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亚慢性给予苯丙胺或安非诺酸对大鼠脑多巴胺能和5-羟色胺能功能的影响。

Effects of subchronic amphetamine or amfonelic acid on rat brain dopaminergic and serotonergic function.

作者信息

McMillen B A, Scott S M, Williams H L

机构信息

Department of Pharmacology, East Carolina University, Greenville, North Carolina.

出版信息

J Neural Transm Gen Sect. 1991;83(1-2):55-66. doi: 10.1007/BF01244452.

Abstract

Repeated doses of direct or indirect CNS stimulants are known to cause behavioral hypersensitivity. The biochemical basis for hypersensitization remains unclear. Since the dopaminergic system uses a large storage pool that is only slowly mobilized to releasable sites, a change in this relationship may underlie the biochemical changes leading to increased responsiveness to stimulants. To test this hypothesis, rats were first tested with low doses of 2.5 mg/kg amphetamine or 1.0 mg/kg amfonelic acid (AFA) for their locomotor response, then 5.0 mg/kg amphetamine or 2.5 mg/kg AFA were injected daily for 7 days and the rats retested with the lower doses of amphetamine or AFA, respectively. Both drugs produced hypersensitivity, but the cataleptic response to acute dopamine (DA) receptor blockade by haloperidol was unaltered. The ability of haloperidol to increase DA metabolism was unaltered and the ability of acute AFA to synergize with haloperidol was similar in the striatum of stimulant and saline treated rats, but reduced in the medial prefrontal cortex of both AFA and d-amphetamine treated rats. Additional rats had DA2 receptor sensitivity measured in the striatum and frontal cortex, but no significant differences were found. Only amphetamine caused a significant decrease in frontal cortex serotonin type 2 receptors. Since there was no alteration in the ability of AFA to increase neurogenic release of DA in the striatum and a decrease occurred in prefrontal cortex, an increase in the storage to functional pool exchange in the nigrostriatal and mesocortical DA containing neurons seems unlikely. In contrast, both the amphetamine and AFA treatment groups had their brain 5HT and 5HIAA levels reduced by about 50%. This suggests that changes in other transmitter systems may have a permissive effect allowing exaggerated responses to excessive DA release.

摘要

已知重复给予直接或间接的中枢神经系统兴奋剂会导致行为超敏反应。超敏反应的生化基础尚不清楚。由于多巴胺能系统使用的是一个大储存池,该储存池仅缓慢地动员到可释放位点,这种关系的改变可能是导致对兴奋剂反应性增加的生化变化的基础。为了验证这一假设,首先用低剂量的2.5毫克/千克苯丙胺或1.0毫克/千克安非他明酸(AFA)测试大鼠的运动反应,然后每天注射5.0毫克/千克苯丙胺或2.5毫克/千克AFA,持续7天,之后分别用较低剂量的苯丙胺或AFA对大鼠进行重新测试。两种药物均产生了超敏反应,但对氟哌啶醇急性阻断多巴胺(DA)受体的僵住反应未改变。氟哌啶醇增加DA代谢的能力未改变,急性AFA与氟哌啶醇协同作用的能力在兴奋剂处理组和生理盐水处理组大鼠的纹状体中相似,但在AFA和右旋苯丙胺处理组大鼠的内侧前额叶皮质中降低。另外的大鼠在纹状体和额叶皮质中测量了DA2受体敏感性,但未发现显著差异。只有苯丙胺导致额叶皮质5-羟色胺2型受体显著减少。由于AFA增加纹状体中DA神经源性释放的能力没有改变,而前额叶皮质中出现了减少,黑质纹状体和中皮质含DA神经元中储存池与功能池交换增加的可能性似乎不大。相反,苯丙胺和AFA处理组的大脑5-羟色胺(5HT)和5-羟吲哚乙酸(5HIAA)水平均降低了约50%。这表明其他递质系统的变化可能具有允许效应,使得对过量DA释放产生过度反应。

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