[Serotonergic neurons and behavior].

Journal de pharmacologie Pub Date : 1986-04-01
P Soubrié
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引用次数: 0

Abstract

The hypothesis linking decreased serotonin transmission to reduced anxiety as the mechanism in the anxiolytic activity of benzodiazepines conflicts with most clinical observations. Serotonin antagonists show no marked capacity to alleviate anxiety. On the other hand, clinical signs of reduced serotonergic transmission (low 5-HIAA levels in the cerebrospinal fluid) are frequently associated with aggressiveness, suicide attempts and increased anxiety. This brief review attempts to reconcile these human and animal findings by investigating whether anxiety reduction or increased impulsivity are likely to account for animal behavioral changes associated with decreased serotonergic transmission. The effects of manipulating central serotonin on experimental anxiety paradigms in animals (punishment, novelty) are reviewed and compared to the effects of anti-anxiety drugs. Anxiety seems neither necessary nor sufficient to induce control by serotonergic neurons on behavior. Further evidence suggests that behavioral effects of anxiolytics thought to be mediated by decreases in anxiety are not caused by the ability of these drugs to reduce serotonin transmission. Blockade of serotonin transmission, especially at the level of the substantia nigra, results in a shift of behavior towards facilitation of responding. This behavioral shift is particularly marked when there is competition between acting and restraining response tendencies and when obstacles prevent the immediate attainment of an anticipated reward. It is proposed that serotonergic neurons are not only involved in behavioral arousal but also in enabling the organism to arrange or tolerate delay before acting. Decreases in serotonin transmission seem to be associated with the increased performance of behaviors which are usually suppressed though not necessarily because of the alleviation of anxiety which might contribute to the suppression.

[血清素能神经元和行为]。
在苯二氮卓类药物抗焦虑活性的机制中,将减少血清素传递与减少焦虑联系起来的假设与大多数临床观察相冲突。血清素拮抗剂对缓解焦虑没有明显的作用。另一方面,血清素能传递减少的临床症状(脑脊液中5-HIAA水平低)通常与攻击性、自杀企图和焦虑增加有关。这篇简短的综述试图通过调查焦虑的减少或冲动的增加是否可能解释与血清素能传递减少相关的动物行为变化来调和这些人类和动物的发现。本文综述了操纵中枢血清素对实验性动物焦虑范式(惩罚、新奇)的影响,并与抗焦虑药物的作用进行了比较。焦虑似乎既不是必要的也不是充分的,以诱导5 -羟色胺能神经元对行为的控制。进一步的证据表明,被认为是通过减少焦虑介导的抗焦虑药的行为影响,并不是由这些药物减少血清素传递的能力引起的。阻断5 -羟色胺的传递,特别是在黑质水平上,导致行为向促进反应的转变。当行动和抑制反应倾向之间存在竞争时,以及当障碍阻碍了预期奖励的立即获得时,这种行为转变尤其明显。有人提出,血清素能神经元不仅参与行为唤醒,而且还参与使生物体在行动前安排或容忍延迟。血清素传递的减少似乎与行为表现的增加有关,这些行为通常被抑制,但不一定是因为焦虑的缓解,而焦虑可能有助于抑制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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