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反复使用育亨宾对即时及事后行为、应激激素和能量稳态参数的影响。

Effect of recurrent yohimbine on immediate and post-hoc behaviors, stress hormones, and energy homeostatic parameters.

作者信息

Figlewicz D P, Hill S R, Jay J L, West C H, Zavosh A S, Sipols A J

机构信息

VA Puget Sound Health Care System (151), Seattle, WA 98108, USA; Dept. of Psychiatry & Behavioral Sciences, University of Washington, Seattle, WA 98195, USA.

Dept. of Psychiatry & Behavioral Sciences, University of Washington, Seattle, WA 98195, USA.

出版信息

Physiol Behav. 2014 Apr 22;129:186-93. doi: 10.1016/j.physbeh.2014.02.019. Epub 2014 Feb 22.

Abstract

Evidence from experimental models has suggested that acute activation of brain stress and anxiety pathways impacts subsequent behaviors that are mediated or modulated by limbic circuitry. There have been limited investigations of prior or chronic activation of these pathways on subsequent limbic-mediated behaviors. In this study, we tested whether recurrent administration of the anxiogenic compound yohimbine (YOH) could have post-injection effects on brain activation, stress hormones, and performance in sucrose self-administration and startle response paradigms. Rats received six injections across two weeks of either 2mg/kg YOH or saline. Behavioral evaluation confirmed the continued efficacy of the YOH regimen, and increased adrenal corticosterone (CORT) was observed. Several days following YOH or SAL administration, cFos, CORT and adrenocorticotropin hormone (ACTH), and behavioral performance were measured. cFos was elevated post-YOH in the hippocampus; ventral tegmental area/zona inserta; and central and medial nuclei of the amygdala. This activation is consistent with a sustained effect of YOH to activate fear and anxiety circuitries in the CNS. CORT but not ACTH was elevated in the YOH-rats following startle testing. Self-administration and startle tests suggested an increase of non-specific activity in the post-YOH rats; there was no increase in sucrose self-administration or startle response per se. Our findings suggest that recurrent YOH administration may prove a useful and reliable model for simulating recurrent stress/anxiety, and that enhancements to the paradigm such as higher or more frequent dosing of YOH could yield stronger or more extensive behavioral effects.

摘要

实验模型的证据表明,大脑应激和焦虑通路的急性激活会影响随后由边缘系统介导或调节的行为。关于这些通路的先前或慢性激活对随后边缘系统介导行为的影响,相关研究较少。在本研究中,我们测试了反复给予致焦虑化合物育亨宾(YOH)是否会对大脑激活、应激激素以及蔗糖自我给药和惊吓反应范式中的行为表现产生注射后效应。大鼠在两周内接受了六次注射,每次注射2mg/kg YOH或生理盐水。行为评估证实了YOH给药方案的持续有效性,并观察到肾上腺皮质酮(CORT)增加。在给予YOH或生理盐水后数天,测量了cFos、CORT和促肾上腺皮质激素(ACTH)以及行为表现。YOH注射后,海马体、腹侧被盖区/插入带以及杏仁核的中央和内侧核中的cFos升高。这种激活与YOH持续激活中枢神经系统中的恐惧和焦虑回路的作用一致。惊吓测试后,YOH处理的大鼠中CORT升高,但ACTH未升高。自我给药和惊吓测试表明,YOH处理后的大鼠非特异性活动增加;蔗糖自我给药或惊吓反应本身没有增加。我们的研究结果表明,反复给予YOH可能是模拟反复应激/焦虑的一种有用且可靠的模型,并且对该范式的改进,如更高剂量或更频繁地给予YOH,可能会产生更强或更广泛的行为效应。

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