首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >The delayed effects of phencyclidine enhance amphetamine-induced behavior and striatal C-Fos expression in the rat.
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The delayed effects of phencyclidine enhance amphetamine-induced behavior and striatal C-Fos expression in the rat.

机译:苯环利定的延迟作用增强了苯丙胺诱导的行为和大鼠纹状体C-Fos表达。

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摘要

The ability for the delayed effects of phencyclidine to model schizophrenia-like symptomatology was investigated by assessing the effects of phencyclidine pretreatment on amphetamine-induced behavior. Corresponding changes in striatal, nucleus accumbens and anterior cingulate cortex c-Fos induction were also assessed in order to test the hypothesis that alterations in the neurochemistry of these regions accompany phencyclidine-induced changes in amphetamine-induced behaviors. Rats were treated with 15.0 mg/kg phencyclidine or vehicle 24 h prior to behavioral testing following vehicle, 0.5, 2.5 or 5.0 mg/kg amphetamine. Phencyclidine pretreatment significantly increased amphetamine-induced locomotion and rearing in response to 0.5 mg/kg amphetamine. Likewise, phencyclidine pretreatment produced an increase in the number of striatal cells expressing c-Fos following treatment with 0.5 mg/kg amphetamine. Phencyclidine pretreatment did not alter c-Fos induction in the nucleus accumbens, but did decrease the basal number of c-Fos-containing cells in the anterior cingulate cortex. While stereotypy rating revealed that phencyclidine pretreatment enhanced the behavioral response to 5.0 mg/kg amphetamine over time, no other alterations in behavior or c-Fos expression in response to the higher doses of amphetamine were induced by phencyclidine pretreatment. These data demonstrate that the delayed effects of a single dose of phencyclidine alter anterior cingulate cortex neurochemistry, and enhance the behavioral and striatal c-Fos response to a low dose of amphetamine. These findings suggest that the delayed effects of a single dose of phencyclidine may produce a reasonable animal model for schizophrenia.
机译:通过评估苯环利定预处理对苯丙胺诱导的行为的影响,研究了苯环利定对精神分裂症样症状模型的延迟作用的能力。还评估了纹状体,伏隔核和前扣带回皮质c-Fos诱导的相应变化,以检验以下假说:这些区域的神经化学变化伴随苯环利定诱导的苯丙胺诱导的行为变化。在行为测试之前的24小时,用0.5、2.5或5.0 mg / kg苯丙胺对大鼠进行15.0 mg / kg苯环利定或介质的处理。苯环利定预处理显着增加了苯丙胺对0.5 mg / kg苯丙胺的诱导的运动和饲养。同样,苯环利定预处理在用0.5 mg / kg苯丙胺处理后,表达c-Fos的纹状体细胞数量增加。苯环利定预处理不会改变伏隔核中c-Fos的诱导,但会减少前扣带回皮层中含c-Fos的细胞的基数。虽然刻板印象等级表明苯环利定预处理可随着时间的推移增强对5.0 mg / kg安非他明的行为反应,但苯环利定预处理未诱导响应于更高剂量苯丙胺的行为或c-Fos表达的其他改变。这些数据表明,单剂量苯环利定的延迟作用改变了前扣带回皮层的神经化学,并增强了行为和纹状体对低剂量苯丙胺的c-Fos反应。这些发现表明,单剂量苯环利定的延迟作用可能为精神分裂症建立合理的动物模型。

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