapse through a nigrostriatal dopamine pathway.

作者信息

Hohorst Alyssa A, Tanner Margaret K, Han Rebecca, Korth Kamryn M, Westerman Jessica D, Mendoza Carolina Sanchez, Dryden Miles Q, Alvarez Lareina A, Abdul Remla A, Loetz Esteban C, Oleson Erik B, Greenwood Benjamin N

机构信息

Department of Psychology, University of Colorado Denver, Denver, CO, USA.

Department of Integrative Biology, University of Colorado Denver, Denver, CO, USA.

出版信息

Biol Sex Differ. 2025 Jun 1;16(1):38. doi: 10.1186/s13293-025-00722-7.

Abstract

BACKGROUND

Elevated ovarian hormones during fear extinction can enhance fear extinction memory retention and reduce fear renewal, but the mechanisms remain unknown. High levels of ovarian hormones are associated with heightened dopamine (DA) transmission, a key player in fear extinction. In males, stimulation of substantia nigra (SN) DA neurons during fear extinction reduces renewal; an effect mimicked by DA D1 receptor agonist administration into the dorsolateral striatum (DLS), a primary target of the SN. The current studies tested the role of the SN-DLS pathway in estrous cycle-modulation of fear extinction and relapse.

METHODS

Male and female Long-Evans rats were used to investigate the effects of sex and ovarian hormone levels during fear extinction on later fear relapse and underlying mechanisms. Fear extinction-induced cFos in SN DA neurons was quantified with double-label immunohistochemistry. An intersectional chemogenetic approach was used to determine whether SN-DLS pathway activity during fear extinction is necessary and sufficient for observed effects of ovarian hormones on fear relapse. Finally, fast scan cyclic voltammetry revealed the effects of sex and ovarian hormones on electrically-evoked DA release in the DLS and verified the effectiveness of chemogenetic approaches.

RESULTS

Female rats exposed to fear extinction during proestrus or estrus (Pro/Est; high hormones) had less relapse (renewal and spontaneous recovery) compared to males or females exposed to fear extinction during metestrus or diestrus (Met/Di; low hormones). Fear extinction-induced cFos within SN DA neurons and electrically-evoked DA release in the DLS was highest in female rats during Pro/Est. The behavioral and neurochemical effects of Pro/Est were mimicked by estradiol administration to ovariectomized female rats. Inhibition of the SN-DLS pathway suppressed electrically-evoked DA release in the DLS and restored fear renewal in females exposed to simultaneous fear extinction and SN-DLS inhibition during Pro/Est. Conversely, stimulation of the SN-DLS pathway during extinction reduced fear renewal in males.

CONCLUSIONS

Results indicate that ovarian hormones present during fear extinction reduce later fear relapse through a SN-DLS dopamine pathway. Data suggest the SN-DLS DA pathway is a novel target for the reduction of fear relapse in both sexes.

摘要

背景

恐惧消退过程中卵巢激素水平升高可增强恐惧消退记忆的保持并减少恐惧复发,但其机制尚不清楚。高水平的卵巢激素与多巴胺(DA)传递增强有关,而多巴胺是恐惧消退中的关键因素。在雄性动物中,恐惧消退过程中刺激黑质(SN)多巴胺能神经元可减少复发;将DA D1受体激动剂注入背外侧纹状体(DLS)(SN的主要靶点)可模拟这种效应。目前的研究测试了SN-DLS通路在发情周期对恐惧消退和复发的调节中的作用。

方法

使用雄性和雌性Long-Evans大鼠来研究恐惧消退过程中的性别和卵巢激素水平对后期恐惧复发及潜在机制的影响。采用双标免疫组织化学法定量恐惧消退诱导的SN多巴胺能神经元中的cFos。采用交叉化学遗传学方法确定恐惧消退过程中SN-DLS通路的活动对于卵巢激素对恐惧复发的观察到的影响是否必要且充分。最后,快速扫描循环伏安法揭示了性别和卵巢激素对DLS中电诱发的DA释放的影响,并验证了化学遗传学方法的有效性。

结果

与在动情后期或间情期(Met/Di;低激素水平)经历恐惧消退的雄性或雌性大鼠相比,在发情前期或发情期(Pro/Est;高激素水平)经历恐惧消退的雌性大鼠复发(重新出现和自发恢复)较少。在Pro/Est期间,雌性大鼠中恐惧消退诱导的SN多巴胺能神经元内的cFos以及DLS中电诱发的DA释放最高。对去卵巢雌性大鼠给予雌二醇可模拟Pro/Est的行为和神经化学效应。抑制SN-DLS通路可抑制DLS中电诱发的DA释放,并恢复在Pro/Est期间同时经历恐惧消退和SN-DLS抑制的雌性大鼠的恐惧重新出现。相反,在消退过程中刺激SN-DLS通路可减少雄性大鼠的恐惧重新出现。

结论

结果表明,恐惧消退过程中存在的卵巢激素通过SN-DLS多巴胺通路减少后期恐惧复发。数据表明,SN-DLS多巴胺通路是减少两性恐惧复发的新靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e5c1/12128558/783851ebc563/13293_2025_722_Fig1_HTML.jpg

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