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FG-7142 对猫的焦虑、攻击行为和边缘生理学的持久影响。

Lasting effects of FG-7142 on anxiety, aggression and limbic physiology in the cat.

机构信息

Department of Psychology, Memorial University, St. John's, Newfoundland, Canada.

出版信息

J Psychopharmacol. 1993 Jan;7(3):232-48. doi: 10.1177/026988119300700302.

Abstract

The effect of the anxiogenic β-carboline, FG-7142, on behavior and limbic physiology was investigated. A single systemic injection of FG-7142 (10 mg/kg) changed behavior for at least 43 days. Two days after drug administration, defensive response to rats was increased. In addition, predatory attack was suppressed in some, but not all, animals. Cats that were more predatory (killers, n=2) before drug administration showed suppression of predatory attack after FG-7142. The attack of less predatory cats (non-killers, n=3) was unaffected by FG-7142. Suppression of attack was not correlated with changes in defense. This finding suggests FG-7142 acts on separate substrates of defense and attack suppression to change these behaviors lastingly. FG-7142 produced long-term potentiation (LTP) in two of three limbic pathways investigated. LTP was observed in the amygdalo-ventromedial hypothalamic (AM-VMH) pathway. AM-VMH LTP depended on changes within the amygdala and not in the efferent synapses or in the VMH. LTP lasted 6 days, returning to baseline by 21 days after FG-7142. The only behavioral change correlated with AM-VMH LTP was defensive response at 2 days after FG-7142. Increased defense from 6 to 43 days after the drug was not correlated with AM-VMH LTP. Therefore, AM-VMH LTP may be necessary for the initiation, but not maintenance, of increased defensive response. LTP of the population spike of the perforant path-CA3 (PP-CA3) field potential in the ventral hippocampus was also seen. LTP appeared 6 days after drug administration, after cats had been exposed to rats. Before the appearance of PP-CA3 LTP, there was a transient failure of recurrent inhibition in area CA3. It is likely that exposure to a rat during the period of failed inhibition facilitated the PP-CA3 LTP. In addition, following FG-7142, facilitation in area CA3 increased lastingly, consistent with a lasting increase in the duration of excitatory neurotransmitter release. Changes in hippocampal inhibition and facilitation correlated with changes in attack behavior, but not with changes in defensive response. Systemic flumazenil (10 mg/kg) partially reversed the lasting changes in defense and approach-attack in a drug-dependent manner. Limbic physiology was unchanged by flumazenil. Flumazenil probably did not affect AM-VMH transmission in the present study because AM-VMH LTP had returned to baseline when flumazenil was given. These findings suggest flumazenil only acts on potentiated AM-VMH transmission.

摘要

研究了致焦虑β-咔啉 FG-7142 对行为和边缘生理学的影响。单次全身注射 FG-7142(10mg/kg)至少可改变 43 天的行为。给药后两天,大鼠的防御反应增强。此外,一些(但不是所有)动物的捕食攻击受到抑制。在给药前更具捕食性的猫(杀手,n=2)在 FG-7142 后显示出捕食攻击的抑制。不太具捕食性的猫(非杀手,n=3)的攻击不受 FG-7142 的影响。攻击的抑制与防御的变化无关。这一发现表明,FG-7142 作用于防御和攻击抑制的独立基质上,以持久地改变这些行为。FG-7142 在三种研究的边缘途径中的两种中产生了长时程增强(LTP)。在杏仁-腹内侧下丘脑(AM-VMH)途径中观察到 AM-VMH LTP。AM-VMH LTP 取决于杏仁核内的变化,而不是传出突触或 VMH 中的变化。LTP 持续 6 天,在 FG-7142 后 21 天恢复到基线。唯一与 AM-VMH LTP 相关的行为变化是 FG-7142 后 2 天的防御反应。在药物后 6 至 43 天,防御反应的增加与 AM-VMH LTP 无关。因此,AM-VMH LTP 可能是增强防御反应的起始所必需的,但不是维持所必需的。腹侧海马的穿通路径-CA3(PP-CA3)场电位的群体峰也出现 LTP。LTP 在药物给予后 6 天出现,此时猫已经接触到老鼠。在出现 PP-CA3 LTP 之前,CA3 区的复发性抑制暂时失效。很可能是在抑制失败期间接触老鼠促进了 PP-CA3 LTP。此外,FG-7142 后,CA3 区的易化作用持久增加,与兴奋性神经递质释放持续增加一致。海马抑制和易化的变化与攻击行为的变化相关,但与防御反应的变化无关。全身氟马西尼(10mg/kg)以药物依赖的方式部分逆转了防御和接近攻击的持久变化。氟马西尼未改变边缘生理学。氟马西尼可能没有影响本研究中的 AM-VMH 传递,因为当给予氟马西尼时,AM-VMH LTP 已经恢复到基线。这些发现表明,氟马西尼仅作用于增强的 AM-VMH 传递。

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