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Acute restraint differently alters defensive responses and fos immunoreactivity in the rat brain

机译:急性抑制以不同方式改变大鼠大脑的防御反应和fos免疫反应性

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Results from a previous study show that rats exposed to acute restraint display anxiogenic-like behavior, evidenced by facilitation of avoidance responses in the elevated T-maze (ETM) model of anxiety. In contrast, escape responses were unaltered by stress exposure. Since ETM avoidance and escape tasks seem to activate distinct sets of brain structures, it is possible that the differences observed with acute restraint are due to particularities in the neurobiological mechanisms which modulate these responses. In the present study, analysis of . fos protein immunoreactivity (. fos-ir) was used to map areas activated by exposure of male Wistar rats to restraint stress (30. min) previously (30. min) to the ETM. Corticosterone levels were also measured in stressed and non-stressed animals. Confirming previous observations restraint facilitated avoidance performance, an anxiogenic result, while leaving escape unaltered. Performance of the avoidance task increased . fos-ir in the frontal cortex, intermediate lateral septum, basolateral amygdala, basomedial amygdala, lateral amygdala, anterior hypothalamus and dorsal raphe nucleus. In contrast, performance of escape increased . fos-ir in the ventromedial hypothalamus, dorsolateral periaqueductal gray and . locus ceruleus. Both behavioral tasks also increased . fos-ir in the dorsomedial hypothalamus. Restraint significantly raised corticosterone levels. Additionally after restraint, . fos-ir was predominantly seen in the basolateral amygdala and dorsal raphe of animals submitted to the avoidance task. This data confirms that different sets of brain structures are activated by ETM avoidance and escape tasks and suggests that acute restraint differently alters ETM behavior and the pattern of . fos activation in the brain.
机译:先前研究的结果表明,暴露于急性约束下的大鼠表现出类似焦虑症的行为,这可通过促进T型迷宫(ETM)焦虑模型中的回避反应来证明。相比之下,压力暴露不会改变逃生反应。由于ETM的回避和逃避任务似乎激活了不同的大脑结构集,因此在急性约束下观察到的差异可能归因于调节这些反应的神经生物学机制的特殊性。在本研究中,对的分析。 fos蛋白免疫反应性(.fos-ir)用于绘制通过雄性Wistar大鼠暴露于先前(30分钟)到ETM的限制压力(30分钟)而激活的区域。还测量了应激和非应激动物的皮质酮水平。确认先前的观察约束有助于避免行为的产生,这是一个焦虑症的结果,而逃生却没有改变。回避任务的表现有所提高。额叶皮质,中间外侧中隔,基底外侧杏仁核,基底体杏仁核,外侧杏仁核,下丘脑前部和背ra核的fos-ir。相反,逃避的性能增加了。 fos-ir在腹侧下丘脑,背外侧导水管周围灰色和。蓝斑。两项行为任务也有所增加。 fos-ir位于背部丘脑下丘脑。克制能显着提高皮质酮水平。此外,约束后,。 fos-ir主要见于接受规避任务的动物的基底外侧杏仁核和背脊。这些数据证实了ETM的回避和逃避任务激活了不同的脑结构集,并暗示了急性束缚会改变ETM的行为和行为模式。大脑中的fos激活。

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