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5-羟色胺3受体激动剂和拮抗剂改变小鼠厌恶行为的神经解剖学作用部位。

Neuroanatomical sites of action of 5-HT3 receptor agonist and antagonists for alteration of aversive behaviour in the mouse.

作者信息

Costall B, Kelly M E, Naylor R J, Onaivi E S, Tyers M B

机构信息

Postgraduate School of Studies in Pharmacology, University of Bradford.

出版信息

Br J Pharmacol. 1989 Feb;96(2):325-32. doi: 10.1111/j.1476-5381.1989.tb11821.x.

Abstract
  1. The cerebral topography of the action of diazepam and the action of the 5-hydroxytryptamine 5-HT3 receptor antagonists GR38032F and ICS 205-930 in attenuating an aversive response was studied in the mouse. 2. Mice which had been cannulated to allow drug injection into the dorsal and median raphe nuclei, the amygdala, nucleus accumbens or caudate-putamen were placed in a two compartment black (dimly illuminated) and white (brightly illuminated) test box. Measurements were made of the time spent, rearing and line crossings in the two sections and the latency of initial movement from the white to the black area. 3. The injection of diazepam (0.1-10 ng), GR38032F (0.01-1.0 ng) and ICS 205-930 (1.0-10 ng) into the dorsal raphe nucleus and amygdala, and the injection of diazepam (0.1-10 ng) into the median raphe nucleus, reduced an aversive response to the brightly illuminated white area, delaying the initial movement into the black section and increasing the time spent, rearings and line crossings in the white area. Concomitantly such activities were decreased in the black section. 4. The injection of the 5-HT3 agonist 2-methyl-5-hydroxytryptamine (0.1-10 ng) into the dorsal raphe nucleus and amygdala caused the opposite response, decreasing the time taken to move into the black section and increasing the time spent, rearings and line crossings in the black section, decreasing such activities in the white area. 5. The 5-HT3 agonist and antagonists showed little or no effect following injection into the median raphe nucleus and there were no changes in exploratory behaviour following their injection, or injection of diazepam, into the nucleus accumbens or caudate-putamen. 6. It is concluded that in the mouse the cerebral topography of action of GR38032F and ICS 205-930 in attenuating an aversive response follows that of diazepam in the dorsal raphe nucleus and amygdala but that diazepam may have additional effects mediated via the median raphe nucleus.
摘要
  1. 在小鼠中研究了地西泮的作用以及5-羟色胺5-HT3受体拮抗剂GR38032F和ICS 205-930在减轻厌恶反应方面的作用的脑地形图。2. 已插管以便将药物注射到背侧和中缝核、杏仁核、伏隔核或尾状壳核的小鼠被置于一个两室的黑(弱光照明)白(强光照明)测试箱中。测量在两个区域花费的时间、竖毛和穿越线条的次数以及从白色区域到黑色区域的初始移动潜伏期。3. 向背侧中缝核和杏仁核注射地西泮(0.1 - 10纳克)、GR38032F(0.01 - 1.0纳克)和ICS 205-930(1.0 - 10纳克),以及向中缝核注射地西泮(0.1 - 10纳克),可减轻对强光照明的白色区域的厌恶反应,延迟进入黑色区域的初始移动,并增加在白色区域花费的时间、竖毛和穿越线条的次数。同时,在黑色区域的此类活动减少。4. 向背侧中缝核和杏仁核注射5-HT3激动剂2-甲基-5-羟色胺(0.1 - 10纳克)会引起相反的反应,减少进入黑色区域所需的时间,并增加在黑色区域花费的时间、竖毛和穿越线条的次数,减少在白色区域的此类活动。5. 向中缝核注射5-HT3激动剂和拮抗剂后几乎没有或没有影响,并且在向伏隔核或尾状壳核注射它们或注射地西泮后,探索行为没有变化。6. 得出结论,在小鼠中,GR38032F和ICS 205-930在减轻厌恶反应方面的作用脑地形图与地西泮在背侧中缝核和杏仁核中的作用脑地形图一致,但地西泮可能还具有通过中缝核介导的其他作用。

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