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首页> 外文期刊>Behavioural pharmacology >Haloperidol-induced within-session response decrement patterns and catalepsy in rats: behavioural dissociation.
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Haloperidol-induced within-session response decrement patterns and catalepsy in rats: behavioural dissociation.

机译:氟哌啶醇诱导的会话中反应减量模式和僵直症在大鼠中:行为分离。

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The typical antipsychotic haloperidol is known to induce extra-pyramidal side-effects (EPS). Catalepsy in rats is generally regarded as a valid model for detecting the EPS liability of compounds in humans. Together with its antipsychotic and cataleptogenic actions, haloperidol causes an attenuation of instrumental responding which becomes larger in the course of a session: a within-session response decrement. The present study compared the time-course of haloperidol-induced catalepsy, measured by a bar test, to the haloperidol-induced within-session response decrements, measured by operant behaviour under a fixed ratio 10 schedule of reinforcement. Rats were trained to press a lever on a Fixed Ratio 10 schedule of food reinforcement during sessions of 15 min. When responding was stable, saline or haloperidol in 0.03 mg/kg, 0.1 mg/kg, or 0.3 mg/kg was administered intra-peritoneally either 30, 90 or 180 min prior to behavioural testing. The number of lever presses, food tray visits and latency to press the lever and to visit the food tray were analysed in five successive blocks of 3 min. Catalepsy was tested 30, 60, 90, 120, and 180 min. after injection, by placing a rat with its forepaws on a horizontal bar. The latency to remove both forepaws from the bar was scored. Within-session response decrements were present at 0.1 mg/kg and at 0.3 mg/kg, from 30 min after administration onward. At these doses, latency to press the lever was increased after 30 and 90 min, but not significantly after 180 min. Latency to visit the tray was affected only after 30 min, at 0.3 mg/kg. Haloperidol induced a dose-dependent increase in catalepsy from 60 min onwards, with maximal effect after 120 min. A dissociation between the time-course of occurrence of within-session response decrement and the cataleptogenic action of haloperidol, as well as between the latter and both latency measures, was found. Consequently, the present data suggest that within-session response decrements are not obviously caused by catalepsy-related impairments.
机译:已知典型的抗精神病药物氟哌啶醇会诱发锥体束外副作用(EPS)。通常认为大鼠的僵直症是检测化合物对人的EPS敏感性的有效模型。氟哌啶醇连同其抗精神病药和致激肽的作用一起,会导致器械反应减弱,在整个疗程过程中会变大:疗程内反应减量。本研究比较了用棒试验测得的氟哌啶醇诱发的僵直的时间过程与按固定比例10强化计划下的手术行为测得的氟哌啶醇诱发的疗程内反应减少。在15分钟的训练中,训练大鼠按固定比例10的食物强化时间表上的杠杆操作。当反应稳定后,在行为测试前30、90或180分钟腹膜内给予0.03 mg / kg,0.1 mg / kg或0.3 mg / kg的生理盐水或氟哌啶醇。在3分钟的连续五个步骤中,分析了压杆次数,食物托盘访问次数以及按下杠杆和访问食物托盘的等待时间。在30、60、90、120和180分钟测试了僵直症。注射后,将大鼠的前额放在单杠上。对从杠上移走两个前爪的潜伏期进行了评分。从给药后30分钟开始,疗程内反应降低量为0.1mg / kg和0.3mg / kg。在这些剂量下,按下杠杆的等待时间在30和90分钟后增加,但在180分钟后没有明显增加。仅在30分钟后(0.3 mg / kg),访问托盘的等待时间受到影响。氟哌啶醇从60分钟起诱导僵直症的剂量依赖性增加,在120分钟后达到最大作用。会议期间内反应减少的发生的时间过程和氟哌啶醇的致致癌作用之间的分离,以及后者和两种潜伏措施之间的分离。因此,目前的数据表明,会议期间的反应减少不是明显的由僵直相关的损伤引起的。

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