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血清素能减肥药的外周和中枢作用机制。

Peripheral and central mechanisms of action of serotoninergic anorectic drugs.

作者信息

Carruba M O, Mantegazza P, Memo M, Missale C, Pizzi M, Spano P F

出版信息

Appetite. 1986;7 Suppl:105-13. doi: 10.1016/s0195-6663(86)80056-3.

Abstract

Several pieces of evidence indicate that brain serotoninergic systems play an inhibitory role in feeding, being specifically involved in regulating satiety and food selection. The anorectic drug fenfluramine has been shown to exert its effects by activating serotoninergic mechanisms. Since fenfluramine influences both central and peripheral serotonin stores, it is difficult to establish the relative contributions of the central and peripheral serotoninergic mechanisms in the regulation of feeding behaviour. In the present paper evidence is presented that changes in feeding come about In the present paper evidence is presented that changes in feeding come about after interventions in either the brain or the periphery. This evidence includes the observation that serotonin itself given subcutaneously causes a dose-related anorexia in rats trained to eat four hours a day, an effect antagonized not only by metergoline but also by xilamidine, a serotonin antagonist that does not cross the blood-brain barrier. Since serotonin given systemically cannot reach the brain, its effect is ascribed to the activation of peripheral mechanisms. Furthermore, as is the case with fenfluramine, subcutaneous administration of serotonin is able to completely counteract the overeating induced by the glucoprivic agents insulin and 2-deoxy-D-glucose (2-DG). It is concluded that activation of peripheral serotoninergic mechanisms is sufficient not only to reduce eating in rats trained to eat four hours a day, but also to control the hyperphagias brought about by insulin or 2-DG.

摘要

多项证据表明,脑内5-羟色胺能系统在进食过程中起抑制作用,尤其参与调节饱腹感和食物选择。已证实食欲抑制药物芬氟拉明通过激活5-羟色胺能机制发挥作用。由于芬氟拉明会影响中枢和外周的5-羟色胺储备,因此很难确定中枢和外周5-羟色胺能机制在调节进食行为中的相对作用。本文提供的证据表明,无论是对脑还是外周进行干预后,进食都会发生变化。这一证据包括以下观察结果:皮下注射5-羟色胺本身会使每天进食4小时的大鼠出现剂量相关的厌食,不仅麦角新碱可拮抗这种作用,不能透过血脑屏障的5-羟色胺拮抗剂西拉米定也可拮抗。由于全身给药的5-羟色胺无法到达脑内,其作用归因于外周机制的激活。此外,与芬氟拉明的情况一样,皮下注射5-羟色胺能够完全抵消由糖缺乏剂胰岛素和2-脱氧-D-葡萄糖(2-DG)诱导的暴饮暴食。得出的结论是,激活外周5-羟色胺能机制不仅足以减少每天进食4小时的大鼠的进食量,还能控制由胰岛素或2-DG引起的食欲亢进。

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