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5-羟色胺拮抗剂甲基麦角新碱、美替戈林和利坦色林诱导饱足大鼠食物摄入量增加。

Increased food intake in satiated rats induced by the 5-HT antagonists methysergide, metergoline and ritanserin.

作者信息

Fletcher P J

机构信息

Neuropsychiatric Research Unit, University of Saskatchewan, Saskatoon, Canada.

出版信息

Psychopharmacology (Berl). 1988;96(2):237-42. doi: 10.1007/BF00177567.

Abstract

Two series of experiments examined whether 5-hydroxytryptamine (5-HT) antagonists induce feeding in rats. In the first series of experiments separate groups of rats were injected with various doses of methysergide, cyproheptadine, metergoline or ritanserin prior to a 2 h period of access to a wet mash diet which induced vigorous feeding under control conditions. None of the antagonists increased food intake in this paradigm. Rather, at certain doses, methysergide, cyproheptadine and ritanserin induced slight decreases in food intake. Since 5-HT may be involved in controlling satiety, it may be that a more appropriate test of the efficacy of these compounds involves administering them to maximally satiated rats. Consequently, the effects of these drugs were investigated in groups of rats which had fed to satiety immediately prior to drug treatment. In this paradigm methysergide, metergoline and ritanserin, but not cyproheptadine, induced definite increases in food intake. It is suggested that this effect occurs via a dissipation of satiety signals, and that these results further support the hypothesis that 5-HT is involved in controlling satiety. The possibility that these antagonists act on peripheral 5-HT systems is discussed.

摘要

两组实验研究了5-羟色胺(5-HT)拮抗剂是否能诱导大鼠进食。在第一组实验中,给不同组的大鼠分别注射不同剂量的麦角新碱、赛庚啶、美替拉酮或利坦色林,然后让它们在2小时内进食软湿食物,在对照条件下这种食物能引起大鼠积极进食。在这种实验模式下,没有一种拮抗剂能增加食物摄入量。相反,在某些剂量下,麦角新碱、赛庚啶和利坦色林会使食物摄入量略有减少。由于5-HT可能参与控制饱腹感,或许对这些化合物功效的更合适测试是将它们给予处于最大饱腹感的大鼠。因此,在药物治疗前刚刚进食至饱腹感的大鼠组中研究了这些药物的作用。在这种实验模式下,麦角新碱、美替拉酮和利坦色林能明确增加食物摄入量,但赛庚啶不能。研究表明,这种效应是通过饱腹感信号的消散产生的,并且这些结果进一步支持了5-HT参与控制饱腹感的假说。文中还讨论了这些拮抗剂作用于外周5-HT系统的可能性。

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