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The Selective Serotonin Reuptake Inhibitor Paroxetine Does Not Alter Consummatory Concentration-Dependent Licking of Prototypical Taste Stimuli by Rats

机译:选择性5-羟色胺再摄取抑制剂帕罗西汀不会改变大鼠原型味觉刺激物的消费浓度依赖性舔法。

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摘要

Serotonin and the 5HT-(1A) receptor are expressed in a subset of taste receptor cells, and the 5HT_3 receptor is expressed on afferent fibers innervating taste buds. Exogenous administration of the selective serotonin reuptake inhibitor, paroxetine, has been shown to increase taste sensitivity to stimuli described by humans as sweet and bitter. Serotonergic agonists also decrease food and fluid intake, and it is possible that modulations of serotonin may alter taste-based hedonic responsiveness; alternatively, or in combination, serotonin may interact with physiological state to impact ingestive behavior. In this study, the unconditioned licking of prototypical taste stimuli by rats in brief-access taste tests was assessed following paroxetine administration (0.3-10 mg/kg intraperitoneal). We also measured sucrose licking by rats in different deprivation states after paroxetine (5 mg/kg). In neither experiment did we find any evidence of an effect of paroxetine on licking relative to water to any of the taste stimuli in the brief-access test at doses that decreased food intake. However, in some conditions, paroxetine decreased trials initiated to tastants. Therefore, a systemic increase in serotonin via paroxetine administration can decrease appetitive behavior in brief-access tests but is insufficient to alter taste-guided consummatory behavior.
机译:血清素和5HT-(1A)受体在一部分味觉受体细胞中表达,而5HT_3受体在支配味蕾的传入纤维中表达。选择性5-羟色胺再摄取抑制剂帕罗西汀的外用给药已显示出增加了对人类描述为甜和苦的刺激的味觉敏感性。血清素能激动剂也会减少食物和液体的摄入,5-羟色胺的调节可能会改变基于味觉的享乐反应。替代地或组合地,5-羟色胺可与生理状态相互作用以影响摄食行为。在这项研究中,在帕罗西汀给药(腹腔注射0.3-10 mg / kg)后评估了短暂访问味觉试验中大鼠对原型味觉刺激的无条件舔conditioned。我们还测量了帕罗西汀(5 mg / kg)后处于不同剥夺状态的大鼠的蔗糖舔食。在这两个实验中,我们都没有发现任何证据表明帕罗西汀在减少食物摄入的剂量下相对于水对任何味觉刺激的舔舔作用相对于水都有效。然而,在某些情况下,帕罗西汀降低了促味剂试验的开始。因此,通过帕罗西汀的全身性增加5-羟色胺可以降低短暂访问测试中的食欲行为,但不足以改变口味指导的消费行为。

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