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纳洛酮、β-内啡肽和促肾上腺皮质激素对程序诱导的过度饮水习得的影响。

Effects of naloxone, beta-endorphin and ACTH on acquisition of schedule-induced polydipsia.

作者信息

Tazi A, Dantzer R, Mormede P, Le Moal M

出版信息

Psychopharmacology (Berl). 1985;85(1):87-91. doi: 10.1007/BF00427328.

Abstract

A series of three experiments examined the possible involvement of endogenous opioid peptides in the development of schedule-induced polydipsia in rats. Repeated pretraining treatment with 2 mg/kg naloxone impaired acquisition of schedule-induced polydipsia, whereas the same treatment injected after training increased drinking. This later effect was time dependent, since a 30-min delay in the injection of naloxone resulted in a disappearance of its effect. Post-training injections of 10 micrograms/kg beta-endorphin or ACTH delayed the development of drinking. These findings are consistent with the hypothesis that endogenous opioid peptides modulate the development of schedule-induced polydipsia.

摘要

一系列三项实验研究了内源性阿片肽在大鼠程序性诱导多饮症发展过程中可能发挥的作用。用2毫克/千克纳洛酮进行重复的预训练处理会损害程序性诱导多饮症的习得,而在训练后注射相同处理则会增加饮水量。后一种效应具有时间依赖性,因为纳洛酮注射延迟30分钟会导致其效应消失。训练后注射10微克/千克的β-内啡肽或促肾上腺皮质激素会延迟饮水行为的发展。这些发现与内源性阿片肽调节程序性诱导多饮症发展的假说一致。

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