5-羟色氨酸、抗精神病药物和5-羟色胺受体拮抗剂在改变啮齿动物对厌恶情境反应中的行为相互作用。
Behavioural interactions between 5-hydroxytryptophan, neuroleptic agents and 5-HT receptor antagonists in modifying rodent responding to aversive situations.
作者信息
Costall B, Naylor R J
机构信息
Postgraduate Studies in Pharmacology, School of Pharmacy, University of Bradford.
出版信息
Br J Pharmacol. 1995 Dec;116(7):2989-99. doi: 10.1111/j.1476-5381.1995.tb15954.x.
Abstract
- The ability of 5-hydroxytryptophan, 5-HT2 receptor antagonists and typical and atypical neuroleptic agents to modify behavioural responding to aversive situations was investigated in the mouse light/dark test and rat social interaction. 2. The administration of 5-hydroxytryptophan inhibited rat social interaction and the exploratory behaviour of mice in the light/dark test. 3. The 5-HT2 receptor antagonists, ketanserin, ritanserin, MDL11939, methysergide and RP62203, the neuroleptic agents, spiperone, haloperidol and benperidol, and the atypical neuroleptic agent, clozapine, when administered alone failed to modify mouse or rat behaviour. In contrast, when administered alone, sulpiride in rats and mice and thioridazine in rats disinhibited behaviour. 4. Methysergide, RP62203, ketanserin, ritanserin and MDL11939 antagonized the inhibitory effects of 5-hydroxytryptophan or reversed the inhibitory effects to one of disinhibition. 5. Low doses of spiperone (but not haloperidol or benperidol) also antagonized the inhibitory effects of 5-hydroxytryptophan in the rat but not the mouse. Higher doses of the three neuroleptic agents caused locomotor depression in both rats and mice which obscured any specific changes in behavioural responding to the aversive situations. 6. The disinhibitory profile of sulpiride in both mice and rats and thioridazine in rats was evident during their interaction with 5-hydroxytryptophan. Thioridazine in the mouse and clozapine in rats and mice also reversed the inhibitory effects of 5-hydroxytryptophan to one of disinhibition. 7. In summary, we present evidence that the atypical neuroleptic agents, thioridazine and clozapine, with their known affinity for the 5-HT2 receptors, can mimic the actions of reference 5-HT2 receptor antagonists to antagonize the inhibitory effects of 5-hydroxytryptophan in rodent models of anxiety. The results are intepreted in terms of drug action on different 5-HT2 and other 5-HT receptor subtypes. In addition, thioridazine and sulpiride have disinhibitory effects in their own right which remain to be explained.
摘要
- 在小鼠明暗试验及大鼠社交互动实验中,研究了5-羟色氨酸、5-HT2受体拮抗剂以及典型和非典型抗精神病药物对厌恶情境下行为反应的影响。2. 给予5-羟色氨酸会抑制大鼠的社交互动以及小鼠在明暗试验中的探索行为。3. 5-HT2受体拮抗剂酮色林、利坦色林、MDL11939、麦角新碱和RP62203,抗精神病药物螺哌隆、氟哌啶醇和苯哌利多,以及非典型抗精神病药物氯氮平,单独给药时未能改变小鼠或大鼠的行为。相比之下,单独给药时,舒必利在大鼠和小鼠中以及硫利达嗪在大鼠中会解除行为抑制。4. 麦角新碱、RP62203、酮色林、利坦色林和MDL11939拮抗了5-羟色氨酸的抑制作用,或将抑制作用逆转至解除抑制作用之一。5. 低剂量的螺哌隆(但氟哌啶醇或苯哌利多无此作用)也拮抗了大鼠中5-羟色氨酸的抑制作用,但对小鼠无此作用。三种抗精神病药物的高剂量会导致大鼠和小鼠的运动抑制,这掩盖了对厌恶情境行为反应的任何特定变化。6. 舒必利在小鼠和大鼠中以及硫利达嗪在大鼠中的解除抑制作用在它们与5-羟色氨酸相互作用时很明显。硫利达嗪在小鼠中以及氯氮平在大鼠和小鼠中也将5-羟色氨酸的抑制作用逆转至解除抑制作用之一。7. 总之,我们提供的证据表明,非典型抗精神病药物硫利达嗪和氯氮平,因其对5-HT2受体的已知亲和力,在焦虑啮齿动物模型中可模拟参考5-HT2受体拮抗剂的作用,拮抗5-羟色氨酸的抑制作用。结果根据药物对不同5-HT2和其他5-HT受体亚型的作用进行解释。此外,硫利达嗪和舒必利本身具有解除抑制作用,其原因尚待解释。
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