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在大鼠中,阶段性和持续性恐惧在药理学上是可分离的。

Phasic and sustained fear are pharmacologically dissociable in rats.

机构信息

Department of Molecular and Systems Pharmacology, Emory University, Atlanta, GA 30329, USA.

出版信息

Neuropsychopharmacology. 2011 Jul;36(8):1563-74. doi: 10.1038/npp.2011.29. Epub 2011 Apr 6.

Abstract

Previous findings suggest differences in the neuroanatomical substrates of short- (seconds) vs longer-duration (minutes) fear responses. We now report that phasic and sustained fear can also be differentiated pharmacologically, based on their response to several treatments that either are or are not clinically effective anxiolytics. For these experiments, short- or long-duration clicker stimuli were paired with footshock. Acoustic startle amplitude was later measured in the absence of the clicker, or within seconds (phasic fear) or minutes (sustained fear) of its onset. Before testing, rats received a single injection of vehicle, the benzodiazepine chlordiazepoxide, the 5HT(1A) agonist and dopamine D2 antagonist buspirone, the selective serotonin reuptake inhibitor fluoxetine, or a 3-week treatment with either vehicle or fluoxetine. Chlordiazepoxide blocked sustained, but not phasic startle increases. Acute buspirone, which is not anxiolytic in human beings, did not affect sustained startle increases, but did disrupt phasic increases. Chronic fluoxetine blocked sustained startle increases and unreliably reduced phasic increases; acute fluoxetine affected neither. The results indicate that phasic and sustained fear responses can be pharmacologically dissociated, further validating this distinction, and suggest that sustained startle increases may be especially useful as anxiety models and anxiolytic screens.

摘要

先前的研究结果表明,短时间(秒级)和长时间(分钟级)恐惧反应的神经解剖学基础存在差异。我们现在报告称,根据几种治疗方法对其的反应,也可以从药理学上区分出瞬态和持续的恐惧,这些治疗方法要么是有效的抗焦虑药物,要么不是。对于这些实验,短时间或长时间的点击刺激与足底电击配对。随后在没有点击器的情况下或在其出现后的几秒钟(瞬态恐惧)或几分钟(持续恐惧)内测量声惊跳幅度。在测试之前,大鼠接受了单次注射载体、苯二氮䓬类氯氮䓬、5HT(1A)激动剂和多巴胺 D2 拮抗剂丁螺环酮、选择性 5-羟色胺再摄取抑制剂氟西汀,或接受载体或氟西汀的 3 周治疗。氯氮䓬阻断了持续的,但不是瞬态的惊跳增加。在人类中没有抗焦虑作用的急性丁螺环酮不会影响持续的惊跳增加,但会破坏瞬态的惊跳增加。慢性氟西汀阻断了持续的惊跳增加,并不可靠地减少了瞬态的惊跳增加;急性氟西汀则没有影响。研究结果表明,瞬态和持续的恐惧反应可以在药理学上区分开来,进一步验证了这种区别,并表明持续的惊跳增加可能特别有用作焦虑模型和抗焦虑筛选。

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