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药理学应激源对小鼠大脑中c-fos和CRF mRNA的影响:与酒精觅求的关系。

Effects of pharmacological stressors on c-fos and CRF mRNA in mouse brain: relationship to alcohol seeking.

作者信息

Funk Douglas, Li Zhaoxia, Coen Kathy, Lê Anh Dzung

机构信息

Department of Neuroscience, Center for Addiction and Mental Health, Toronto, Canada.

出版信息

Neurosci Lett. 2008 Oct 31;444(3):254-8. doi: 10.1016/j.neulet.2008.08.043. Epub 2008 Aug 19.

Abstract

A marked heterogeneity exists among stressors in their ability to reinstate alcohol seeking in rats. We have reported that the pharmacological stressor yohimbine, an alpha-2 adrenoceptor antagonist, potently reinstated alcohol seeking, but FG-7142, a benzodiazepine inverse agonist was ineffective. In rats, we determined that yohimbine elicits patterns of brain expression of the mRNAs for c-fos, a marker of neuronal activation, and corticotropin-releasing factor (CRF) a stress-related peptide, distinct from that produced by FG-7142. The purpose of the present experiment is to determine if these differential effects of yohimbine and FG-7142 on regional c-fos and CRF mRNA expression generalize to another animal commonly used in alcohol research, the C57 BL/6J mouse. In comparing the results of the present study to those of our previous one, we found a number of commonalities in the patterns of activation elicited by yohimbine and FG-7142 between the two species, and some notable differences. As we found in the rat, yohimbine selectively increased c-fos mRNA in the mouse NACs, BLA and CeA. Yohimbine increased CRF mRNA only in the mouse PVN, but was without effect on CRF mRNA in extrahypothalamic sites, the BNST and CeA. This differs from what we saw in the rat, where yohimbine increased CRF mRNA in these extrahypothalamic regions, but not the PVN. The selective induction of c-fos in the NACs, BLA and CeA of mice and rats by yohimbine offers further support for the idea that activation of these structures participates in reinstatement induced by such stressors.

摘要

应激源在恢复大鼠酒精觅求行为的能力方面存在显著的异质性。我们曾报道,药理应激源育亨宾(一种α-2肾上腺素能受体拮抗剂)能有效恢复酒精觅求行为,但苯二氮䓬反向激动剂FG-7142却无效。在大鼠中,我们确定育亨宾引发的神经元激活标志物c-fos的mRNA以及应激相关肽促肾上腺皮质激素释放因子(CRF)的脑表达模式,与FG-7142产生的模式不同。本实验的目的是确定育亨宾和FG-7142对区域c-fos和CRF mRNA表达的这些差异效应是否适用于另一种常用于酒精研究的动物——C57 BL/6J小鼠。在将本研究结果与我们之前的研究结果进行比较时,我们发现育亨宾和FG-7142在两种物种中引发的激活模式存在一些共性,也有一些显著差异。正如我们在大鼠中发现的那样,育亨宾选择性地增加了小鼠伏隔核、杏仁基底外侧核和中央杏仁核中的c-fos mRNA。育亨宾仅在小鼠室旁核中增加了CRF mRNA,但对下丘脑外部位、终纹床核和中央杏仁核中的CRF mRNA没有影响。这与我们在大鼠中看到的情况不同,在大鼠中育亨宾增加了这些下丘脑外区域的CRF mRNA,但对室旁核没有影响。育亨宾对小鼠和大鼠的伏隔核、杏仁基底外侧核和中央杏仁核中c-fos的选择性诱导,进一步支持了这些结构的激活参与此类应激源诱导的恢复这一观点。

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