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雄性Wistar大鼠自由探索范式的药理学验证:一种特质焦虑的拟议测试。

Pharmacological validation of the free-exploratory paradigm in male Wistar rats: A proposed test of trait anxiety.

作者信息

Almeida-Souza Thiago Henrique, Goes Tiago Costa, Teixeira-Silva Flavia

机构信息

Departamento de Fisiologia, Centro de Ciências Biológicas e da Saúde, Universidade Federal de Sergipe, 49100-000 São Cristóvão, SE, Brazil.

出版信息

Pharmacol Biochem Behav. 2015 Aug;135:114-20. doi: 10.1016/j.pbb.2015.03.024. Epub 2015 May 28.

Abstract

The free-exploratory paradigm (FEP) has been proposed as a model of trait anxiety for both mice and rats. However, its pharmacological validation has only been carried out for the mice. Thus, the aim of the present study was to pharmacologically validate FEP for Wistar rats, by testing the effects of clinically established anxiolytic and anxiogenic drugs, in four different experiments. In all experiments, male Wistar rats were first tested in FEP to be categorized according to their levels of trait anxiety (high, medium and low). Then, only medium trait anxiety rats were selected to be tested again in FEP, two weeks later, after being pharmacologically treated, according to each experiment as follows: Experiment I: 0.5mg/kg of diazepam (DZP) or vehicle; Experiment II: 20mg/kg of pentylenetetrazole (PTZ) or vehicle; Experiment III: 5mg/kg of fluoxetine (FLX5) or vehicle: and Experiment IV: 0.5mg/kg of fluoxetine (FLX0.5) or vehicle. As a group, the results showed that PTZ and FLX5 increased levels of trait anxiety and reduced locomotor activity, whereas DZP and FLX0.5 decreased levels of trait anxiety, without impairing locomotor activity. These results demonstrate that FEP for rats is able to predict clinical anxiolytic and anxiogenic activities of different drugs, including fluoxetine, which is believed to present a dual effect on anxiety. Therefore, this paradigm can be proposed as an effective method for testing potential trait anxiety-reducing drugs, in rats.

摘要

自由探索范式(FEP)已被提出作为小鼠和大鼠特质焦虑的一种模型。然而,其药理学验证仅在小鼠中进行。因此,本研究的目的是通过在四个不同实验中测试临床确定的抗焦虑和致焦虑药物的效果,对Wistar大鼠的FEP进行药理学验证。在所有实验中,雄性Wistar大鼠首先在FEP中进行测试,以根据其特质焦虑水平(高、中、低)进行分类。然后,仅选择中等特质焦虑的大鼠,在两周后经过药理学处理后,再次在FEP中进行测试,每个实验如下:实验I:0.5mg/kg地西泮(DZP)或赋形剂;实验II:20mg/kg戊四氮(PTZ)或赋形剂;实验III:5mg/kg氟西汀(FLX5)或赋形剂;实验IV:0.5mg/kg氟西汀(FLX0.5)或赋形剂。总体而言,结果表明PTZ和FLX5增加了特质焦虑水平并降低了运动活性,而DZP和FLX0.5降低了特质焦虑水平,且不损害运动活性。这些结果表明,大鼠的FEP能够预测不同药物(包括氟西汀)的临床抗焦虑和致焦虑活性,氟西汀被认为对焦虑具有双重作用。因此,该范式可被提议作为测试大鼠潜在特质焦虑减轻药物的有效方法。

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