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对暴露于高架十字迷宫的大鼠,将利坦色林微量注入其基底外侧杏仁核可预防系统给予MK - 212产生的行为效应。

Behavioral effects of systemically administered MK-212 are prevented by ritanserin microinfusion into the basolateral amygdala of rats exposed to the elevated plus-maze.

作者信息

de Mello Cruz Antonio Pedro, Pinheiro Gilson, Alves Sérgio Henrique, Ferreira Graziela, Mendes Marília, Faria Letícia, Macedo Carlos Eduardo, Motta Vitor, Landeira-Fernandez J

机构信息

Laboratório de Psicobiologia, Departamento de Processos Psicológicos Básicos, Instituto de Psicologia, Universidade de Brasília, Brasília, DF, Brazil.

出版信息

Psychopharmacology (Berl). 2005 Nov;182(3):345-54. doi: 10.1007/s00213-005-0108-2. Epub 2005 Oct 19.

Abstract

RATIONALE

Although 5-HT2 receptors seem to play an important role in anxiety, results from numerous studies are still highly variable. Moreover, little is known about the behavioral effects of centrally administered 5-HT2 compounds in animal models of anxiety.

OBJECTIVE

The current study was performed to: (1) further investigate the effects of 5-HT2 receptor activation in rats exposed to the elevated plus-maze (EPM) and the open-field arena, two widely used animal models for studying anxiety and locomotor activity; and (2) evaluate the involvement of the 5-HT2 receptors within the basolateral nucleus of the amygdala (BLA) in the modulation of such effects.

METHODS

In the first experiment, male Wistar rats were exposed for 5 min to the EPM 27 min following intraperitoneal (i.p.) (1.0 ml/kg) injections of the preferential 5-HT2C receptor agonist 6-chloro-2[1-piperazinyl]pyrazine (MK-212) at doses of 1.0, 2.0, or 4.0 mg/kg. Control animals were injected with saline. The percentage of open-arm entries and the percentage of time spent in these arms were employed as anxiety indexes, whereas the number of closed-arm entries was calculated as indicative of locomotor activity. In the second experiment, rats were exposed for 10 min in an open-field arena to further assess the interference of the same MK-212 doses upon locomotor activity. In Experiment 3, rats were microinjected (0.2 microl) either with the mixed 5-HT 2A/2C receptor antagonist ritanserin (0.5, 1.25, 2.5, and 5.0 microg) or its vehicle into the BLA 12 min following i.p. injections of saline or the intermediate dose of MK-212 (2.0 mg/kg). Fifteen minutes later, each animal was exposed to the EPM as before.

RESULTS

Whereas the highest dose of MK-212 (4.0 mg/kg) induced motor-suppressant effects in both EPM and open-field arena, the intermediate dose of the drug (2.0 mg/kg) reduced open-arm exploration without significantly affecting the number of closed-arm entries. This behavioral profile, consistent with selective anxiogenic effect in the EPM, was dose-dependently prevented by ritanserin microinfusion into the BLA. In saline-pretreated animals, however, ritanserin (all doses) was ineffective.

CONCLUSIONS

MK-212 increases anxiety and decreases locomotor activity. The anxiogenic-like profile of 5-HT2 receptor activation is prevented by the blockade of 5-HT2 receptors within the BLA, which does not have an effect by itself upon basal anxiety levels triggered by the EPM.

摘要

理论依据

尽管5-羟色胺2(5-HT2)受体似乎在焦虑中发挥重要作用,但众多研究的结果仍存在很大差异。此外,关于在焦虑动物模型中中枢给予5-HT2化合物的行为效应,人们了解甚少。

目的

进行本研究以:(1)进一步研究5-HT2受体激活对暴露于高架十字迷宫(EPM)和旷场试验箱的大鼠的影响,这是两种广泛用于研究焦虑和运动活动的动物模型;(2)评估杏仁核基底外侧核(BLA)内的5-HT2受体在调节此类效应中的作用。

方法

在第一个实验中,雄性Wistar大鼠在腹腔内(i.p.)(1.0 ml/kg)注射剂量为1.0、2.0或4.0 mg/kg的选择性5-HT2C受体激动剂6-氯-2-[1-哌嗪基]吡嗪(MK-212)27分钟后,暴露于EPM 5分钟。对照动物注射生理盐水。将进入开放臂的百分比和在这些臂中花费的时间百分比用作焦虑指标,而将进入封闭臂的次数计算为运动活动的指标。在第二个实验中,大鼠在旷场试验箱中暴露10分钟,以进一步评估相同剂量的MK-212对运动活动的干扰。在实验3中,大鼠在腹腔注射生理盐水或MK-212中间剂量(2.0 mg/kg)12分钟后,向BLA微量注射(0.2微升)混合的5-HT2A/2C受体拮抗剂利坦色林(0.5、1.25、2.5和5.0微克)或其溶媒。15分钟后,每只动物如前一样暴露于EPM。

结果

虽然MK-212的最高剂量(4.0 mg/kg)在EPM和旷场试验箱中均诱导运动抑制作用,但该药物的中间剂量(2.0 mg/kg)减少了开放臂探索,而对封闭臂进入次数没有显著影响。这种行为特征与EPM中的选择性致焦虑效应一致,通过向BLA微量注射利坦色林可剂量依赖性地预防。然而,在生理盐水预处理的动物中,利坦色林(所有剂量)均无效。

结论

MK-212增加焦虑并降低运动活动。通过阻断BLA内的5-HT2受体可预防5-HT2受体激活的致焦虑样特征,而其本身对EPM引发的基础焦虑水平没有影响。

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