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克仑特罗的辨别刺激特性:β肾上腺素能参与的证据。

Discriminative stimulus properties of clenbuterol: evidence for beta adrenergic involvement.

作者信息

McElroy J F, O'Donnell J M

机构信息

Life Sciences Division, Los Alamos National Laboratory, New Mexico.

出版信息

J Pharmacol Exp Ther. 1988 Apr;245(1):155-63.

PMID:2834535
Abstract

Thirty rats were trained to discriminate the centrally acting beta adrenergic agonist clenbuterol (0.1 mg/kg) from saline using a water-reinforced (fixed-ratio 10 schedule) two-lever operant task. Discrimination acquisition required a mean +/- S.E.M. of 42 +/- 7 training sessions (median of 26 training sessions). The clenbuterol stimulus was dose-dependent (ED50 = 0.03 mg/kg) and stereoselective, and had a rapid onset (5 min) and a duration of approximately 1 hr. The beta adrenergic antagonist propranolol fully antagonized the clenbuterol discriminative stimulus (IC50 = 0.18 mg/kg). Other beta adrenergic agonists such as SOM 1122 (ED50 = 0.01 mg/kg), zinterol (ED50 = 0.03 mg/kg), salbutamol (ED50 = 0.23 mg/kg) and prenalterol (ED50 = 1.91 mg/kg) substituted for clenbuterol. The monoamine uptake inhibitor despiramine (ED50 = 2.25 mg/kg), the psychomotor stimulants amphetamine (ED50 = 0.33 mg/kg) and pentylenetetrazol (ED50 = 0.31 mg/kg), and the dopamine receptor antagonists haloperidol (ED50 = 0.08 mg/kg) and chlorpromazine (ED50 = 2.32 mg/kg) similarly substituted for clenbuterol. However, chlordiazepoxide, pentobarbital, fentanyl, cocaine and fenfluramine produced little or no clenbuterol lever selection up to doses that decreased response rate markedly. The ability of SOM 1122, zinterol, salbutamol, despiramine, amphetamine, pentylenetetrazol and haloperiol to substitute for the clenbuterol stimulus was antagonized by prior treatment with propranolol. Taken together, these results suggest that the discriminative stimulus properties of clenbuterol are mediated, at least in part, through an interaction with beta adrenergic receptors. The same drugs also were assayed for in vitro inhibition of [125I]iodopindolol binding to beta adrenergic receptor preparations of rat cerebral cortex and cerebellum.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

30只大鼠通过水强化(固定比率10程序)双杠杆操作性任务,接受训练以区分中枢作用的β肾上腺素能激动剂克伦特罗(0.1毫克/千克)和生理盐水。辨别性训练习得平均需要42±7次训练(中位数为26次训练)。克伦特罗刺激具有剂量依赖性(半数有效剂量[ED50]=0.03毫克/千克)且具有立体选择性,起效迅速(5分钟),持续时间约为1小时。β肾上腺素能拮抗剂普萘洛尔完全拮抗克伦特罗的辨别性刺激(半数抑制浓度[IC50]=0.18毫克/千克)。其他β肾上腺素能激动剂,如SOM 1122(ED50=0.01毫克/千克)、辛特罗(ED50=0.03毫克/千克)、沙丁胺醇(ED50=0.23毫克/千克)和普瑞特罗(ED50=1.91毫克/千克)可替代克伦特罗。单胺摄取抑制剂地昔帕明(ED50=2.25毫克/千克)、精神运动兴奋剂苯丙胺(ED50=0.33毫克/千克)和戊四氮(ED50=0.31毫克/千克)以及多巴胺受体拮抗剂氟哌啶醇(ED50=0.08毫克/千克)和氯丙嗪(ED50=2.32毫克/千克)同样可替代克伦特罗。然而,氯氮卓、戊巴比妥、芬太尼、可卡因和芬氟拉明在剂量显著降低反应率之前,几乎不产生或不产生克伦特罗杠杆选择。预先用普萘洛尔治疗可拮抗SOM 1122、辛特罗、沙丁胺醇、地昔帕明、苯丙胺、戊四氮和氟哌啶醇替代克伦特罗刺激的能力。综上所述,这些结果表明,克伦特罗的辨别性刺激特性至少部分是通过与β肾上腺素能受体相互作用介导的。还对相同药物在体外抑制[125I]碘吲哚洛尔与大鼠大脑皮层和小脑的β肾上腺素能受体制剂结合的情况进行了测定。(摘要截断于250字)

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