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渗透压应激模拟血管加压素对学习行为的影响。

Osmotic stress mimics effects of vasopressin on learned behaviour.

作者信息

Koob G F, Dantzer R, Rodriguez F, Bloom F E, Le Moal M

出版信息

Nature. 1985;315(6022):750-2. doi: 10.1038/315750a0.

Abstract

It has been suggested that arginine vasopressin (AVP) is involved in the retention of learned responses, in addition to its classical physiological functions of water retention and modulation of blood pressure. AVP administered subcutaneously (s.c.), intraventricularly or intracerebrally can prolong extinction of active avoidance behaviour and can enhance retention in inhibitory (passive) avoidance. These effects have been interpreted as a direct action of AVP on the central nervous system to facilitate memory consolidation. AVP also has facilitatory effects on cognitive function in humans, and marked deficits in AVP function have been associated with certain types of psychopathology. Alternative hypotheses for the behavioural actions of AVP have involved motivational constructs such as arousal, and our recent work has focused on the role of arousal resulting from the activation of peripheral visceral signals in the behavioural effects of peripherally administered AVP. The development of a specific antagonist for AVP, 1-deaminopenicillamine-2-O-methyl tyrosine arginine vasopressin (dPTyr(Me)AVP), which can reverse the behavioural effects of exogenously administered AVP, has provided a powerful tool for examining the role of AVP in the behavioural responses produced by physiological challenges known to release vasopressin. However, the relationship between the behavioural effects of exogenously administered AVP and the behavioural function of endogenously released AVP has not been evaluated. We report here that a potent peripheral osmotic stimulus, the intraperitoneal (i.p.) injection of hypertonic saline, at doses known to release AVP both centrally and peripherally, will produce behavioural effects similar to those of exogenously administered AVP. Furthermore, the prolongation of active avoidance induced by this osmotic stimulus is reversed by pretreatment with dPTyr(Me)AVP, suggesting that endogenously released AVP may also produce behavioural effects.

摘要

有人提出,精氨酸加压素(AVP)除了具有保水和调节血压的经典生理功能外,还参与了习得反应的保留。皮下(s.c.)、脑室内或脑内注射AVP可以延长主动回避行为的消退时间,并增强抑制性(被动)回避中的记忆保留。这些作用被解释为AVP对中枢神经系统的直接作用,以促进记忆巩固。AVP对人类认知功能也有促进作用,AVP功能的显著缺陷与某些类型的精神病理学有关。关于AVP行为作用的其他假说是涉及诸如唤醒等动机结构,我们最近的工作集中在外周内脏信号激活所引起的唤醒在经外周给予AVP的行为效应中的作用。一种AVP特异性拮抗剂,1-脱氨青霉胺-2-O-甲基酪氨酸精氨酸加压素(dPTyr(Me)AVP)的开发,它可以逆转外源性给予AVP的行为效应,为研究AVP在已知释放加压素的生理挑战所产生的行为反应中的作用提供了一个有力工具。然而,外源性给予AVP的行为效应与内源性释放AVP的行为功能之间的关系尚未得到评估。我们在此报告,一种有效的外周渗透刺激,即腹腔内(i.p.)注射高渗盐水,在已知能在中枢和外周释放AVP的剂量下,将产生与外源性给予AVP相似的行为效应。此外,这种渗透刺激诱导的主动回避延长可被dPTyr(Me)AVP预处理所逆转,这表明内源性释放的AVP也可能产生行为效应。

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