Effects of repeated low dose administration and withdrawal of haloperidol on sexual behaviour of male rats.

E Tupala, A Haapalinna, T Viitamaa, P T Männistö, V Saano
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引用次数: 3

Abstract

Neuroleptics are known to cause anhedonia and attenuate sexual behaviour at therapeutic doses in humans. These effects are assumed to result from the dopamine antagonism of the drugs. It has been observed that a mixed dopamine D1/D2 antagonist, haloperidol, may cause a reduction in the number of intromissions required to achieve ejaculation. On the other hand, dopamine antagonists are considered unable to modify sexual behaviour once the copulatory sequence is initiated. In this study, male rats received low doses of haloperidol (30 or 60 microg/kg) before the investigation of sexual behaviour in five consecutive days and the mating test was repeated after withdrawal periods of four and five days. Haloperidol dose-dependently reduced intromission frequency, and this effect was maintained for four days after withdrawal. Ejaculation latency was reduced in all groups, including controls. The results indicate that at low doses haloperidol dose-dependently reduces intromission frequency, and the effect of a repeated dosage may persist several days after cessation of medication.

氟哌啶醇反复小剂量给药和停药对雄性大鼠性行为的影响。
已知抗精神病药在治疗剂量下会引起快感缺乏和减少性行为。这些影响被认为是由药物的多巴胺拮抗作用引起的。据观察,混合多巴胺D1/D2拮抗剂氟哌啶醇可能导致射精所需的射精次数减少。另一方面,多巴胺拮抗剂被认为不能改变性行为一旦交配序列启动。在本研究中,雄性大鼠在性行为调查前连续5天接受低剂量氟哌啶醇(30或60微克/千克),在停药4天和5天后重复交配试验。氟哌啶醇剂量依赖性降低了渗滤频率,这种效果在停药后持续4天。射精潜伏期在所有组中都减少了,包括对照组。结果表明,在低剂量氟哌啶醇剂量依赖性降低渗滤频率,重复剂量的效果可能持续数天后停止用药。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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