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组胺H1拮抗剂对松鼠猴的一些行为影响。

Some behavioral effects of histamine H1 antagonists in squirrel monkeys.

作者信息

Bergman J, Spealman R D

出版信息

J Pharmacol Exp Ther. 1986 Oct;239(1):104-10.

PMID:2876090
Abstract

Graded dose of the histamine H1 antagonists tripelennamine (0.1-3.0 mg/kg), promethazine (0.1-3.0 mg/kg), diphenhydramine (0.3-10.0 mg/kg) and chlorpheniramine (0.3-1.7 mg/kg) increased rates of nonsuppressed responding under a second-order schedule of food presentation to a maximum beyond which responding was increased less or decreased. In contrast, the H2 antagonist, cimetidine, had no effect or decreased responding at the highest doses studied (56.0-100.0 mg/kg). Intermediate doses of tripelennamine, diphenhydramine and promethazine also increased rates of food-maintained responding that were suppressed by electric shock. Maximal increases in rates of suppressed responding were comparable to those produced by effective doses of chlordiazepoxide (3.0-10.0 mg/kg). Under identical conditions, clozapine (0.1-1.0 mg/kg) increased responding to a lesser extent, and d-amphetamine (0.01-0.3 mg/kg) and cimetidine (3.0-100.0 mg/kg) either did not increase or, at the highest doses, only decreased rates of suppressed responding. Doses of tripelennamine and diphenhydramine that increased rates of nonsuppressed and suppressed responding also maintained self-administration in cocaine-trained squirrel monkeys under a second-order schedule of i.v. injection. Rates and patterns of responding maintained by tripelennamine and diphenhydramine were comparable to those maintained by cocaine and d-amphetamine under identical conditions. The results show that histamine H1 antagonists can have pronounced rate-increasing effects on nonsuppressed and suppressed behavior, and that they can serve as reinforcers in monkeys. These effects occur at doses that probably are greater than those required to saturate H1 sites of action in central nervous system and may not be mediated solely through histaminic mechanisms.

摘要

组胺H1拮抗剂曲吡那敏(0.1 - 3.0毫克/千克)、异丙嗪(0.1 - 3.0毫克/千克)、苯海拉明(0.3 - 10.0毫克/千克)和氯苯那敏(0.3 - 1.7毫克/千克)的分级剂量,在食物呈现的二级强化程序下增加了非抑制反应率,达到最大值后反应增加较少或减少。相比之下,H2拮抗剂西咪替丁在研究的最高剂量(56.0 - 100.0毫克/千克)下没有效果或降低了反应。曲吡那敏、苯海拉明和异丙嗪的中等剂量也增加了被电击抑制的食物维持反应率。抑制反应率的最大增加与有效剂量的氯氮卓(3.0 - 10.0毫克/千克)产生的增加相当。在相同条件下,氯氮平(0.1 - 1.0毫克/千克)增加反应的程度较小,而右旋苯丙胺(0.01 - 0.3毫克/千克)和西咪替丁(3.0 - 100.0毫克/千克)要么没有增加,要么在最高剂量下仅降低了抑制反应率。增加非抑制和抑制反应率的曲吡那敏和苯海拉明剂量,在静脉注射的二级强化程序下,也维持了可卡因训练的松鼠猴的自我给药行为。在相同条件下,曲吡那敏和苯海拉明维持的反应率和模式与可卡因和右旋苯丙胺维持的相当。结果表明,组胺H1拮抗剂对非抑制和抑制行为可产生显著的增加反应率的作用,并且它们可作为猴子的强化物。这些作用发生的剂量可能大于使中枢神经系统中H1作用位点饱和所需的剂量,并且可能不仅仅通过组胺机制介导。

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