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慢性合成代谢雄激素类固醇暴露改变了雌性小鼠的促肾上腺皮质激素释放因子表达和焦虑样行为。

Chronic anabolic androgenic steroid exposure alters corticotropin releasing factor expression and anxiety-like behaviors in the female mouse.

机构信息

Department of Surgery, Dartmouth Medical School, Lebanon, NH 03756, United States.

出版信息

Psychoneuroendocrinology. 2010 Nov;35(10):1473-85. doi: 10.1016/j.psyneuen.2010.04.015. Epub 2010 May 26.

Abstract

In the past several decades, the therapeutic use of anabolic androgenic steroids (AAS) has been overshadowed by illicit use of these drugs by elite athletes and a growing number of adolescents to enhance performance and body image. As with adults, AAS use by adolescents is associated with a range of behavioral effects, including increased anxiety and altered responses to stress. It has been suggested that adolescents, especially adolescent females, may be particularly susceptible to the effects of these steroids, but few experiments in animal models have been performed to test this assertion. Here we show that chronic exposure of adolescent female mice to a mixture of three commonly abused AAS (testosterone cypionate, nandrolone decanoate and methandrostenolone; 7.5 mg/kg/day for 5 days) significantly enhanced anxiety-like behavior as assessed by the acoustic startle response (ASR), but did not augment the fear-potentiated startle response (FPS) or alter sensorimotor gating as assessed by prepulse inhibition of the acoustic startle response (PPI). AAS treatment also significantly increased the levels of corticotropin releasing factor (CRF) mRNA and somal-associated CRF immunoreactivity in the central nucleus of the amygdala (CeA), as well as neuropil-associated immunoreactivity in the dorsal aspect of the anterolateral division of the bed nucleus of the stria terminalis (dBnST). AAS treatment did not alter CRF receptor 1 or 2 mRNA in either the CeA or the dBnST; CRF immunoreactivity in the ventral BnST, the paraventricular nucleus (PVN) or the median eminence (ME); or peripheral levels of corticosterone. These results suggest that chronic AAS treatment of adolescent female mice may enhance generalized anxiety, but not sensorimotor gating or learned fear, via a mechanism that involves increased CRF-mediated signaling from CeA neurons projecting to the dBnST.

摘要

在过去几十年中,由于精英运动员和越来越多的青少年为了提高运动表现和身体形象而非法使用这些药物,合成代谢雄激素类固醇(AAS)的治疗用途受到了影响。与成年人一样,青少年使用 AAS 与一系列行为效应有关,包括焦虑增加和对压力的反应改变。有人认为,青少年,尤其是青春期女性,可能特别容易受到这些类固醇的影响,但在动物模型中进行的很少实验来检验这一说法。在这里,我们显示慢性暴露于混合三种常用 AAS(睾丸酮 Cypionate、十一酸睾酮和 Methandrostenolone;7.5 毫克/千克/天,共 5 天)的青春期雌性小鼠显著增强了焦虑样行为,如声惊反射(ASR)评估,但并未增强恐惧增强的惊反射(FPS)或改变感觉运动门控,如声惊反射的前脉冲抑制(PPI)评估。AAS 治疗还显著增加了中央杏仁核(CeA)中促肾上腺皮质释放因子(CRF)mRNA 和体相关 CRF 免疫反应,以及终纹床核前外侧分支(dBNST)背侧神经突相关免疫反应。AAS 治疗并未改变 CeA 或 dBNST 中的 CRF 受体 1 或 2 mRNA;BnST 腹侧、室旁核(PVN)或正中隆起(ME)中的 CRF 免疫反应;或外周皮质酮水平。这些结果表明,慢性 AAS 治疗青春期雌性小鼠可能通过涉及从 CeA 神经元投射到 dBNST 的 CRF 介导信号增加的机制增强了一般焦虑,但不会增强感觉运动门控或习得性恐惧。

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