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将社会不稳定应激作为成年雌性大鼠应激相关障碍模型的行为和分子效应评估

The behavioral and molecular evaluation of effects of social instability stress as a model of stress-related disorders in adult female rats.

作者信息

Nowacka-Chmielewska Marta Maria, Kasprowska-Liśkiewicz Daniela, Barski Jarosław Jerzy, Obuchowicz Ewa, Małecki Andrzej

机构信息

a Laboratory of Molecular Biology, Faculty of Physiotherapy , The Jerzy Kukuczka Academy of Physical Education , Katowice , Poland.

b Department of Experimental Medicine, School of Medicine in Katowice , Medical University of Silesia , Katowice , Poland.

出版信息

Stress. 2017 Nov;20(6):549-561. doi: 10.1080/10253890.2017.1376185. Epub 2017 Sep 15.

Abstract

The study aimed to test the hypotheses that chronic social instability stress (CSIS) alters behavioral and physiological parameters and expression of selected genes important for stress response and social behaviors. Adult female Sprague-Dawley rats were subjected to the 4-week CSIS procedure, which involves unpredictable rotation between phases of isolation and overcrowding. Behavioral analyses (Experiment 1) were performed on the same rats before and after CSIS (n = 16) and physiological and biochemical measurements (Experiment 2) were made on further control (CON; n = 7) and stressed groups (CSIS; n = 8). Behaviors in the open field test (locomotor and exploratory activities) and elevated-plus maze (anxiety-related behaviors) indicated anxiety after CSIS. CSIS did not alter the physiological parameters measured, i.e. body weight gain, regularity of estrous cycles, and circulating concentrations of stress hormones and sex steroids. QRT-PCR analysis of mRNA expression levels was performed on amygdala, hippocampus, prefrontal cortex (PFC), and hypothalamus. The main finding is that CSIS alters the mRNA levels for the studied genes in a region-specific manner. Hence, expression of POMC (pro-opiomelanocortin), AVPR1a (arginine vasopressin receptor), and OXTR (oxytocin receptor) significantly increased in the amygdala following CSIS, while in PFC and/or hypothalamus, POMC, AVPR1a, AVPR1b, OXTR, and ERβ (estrogen receptor beta) expression decreased. CSIS significantly reduced expression of CRH-R1 (corticotropin-releasing hormone receptor type 1) in the hippocampus. The directions of change in gene expression and the genes and regions affected indicate a molecular basis for the behavior changes. In conclusion, CSIS may be valuable for further analyzing the neurobiology of stress-related disorders in females.

摘要

该研究旨在检验以下假设

慢性社会不稳定应激(CSIS)会改变行为和生理参数,以及对应激反应和社会行为重要的特定基因的表达。成年雌性斯普拉格-道利大鼠接受为期4周的CSIS程序,该程序包括在隔离和拥挤阶段之间进行不可预测的轮换。对相同的大鼠在CSIS前后进行行为分析(实验1,n = 16),并对另外的对照组(CON;n = 7)和应激组(CSIS;n = 8)进行生理和生化测量(实验2)。旷场试验中的行为(运动和探索活动)以及高架十字迷宫中的行为(与焦虑相关的行为)表明CSIS后出现焦虑。CSIS并未改变所测量的生理参数,即体重增加、发情周期规律以及应激激素和性类固醇的循环浓度。对杏仁核、海马体、前额叶皮质(PFC)和下丘脑进行了mRNA表达水平的定量实时聚合酶链反应(QRT-PCR)分析。主要发现是CSIS以区域特异性方式改变了所研究基因的mRNA水平。因此,CSIS后杏仁核中阿黑皮素原(POMC)、精氨酸加压素受体1a(AVPR1a)和催产素受体(OXTR)的表达显著增加,而在PFC和/或下丘脑,POMC、AVPR1a、AVPR1b、OXTR和雌激素受体β(ERβ)的表达下降。CSIS显著降低了海马体中促肾上腺皮质激素释放激素受体1(CRH-R1)的表达。基因表达变化的方向以及受影响的基因和区域表明了行为变化的分子基础。总之,CSIS对于进一步分析女性应激相关障碍的神经生物学可能具有重要价值。

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